anatomy_function.ace

Anatomy_function : "WBbtf0001"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001446"
Gene	"WBGene00001681"
Involved	"WBbt:0005666"	Sufficient
Involved	"WBbt:0005665"	Sufficient
Involved	"WBbt:0005661"	Sufficient
Remark	"NaCl gustatory plasticity defective"
Remark	"Published_as gpc-1"
Remark	"in gpc-1 mutant, expression of GPC-1 in ADL and ASH neurons resulted in better rescue than expression in ASH neurons alone."
Remark	"partial rescue of gpc-1 mutant by ASH-specific expression of GPC-1."
Remark	"partial rescue of gpc-1 mutant by ASI-specific expression of GPC-1."
Reference	"WBPaper00027029"


Anatomy_function : "WBbtf0002"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0001446"
Involved	"WBbt:0005666"	Necessary
Involved	"WBbt:0005665"	Necessary
Remark	"NaCl gustatory plasticity defective"
Remark	"targeted by cell-specific expression of mec-4d/mec-2"
Reference	"WBPaper00027029"


Anatomy_function : "WBbtf0003"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000992"
Gene	"WBGene00003850"
Involved	"WBbt:0005665"	Sufficient
Remark	"Published_as odr-3"
Remark	"avoidance of 1M NaCl"
Remark	"expression of ODR-3 in ASH of odr-3 animals fully restored avoidance of 1M NaCl."
Reference	"WBPaper00027029"


Anatomy_function : "WBbtf0004"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001446"
Gene	"WBGene00003850"
Involved	"WBbt:0005660"	Sufficient
Remark	"ADF specific expression of odr-3 restored NaCl avoidance after pre-exposure."
Remark	"NaCl gustatory plasticity defective"
Remark	"Published_as odr-3"
Reference	"WBPaper00027029"


Anatomy_function : "WBbtf0005"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001084"
Gene	"WBGene00001709"
Involved	"WBbt:0005665"	Sufficient
Involved	"WBbt:0005661"	Sufficient
Remark	"Published_as grk-2"
Remark	"attractive response to NaCl defective"
Remark	"expression of grk-2 by srb-6::grk-2 can restore NaCl chemoattraction in grk-2 mutant."
Remark	"expression of grk-2, by srb-6::grk-2 or osm-10::grk-2, can restore NaCl chemoattraction in grk-2 mutant."
Reference	"WBPaper00027029"


Anatomy_function : "WBbtf0006"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000249"
Gene	"WBGene00001709"
Involved	"WBbt:0005665"	Sufficient
Remark	"Published_as grk-2"
Remark	"avoidance of 1M glycerol defective"
Remark	"specific expression of grk-2 in ASH could restore avoidance of 1M glycerol."
Reference	"WBPaper00027029"


Anatomy_function : "WBbtf0007"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000412"
Gene	"WBGene00001709"
Involved	"WBbt:0005665"	Sufficient
Remark	"0000412"
Remark	"Published_as grk-2"
Remark	"specific expression of grk-2 in ASH could restore avoidance of octanol."
Reference	"WBPaper00027029"


Anatomy_function : "WBbtf0008"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0001446"
Involved	"WBbt:0003927"	Necessary
Involved	"WBbt:0004096"	Necessary
Involved	"WBbt:0006846"	Necessary
Remark	"NaCl gustatory plasticity defective"
Remark	"neuronal activity inhibited by a gcy-32::egl-2(gf) construct."
Reference	"WBPaper00027029"


Anatomy_function : "WBbtf0009"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001446"
Gene	"WBGene00001555"
Involved	"WBbt:0003927"	Sufficient
Involved	"WBbt:0004096"	Sufficient
Involved	"WBbt:0006846"	Sufficient
Remark	"NaCl gustatory plasticity defective"
Remark	"Published_as gcy-35"
Remark	"avoidance after pre-exposure was restored in gcy-32 animals expressing a gcy-32::gcy-35 construct."
Reference	"WBPaper00027029"


Anatomy_function : "WBbtf0010"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000184"	Autonomous
Gene	"WBGene00000417"
Involved	"WBbt:0006925"	Sufficient
Involved	"WBbt:0006925"	Necessary
Involved	"WBbt:0006925"	Remark
Remark	"Five obviously mosaic animals are described in categories 1 and 2 of Table 2. The category 1 mosaics are semi-Dpy and Unc. These animals were found to have cell death survivors only among cells generated from the ABp lineage. The category 2 mosaic, with an apparent ABa loss, was semiDpy and non-Unc (although this animal moved more slowly than does a wild-type animal). These results again indicate that ced-3 is cell autonomous and reveal that unc-26, like unc-30, acts in the ABp lineage."
Remark	"Genotype \"unc-30(e191) ced-3(n717) dpy-4(e1166); nDp3(IV,V;f)\""
Remark	"Published_as ced-3"
Remark	"Strain used for ced-3 mosaic analysis"
Remark	"ced-3 acts within a dying cell or, possibly, its ancestors."
Reference	"WBPaper00001254"


Anatomy_function : "WBbtf0011"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000184"	Autonomous
Gene	"WBGene00000418"
Involved	"WBbt:0006925"	Sufficient
Involved	"WBbt:0006925"	Necessary
Involved	"WBbt:0006925"	Remark
Remark	"Genotype \"ced-4(n1162) dpy-17(e164) unc-36(e251); sDp3(III;f)\""
Remark	"Published_as ced-4"
Remark	"Strain used for ced-4 mosaic analysis"
Remark	"ced-4 acts within a dying cell or, possibly, its ancestors."
Reference	"WBPaper00001254"


Anatomy_function : "WBbtf0012"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000443"
Involved	"WBbt:0005309"	Necessary
Remark	"no spicule structure or spicule cuticle material is formed when socket cell is ablated."
Reference	"WBPaper00003579"


Anatomy_function : "WBbtf0013"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000430"
Involved	"WBbt:0005309"	Necessary
Remark	"male spicule development abnormal."
Remark	"no spicule structure or spicule cuticle material is formed when socket cell is ablated."
Reference	"WBPaper00003579"


Anatomy_function : "WBbtf0014"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001487"
Involved	"WBbt:0005309"	Necessary
Remark	"no spicule structure or spicule cuticle material is formed when socket cell is ablated."
Reference	"WBPaper00003579"


Anatomy_function : "WBbtf0015"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001487"
Not_involved	"WBbt:0005831"	Unnecessary
Not_involved	"WBbt:0005311"	Unnecessary
Remark	"elimination of all spicule neurons and sheath cells does not affect spicule morphology."
Reference	"WBPaper00003579"


Anatomy_function : "WBbtf0016"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000443"
Not_involved	"WBbt:0005831"	Unnecessary
Not_involved	"WBbt:0005311"	Unnecessary
Remark	"elimination of all spicule neurons and sheath cells does not affect spicule morphology."
Reference	"WBPaper00003579"


Anatomy_function : "WBbtf0017"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001488"
Involved	"WBbt:0004812"	Necessary
Remark	"ablation of the B.paa cell eliminates the gubernaculum."
Reference	"WBPaper00003579"


Anatomy_function : "WBbtf0018"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001489"
Involved	"WBbt:0004812"	Necessary
Remark	"ablation of the B.paa cell eliminates the gubernaculum."
Reference	"WBPaper00003579"


Anatomy_function : "WBbtf0019"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0001073"
Not_involved	"WBbt:0006830"	Unnecessary
Remark	"Genotype \"egl-1(n986)\""
Remark	"egl-1 mutant showed a significantly lower egg-laying rate in the absence of food, similar to that of wild type."
Reference	"WBPaper00003951"


Anatomy_function : "WBbtf0020"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000800"	Autonomous
Gene	"WBGene00003912"
Involved	"WBbt:0008588"	Necessary
Remark	"Genotype \"pal-1(ct224) dpy-17(e164) ncl-1(e1865) unc-36(e251) III; sDp3(III,f); him-8(e1489) IV\""
Remark	"Published_as pal-1"
Remark	"To identify cells in which pal-1 function is required, we performed  a  limited  mosaic  analysis,  using  two  different strains. CF353 carried mutant markers in dpy-17, unc-36, ncl-1, and pal-1(ct224) on LGIII, complemented by wild-type copies on the free duplication sDp3. The losses resulting in posterior phenotypes that we were  able to score are summarized in Table 5. Three embryos that appeared to have lost the  duplication in either P2 or C [so that the entire C lineage was pal-1(2)] displayed  the Nob phenotype."
Remark	"posterior development defective, Nob (no back end) phenotype."
Reference	"WBPaper00004499"


Anatomy_function : "WBbtf0021"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000254"
Involved	"WBbt:0003903"	Necessary
Remark	"chloride chemotaxis was disrupted by ablation of ASER."
Reference	"WBPaper00004609"


Anatomy_function : "WBbtf0022"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001058"
Involved	"WBbt:0003903"	Necessary
Remark	"potassium chemotaxis was disrupted by ablation of ASER."
Reference	"WBPaper00004609"


Anatomy_function : "WBbtf0023"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000247"
Involved	"WBbt:0003903"	Necessary
Involved	"WBbt:0003904"	Necessary
Remark	"Although ablation of ASER had little or no effect on sodium chemotaxis, the effect of bilateral ablation of the ASE neurons was greater than the effect of unilateral ablation of ASEL."
Remark	"sodium chemotaxis was disrupted by ablation of ASEL."
Reference	"WBPaper00004609"


Anatomy_function : "WBbtf0024"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000265"
Involved	"WBbt:0005833"	Necessary
Remark	"AWC-off ablated animals did not detect 2,3-pentanedione."
Remark	"chemotaxis towards 2,3-pentanedione abnormal."
Reference	"WBPaper00004610"


Anatomy_function : "WBbtf0025"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000265"
Involved	"WBbt:0005833"	Necessary
Remark	"AWC-off ablated animals did not discriminate benzaldehyde from butanone."
Remark	"discrimination of benzaldehyde from butanone abnormal."
Reference	"WBPaper00004610"


Anatomy_function : "WBbtf0026"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001503"
Involved	"WBbt:0004070"	Necessary
Involved	"WBbt:0004070"	Remark
Remark	"30% of animals in which PVT was laser ablated in the L1 stage contained axons that were aberrantly placed across the ventral midline."
Remark	"aberrantly placed axons across the midline of ventral nerve cord."
Remark	"necessary for L1 stage only."
Reference	"WBPaper00005064"


Anatomy_function : "WBbtf0027"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000515"	Nonautonomous
Gene	"WBGene00006981"
Involved	"WBbt:0004070"	Sufficient
Involved	"WBbt:0005278"	Sufficient
Involved	"WBbt:0005339"	Sufficient
Involved	"WBbt:0005304"	Sufficient
Remark	"ZIG-4 rescuing activity can be disrupted by adding a synthetic transmembrane domain."
Remark	"aberrantly placed axons across the ventral midline of ventral nerve cord, including exons of AVK and PVQ but not those of HSN or RMEV."
Remark	"expression of ZIG-4 under the control of an unc-4 promoter can rescue the axon defect of PVQ in zig-4 mutants."
Remark	"expression of ZIG-4 under the control of its own promoter can rescue the axon defect of PVQ in zig-4 mutants."
Reference	"WBPaper00005064"


Anatomy_function : "WBbtf0028"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001084"
Involved	"WBbt:0005663"	Necessary
Remark	"ASE activity is the major determinant of the downstep turn but not of the other (NaCl chemo-attration step) response components."
Reference	"WBPaper00025064"


Anatomy_function : "WBbtf0029"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000111"
Involved	"WBbt:0006744"	Necessary
Remark	"ref-1 expression on both the left and right sides of the E16 primordium after killing the precursor of the ligand(LAG-2)-expressing cell for the E4 interaction."
Reference	"WBPaper00025235"


Anatomy_function : "WBbtf0030"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001506"
Not_involved	"WBbt:0004577"	Unnecessary
Not_involved	"WBbt:0004574"	Unnecessary
Remark	"laser ablation of Z1 and Z4 does not affect rate of spontaneous reversal during normal locomotion."
Remark	"rate of spontaneous reversal during normal locomotion (~10 per 3 minutes) abnormal."
Reference	"WBPaper00026650"


Anatomy_function : "WBbtf0031"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001506"
Gene	"WBGene00003001"
Not_involved	"WBbt:0004577"	Unnecessary
Not_involved	"WBbt:0004574"	Unnecessary
Remark	"Z1-Z4-killed lin-12(RNAi) animals maintained high reversal rates comparable to mock treated animals."
Remark	"rate of spontaneous reversal during normal locomotion (~10 per 3 minutes) abnormal."
Reference	"WBPaper00026650"


Anatomy_function : "WBbtf0032"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001506"
Gene	"WBGene00003001"
Not_involved	"WBbt:0004577"	Unnecessary
Not_involved	"WBbt:0004574"	Unnecessary
Remark	"Z1-Z4-killed lin-12p::lin-12(OE) animals maintained high reversal rates comparable to mock treated animals."
Remark	"rate of spontaneous reversal during normal locomotion (~10 per 3 minutes) abnormal."
Reference	"WBPaper00026650"


Anatomy_function : "WBbtf0033"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001506"
Gene	"WBGene00003001"
Involved	"WBbt:0006836"	Necessary
Remark	"increased lin-12 activity in the RIG neurons of adult animals increases reversal rates."
Remark	"rate of spontaneous reversal during normal locomotion (~10 per 3 minutes) abnormal."
Reference	"WBPaper00026650"


Anatomy_function : "WBbtf0034"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001506"
Gene	"WBGene00003001"
Involved	"WBbt:0006836"	Necessary
Remark	"Genotype \"lin-12(n137n460)\""
Remark	"increased lin-12 activity in the RIG neurons of adult animals increases reversal rates."
Remark	"lin-12(gfcs)"
Remark	"rate of spontaneous reversal during normal locomotion (~10 per 3 minutes) abnormal."
Reference	"WBPaper00026650"


Anatomy_function : "WBbtf0035"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001506"
Gene	"WBGene00003001"
Involved	"WBbt:0005842"	Sufficient
Involved	"WBbt:0005842"	Necessary
Involved	"WBbt:0005841"	Sufficient
Involved	"WBbt:0005841"	Necessary
Involved	"WBbt:0006818"	Sufficient
Involved	"WBbt:0006818"	Necessary
Involved	"WBbt:0006819"	Sufficient
Involved	"WBbt:0006819"	Necessary
Involved	"WBbt:0005840"	Sufficient
Involved	"WBbt:0005840"	Necessary
Involved	"WBbt:0006813"	Sufficient
Involved	"WBbt:0006813"	Necessary
Involved	"WBbt:0003850"	Sufficient
Involved	"WBbt:0003850"	Necessary
Involved	"WBbt:0006822"	Sufficient
Involved	"WBbt:0006822"	Necessary
Involved	"WBbt:0004821"	Sufficient
Involved	"WBbt:0004821"	Necessary
Involved	"WBbt:0006976"	Sufficient
Involved	"WBbt:0006976"	Necessary
Involved	"WBbt:0006836"	Sufficient
Involved	"WBbt:0006836"	Necessary
Involved	"WBbt:0005835"	Sufficient
Involved	"WBbt:0005835"	Necessary
Involved	"WBbt:0005045"	Sufficient
Involved	"WBbt:0005045"	Necessary
Involved	"WBbt:0005400"	Sufficient
Involved	"WBbt:0005400"	Necessary
Involved	"WBbt:0005025"	Sufficient
Involved	"WBbt:0005025"	Necessary
Involved	"WBbt:0005023"	Sufficient
Involved	"WBbt:0005023"	Necessary
Involved	"WBbt:0005353"	Sufficient
Involved	"WBbt:0005353"	Necessary
Involved	"WBbt:0005346"	Sufficient
Involved	"WBbt:0005346"	Necessary
Remark	"effects of all the cells were tested together as a whole set, using glr-1 promoter, rather than individually."
Remark	"each configuration was used separately to affect lin-12 expression in glr-1-expressing cells"
Remark	"rate of spontaneous reversal during normal locomotion (~10 per 3 minutes) abnormal."
Reference	"WBPaper00026650"


Anatomy_function : "WBbtf0036"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000117"
Gene	"WBGene00000035"
Involved	"WBbt:0006804"	Necessary
Remark	"Genotype \"ace-2 I; ace-3 II; unc-3 daf-6 ace-1 X; mnDp14(X,f)\""
Remark	"lack of ace-1(+) in the P1 lineage (which includes 94 of the 95 body muscle cells) is responsible for the Ace-Let phenotype."
Remark	"multiple strains were used for mosaic analysis"
Reference	"WBPaper00001039"


Anatomy_function : "WBbtf0037"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000646"
Gene	"WBGene00000035"
Involved	"WBbt:0006804"	Necessary
Remark	"Ace-Unc"
Remark	"Genotype \"ace-2 I; daf-6 ace-1 X; mnDp14(X;f)\""
Remark	"loss of ace-1+ at P1 leads to an Ace-Unc phenotype."
Remark	"two different genotypes were used separately"
Reference	"WBPaper00000761"


Anatomy_function : "WBbtf0038"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000177"
Gene	"WBGene00000035"
Involved	"WBbt:0006804"	Necessary
Remark	"Genotype \"ace-2 I; daf-6 ace-1 X; mnDp14(X;f)\""
Remark	"acetylcholinesterase activity, histochemically staining, reduced."
Remark	"loss of ace-1+ at P1 leads to loss of detectable acetylcholinesterase activity."
Remark	"two different genotypes were used separately"
Reference	"WBPaper00000761"


Anatomy_function : "WBbtf0039"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001071"
Gene	"WBGene00001444"
Not_involved	"WBbt:0006830"	Insufficient
Remark	"Genotype \"flp-1(yn2)\""
Remark	"HSN-ablated flp-1 animals were no more severely egg-laying defective than HSN-ablated wild-type animals. In the presence of exogenous serotonin, HSN-ablated flp-1 animals laid eggs significantly more slowly than HSN-ablated wild-type animals."
Reference	"WBPaper00003951"


Anatomy_function : "WBbtf0040"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0001073"
Not_involved	"WBbt:0006830"	Unnecessary
Remark	"Genotype \"egl-1(n986)\""
Remark	"egl-1 mutant lay eggs significantly less in the absence of food."
Reference	"WBPaper00003951"


Anatomy_function : "WBbtf0041"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001070"
Gene	"WBGene00001648"
Involved	"WBbt:0006830"	Necessary
Remark	"Genotype \"goa-1(n1134)\""
Remark	"The egg-laying inactive phase in HSN-ablated goa-1 mutants was no shorter than in HSN-ablated wild-type animals."
Reference	"WBPaper00003951"


Anatomy_function : "WBbtf0042"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000127"
Gene	"WBGene00014025"
Involved	"WBbt:0006816"	Sufficient
Remark	"Constitutive asna-1 expression under the control of a sensory neuron-specific promoter from the osm-6 gene promoted dauer exit of daf-7(e1372) mutant animals."
Remark	"Genotype \"daf-7(e1372); svEx412[Posm-6:asna-1(++)]\""
Reference	"WBPaper00029101"


Anatomy_function : "WBbtf0043"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000229"
Gene	"WBGene00014025"
Involved	"WBbt:0006816"	Sufficient
Remark	"Constitutive asna-1 expression under the control of a ciliated sensory neuron-specific promoter from the osm-6 gene rescued the small body size phenotype of asna-1(sv42) mutant animals."
Remark	"Genotype \"asna-1(sv42); svEx412[Posm-6::asna-1::gfp]\""
Reference	"WBPaper00029101"


Anatomy_function : "WBbtf0044"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000229"
Gene	"WBGene00014025"
Involved	"WBbt:0005792"	Sufficient
Remark	"Constitutive asna-1 expression under the control of an intestine-specific promoter from the elt-2 gene rescued the small body size phenotype of asna-1(sv42) mutant animals."
Remark	"Genotype \"asna-1(sv42); svEx439[Pelt-2::asna-1::gfp]\""
Reference	"WBPaper00029101"


Anatomy_function : "WBbtf0045"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000229"	Nonautonomous
Gene	"WBGene00014025"
Reference	"WBPaper00029101"


Anatomy_function : "WBbtf0046"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001272"
Involved	"WBbt:0004522"	Necessary
Remark	"Genotype \"let-60(n1046); let-341(s1031); gap-1(n1691)\""
Remark	"gonad ablation significantly reduces the vulval induction of let-60(gf); let-341(null);gap-1(null) animals."
Reference	"WBPaper00004213"


Anatomy_function : "WBbtf0047"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000083"	Nonautonomous
Gene	"WBGene00000229"
Remark	"Genotype \"atp-2(ua2) unc-32(e189) III; svDp1[sDp3[atp-2(+)]-svEx12[unc-4(+)-sur-5::gfp]] Strain WBStrain00047012Reference \""
Remark	"Strain name LB146"
Reference	"WBPaper00005808"


Anatomy_function : "WBbtf0048"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000061"
Gene	"WBGene00000912"
Involved	"WBbt:0003679"	Sufficient
Involved	"WBbt:0005792"	Sufficient
Remark	"Genotype \"daf-16(mu86); daf-2(e1370)\""
Remark	"expressing daf-16 in the intestine (with a ges-1 promoter) increased lifespan by 50%-60%."
Remark	"neuronal (unc-119 promoter-driven) daf-16 expression increased lifespan 5%-20%, up to that of wild-type."
Reference	"WBPaper00006226"


Anatomy_function : "WBbtf0049"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000013"
Gene	"WBGene00000912"
Involved	"WBbt:0003679"	Sufficient
Involved	"WBbt:0005792"	Sufficient
Remark	"Genotype \"daf-16(mu86); daf-2(e1370)\""
Remark	"expressing daf-16::gfp in the intestine (with a ges-1 promoter) had a small effect on dauer formation."
Remark	"neuronal (unc-119 promoter-driven) daf-16 expression was sufficient to promote dauer formation in daf-16(mu86); daf-2(e1370) mutants."
Reference	"WBPaper00006226"


Anatomy_function : "WBbtf0050"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000013"	Nonautonomous
Gene	"WBGene00000912"
Involved	"WBbt:0004015"	Sufficient
Involved	"WBbt:0006874"	Sufficient
Remark	"AB-mosaics were able to become dauers."
Remark	"Genotype \"daf-16(mu86); daf-2(e1370) ncl-1(e1865); muEx258\""
Remark	"P1-mosaics were able to become dauers."
Remark	"actual experimental temperature is 25.5 degrees"
Reference	"WBPaper00006226"


Anatomy_function : "WBbtf0051"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000039"	Nonautonomous
Gene	"WBGene00000912"
Involved	"WBbt:0006874"	Sufficient
Involved	"WBbt:0004015"	Sufficient
Remark	"AB-mosaics had extended lifespans."
Remark	"Genotype \"daf-16(mu86); daf-2(e1370) ncl-1(e1865); muEx258\""
Remark	"P1-mosaics had extended lifespans."
Remark	"Strain name CF1803"
Reference	"WBPaper00006226"


Anatomy_function : "WBbtf0052"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000061"
Gene	"WBGene00000912"
Involved	"WBbt:0005792"	Sufficient
Remark	"Genotype \"daf-16(mu86); mes-1(bn7)\""
Remark	"expressing daf-16 in the intestine (with a ges-1 promoter) completely restored the longevity of daf-16(-); mes-1(bn7) germline-less animals."
Reference	"WBPaper00006226"


Anatomy_function : "WBbtf0053"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000245"
Involved	"WBbt:0006780"	Sufficient
Involved	"WBbt:0006781"	Sufficient
Involved	"WBbt:0004522"	Sufficient
Involved	"WBbt:0007809"	Sufficient
Remark	"Anchor cell, ventral and dorsal uterine precursor cells and the induced VPC cells appear to all be sources of attraction and repulsion to sex myoblast migration."
Reference	"WBPaper00004362"


Anatomy_function : "WBbtf0054"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001272"	Autonomous
Gene	"WBGene00000238"
Involved	"WBbt:0008117"	Necessary
Remark	"Analysed 13 mosaic animals in which P4.p lacked the extrachromosomal array and found that this cell adopted the F (mutant) fate in 11 cases."
Remark	"ENTITY:WBbt:0006892(P4.p)|GO:0001708(cell fate specification) QUALITY:PATO:0001507(disrupted)"
Remark	"Genotype \"unc-29(e1072); ncl-1(e1942); unc-30(e191); bar-1(ga80); gaEx117[F35D3; C33C3; pSC11; pDE204]\""
Remark	"Published_as bar-1"
Reference	"WBPaper00003200"


Anatomy_function : "WBbtf0055"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001507"
Gene	"WBGene00000270"
Involved	"WBbt:0005792"	Necessary
Remark	"among progeny of transgenic animals, all mosaic, toxin-resistant animals have lost extra-chromosomal array carrying bre-5(+) in the gut lineage."
Reference	"WBPaper00004776"


Anatomy_function : "WBbtf0056"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000717"
Involved	"WBbt:0005175"	Necessary
Remark	"ceh-14::lacZ (pLZ14-2 reporter) expression in hypodermis was affected."
Remark	"no hypodermal expression of ceh-14::lacZ is seen in animals underwent laser ablation of Z1, Z2, Z3, Z4 gonadal precursors."
Reference	"WBPaper00004435"


Anatomy_function : "WBbtf0057"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000232"	Autonomous
Gene	"WBGene00000289"
Involved	"WBbt:0006827"
Remark	"Genotype \"cam-1(gm122); ncl-1(e1865); kyls5[ceh-23-unc-76-gfp; lin-15];gmEx188[pCAM-1; ncl-1(+); pRF4rol-6(dm)]\""
Reference	"WBPaper00003653"


Anatomy_function : "WBbtf0058"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000220"
Involved	"WBbt:0004522"	Necessary
Remark	"ablation of AC at the late P6.px to early P6.pxx stage (but not at the late P6.pxx stage) affects zmp-1::GFP expression in P6.pxxx during L4 lethargus."
Remark	"vulval primary lineage patterning (P6.pxx, vulE vs. vulF fates) defective."
Reference	"WBPaper00004481"


Anatomy_function : "WBbtf0059"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000885"
Gene	"WBGene00000420"
Involved	"WBbt:0007803"	Remark
Remark	"Genotype \"dpy-17(e164) ced-6(n1813) mec-14(u55) ncl-1(e1865) unc-36(e251)III; sDp3\""
Remark	"mosaic analysis demonstrates that ced-6 acts within the engulfing gonadal sheath cells rather than the germline apoptotic cells."
Reference	"WBPaper00003090"


Anatomy_function : "WBbtf0060"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000707"
Involved	"WBbt:0005793"
Remark	"specific defect: anterior pharyngeal extension abnormal."
Reference	"WBPaper00004707"


Anatomy_function : "WBbtf0061"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000885"
Gene	"WBGene00000421"
Involved	"WBbt:0006925"	Necessary
Involved	"WBbt:0007803"	Necessary
Remark	"Genotype \"ncl-1(e1865) unc-36(e251) ced-7(n1892); qDp3(ncl-1(+) unc-36(+) ced-7(+))\""
Remark	"mosaic animals that lost qDp3 in sheath cells of the gonad arms showed the Ced-7 phenotype."
Remark	"mosaic animals that lost qDp3 in the germline showed the Ced-7 phenotype."
Remark	"strain name MT9149"
Reference	"WBPaper00003091"


Anatomy_function : "WBbtf0062"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0004026"
Gene	"WBGene00001172"
Involved	"WBbt:0007804"	Sufficient
Remark	"Genotype \"glr-1(n2461);egl-3(nu349)\""
Remark	"expression of egl-3 in the command neurons (using the glr-1 promoter) rescued the glr-1 (nose touch defective) suppression defect."
Remark	"glr-1 single mutants are nose-touch insensitive, whereas glr-1;egl-3 double mutants are nose-touch sensitive."
Reference	"WBPaper00004977"


Anatomy_function : "WBbtf0063"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000643"
Involved	"WBbt:0006830"	Necessary
Remark	"Genotype \"egl-1(n986)\""
Remark	"egl-1 mutant animals (lack HSN neurons) did not display the velocity peak prior to egg-laying, nor did they exhibit the reversal frequency peak after egg-laying."
Remark	"specific defect: execution of the egg-laying motor program correlates with two changes in locomotive behavior: an increased propensity for forward locomotion before egg-laying, and an increased propensity for directional changes, in particular reversals, during and after an egg-laying event."
Reference	"WBPaper00004978"


Anatomy_function : "WBbtf0064"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000643"
Involved	"WBbt:0003851"	Necessary
Remark	"in AVF-ablated animals, the velocity burst prior to egg-laying was reduced if not eliminated, and the average velocity overall was significantly reduced; in addition, the peak in directional change probability after egg-laying was eliminated."
Remark	"specific defect: execution of the egg-laying motor program correlates with two changes in locomotive behavior: an increased propensity for forward locomotion before egg-laying, and an increased propensity for directional changes, in particular reversals, during and after an egg-laying event."
Reference	"WBPaper00004978"


Anatomy_function : "WBbtf0065"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000643"
Not_involved	"WBbt:0005842"	Unnecessary
Not_involved	"WBbt:0005840"	Unnecessary
Remark	"Genotype \"akIs11\""
Remark	"akIs11 uses the nmr-1 promoter to express ICE protease, which induces cell death, in a subset of command interneurons."
Remark	"nmr-1::ICE strain exhibited a significant velocity burst prior to egg-laying."
Remark	"specific defect: execution of the egg-laying motor program correlates with two changes in locomotive behavior: an increased propensity for forward locomotion before egg-laying, and an increased propensity for directional changes, in particular reversals, during and after an egg-laying event."
Reference	"WBPaper00004978"


Anatomy_function : "WBbtf0066"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000643"
Not_involved	"WBbt:0005842"	Unnecessary
Not_involved	"WBbt:0005840"	Unnecessary
Not_involved	"WBbt:0005841"	Unnecessary
Not_involved	"WBbt:0006822"	Unnecessary
Remark	"Genotype \"kyIs36\""
Remark	"glr-1::ICE strain exhibited a significant velocity burst prior to egg-laying."
Remark	"kyIs36 uses the glr-1 promoter to express ICE protease, which induces cell death, in a subset of command interneurons."
Remark	"specific defect: execution of the egg-laying motor program correlates with two changes in locomotive behavior: an increased propensity for forward locomotion before egg-laying, and an increased propensity for directional changes, in particular reversals, during and after an egg-laying event."
Reference	"WBPaper00004978"


Anatomy_function : "WBbtf0067"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000529"	Autonomous
Gene	"WBGene00000439"
Involved	"WBbt:0005753"	Sufficient
Involved	"WBbt:0005753"	Necessary
Remark	"specific phenotype: embryonic seam cell development abnormal."
Reference	"WBPaper00024903"


Anatomy_function : "WBbtf0068"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000471"	Nonautonomous
Gene	"WBGene00000478"
Not_involved	"WBbt:0005406"	Insufficient
Not_involved	"WBbt:0005406"	Unnecessary
Remark	"to generate transgenic animals, a PCR fragment containing all of the predicted cfz-2 coding region plus 4.7 kb of upstream sequence from wild type was coinjected with pTG96 (plasmid carrying a sur-5::gfp transgene) into cfz-2(cw49) homozygous mutants."
Reference	"WBPaper00026706"


Anatomy_function : "WBbtf0069"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0004007"
Involved	"WBbt:0007806"	Necessary
Involved	"WBbt:0006859"	Necessary
Involved	"WBbt:0006930"	Necessary
Remark	"removal of both the hook sensillum and the postcloacal sensilla neurons PCA and PCB resulted in males that showed no spicule activity."
Reference	"WBPaper00005027"


Anatomy_function : "WBbtf0070"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000279"
Involved	"WBbt:0004968"	Necessary
Involved	"WBbt:0004967"	Necessary
Not_involved	"WBbt:0006862"	Unnecessary
Not_involved	"WBbt:0007805"	Unnecessary
Remark	"although each SPC neuron is associated with a separate spicule, either cell facilitates insertion of both copulatory structures."
Reference	"WBPaper00005027"


Anatomy_function : "WBbtf0071"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0004008"
Involved	"WBbt:0006794"	Necessary
Remark	"somatic cells of the gonad can lengthen the duration of protractor contraction; maximal duration of protractor contraction requires proper connection of the gonad to the cloaca."
Reference	"WBPaper00005027"


Anatomy_function : "WBbtf0072"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0004008"
Gene	"WBGene00001187"
Involved	"WBbt:0005826"	Necessary
Remark	"EGL-19 in the protractors promotes prolonged contractions."
Remark	"Genotype \"egl-19(st556); him-5; syEx515\""
Reference	"WBPaper00005027"


Anatomy_function : "WBbtf0073"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0004004"
Involved	"WBbt:0006942"	Necessary
Involved	"WBbt:0006950"	Necessary
Involved	"WBbt:0006952"	Necessary
Remark	"males with dorsally opening (of sensory openings) rays ablated failed to respond to dorsal contact with the hermaphrodite."
Remark	"specific phenotype: male response to dorsal tail contact of hermaphrodite abnormal."
Reference	"WBPaper00002109"


Anatomy_function : "WBbtf0074"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0004004"
Involved	"WBbt:0006945"	Necessary
Involved	"WBbt:0006949"	Necessary
Involved	"WBbt:0006953"	Necessary
Involved	"WBbt:0006930"	Necessary
Involved	"WBbt:0005487"	Necessary
Involved	"WBbt:0005312"	Necessary
Remark	"males lacking ventral sensory organs and the ventrally opening rays do not respond to ventral contact with the hermaphrodite."
Remark	"males lacking ventral sensory organs and the ventrally opening rays do not respond to ventral contact with the hermaphrodite."
Remark	"specific phenotype: male response to ventral tail contact of hermaphrodite abnormal."
Reference	"WBPaper00002109"


Anatomy_function : "WBbtf0075"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000227"
Involved	"WBbt:0006952"	Necessary
Involved	"WBbt:0006953"	Necessary
Involved	"WBbt:0006954"	Necessary
Remark	"TL/R.ap ablated (missing rays 7-9) males swim past the end of the hermaphrodite, losing contact and ending with their tail in a tight ventral coil."
Reference	"WBPaper00002109"


Anatomy_function : "WBbtf0076"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0004004"
Involved	"WBbt:0006942"	Necessary
Involved	"WBbt:0006945"	Necessary
Involved	"WBbt:0006948"	Necessary
Involved	"WBbt:0006949"	Necessary
Involved	"WBbt:0006950"	Necessary
Involved	"WBbt:0006951"	Necessary
Remark	"ablation of V5L/R.p and V6L/R.p results in males missing rays 1-6; these males are incapable of responding to contact with hermaphrodites."
Reference	"WBPaper00002109"


Anatomy_function : "WBbtf0077"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000227"
Involved	"WBbt:0006856"	Necessary
Involved	"WBbt:0006857"	Necessary
Involved	"WBbt:0006858"	Necessary
Remark	"ablation of R(5/7/9).a neurons results in males that turn at the of the hermaphrodite but tend to do so in a large, sloppy arc instead of the tight ventral coil seen in intact animals."
Remark	"specific phenotype: males that turn at the of the hermaphrodite but tend to do so in a large, sloppy arc instead of the tight ventral coil seen in intact animals."
Reference	"WBPaper00002109"


Anatomy_function : "WBbtf0078"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0004009"
Involved	"WBbt:0006930"	Necessary
Remark	"operated males fail to stop at the vulva, circling the hermaphrodite many times."
Reference	"WBPaper00002109"


Anatomy_function : "WBbtf0079"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0004010"
Involved	"WBbt:0005487"	Necessary
Remark	"operated animals respond, turn, and readily stop in the general area of the vulva but they tend to lose the vulva while attempting to locate its precise position."
Reference	"WBPaper00002109"


Anatomy_function : "WBbtf0080"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000284"
Involved	"WBbt:0006862"	Necessary
Reference	"WBPaper00002109"


Anatomy_function : "WBbtf0081"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000279"
Involved	"WBbt:0006861"	Necessary
Involved	"WBbt:0007805"	Necessary
Remark	"ablation of either the SPC motoneurons or the SPD sensory neurons resulted in males defective in spicule insertion."
Reference	"WBPaper00002109"


Anatomy_function : "WBbtf0082"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001450"
Involved	"WBbt:0005665"	Necessary
Involved	"WBbt:0005668"	Necessary
Remark	"animals in which the ASH neurons were ablated showed reduced response to SDS; animals in which the ASH and the ASK neurons had both been ablated showed a response to SDS that was significantly lower than that of animals in which only the ASH neurons had been ablated."
Remark	"specific phenotype: SDS avoidance"
Reference	"WBPaper00005242"


Anatomy_function : "WBbtf0083"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001450"
Involved	"WBbt:0005665"	Necessary
Involved	"WBbt:0005668"	Necessary
Remark	"animals in which the ASH neurons were ablated showed reduced response to SDS; animals in which the ASH and the ASK neurons had both been ablated showed a response to SDS that was significantly lower than that of animals in which only the ASH neurons had been ablated."
Remark	"specific phenotype: SDS avoidance defect"
Reference	"WBPaper00005242"


Anatomy_function : "WBbtf0084"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001450"
Involved	"WBbt:0007807"	Necessary
Involved	"WBbt:0007808"	Necessary
Remark	"ablation of PHA and PHB did not result in an avoidance defect; however, animals in which ASH, PHA, and PHB were killed showed a significantly stronger avoidance response to SDS than animals in which ASH alone was killed."
Remark	"specific phenotype: SDS avoidance defect"
Reference	"WBPaper00005242"


Anatomy_function : "WBbtf0085"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001291"
Gene	"WBGene00003839"
Involved	"WBbt:0005665"	Sufficient
Involved	"WBbt:0005661"	Sufficient
Remark	"Genotype \"ocr-2(ak47) IV; npr-1(ad609) lin-15(n765ts)\""
Remark	"expression of ocr-2 in the ASH or ADL neurons restores aggregation behavior to ocr-2; npr-1 mutant animals."
Remark	"strain name CX4827"
Reference	"WBPaper00005511"


Anatomy_function : "WBbtf0086"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001291"
Gene	"WBGene00003851"
Involved	"WBbt:0005661"	Sufficient
Remark	"Genotype \"odr-4(n2144) III; npr-1(ad609) lin-15(n765ts) X\""
Remark	"odr-4 expression in ADL restores social behavior to odr-4; npr-1 mutant animals."
Remark	"strain name AX215"
Reference	"WBPaper00005511"


Anatomy_function : "WBbtf0087"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001291"
Involved	"WBbt:0005661"	Necessary
Involved	"WBbt:0005665"	Necessary
Remark	"ablatin of both pairs of ADL and ASH neurons suppresses aggregation; ablation of the ASH neuron pair, the ADL neuron pair, or the ASH neuron pair and 1 ADL neuron, does not suppress aggregation."
Reference	"WBPaper00005511"


Anatomy_function : "WBbtf0088"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001472"
Gene	"WBGene00002335"
Involved	"WBbt:0005672"	Sufficient
Remark	"Genotype \"let-60(n2021)\""
Remark	"gcy-10::let-60(gf) transgenic line showed a chemotaxis defect towards isoamylalcohol; gcy-10::let-60(+) restored the response of let-60(lf) mutants to isoamylalcohol. gcy-10 promoter is active in AWC, AWB, and I1."
Reference	"WBPaper00003955"


Anatomy_function : "WBbtf0089"
Assay	"Blastomere_isolation"
Phenotype	"WBPhenotype:0000080"
Gene	"WBGene00000148"
Involved	"WBbt:0004458"	Sufficient
Involved	"WBbt:0005865"	Sufficient
Involved	"WBbt:0006162"	Sufficient
Remark	"AB blastomeres were isolated from hermaphrodites from the strain PD8260 (ceh-22::lacZ) or unc-29 hermaphrodites from the strain JJ977 [unc-29(e1072) aph-2(zu181)/hT2; ceh-22::lacZ]. The P1 blastomeres were isolated from N2 hermaphrodites or unc-29 hermaphrodites from the strain JJ1077 [unc-29(e1072) aph-2(zu181)/hT2]"
Remark	"aph-2(+) function apparently can be supplied by either the signaling cell (MS), or by the responding cells (AB descendants)."
Reference	"WBPaper00004188"


Anatomy_function : "WBbtf0090"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000384"	Autonomous
Gene	"WBGene00003143"
Involved	"WBbt:0005270"	Sufficient
Involved	"WBbt:0005303"	Sufficient
Remark	"specific expression of MAX-1 the DD and VD neurons using the unc-25 promoter fully rescued the axon guidance defects of DD and VD neurons in max-1 mutants."
Reference	"WBPaper00005251"


Anatomy_function : "WBbtf0091"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000699"	Autonomous
Phenotype	"WBPhenotype:0000699"	Nonautonomous
Gene	"WBGene00000393"
Involved	"WBbt:0007809"	Sufficient
Involved	"WBbt:0005792"	Sufficient
Remark	"CDF-1 expression in the Pn.p cells (under the control of lin-31 promoter) is sufficient to rescue the mutant phenotype."
Remark	"CDF-1 expression in the intestinal cells (under the control of ges-1 promoter) can partially rescue the defects in vulval development."
Remark	"Genotype \"let-60(n1046gf); cdf-1(n2527)\""
Reference	"WBPaper00005255"


Anatomy_function : "WBbtf0092"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000047"
Gene	"WBGene00004215"
Involved	"WBbt:0003679"	Sufficient
Remark	"Genotype \"vab-1(e2) ptp-3(op147)\""
Remark	"expression of PTP-3 under the control of the pan-neural unc-119 promoter caused a significant decrease in teh lethality of vab-1 ptp-3 double mutants."
Reference	"WBPaper00005259"


Anatomy_function : "WBbtf0093"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000525"	Nonautonomous
Gene	"WBGene00001841"
Involved	"WBbt:0005663"	Sufficient
Remark	"Genotype \"hen-1(tm501)\""
Remark	"hen-1 mutant expressing the wild-type HEN-1 protein in ASE neurons (using pgcy-5/7::HEN-1) crossed the Cu2+ barrier to reach diacetyl like wild-type animals."
Remark	"specific phenotype: sensory signals integration (overcoming Cu2+ inhibition by attraction to diacetyl) defective."
Reference	"WBPaper00005300"


Anatomy_function : "WBbtf0094"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000525"	Nonautonomous
Gene	"WBGene00001841"
Involved	"WBbt:0005413"	Sufficient
Remark	"Genotype \"hen-1(tm501)\""
Remark	"hen-1 mutant expressing the wild-type HEN-1 protein in AIY neurons (using pttx-3::HEN-1) crossed the Cu2+ barrier to reach diacetyl like wild-type animals."
Remark	"specific phenotype: sensory signals integration (overcoming Cu2+ inhibition by attraction to diacetyl) defective."
Reference	"WBPaper00005300"


Anatomy_function : "WBbtf0095"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000525"	Nonautonomous
Gene	"WBGene00001841"
Involved	"WBbt:0005671"	Sufficient
Involved	"WBbt:0005672"	Sufficient
Remark	"Genotype \"hen-1(tm501)\""
Remark	"hen-1 mutant expressing the wild-type HEN-1 protein in AWB/C neurons (using pgcy-10::HEN-1) crossed the Cu2+ barrier to reach diacetyl like wild-type animals."
Remark	"specific phenotype: sensory signals integration (overcoming Cu2+ inhibition by attraction to diacetyl) defective."
Reference	"WBPaper00005300"


Anatomy_function : "WBbtf0096"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000525"	Nonautonomous
Gene	"WBGene00001841"
Involved	"WBbt:0005237"	Sufficient
Remark	"Genotype \"hen-1(tm501)\""
Remark	"hen-1 mutant expressing the wild-type HEN-1 protein in touch neurons (using pmec-7::HEN-1) crossed the Cu2+ barrier to reach diacetyl like wild-type animals."
Remark	"specific phenotype: sensory signals integration (overcoming Cu2+ inhibition by attraction to diacetyl) defective."
Reference	"WBPaper00005300"


Anatomy_function : "WBbtf0097"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000525"	Nonautonomous
Gene	"WBGene00001841"
Not_involved	"WBbt:0006804"	Insufficient
Remark	"Genotype \"hen-1(tm501)\""
Remark	"hen-1 mutant expressing the wild-type HEN-1 protein in body wall muscles (using pmyo-3::HEN-1) did not rescue the behavioral phenotype (crossing the Cu2+ barrier to reach diacetyl like wild-type animals)."
Remark	"specific phenotype: sensory signals integration (overcoming Cu2+ inhibition by attraction to diacetyl) defective."
Reference	"WBPaper00005300"


Anatomy_function : "WBbtf0098"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000525"	Nonautonomous
Gene	"WBGene00001841"
Not_involved	"WBbt:0006804"	Insufficient
Remark	"Genotype \"hen-1(tm501)\""
Remark	"expression of the wild-type HEN-1 protein in body wall muscle (using pmyo-3::HEN-1) did not rescue the behavioral plasticity phenotype."
Remark	"specific phenotype: behavioral plasticity induced by paired stimuli (reduced chemotaxis toward NaCl of animals conditioned without food and with NaCl vs. without food and without NaCl) defective."
Reference	"WBPaper00005300"


Anatomy_function : "WBbtf0099"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000525"	Nonautonomous
Gene	"WBGene00001841"
Involved	"WBbt:0005663"	Sufficient
Remark	"Genotype \"hen-1(tm501)\""
Remark	"expression of the wild-type HEN-1 protein in ASE (using pgcy-5/7::HEN-1) rescued the behavioral plasticity phenotype."
Remark	"specific phenotype: behavioral plasticity induced by paired stimuli (reduced chemotaxis toward NaCl of animals conditioned without food and with NaCl vs. without food and without NaCl) defective."
Reference	"WBPaper00005300"


Anatomy_function : "WBbtf0100"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000525"	Nonautonomous
Gene	"WBGene00001841"
Involved	"WBbt:0005663"	Sufficient
Remark	"Genotype \"hen-1(tm501)\""
Remark	"expression of the wild-type HEN-1 protein in AIY (using pttx-3::HEN-1) rescued the behavioral plasticity phenotype."
Remark	"specific phenotype: behavioral plasticity induced by paired stimuli (reduced chemotaxis toward NaCl of animals conditioned without food and with NaCl vs. without food and without NaCl) defective."
Reference	"WBPaper00005300"


Anatomy_function : "WBbtf0101"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001381"
Gene	"WBGene00000898"
Involved	"WBbt:0003679"	Sufficient
Remark	"Genotype \"daf-2(e1370)\""
Remark	"pan-neuronal expression of daf-2(+) in a daf-2(e1370) background significantly increased hypoxia-induced death."
Reference	"WBPaper00005310"


Anatomy_function : "WBbtf0102"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001381"
Gene	"WBGene00000898"
Involved	"WBbt:0003675"	Sufficient
Remark	"Genotype \"daf-2(e1370)\""
Remark	"muscle expression of daf-2(+) in a daf-2(e1370) background significantly increased hypoxia-induced death."
Reference	"WBPaper00005310"


Anatomy_function : "WBbtf0103"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001381"
Gene	"WBGene00000898"
Involved	"WBbt:0005792"	Sufficient
Remark	"Genotype \"daf-2(e1370)\""
Remark	"intestinal expression of daf-2(+) in a daf-2(e1370) background did not increase hypoxia-induced death after the standard 20-hour incubation but it did after longer (41-hour) incubations."
Reference	"WBPaper00005310"


Anatomy_function : "WBbtf0104"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000022"
Gene	"WBGene00003055"
Involved	"WBbt:0007846"	Sufficient
Remark	"Genotype \"lon-1(wk50)\""
Remark	"lon-1 genomic DNA under control of the hypodermal specific promoters, rol-6 or elt-3, is able to rescue the long body size phenotype of lon-1(wk50)."
Reference	"WBPaper00005325"


Anatomy_function : "WBbtf0105"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000022"
Gene	"WBGene00003055"
Not_involved	"WBbt:0005792"	Insufficient
Remark	"Genotype \"lon-1(wk50)\""
Remark	"lon-1 genomic DNA under control of elt-2, the intestinal-specific promoter, did not rescue the long body size phenotype of lon-1(wk50)."
Reference	"WBPaper00005325"


Anatomy_function : "WBbtf0106"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000933"
Gene	"WBGene00004077"
Involved	"WBbt:0006876"	Sufficient
Remark	"Genotype \"pop-1(zu189)\""
Remark	"specific phenotype: MS specification abnormal (adopting an E-like fate)."
Remark	"zygotic expression of POP-1 in EMS (using a med-1-driven POP-1 construct) rescues the excess intestine and small pharynx phenotype of pop-1 mutants."
Reference	"WBPaper00005341"


Anatomy_function : "WBbtf0107"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001140"
Involved	"WBbt:0003666"	Necessary
Involved	"WBbt:0005660"	Necessary
Remark	"ablation of all four NSM and ADF neurons resulted in a migration defect that was essentially identical in penetrance to the tph-1 deletion mutant."
Remark	"specific phenotype: AVM and SDQR neuron migration defect."
Reference	"WBPaper00005551"


Anatomy_function : "WBbtf0108"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001140"
Involved	"WBbt:0003666"	Necessary
Remark	"ablation of the NSMs alone resulted in a significant (penetrance = 20%-25%) migration defect."
Remark	"specific phenotype: AVM and SDQR neuron migration defect."
Reference	"WBPaper00005551"


Anatomy_function : "WBbtf0109"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001140"
Involved	"WBbt:0005660"	Necessary
Remark	"ablation of the ADFs alone caused a significant defect in AVM and SDQR migration (penetrance = 45% - 50%)."
Remark	"specific phenotype: AVM and SDQR neuron migration defect."
Reference	"WBPaper00005551"


Anatomy_function : "WBbtf0110"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000134"
Involved	"WBbt:0005666"	Necessary
Remark	"Genotype \"oyIs14(sra-6::gfp)\""
Remark	"killing the ASI neurons in L1 larvae resulted in the loss of sra-6 expression in the ASH neurons of young adult animals, whereas killing both the ASI neurons in adult animals did not significantly affect sra-6 expression in the ASH neurons, even after four days."
Remark	"specific phenotype: loss of sra-6::gfp exprssion in ASH neurons."
Reference	"WBPaper00005612"


Anatomy_function : "WBbtf0111"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000134"	Autonomous
Involved	"WBbt:0005665"	Sufficient
Involved	"WBbt:0005666"	Sufficient
Remark	"DAF-4 expression driven by either the odr-4 or the osm-10 promoter but not the myo-3 promoter is sufficient to restore sra-6::gfp expression in the ASH and ASI neurons."
Remark	"DAF-4 expression driven by either the odr-4 or the osm-10 promoter but not the myo-3 promoter is sufficient to restore sra-6::gfp expression in the ASH and ASI neurons."
Remark	"Genotype \"daf-4(m63); oyIs14(sra-6::gfp)\""
Remark	"specific phenotype: loss of sra-6::gfp exprssion in ASH and ASI neurons."
Reference	"WBPaper00005612"


Anatomy_function : "WBbtf0112"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000134"
Gene	"WBGene00000900"
Not_involved	"WBbt:0003675"	Insufficient
Remark	"DAF-4 expression driven by either the odr-4 or the osm-10 promoter but not the myo-3 promoter is sufficient to restore sra-6::gfp expression in the ASH and ASI neurons."
Remark	"specific phenotype: loss of sra-6::gfp exprssion in ASH and ASI neurons."
Reference	"WBPaper00005612"


Anatomy_function : "WBbtf0113"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000904"	Autonomous
Gene	"WBGene00006788"
Involved	"WBbt:0005821"	Sufficient
Remark	"Genotype \"unc-53(n152)\""
Remark	"pB::unc-53 fusion is expressed in the sex muscles and showed rescue of Egl phenotype and this rescue was associated with a restoration of wild-type morphology and attachment of the sex muscles, whereas pA::unc-53 fusion, which is not expressed in the sex muscles, failed to rescue the Egl phenotype."
Remark	"specific phenotype: anterior-posterior (A-P) cell migration and extension of vulval muscle abnormal."
Reference	"WBPaper00005353"


Anatomy_function : "WBbtf0114"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000904"
Gene	"WBGene00006788"
Involved	"WBbt:0007810"	Sufficient
Remark	"in comparison with wild-type body wall muscle growth cones, the processes of punc-54::unc-54 embryos were overextended along the anteroposterior axis of the animal."
Remark	"specific phenotype: anterior-posterior (A-P) muscle cell extension abnormal."
Reference	"WBPaper00005353"


Anatomy_function : "WBbtf0115"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000006"
Gene	"WBGene00003000"
Involved	"WBbt:0007256"	Sufficient
Involved	"WBbt:0004477"	Sufficient
Involved	"WBbt:0004448"	Sufficient
Involved	"WBbt:0007264"	Sufficient
Involved	"WBbt:0006763"	Sufficient
Involved	"WBbt:0006764"	Sufficient
Involved	"WBbt:0006765"	Sufficient
Involved	"WBbt:0006766"	Sufficient
Involved	"WBbt:0007813"	Sufficient
Remark	"lin-11-A also drives GFP expression in VC and PVQ neurons."
Remark	"Genotype \"lin-11(n389)\""
Remark	"Vulval-specific (controlled by lin-11-A element) and uterine-specific (controlled by lin-11-B element) expression of lin-11 together rescues the Egg-laying defect of lin-11(n389) mutant."
Reference	"WBPaper00005357"


Anatomy_function : "WBbtf0116"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000695"
Gene	"WBGene00003000"
Involved	"WBbt:0007256"	Sufficient
Involved	"WBbt:0004477"	Sufficient
Involved	"WBbt:0004448"	Sufficient
Involved	"WBbt:0007264"	Sufficient
Involved	"WBbt:0006763"	Sufficient
Involved	"WBbt:0006764"	Sufficient
Involved	"WBbt:0006765"	Sufficient
Involved	"WBbt:0006766"	Sufficient
Remark	"lin-11-A also drives GFP expression in VC and PVQ neurons."
Remark	"Genotype \"lin-11(n389)\""
Remark	"lin-11(n389) animals carrying the lin-11-A (vulval-specific expression) mini-gene construct showed normal vulval morphology but no visible utse."
Reference	"WBPaper00005357"


Anatomy_function : "WBbtf0117"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000289"
Gene	"WBGene00003000"
Involved	"WBbt:0007813"	Sufficient
Remark	"Genotype \"lin-11(n389)\""
Remark	"uterine pi-specific (controlled by lin-11-B element) expression of lin-11 rescued only the utse defect (as revealed by the expression of cog-2::GFP) of lin-11(n389) mutant."
Reference	"WBPaper00005357"


Anatomy_function : "WBbtf0118"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000905"	Autonomous
Gene	"WBGene00006788"
Involved	"WBbt:0006851"	Sufficient
Involved	"WBbt:0006855"	Sufficient
Involved	"WBbt:0006855"	Remark
Remark	"Genotype \"unc-53(n152)\""
Remark	"pA is occasionally associated with expression in the excretory cell."
Remark	"pA::unc-53 fusion is expressed in ALN and PLN neurones, and gives a high degree of rescue of their extension phenotypes in n152."
Remark	"specific phenotype: anterior-posterior neuronal process extension of ALN and PLN."
Reference	"WBPaper00005353"


Anatomy_function : "WBbtf0119"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000704"	Autonomous
Gene	"WBGene00006788"
Involved	"WBbt:0005812"	Sufficient
Remark	"Genotype \"unc-53(n152)\""
Remark	"pA is occasionally associated with expression in the excretory cell and only pA::unc-53 (but not pB::unc-53) produced some rescue of excretory canal extension."
Remark	"pA::unc-53 fusion is also expressed in ALN and PLN neurones."
Remark	"specific phenotype: posterior excretory canal process extension abnormal."
Reference	"WBPaper00005353"


Anatomy_function : "WBbtf0120"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000668"
Gene	"WBGene00003043"
Not_involved	"WBbt:0007815"	Insufficient
Remark	"Genotype \"lip-1(zh15) let-60(n1046gf)\""
Remark	"a lip-1::gfp transgene (zh29) that was expressed in most somatic cells including the somatic gonad but not in the germline, failed to rescue the lip-1(0) let-60(n1046gf) Emo phenotype, while the somatic lip-1(0) phenotypes such as the vulval lineage defects and the larval lethality were rescued efficiently."
Reference	"WBPaper00005425"


Anatomy_function : "WBbtf0121"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001291"
Gene	"WBGene00003807"
Involved	"WBbt:0003927"	Sufficient
Involved	"WBbt:0004096"	Sufficient
Involved	"WBbt:0006846"	Sufficient
Involved	"WBbt:0006817"	Sufficient
Remark	"Expression of NPR-1 215V specifically in the AQR, PQR and URX sensory neurons, using the gcy-32 promoter, suppressed both aggregation and bordering of npr-1(ad609) mutant animals. Stronger suppression of social feeding was obtained if npr-1 was expressed in the AUA interneuron in addition to AQR,PQR and URX, using the flp-8 promoter."
Remark	"Genotype \"npr-1(ad609)\""
Remark	"specific phenotype: aggregation abnormal (animals in groups); bordering."
Reference	"WBPaper00005512"


Anatomy_function : "WBbtf0122"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0001291"
Involved	"WBbt:0003927"	Necessary
Involved	"WBbt:0004096"	Necessary
Involved	"WBbt:0006846"	Necessary
Remark	"Expression of EGL-2(gf) in AQR, PQR, and URX (with a gcy-32 promoter) was sufficient to suppress strongly the aggregation and bordering phenotypes of npr-1(ad609)."
Remark	"Genotype \"npr-1(ad609); gcy-32::egl-2(gf)\""
Remark	"specific phenotype: aggregation and bordering."
Reference	"WBPaper00005512"


Anatomy_function : "WBbtf0123"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001291"
Gene	"WBGene00006525"
Involved	"WBbt:0003927"	Necessary
Involved	"WBbt:0005663"	Necessary
Involved	"WBbt:0005662"	Necessary
Involved	"WBbt:0006825"	Necessary
Remark	"A promoter mutation (p694) that disrupts tax-2 expression in the AQR, ASE, AFD and BAG sensory neurons also disrupted social feeding of npr-1(ad609) animal."
Remark	"Genotype \"npr-1(ad609); tax-2(p694)\""
Remark	"specific phenotype: aggregation in groups and bordering."
Reference	"WBPaper00005512"


Anatomy_function : "WBbtf0124"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0004028"
Gene	"WBGene00006525"
Involved	"WBbt:0003927"	Necessary
Involved	"WBbt:0005663"	Necessary
Involved	"WBbt:0005662"	Necessary
Involved	"WBbt:0006825"	Necessary
Remark	"A promoter mutation (p694) that disrupts tax-2 expression in the AQR, ASE, AFD and BAG sensory neurons restored a slowing response to food of npr-1(ad609) animal."
Remark	"Genotype \"npr-1(ad609); tax-2(p694)\""
Reference	"WBPaper00005512"


Anatomy_function : "WBbtf0125"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001291"
Gene	"WBGene00006526"
Involved	"WBbt:0003927"	Sufficient
Involved	"WBbt:0004096"	Sufficient
Involved	"WBbt:0006846"	Sufficient
Involved	"WBbt:0005664"	Sufficient
Involved	"WBbt:0005666"	Sufficient
Involved	"WBbt:0005667"	Sufficient
Involved	"WBbt:0005668"	Sufficient
Involved	"WBbt:0005671"	Sufficient
Involved	"WBbt:0005672"	Sufficient
Remark	"The odr-4 promoter drives expression in 12 neurons, but only 6 of which also express tax-4 and thus are considered relevant."
Remark	"Combined expression of tax-4 from the gcy-32 promoter and the odr-4 promoter fully restored the social behavior to tax-4; npr-1 animals, whereas from either promoter alone did not."
Remark	"Genotype \"tax-4(p678); npr-1(ad609)\""
Remark	"specific phenotype: aggregation in groups and bordering."
Reference	"WBPaper00005512"


Anatomy_function : "WBbtf0126"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000279"
Involved	"WBbt:0006861"	Necessary
Involved	"WBbt:0004292"	Necessary
Remark	"Genotype \"unc-103(sy557)\""
Remark	"unc-103(sy557) causes spontaneous spicule protraction; ablation of both the SPC neurons and the anal depressor muscle is required to suppress this phenotype."
Reference	"WBPaper00005799"


Anatomy_function : "WBbtf0127"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000306"
Not_involved	"WBbt:0006762"	Unnecessary
Not_involved	"WBbt:0006763"	Unnecessary
Not_involved	"WBbt:0006764"	Unnecessary
Remark	"Genotype \"ayIs4(egl-17::GFP)\""
Remark	"egl-17::GFP expression in remaining vulval cells was not affected by ablation of vulA , vulB1 and vulB2 cells during Pn.px and Pn.pxx stages."
Remark	"specific phenotype: egl-17::GFP expression in vulC and vulD cells and the lack of expression in vulE and vulF."
Reference	"WBPaper00005954"


Anatomy_function : "WBbtf0128"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000306"
Not_involved	"WBbt:0006767"	Unnecessary
Not_involved	"WBbt:0006768"	Unnecessary
Remark	"Genotype \"ayIs4(egl-17::GFP)\""
Remark	"egl-17::GFP expression in remaining vulval cells was not affected by ablation of vulE and vulF cells during Pn.px and Pn.pxx stages."
Remark	"specific phenotype: egl-17::GFP expression in vulC and vulD cells and the lack of expression in vulA, vulB1 and vulB2 cells."
Reference	"WBPaper00005954"


Anatomy_function : "WBbtf0129"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000306"
Not_involved	"WBbt:0006765"	Unnecessary
Not_involved	"WBbt:0006766"	Unnecessary
Remark	"Genotype \"ayIs4(egl-17::GFP)\""
Remark	"egl-17::GFP expression in remaining vulval cells was not affected by ablation of vulC and vulD cells during Pn.px and Pn.pxx stages."
Remark	"specific phenotype: the lack of egl-17::GFP expression in vulA, vulB1, vulB2, vulE and vulF cells."
Reference	"WBPaper00005954"


Anatomy_function : "WBbtf0130"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000306"
Not_involved	"WBbt:0006765"	Unnecessary
Not_involved	"WBbt:0006766"	Unnecessary
Not_involved	"WBbt:0006762"	Unnecessary
Not_involved	"WBbt:0006763"	Unnecessary
Not_involved	"WBbt:0006764"	Unnecessary
Remark	"Genotype \"ayIs4(egl-17::GFP)\""
Remark	"egl-17::GFP expression in remaining vulval cells was not affected by ablation of vulA, vulB1, vulB2, vulC and vulD cells during Pn.px and Pn.pxx stages."
Remark	"specific phenotype: the lack of egl-17::GFP expression in vulE and vulF cells."
Reference	"WBPaper00005954"


Anatomy_function : "WBbtf0131"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000306"
Not_involved	"WBbt:0006767"	Unnecessary
Not_involved	"WBbt:0006768"	Unnecessary
Remark	"Genotype \"syIs49(zmp-1::GFP)\""
Remark	"specific phenotype: zmp-1::GFP expression in vulA and vulD cells and the lack of expression in vulB1, vulB2 and vulC cells."
Remark	"zmp-1::GFP expression in remaining vulval cells was not affected by ablation of vulE and vulF cells during Pn.px and Pn.pxx stages."
Reference	"WBPaper00005954"


Anatomy_function : "WBbtf0132"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000306"
Not_involved	"WBbt:0006765"	Unnecessary
Not_involved	"WBbt:0006766"	Unnecessary
Remark	"Genotype \"syIs49(zmp-1::GFP)\""
Remark	"specific phenotype: expression of zmp-1::GFP expression in vulA and vulE, and the lack of expression vulB1, vulB2 and vulF cells."
Remark	"zmp-1::GFP expression in remaining vulval cells was not affected by ablation of vulC and vulD cells during Pn.px and Pn.pxx stages."
Reference	"WBPaper00005954"


Anatomy_function : "WBbtf0133"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000306"
Not_involved	"WBbt:0006765"	Unnecessary
Not_involved	"WBbt:0006766"	Unnecessary
Not_involved	"WBbt:0006762"	Unnecessary
Not_involved	"WBbt:0006763"	Unnecessary
Not_involved	"WBbt:0006764"	Unnecessary
Remark	"Genotype \"syIs49(zmp-1::GFP)\""
Remark	"specific phenotype: the lack of zmp-1::GFP expression in vulE and vulF cells."
Remark	"zmp-1::GFP expression in remaining vulval cells was not affected by ablation of vulA, vulB1, vulB2, vulC and vulD cells during Pn.px and Pn.pxx stages."
Reference	"WBPaper00005954"


Anatomy_function : "WBbtf0134"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000306"
Not_involved	"WBbt:0006762"	Unnecessary
Not_involved	"WBbt:0006763"	Unnecessary
Not_involved	"WBbt:0006764"	Unnecessary
Remark	"Genotype \"syIs50(cdh-3::GFP)\""
Remark	"cdh-3::GFP expression in remaining vulval cells was not affected by ablation of vulA , vulB1 and vulB2 cells during Pn.px and Pn.pxx stages."
Remark	"specific phenotype: cdh-3::GFP expression in vulC, vulD, vulE and vulF cells."
Reference	"WBPaper00005954"


Anatomy_function : "WBbtf0135"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000306"
Not_involved	"WBbt:0006767"	Unnecessary
Not_involved	"WBbt:0006768"	Unnecessary
Remark	"Genotype \"syIs50(cdh-3::GFP)\""
Remark	"cdh-3::GFP expression in remaining vulval cells was not affected by ablation of vulE and vulF cells during Pn.px and Pn.pxx stages."
Remark	"specific phenotype: cdh-3::GFP expression in vulC and vulD cells and the lack of expression in vulA, vulB1 and vulB2 cells."
Reference	"WBPaper00005954"


Anatomy_function : "WBbtf0136"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000306"
Not_involved	"WBbt:0006765"	Unnecessary
Not_involved	"WBbt:0006766"	Unnecessary
Remark	"Genotype \"syIs50(cdh-3::GFP)\""
Remark	"cdh-3::GFP expression in remaining vulval cells was not affected by ablation of vulC and vulD cells during Pn.px and Pn.pxx stages."
Remark	"specific phenotype: the lack of cdh-3::GFP expression in vulA, vulB1, vulB2 and the expression in vulE and vulF cells."
Reference	"WBPaper00005954"


Anatomy_function : "WBbtf0137"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000306"
Not_involved	"WBbt:0006765"	Unnecessary
Not_involved	"WBbt:0006766"	Unnecessary
Not_involved	"WBbt:0006762"	Unnecessary
Not_involved	"WBbt:0006763"	Unnecessary
Not_involved	"WBbt:0006764"	Unnecessary
Remark	"Genotype \"syIs50(cdh-3::GFP)\""
Remark	"cdh-3::GFP expression in remaining vulval cells was not affected by ablation of vulA, vulB1, vulB2, vulC and vulD cells during Pn.px and Pn.pxx stages."
Remark	"specific phenotype: the expression of cdh-3::GFP expression in vulE and vulF cells."
Reference	"WBPaper00005954"


Anatomy_function : "WBbtf0138"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000306"
Not_involved	"WBbt:0006762"	Unnecessary
Not_involved	"WBbt:0006763"	Unnecessary
Not_involved	"WBbt:0006764"	Unnecessary
Remark	"Genotype \"syIs54(ceh-2::GFP)\""
Remark	"ceh-2::GFP expression in remaining vulval cells was not affected by ablation of vulA , vulB1 and vulB2 cells during Pn.px and Pn.pxx stages."
Remark	"specific phenotype: ceh-2::GFP expression in vulC cells and the lack of expression in vulE and vulF."
Reference	"WBPaper00005954"


Anatomy_function : "WBbtf0139"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000306"
Not_involved	"WBbt:0006767"	Unnecessary
Not_involved	"WBbt:0006768"	Unnecessary
Remark	"Genotype \"syIs54(ceh-2::GFP)\""
Remark	"ceh-2::GFP expression in remaining vulval cells was not affected by ablation of vulE and vulF cells during Pn.px and Pn.pxx stages."
Remark	"specific phenotype: ceh-2::GFP expression in vulB1, vulB2 and vulC cells and the lack of expression in vulA and vulD cells."
Reference	"WBPaper00005954"


Anatomy_function : "WBbtf0140"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000306"
Not_involved	"WBbt:0006765"	Unnecessary
Not_involved	"WBbt:0006766"	Unnecessary
Remark	"Genotype \"syIs54(ceh-2::GFP)\""
Remark	"ceh-2::GFP expression in remaining vulval cells was not affected by ablation of vulC and vulD cells during Pn.px and Pn.pxx stages."
Remark	"specific phenotype: expression of ceh-2::GFP in vulB1, vulB2, and the lack of expression in vulA, vulE and vulF cells."
Reference	"WBPaper00005954"


Anatomy_function : "WBbtf0141"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000306"
Not_involved	"WBbt:0006765"	Unnecessary
Not_involved	"WBbt:0006766"	Unnecessary
Not_involved	"WBbt:0006762"	Unnecessary
Not_involved	"WBbt:0006763"	Unnecessary
Not_involved	"WBbt:0006764"	Unnecessary
Remark	"Genotype \"syIs54(ceh-2::GFP)\""
Remark	"ceh-2::GFP expression in remaining vulval cells was not affected by ablation of vulA, vulB1, vulB2, vulC and vulD cells during Pn.px and Pn.pxx stages."
Remark	"specific phenotype: the lack of ceh-2::GFP expression in vulE and vulF cells."
Reference	"WBPaper00005954"


Anatomy_function : "WBbtf0142"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000306"
Not_involved	"WBbt:0006762"	Unnecessary
Not_involved	"WBbt:0006763"	Unnecessary
Not_involved	"WBbt:0006764"	Unnecessary
Remark	"Genotype \"syIs49(zmp-1::GFP)\""
Remark	"specific phenotype: zmp-1::GFP expression in vulD and vulE cells and the lack of expression in vulC and vulF."
Remark	"zmp-1::GFP expression in remaining vulval cells was not affected by ablation of vulA , vulB1 and vulB2 cells during Pn.px and Pn.pxx stages."
Reference	"WBPaper00005954"


Anatomy_function : "WBbtf0143"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000529"
Not_involved	"WBbt:0004576"	Unnecessary
Not_involved	"WBbt:0004575"	Unnecessary
Not_involved	"WBbt:0004574"	Unnecessary
Not_involved	"WBbt:0007026"	Unnecessary
Not_involved	"WBbt:0007027"	Unnecessary
Not_involved	"WBbt:0007595"	Unnecessary
Not_involved	"WBbt:0007607"	Unnecessary
Not_involved	"WBbt:0007628"	Unnecessary
Remark	"Genotype \"syIs50(cdh-3::GFP)X\""
Remark	"gonadal cells neighboring the AC (Z1.ppp) do not regulate AC invasion."
Remark	"specific phenotype: anchor cell (AC) invasion into the underlying vulval cells (P6.p descendants) abnormal."
Reference	"WBPaper00005989"


Anatomy_function : "WBbtf0144"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000529"
Involved	"WBbt:0007831"	Necessary
Involved	"WBbt:0007831"	Remark
Remark	"Genotype \"lin-3(n1059)/lin-3(n378); syIs50(cdh-3::GFP)X\""
Remark	"incomplete necessity."
Remark	"only 20% of ACs invaded into the underlying epidermis in vulvaless animals, suggesting that induced vulval cells stimulate invasion at the mid-to-late L3 stage."
Remark	"specific phenotype: anchor cell (AC) invasion into the underlying epidermis (vulval cells) abnormal."
Reference	"WBPaper00005989"


Anatomy_function : "WBbtf0145"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000529"
Involved	"WBbt:0007809"	Necessary
Involved	"WBbt:0007809"	Remark
Remark	"Genotype \"syIs50(cdh-3::GFP)X\""
Remark	"VPC removal by laser ablation at the L1 molt resulted in only 24% of ACs invading."
Remark	"incomplete necessity."
Remark	"specific phenotype: anchor cell (AC) invasion into the underlying epidermis (vulval cells) abnormal."
Reference	"WBPaper00005989"


Anatomy_function : "WBbtf0146"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000594"
Not_involved	"WBbt:0008112"	Unnecessary
Not_involved	"WBbt:0008117"	Unnecessary
Not_involved	"WBbt:0008121"	Unnecessary
Not_involved	"WBbt:0008129"	Unnecessary
Not_involved	"WBbt:0008133"	Unnecessary
Remark	"Genotype \"ayIs4(egl-17::GFP) X\""
Remark	"all VPCs except for P6.p were ablated at the L1 molt; isolated P6.p descendants expressed egl-17::GFP at the mid-to-late L3 and stimulated AC invasion between the P6.pap and P6.ppa cells normally (30/30 animals)."
Remark	"specific phenotype: anchor cell (AC) invasion into the underlying epidermis (vulval cells) abnormal."
Remark	"EQ:GO:0030030(cell projection organization and biogenesis)|WBbt:0004522(anchor cell)|Life_stage:L3 larva|PATO:0000461(normal)"
Reference	"WBPaper00005989"


Anatomy_function : "WBbtf0147"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000594"
Involved	"WBbt:0008125"	Necessary
Remark	"AC cell invasion occurred in only 20% of late L3 to early L4 animals containing only secondary vulval cells (similar to the quantitative level of invasion observed in animals where both primary and secondary VPCs are missing)."
Remark	"Genotype \"lin-10(e1439); lin-12(n137)/lin-12(n137n720)\""
Remark	"specific phenotype: anchor cell (AC) invasion into the underlying epidermis (vulval cells) abnormal."
Remark	"EQ:GO:0030030(cell projection organization and biogenesis)|WBbt:0004522(anchor cell)|Life_stage:L3 larva|PATO:0000761(hypoactive)"
Reference	"WBPaper00005989"


Anatomy_function : "WBbtf0148"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001215"
Involved	"WBbt:0004520"	Necessary
Involved	"WBbt:0004506"	Necessary
Involved	"WBbt:0007667"	Necessary
Involved	"WBbt:0007688"	Necessary
Remark	"ablation of all four lag-2-expressing cells (Z1.aa, Z4.pp, Z1.ppp, Z4.aaa) results in earliest meiotic entry of germ cells."
Remark	"ablation of all four lag-expressing cells (Z1.aa, Z4.pp, Z1.ppp, Z4.aaa) results in earliest meiotic entry of germ cells."
Remark	"specific phenotype: premature entering into meiosis of germ cells."
Remark	"EQ: GO:0051728(cell cycle switching, mitotic to meiotic cell cycle)|WBbt:0005784(germ line)|Life_stage: L3 larva|PATO:0000694(premature)"
Reference	"WBPaper00005992"


Anatomy_function : "WBbtf0149"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0001506"
Involved	"WBbt:0005413"	Necessary
Remark	"AIY-specific expression of a gain-of-function potassium channel subunit [EGL-2(A478V)] caused animals to display hyper-reversal defects."
Remark	"ENTITY=GO:(transition from forward to backward locomotion)|WBbt:0007833(organism)|LifeExperience(well fed) QUALITY=PATO:(increased frequency of occurant) ENVIROTYPE=plate without food"
Remark	"specific phenotpe: more frequent (from forward to backward) reversal of locomotion direction when a well-fed animal is placed on a plate without food."
Remark	"Genotype \"otIs73[pAIY-egl-2(gf); unc-122::gfp]\""
Reference	"WBPaper00005998"


Anatomy_function : "WBbtf0150"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001506"
Gene	"WBGene00006654"
Involved	"WBbt:0005413"	Sufficient
Remark	"ENTITY=GO:(transition from forward to backward locomotion)|WBbt:0007833(organism)|LifeExperience(well fed) QUALITY=PATO:(frequency of occurant)|PATO:0000461(normal) ENVIROTYPE=plate without food"
Remark	"specific phenotpe: normal frequency of (from forward to backward) reversal of locomotion direction when a well-fed animal is placed on a plate without food."
Remark	"Genotype \"ttx-3(ot22); otEx[AIY-promoter::TTX-3]\""
Remark	"a ttx-3 cDNA expressed under the control of a promoter element of the ttx-3 gene that is exclusively active in AIY completely rescues the hyper-reversal defects of ttx-3."
Reference	"WBPaper00005998"


Anatomy_function : "WBbtf0151"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001506"
Involved	"WBbt:0005413"	Necessary
Remark	"ENTITY=GO:(transition from forward to backward locomotion)|WBbt:0007833(organism)|LifeExperience(well fed) QUALITY=PATO:(increased frequency of occurant) ENVIROTYPE=plate without food"
Remark	"specific phenotpe: increased frequency of (from forward to backward) reversal of locomotion direction when a well-fed animal is placed on a plate without food."
Remark	"Genotype \"mgIs18\""
Remark	"laser ablation of AIY causes locomotory defects (increased reversal frequency)."
Reference	"WBPaper00005998"


Anatomy_function : "WBbtf0152"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001506"
Involved	"WBbt:0005834"	Necessary
Remark	"ENTITY=GO:(transition from forward to backward locomotion)|WBbt:0007833(organism)|LifeExperience(well fed) QUALITY=PATO:(increased frequency of occurant) ENVIROTYPE=plate without food"
Remark	"specific phenotpe: increased frequency of (from forward to backward) reversal of locomotion direction when a well-fed animal is placed on a plate without food."
Remark	"Genotype \"kyIs123/+\""
Remark	"laser ablation of RIB causes locomotory defects (increased reversal frequency)."
Reference	"WBPaper00005998"


Anatomy_function : "WBbtf0153"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001506"
Involved	"WBbt:0005836"	Necessary
Remark	"ENTITY=GO:(transition from forward to backward locomotion)|WBbt:0007833(organism)|LifeExperience(well fed) QUALITY=:(reduced frequency of occurant) ENVIROTYPE=plate without food"
Remark	"specific phenotpe: reduced frequency of (from forward to backward) reversal of locomotion direction when a well-fed animal is placed on a plate without food."
Remark	"Genotype \"otEx536\""
Remark	"laser ablation of AIZ causes a hypo-reversal phenotype."
Reference	"WBPaper00005998"


Anatomy_function : "WBbtf0154"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001506"
Not_involved	"WBbt:0005045"	Unnecessary
Remark	"ENTITY=GO:(transition from forward to backward locomotion)|WBbt:0007833(organism)|LifeExperience(well fed) QUALITY=PATO:(frequency of occurant)|PATO:0000461(normal) ENVIROTYPE=plate without food"
Remark	"specific phenotpe: normal frequency of (from forward to backward) reversal of locomotion direction when a well-fed animal is placed on a plate without food."
Remark	"Genotype \"otIs39\""
Remark	"laser ablation of RIS does not cause locomotory defects (reversal frequency normal)."
Reference	"WBPaper00005998"


Anatomy_function : "WBbtf0155"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001506"
Not_involved	"WBbt:0006834"	Unnecessary
Remark	"ENTITY=GO:(transition from forward to backward locomotion)|WBbt:0007833(organism)|LifeExperience(well fed) QUALITY=PATO:(frequency of occurant)|PATO:0000461(normal) ENVIROTYPE=plate without food"
Remark	"specific phenotpe: normal frequency of (from forward to backward) reversal of locomotion direction when a well-fed animal is placed on a plate without food."
Remark	"Genotype \"nIs107\""
Remark	"laser ablation of RIC does not cause locomotory defects (reversal frequency normal)."
Reference	"WBPaper00005998"


Anatomy_function : "WBbtf0156"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001506"
Not_involved	"WBbt:0006833"	Unnecessary
Remark	"ENTITY=GO:(transition from forward to backward locomotion)|WBbt:0007833(organism)|LifeExperience(well fed) QUALITY=PATO:(frequency of occurant)|PATO:0000461(normal) ENVIROTYPE=plate without food"
Remark	"specific phenotpe: normal frequency of (from forward to backward) reversal of locomotion direction when a well-fed animal is placed on a plate without food."
Remark	"Genotype \"otIs107\""
Remark	"laser ablation of RIA does not cause locomotory defects (reversal frequency normal)."
Reference	"WBPaper00005998"


Anatomy_function : "WBbtf0157"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001506"
Involved	"WBbt:0005663"	Necessary
Remark	"ENTITY=GO:(transition from forward to backward locomotion)|WBbt:0007833(organism)|LifeExperience(well fed) QUALITY=PATO:(increased frequency of occurant) ENVIROTYPE=plate without food"
Remark	"specific phenotpe: increased frequency of (from forward to backward) reversal of locomotion direction when a well-fed animal is placed on a plate without food."
Remark	"Genotype \"otIs3\""
Remark	"laser ablation of ASE causes a hyper-reversal phenotype."
Reference	"WBPaper00005998"


Anatomy_function : "WBbtf0158"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001506"
Involved	"WBbt:0005662"	Necessary
Remark	"ENTITY=GO:(transition from forward to backward locomotion)|WBbt:0007833(organism)|LifeExperience(well fed) QUALITY=PATO:(reduced frequency of occurant) ENVIROTYPE=plate without food"
Remark	"specific phenotpe: reduced frequency of (from forward to backward) reversal of locomotion direction when a well-fed animal is placed on a plate without food."
Remark	"Genotype \"oyIs17\""
Remark	"laser ablation of AFD causes a hypo-reversal phenotype."
Reference	"WBPaper00005998"


Anatomy_function : "WBbtf0159"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001506"
Not_involved	"WBbt:0005670"	Unnecessary
Remark	"ENTITY=GO:(transition from forward to backward locomotion)|WBbt:0007833(organism)|LifeExperience(well fed) QUALITY=PATO:(frequency of occurant)|PATO:0000461(normal) ENVIROTYPE=plate without food"
Remark	"specific phenotpe: normal frequency of (from forward to backward) reversal of locomotion direction when a well-fed animal is placed on a plate without food."
Remark	"Genotype \"kyIs37\""
Remark	"laser ablation of AWA does not cause locomotory defects (reversal frequency normal)."
Reference	"WBPaper00005998"


Anatomy_function : "WBbtf0160"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001506"
Not_involved	"WBbt:0005671"	Unnecessary
Not_involved	"WBbt:0005672"	Unnecessary
Remark	"ENTITY=GO:(transition from forward to backward locomotion)|WBbt:0007833(organism)|LifeExperience(well fed) QUALITY=PATO:(frequency of occurant)|PATO:0000461(normal) ENVIROTYPE=plate without food"
Remark	"specific phenotpe: normal frequency of (from forward to backward) reversal of locomotion direction when a well-fed animal is placed on a plate without food."
Remark	"Genotype \"oyIs28\""
Remark	"laser ablation of AWB and AWC together does not cause locomotory defects (reversal frequency normal)."
Reference	"WBPaper00005998"


Anatomy_function : "WBbtf0161"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001506"
Involved	"WBbt:0005836"	Necessary
Remark	"AIZ-ablated animals fail to respond to the AWB cue (2-nonanone-induced increase in reversal frequency)."
Remark	"ENTITY=GO:(transition from forward to backward locomotion)|WBbt:0007833(organism)|LifeExperience(well fed) QUALITY=PATO:PATO:0001550(decreased sensitivity toward) ENTITY:CHEBI(2-nonanone) ENVIROTYPE=plate without food"
Remark	"specific phenotpe: unchanged frequency of (from forward to backward) reversal of locomotion direction when a well-fed animal is placed on a plate without food, with or without 2-Nonanone."
Remark	"Genotype \"otEx536\""
Reference	"WBPaper00005998"


Anatomy_function : "WBbtf0162"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001506"
Involved	"WBbt:0005834"	Necessary
Remark	"ENTITY=GO:(transition from forward to backward locomotion)|WBbt:0007833(organism)|LifeExperience(well fed) QUALITY=PATO:PATO:0001550(decreased sensitivity toward) ENTITY:CHEBI(2-nonanone) ENVIROTYPE=plate without food"
Remark	"specific phenotpe: unchanged frequency of (from forward to backward) reversal of locomotion direction when a well-fed animal is placed on a plate without food, with or without 2-Nonanone."
Remark	"Genotype \"otEx536\""
Remark	"RIB-ablated animals fail to respond to the AWB cue (2-nonanone-induced increase in reversal frequency)."
Reference	"WBPaper00005998"


Anatomy_function : "WBbtf0163"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000637"
Involved	"WBbt:0004581"	Necessary
Involved	"WBbt:0004579"	Necessary
Remark	"Genotype \"Ex[sdf-9p::GFP(pKOG8), gcy-10::GFP]\""
Remark	"killing XXXL/R cells in L1 larvae, at 25C, about 30% of the operated wild-type animals became dauer-like larvae resembing those of sdf-9 and having a non-constricted, pumping pharynx."
Remark	"specific phenotype: formation of dauer-like larvae under replete conditions."
Remark	"ENTITY:GO:0002164(larval development)|WBbt:0007833(organism)|LifeExperience:(replete condition)|LifeExperience:(25C temperature) QUALITY:PATO:0001561(having extra processual parts) ENTITY:GO:0040024(dauer larval development)"
Reference	"WBPaper00006015"


Anatomy_function : "WBbtf0164"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000525"
Not_involved	"WBbt:0005662"	Unnecessary
Remark	"AFD-killed animals clearly avoided warm temperatures above 23 deg in the same way as did wild-type worms. Furthermore, these animals were distributed in a temperature range similar to the wild-type worms, and movement assays indicated that they migrated both up and down the gradient in a region below 22 deg."
Remark	"Genotype \"gcy-8::gfp\""
Remark	"specific phenotype: warm temperature (above 23 deg) avoidance abnormal."
Remark	"ENTITY:WBbt:0007833(organism)|GO:0043052(thermotaxis) QUALITY:PATO:0000461(normal)"
Reference	"WBPaper00006045"


Anatomy_function : "WBbtf0165"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000525"
Gene	"WBGene00006526"
Not_involved	"WBbt:0005662"	Insufficient
Remark	"Genotype \"tax-4(p678); Ex[gcy-8::TAX-4::gfp]\""
Remark	"expression of tax-4 cDNA fused to a gfp reporter gene under the control of AFD specific promoter nhr-38 or gcy-8 in tax-4 worms did not rescue the defects in both (thermal behavior) population distribution tests and movement analysis."
Remark	"specific phenotype: warm temperature (above 23 deg) avoidance abnormal."
Remark	"ENTITY:WBbt:0007833(organism)|GO:0043052(thermotaxis) QUALITY:PATO:0000460(abnormal)"
Reference	"WBPaper00006045"


Anatomy_function : "WBbtf0166"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000005"
Involved	"WBbt:0004617"	Necessary
Involved	"WBbt:0004613"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|Life_stage:adult hermaphrodite|GO:0018991(oviposition) QUALITY:PATO:0000760(hyperactive)"
Remark	"Genotype \"vsIs13\""
Remark	"Of 20 VC 4/5 ablated animals, six were strongly hyperactive for egg laying (ablation of all six VC neurons resulted in small adults that produced few eggs)."
Remark	"VC neuron specific promoter::gfp"
Reference	"WBPaper00006049"


Anatomy_function : "WBbtf0167"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000005"
Gene	"WBGene00006744"
Involved	"WBbt:0005304"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|Life_stage:adult hermaphrodite|GO:0018991(oviposition) QUALITY:PATO:0000461(normal)"
Remark	"VC neuron specific promoter::unc-4 cDNA"
Remark	"expression of the unc-4 cDNA using a modified lin-11 promoter (from pMD64, that is active in the six VC neurons, cells of the posterior intestine and in the secondary cells of the vulva) rescued the hyperactive egg-laying defect of unc-4 mutants."
Reference	"WBPaper00006049"


Anatomy_function : "WBbtf0168"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000005"
Gene	"WBGene00006744"
Involved	"WBbt:0005304"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|Life_stage:adult hermaphrodite|GO:0018991(oviposition) QUALITY:PATO:0000461(normal)"
Remark	"VC neuron specific promoter::cha-1 cDNA"
Remark	"expression of the cha-1 cDNA in the VC neurons of cha-1 mutants rescued the hyperactive egg-laying phenotype."
Reference	"WBPaper00006049"


Anatomy_function : "WBbtf0169"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000005"
Gene	"WBGene00006744"
Involved	"WBbt:0005304"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|Life_stage:adult hermaphrodite|GO:0018991(oviposition) QUALITY:PATO:0000461(normal)"
Remark	"VC neuron specific promoter::unc-17 cDNA"
Remark	"expression of the unc-17 cDNA in the VC neurons of unc-17 mutants rescued the hyperactive egg-laying phenotype."
Reference	"WBPaper00006049"


Anatomy_function : "WBbtf0170"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000218"
Gene	"WBGene00001196"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBbt:0007831(vulval cell) QUALITY:PATO:0000420(increased number)"
Remark	"ENTITY:WBbt:0007831(vulval cell)|GO:0001708(cell fate specification) QUALITY:PATO:0000470(increased)"
Remark	"Genotype \"lin-3(n378); aex-3::egl-30(tg26gf)\""
Remark	"in F1 transgenic animals, aex-3 or unc-18-driven EGL-30(R243Q) could only rescue the vulvaless phenotype of lin-3(n378) when expressed in cells at levels sufficient to confer a hyperactive phenotype."
Reference	"WBPaper00006284"


Anatomy_function : "WBbtf0171"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000218"
Gene	"WBGene00001196"
Involved	"WBbt:0005304"	Sufficient
Involved	"WBbt:0005396"	Sufficient
Involved	"WBbt:0005278"	Sufficient
Involved	"WBbt:0005339"	Sufficient
Remark	"ENTITY:WBbt:0007831(vulval cell) QUALITY:PATO:0000420(increased number)"
Remark	"ENTITY:WBbt:0007831(vulval cell)|GO:0001708(cell fate specification) QUALITY:PATO:0000470(increased)"
Remark	"Genotype \"lin-3(n378); unc-4::egl-30(tg26gf)\""
Remark	"expression of EGL-30(gf) in the A-type motor neurons using unc-4 promoter showed clear functional rescue of the lin-3(n378) vulvaless phenotype (in 1 of 3 stable transgenic lines)."
Reference	"WBPaper00006284"


Anatomy_function : "WBbtf0172"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000218"
Gene	"WBGene00001196"
Not_involved	"WBbt:0007809"	Insufficient
Remark	"ENTITY:WBbt:0007831(vulval cell) QUALITY:PATO:(unchanged number)"
Remark	"ENTITY:WBbt:0007831(vulval cell)|GO:0001708(cell fate specification) QUALITY:PATO:(unchanged)"
Remark	"Genotype \"lin-3(n378); lin-31::egl-30(tg26gf)\""
Remark	"lin-31 promoter drives egl-30(tg26gf) expression transgenic construct was not able to rescue the vulvaless phenotype of lin-3(n378) mutant."
Reference	"WBPaper00006284"


Anatomy_function : "WBbtf0173"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000218"
Gene	"WBGene00001187"
Involved	"WBbt:0007810"	Sufficient
Remark	"ENTITY:WBbt:0007831(vulval cell) QUALITY:PATO:0000420(increased number)"
Remark	"ENTITY:WBbt:0007831(vulval cell)|GO:0001708(cell fate specification) QUALITY:PATO:0000470(increased)"
Remark	"Genotype \"egl-30(tg26gf); let-23(sy1); egl-19(n582); syEx465[pmyo-3::egl-19]\""
Remark	"wild-type EGL-19 expressed from the myo-3 promoter restores vulval induction to egl-30(tg26gf); let-23(sy1); egl-19(n582) triple mutants."
Reference	"WBPaper00006284"


Anatomy_function : "WBbtf0174"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001224"
Involved	"WBbt:0003850"	Necessary
Remark	"(less than half of the) AVG-ablated animals were abnormal with respect to outgrowth of some labeled axons (in the ventral nerve cord)."
Remark	"ENTITY:WBbt:0005829(ventral nerve cord)|GO:0048812(neurite morphogenesis) QUALITY:PATO:0000460(abnormal)"
Remark	"Genotype \"hdIs10[unc-129::CFP, glr-1::YFP, unc-47::DsRed, hsp16::rol-6] V\""
Reference	"WBPaper00006288"


Anatomy_function : "WBbtf0175"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001224"
Not_involved	"WBbt:0003934"	Unnecessary
Not_involved	"WBbt:0003936"	Unnecessary
Not_involved	"WBbt:0003930"	Unnecessary
Not_involved	"WBbt:0003932"	Unnecessary
Not_involved	"WBbt:0004997"	Unnecessary
Not_involved	"WBbt:0004998"	Unnecessary
Remark	"ENTITY:WBbt:0005829(ventral nerve cord)|GO:0048812(neurite morphogenesis) QUALITY:PATO:0000461(normal)"
Remark	"Genotype \"hdIs14[odr-2::CFP, unc-129::YFP, glr-1::DsRed, hsp16::rol-6] V\""
Remark	"the ablation of all six RIF/SABV/RIG neurons failed to cause any effect in the outgrowth of glr-1::DsRed-expressing interneuron axons; these interneuron axons were found to cross into the right ventral cord fascicle at the correct position."
Reference	"WBPaper00006288"


Anatomy_function : "WBbtf0176"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000399"	Autonomous
Gene	"WBGene00005006"
Involved	"WBbt:0007813"	Sufficient
Remark	"ENTITY:WBbt:0007813(uterine pi cell)|GO:0001708(cell fate specification) QUALITY:PATO:0000460(abnormal)"
Remark	"ENTITY:GO:0018991(oviposition) QUALITY:PATO:0000461(normal)"
Remark	"Genotype \"spr-1(ar200); sel-12(ar171) unc-1(e538); [pcog-2::SPR1::MYC]\""
Remark	"expression of SPR-1(+) in uterine pi cells complements spr-1(ar200)."
Reference	"WBPaper00005525"


Anatomy_function : "WBbtf0177"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000384"	Autonomous
Gene	"WBGene00004729"
Involved	"WBbt:0003832"	Sufficient
Remark	"ENTITY:WBbt:0003832(AVM)|GO:0007411(axon guidance) QUALITY:PATO:0000460(abnormal)"
Remark	"Genotype \"kyIs218(myo-3:SLT-1); sax-3(ky123); mec-7:SAX-3\""
Remark	"expression of sax-3 within AVM using a mec-7:SAX-3 transgene restored the myo-3:SLT-1 posterior defect, indicating that sax-3 acts cell-autonomously in AVM."
Reference	"WBPaper00005544"


Anatomy_function : "WBbtf0178"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000384"	Autonomous
Gene	"WBGene00006770"
Involved	"WBbt:0003832"	Sufficient
Remark	"ENTITY:WBbt:0003832(AVM)|GO:0007411(axon guidance) QUALITY:PATO:0000460(abnormal)"
Remark	"Genotype \"kyIs218(myo-3:SLT-1); unc-34(e951); mec-7:UNC-34\""
Remark	"expression of unc-34 cDNA in AVM caused a reappearance of (AVM) posterior guidance defects (of myo-3:SLT-1 transgenic animals), demonstrating that unc-34 acts cell-autonomously to potentiate slt-1/sax-3 signaling."
Reference	"WBPaper00005544"


Anatomy_function : "WBbtf0179"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000384"	Autonomous
Gene	"WBGene00006776"
Involved	"WBbt:0003832"	Sufficient
Remark	"ENTITY:WBbt:0003832(AVM)|GO:0007411(axon guidance) QUALITY:PATO:0000460(abnormal)"
Remark	"Genotype \"kyIs218(myo-3:SLT-1); unc-40(e1430); mec-7:UNC-40\""
Remark	"expression of unc-40 in touch neurons under the mec-7 promoter was sufficient to restore posterior AVM axons to unc-40; myo-3:SLT-1 animals."
Reference	"WBPaper00005544"


Anatomy_function : "WBbtf0180"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001140"
Involved	"WBbt:0006837"	Necessary
Remark	"ENTITY:WBbt:0003832(AVM)|GO:0016477(cell migration) QUALITY:PATO:0000460(abnormal)"
Remark	"ablation of the NSMs alone resulted in a significant migration defect; likewise, ablation of the ADFs alone also caused a significant defect in AVM and SDQR migration; ablation of all four serotonergic neurons resulted in no greater in penetrance than that of the ADF singly ablated animals."
Reference	"WBPaper00005551"


Anatomy_function : "WBbtf0181"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001140"
Involved	"WBbt:0006837"	Necessary
Remark	"ENTITY:WBbt:0004991(SDQR)|GO:0016477(cell migration) QUALITY:PATO:0000460(abnormal)"
Remark	"ablation of the NSMs alone resulted in a significant migration defect; likewise, ablation of the ADFs alone also caused a significant defect in AVM and SDQR migration; ablation of all four serotonergic neurons resulted in no greater in penetrance than that of the ADF singly ablated animals."
Reference	"WBPaper00005551"


Anatomy_function : "WBbtf0182"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001140"	Autonomous
Gene	"WBGene00001648"
Involved	"WBbt:0003832"	Sufficient
Remark	"ENTITY:WBbt:0003832(AVM)|GO:0016477(cell migration) QUALITY:PATO:0000461(normal)"
Remark	"Genotype \"goa-1(n1134lf); Ex[pegl-46::goa-1(Q205L)]\""
Remark	"an egl-46::goa-1(dm) transgene was able to rescue the AVM/SDQR migration defects of a goa-1(n1134) mutant. egl-46 promoter drives expression in developing AVM and SDQR and some other neurons but not in ADF and NSM neurons."
Reference	"WBPaper00005551"


Anatomy_function : "WBbtf0183"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001140"	Autonomous
Gene	"WBGene00001648"
Involved	"WBbt:0004991"	Sufficient
Remark	"ENTITY:WBbt:0004991(SDQR)|GO:0016477(cell migration) QUALITY:PATO:0000461(normal)"
Remark	"Genotype \"goa-1(n1134lf); Ex[pegl-46::goa-1(Q205L)]\""
Remark	"an egl-46::goa-1(dm) transgene was able to rescue the AVM/SDQR migration defects of a goa-1(n1134) mutant. egl-46 promoter drives expression in developing AVM and SDQR and some other neurons but not in ADF and NSM neurons."
Reference	"WBPaper00005551"


Anatomy_function : "WBbtf0184"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000006"
Gene	"WBGene00004769"
Involved	"WBbt:0004489"	Sufficient
Involved	"WBbt:0004489"	Remark
Remark	"ENTITY:WBls:0000057(adult hermaphrodite)|GO:0018991(oviposition) QUALITY:PATO:0000911(decreased rate)"
Remark	"Egl phenotype is likely caused by vm1 and vm2 morphology and attachment defects."
Remark	"Genotype \"sel-12(ar131,ar171); Ex[hlh-8::sel-12]\""
Remark	"Published_as sel-12"
Remark	"expression of sel-12 in M lineage by hlh-8::sel-12 transgene rescued Egl phenotype in non-Pvl animals (those that did not have pi cell defects)."
Reference	"WBPaper00005557"


Anatomy_function : "WBbtf0185"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000227"
Gene	"WBGene00004769"
Involved	"WBbt:0004489"	Sufficient
Involved	"WBbt:0004489"	Remark
Remark	"ENTITY:WBls:0000056(adult male)|WBbt:0005741(tail)|GO:0035178(turning behavior)|GO:0007617(mating behavior) QUALITY:PATO:0001677(inefficient)"
Remark	"Published_as sel-12"
Remark	"expression of sel-12 in M lineage by hlh-8::sel-12 transgene rescued defects in male tail turning behavior."
Remark	"turning behavior deficiency is likely caused by male sex muscle defects."
Reference	"WBPaper00005557"


Anatomy_function : "WBbtf0186"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001623"
Gene	"WBGene00004769"
Involved	"WBbt:0004489"	Sufficient
Involved	"WBbt:0004489"	Remark
Remark	"ENTITY:WBls:0000056(adult male)|WBbt:0005741(tail)|PATO:0000617(bent)|PATO:0000077(response to)|CHEBI:28790(SEROTONIN) QUALITY:PATO:0000468(reduced)"
Remark	"Published_as sel-12"
Remark	"expression of sel-12 in M lineage by hlh-8::sel-12 transgene rescued defects in male curling response to 20 mM serotonin."
Remark	"tail curling in response to 5-HT deficiency is likely caused by male sex muscle defects."
Reference	"WBPaper00005557"


Anatomy_function : "WBbtf0187"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000697"
Gene	"WBGene00004769"
Not_involved	"WBbt:0004489"	Insufficient
Remark	"ENTITY:WBls:0000057(adult hermaphrodite)|WBbt:0006748(vulva) QUALITY:PATO:0001646(protruding out of)"
Remark	"Published_as sel-12"
Remark	"expression of sel-12 in M lineage by hlh-8::sel-12 transgene does not rescue the Pvl phenotype which is likely caused by pi-cell defects."
Reference	"WBPaper00005557"


Anatomy_function : "WBbtf0188"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000070"
Gene	"WBGene00004769"
Not_involved	"WBbt:0004489"	Insufficient
Remark	"ENTITY:WBls:0000056(adult male)|WBbt:0005741(tail) QUALITY:PATO:0000940(irregular shape)"
Remark	"Published_as sel-12"
Remark	"expression of sel-12 in M lineage by hlh-8::sel-12 transgene did not rescue male tail morphology defects."
Reference	"WBPaper00005557"


Anatomy_function : "WBbtf0189"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000636"	Autonomous
Gene	"WBGene00004095"
Involved	"WBbt:0005665"	Sufficient
Remark	"ENTITY:WBbt:0005665(ASH)|GO:0008219(cell death)|ChemBI:(Htn-Q150) QUALITY:PATO:0000468(reduced)"
Remark	"Genotype \"pqe-1(rt13); Htn-Q150; PQE-1::GFP\""
Remark	"Published_as pqe-1"
Remark	"expression of PQE-1A and PQE-1C but not PQE-1B under osm-10 promoter (expressed in ASH and few other neurons) was able to rescue pqe-1 and thereby restored ASH survival in animals expressing Htn-Q150."
Reference	"WBPaper00005585"


Anatomy_function : "WBbtf0190"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000134"	Autonomous
Gene	"WBGene00000899"
Involved	"WBbt:0005665"	Sufficient
Remark	"ENTITY:Genotype:daf-7(e1372)|WBbt:0005665(ASH)|WBGene00005032(sra-6)|GO:0010467(gene expression) QUALITY:PATO:0000071(amount)"
Remark	"Genotype \"daf-7(e1372); daf-3(mgDf90); oyIs14(sra-6::gfp); Ex(osm-10::daf-3)\""
Remark	"Published_as daf-3"
Remark	"expression of daf-3 driven by the osm-10 promoter resulted in reduced expression primarily in ASH neurons."
Reference	"WBPaper00005612"


Anatomy_function : "WBbtf0191"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000134"
Gene	"WBGene00000899"
Involved	"WBbt:0005665"	Sufficient
Involved	"WBbt:0005666"	Sufficient
Remark	"ENTITY:Genotype:daf-7(e1372)|WBbt:0005665(ASH)|WBGene00005032(sra-6)|GO:0010467(gene expression) QUALITY:PATO:0000071(amount)"
Remark	"Genotype \"daf-7(e1372); daf-3(mgDf90); oyIs14(sra-6::gfp); Ex(odr-4::daf-3)\""
Remark	"Published_as daf-3"
Remark	"expression of daf-3 driven by the odr-4 promoter resulted in reduced sra-6::gfp expression in ASH and ASI neurons."
Reference	"WBPaper00005612"


Anatomy_function : "WBbtf0192"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000134"
Gene	"WBGene00000899"
Involved	"WBbt:0005665"	Sufficient
Involved	"WBbt:0005666"	Sufficient
Remark	"ENTITY:Genotype:daf-7(e1372)|WBbt:0005666(ASI)|WBGene00005032(sra-6)|GO:0010467(gene expression) QUALITY:PATO:0000071(amount)"
Remark	"Published_as daf-3"
Remark	"expression of daf-3 driven by the odr-4 promoter resulted in reduced sra-6::gfp expression in ASH and ASI neurons."
Reference	"WBPaper00005612"


Anatomy_function : "WBbtf0193"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000637"
Gene	"WBGene00000899"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:Genotype:daf-7(e1372)|WBls:0000032(dauer larva)|GO:0032502(developmental process) QUALITY:PATO:0001707(active)"
Remark	"Genotype \"daf-7(e1372); daf-3(mgDf90); oyIs14(sra-6::gfp); Ex(unc-14::daf-3)\""
Remark	"Published_as daf-3"
Remark	"The dauer defects of daf-7 mutants were weakly rescued by daf-3 expression driven by the unc-14 but not the odr-4 or osm-10 promoters."
Reference	"WBPaper00005612"


Anatomy_function : "WBbtf0194"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000640"
Gene	"WBGene00001179"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBbt:0007849(hermaphrodite)|WBls:0000041(adult)|GO:0018991(oviposition) QUALITY:PATO:0000161(rate)"
Remark	"Genotype \"egl-10(md176); Ex[rgs-1::EGL-10]\""
Remark	"Published_as egl-10"
Remark	"transgenic expression of EGL-10 (using rgs-1 promoter, which is active in all neurons) rescued the egl-10 egg-laying defect."
Reference	"WBPaper00005615"


Anatomy_function : "WBbtf0195"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000640"
Gene	"WBGene00001145"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBbt:0007849(hermaphrodite)|WBls:0000041(adult)|GO:0018991(oviposition) QUALITY:PATO:0000161(rate)"
Remark	"Genotype \"eat-16(ad702); Ex[rgs-1::EAT-16]\""
Remark	"Published_as eat-16"
Remark	"transgenic expression of EAT-16 (using rgs-1 promoter, which is active in all neurons) resulted in substantial rescue of the eat-16 mutant hyperactive egg-laying defect."
Reference	"WBPaper00005615"


Anatomy_function : "WBbtf0196"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000203"
Gene	"WBGene00001173"
Involved	"WBbt:0005672"	Sufficient
Remark	"Both odr-3::egl-4 and odr-1::egl-4 transgenes rescued the benzaldehyde adaptation defects of egl-4 mutants. The odr-3 promoter drives strong expression in AWC olfactory neurons and weak expression in AWB, AWA, ADF, and ASH sensory neurons. A 2.5 kb fragment of the odr-1/gcy-10 upstream region drives expression only in AWC and AWB sensory neurons."
Remark	"ENTITY:WBbt:0007833(organism)|GO:0022401(adaptation of signaling pathway)|GO:0050911(detection of chemical stimulus involved in sensory perception of smell)|CHEBI:17169(benzaldehyde) QUALITY:PATO:0000468(reduced)"
Remark	"Genotype \"egl-4(n479); Ex[odr-3::egl-4]\""
Reference	"WBPaper00005620"


Anatomy_function : "WBbtf0197"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001468"
Gene	"WBGene00003149"
Involved	"WBbt:0005672"	Sufficient
Involved	"WBbt:0005671"	Sufficient
Involved	"WBbt:0003649"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050911(detection of chemical stimulus involved in sensory perception of smell)|CHEBI:17169(benzaldehyde) QUALITY:PATO:0000468(reduced)"
Remark	"Genotype \"gcy-10::mbk-1\""
Remark	"Published_as mbk-1"
Remark	"gcy-10::mbk-1 transgenic lines showed impaired odortaxis toward benzaldehyde."
Reference	"WBPaper00005756"


Anatomy_function : "WBbtf0198"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000102"
Not_involved	"WBbt:0005821"	Unnecessary
Not_involved	"WBbt:0005304"	Unnecessary
Remark	"ENTITY:WBbt:0004758(HSNL)|GO:0008021(synaptic vesicle)|GO:0051179(localization) QUALITY:PATO:0000461(normal)"
Remark	"Genotype \"kyIs235(unc-86::snb-1::yfp);lin-39(n709ts)\""
Remark	"The two postsynaptic targets of HSNL were eliminated during the L1 stage by killing the M cell, the precursor to all vulval muscles, in lin-39(n709ts) mutant animals, in which the VC neurons undergo programmed cell death in the L1 stage, the position and intensity of HSNL SNB-1-labeled synaptic vesicles were indistinguishable from those of wild-type animals."
Reference	"WBPaper00005760"


Anatomy_function : "WBbtf0199"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000102"
Involved	"WBbt:0005178"	Necessary
Remark	"ENTITY:WBbt:0004758(HSNL)|GO:0008021(synaptic vesicle)|GO:0051179(localization) QUALITY:PATO:0000628(mislocalized)"
Remark	"Genotype \"kyIs235(unc-86::snb-1::yfp)\""
Remark	"in Z1, Z4 ablated animals, SNB-1::YFP failed to localize in punctate clusters at the normal location in HSNL."
Reference	"WBPaper00005760"


Anatomy_function : "WBbtf0200"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000102"
Involved	"WBbt:0007831"	Necessary
Remark	"ENTITY:WBbt:0004758(HSNL)|GO:0008021(synaptic vesicle)|GO:0051179(localization) QUALITY:PATO:0000628(mislocalized)"
Remark	"Genotype \"kyIs235(unc-86::snb-1::yfp);syg-1(ky652);lin-3(e1417)\""
Remark	"lin-3 mutants, in which the gonad is present but the vulval epithelium is absent due to a loss of EGF signaling, had abnormal anteriorly displaced SNB-1 clusters."
Reference	"WBPaper00005760"


Anatomy_function : "WBbtf0201"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000102"
Involved	"WBbt:0007831"	Sufficient
Remark	"ENTITY:WBbt:0004758(HSNL)|GO:0008021(synaptic vesicle)|GO:0051179(localization) QUALITY:PATO:0000628(mislocalized)"
Remark	"Genotype \"kyIs235(unc-86::snb-1::yfp);lin-15(n765ts)\""
Remark	"in lin-15 mutants, which have vulval epithelium at multiple ectopic pseudovulvae in addition to the normal vulva, multiple SNB-1::YFP clusters formed at the ectopic pseudovulvae, even when the gonad was killed."
Reference	"WBPaper00005760"


Anatomy_function : "WBbtf0202"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000102"	Autonomous
Gene	"WBGene00006365"
Involved	"WBbt:0006830"	Sufficient
Remark	"ENTITY:WBbt:0004758(HSNL)|GO:0008021(synaptic vesicle)|GO:0051179(localization) QUALITY:PATO:0000461(normal)"
Remark	"Genotype \"kyIs235(unc-86::snb-1::yfp);syg-1(ky652);syg-1(ky652);kyEx(unc-86::syg-1)\""
Remark	"Published_as syg-1"
Remark	"syg-1 synaptic vesicle defects were rescued when the expression of SYG-1 was driven by the unc-86 promoter, which is active in HSN neurons."
Reference	"WBPaper00005760"


Anatomy_function : "WBbtf0203"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000102"
Gene	"WBGene00006365"
Not_involved	"WBbt:0005304"	Insufficient
Remark	"ENTITY:WBbt:0004758(HSNL)|GO:0008021(synaptic vesicle)|GO:0051179(localization) QUALITY:PATO:0000628(mislocalized)"
Remark	"Genotype \"kyIs235(unc-86::snb-1::yfp);syg-1(ky652);kyEx(unc-4::syg-1)\""
Remark	"Published_as syg-1"
Remark	"syg-1 synaptic vesicle defects were not rescued when the expression of SYG-1 was driven by the unc-4 promoter, which is active in VC neurons."
Reference	"WBPaper00005760"


Anatomy_function : "WBbtf0204"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000102"
Gene	"WBGene00006365"
Not_involved	"WBbt:0005304"	Insufficient
Not_involved	"WBbt:0007831"	Insufficient
Remark	"ENTITY:WBbt:0004758(HSNL)|GO:0008021(synaptic vesicle)|GO:0051179(localization) QUALITY:PATO:0000628(mislocalized)"
Remark	"Genotype \"kyIs235(unc-86::snb-1::yfp);syg-1(ky652);kyEx(lin-11B::syg-1)\""
Remark	"Published_as syg-1"
Remark	"syg-1 synaptic vesicle defects were not rescued when the expression of SYG-1 was driven by the lin-11B promoter, which is active in VC neurons and vulval epithelium."
Reference	"WBPaper00005760"


Anatomy_function : "WBbtf0205"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000102"
Gene	"WBGene00006365"
Not_involved	"WBbt:0007831"	Insufficient
Remark	"ENTITY:WBbt:0004758(HSNL)|GO:0008021(synaptic vesicle)|GO:0051179(localization) QUALITY:PATO:0000628(mislocalized)"
Remark	"Genotype \"kyIs235(unc-86::snb-1::yfp);syg-1(ky652);kyEx(egl-17::syg-1)\""
Remark	"Published_as syg-1"
Remark	"syg-1 synaptic vesicle defects were not rescued when the expression of SYG-1 was driven by the egl-17 promoter, which is active in vulval epithelium."
Reference	"WBPaper00005760"


Anatomy_function : "WBbtf0206"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000102"
Gene	"WBGene00006365"
Not_involved	"WBbt:0006976"	Insufficient
Not_involved	"WBbt:0005665"	Insufficient
Remark	"ENTITY:WBbt:0004758(HSNL)|GO:0008021(synaptic vesicle)|GO:0051179(localization) QUALITY:PATO:0000628(mislocalized)"
Remark	"Genotype \"kyIs235(unc-86::snb-1::yfp);syg-1(ky652);kyEx(sra-6::syg-1)\""
Remark	"Published_as syg-1"
Remark	"syg-1 synaptic vesicle defects were not rescued when the expression of SYG-1 was driven by the sra-6 promoter, which is active in PVQ and ASH neurons."
Reference	"WBPaper00005760"


Anatomy_function : "WBbtf0207"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001758"	Autonomous
Gene	"WBGene00001189"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBbt:0003679(neuron)|GO:0051605(protein maturation via proteolysis)|IMR:0100129(peptide-neurotransmitter)|FaRP QUALITY:PATO:0000461(normal)"
Remark	"Genotype \"egl-21(n476); Ex[glr-1::gfp::egl-21]\""
Remark	"Published_as egl-21"
Remark	"When expression of egl-21 was restored in a subset of cells (using the glr-1 promoter), FaRP staining was restored only in those cells expressing egl-21 CPE (carboxypeptidase type E)."
Reference	"WBPaper00005776"


Anatomy_function : "WBbtf0208"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000680"
Gene	"WBGene00001189"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|GO:0006936(muscle contraction)|PATO:0000085(sensitivity toward)|CHEBI:2555(aldicarb) QUALITY:PATO:0000468(decreased amount)|NOT"
Remark	"ENTITY:GO:0031594(neuromuscular junction)|GO:0007269(neurotransmitter secretion)|CHEBI:15355(acetylcholine) QUALITY:PATO:0000468(decreased amount)|NOT"
Remark	"Expression of egl-21 using the snb-1 pan-neuronal promoter restored wild-type aldicarb sensitivity to egl-21 mutants."
Remark	"Genotype \"egl-21(n476); Ex[snb-1::egl-21]\""
Remark	"Published_as egl-21"
Reference	"WBPaper00005776"


Anatomy_function : "WBbtf0209"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000680"
Gene	"WBGene00001172"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|GO:0006936(muscle contraction)|PATO:0000085(sensitivity toward)|CHEBI:2555(aldicarb) QUALITY:PATO:0000468(decreased amount)|NOT"
Remark	"ENTITY:GO:0031594(neuromuscular junction)|GO:0007269(neurotransmitter secretion)|CHEBI:15355(acetylcholine) QUALITY:PATO:0000468(decreased amount)|NOT"
Remark	"Expression of egl-3 using the snb-1 pan-neuronal promoter restored wild-type aldicarb sensitivity to egl-3 mutants."
Remark	"Genotype \"egl-3; Ex[snb-1::egl-3]\""
Remark	"Published_as egl-3"
Reference	"WBPaper00005776"


Anatomy_function : "WBbtf0210"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000680"
Gene	"WBGene00001172"
Not_involved	"WBbt:0005409"	Insufficient
Not_involved	"WBbt:0007804"	Insufficient
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|GO:0006936(muscle contraction)|PATO:0000085(sensitivity toward)|CHEBI:2555(aldicarb) QUALITY:PATO:0000468(decreased amount)"
Remark	"ENTITY:GO:0031594(neuromuscular junction)|GO:0007269(neurotransmitter secretion)|CHEBI:15355(acetylcholine) QUALITY:PATO:0000468(decreased amount)"
Remark	"Genotype \"egl-3; Ex[acr-2::egl-3 unc-4::egl-3 glr-1::egl-3]\""
Remark	"Published_as egl-3"
Remark	"transgenes containing a combination of acr-2, unc-4 and glr-1 promoter driven egl-3 failed to rescue the aldicarb sensitivity of egl-3 mutants."
Reference	"WBPaper00005776"


Anatomy_function : "WBbtf0211"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000680"
Gene	"WBGene00001189"
Not_involved	"WBbt:0005409"	Insufficient
Not_involved	"WBbt:0007804"	Insufficient
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|GO:0006936(muscle contraction)|PATO:0000085(sensitivity toward)|CHEBI:2555(aldicarb) QUALITY:PATO:0000468(decreased amount)"
Remark	"ENTITY:GO:0031594(neuromuscular junction)|GO:0007269(neurotransmitter secretion)|CHEBI:15355(acetylcholine) QUALITY:PATO:0000468(decreased amount)"
Remark	"Genotype \"egl-21(n476); Ex[acr-2::egl-21 unc-4::egl-21 glr-1::egl-21]\""
Remark	"Published_as egl-21"
Remark	"transgenes containing a combination of acr-2, unc-4 and glr-1 promoter driven egl-21 failed to rescue the aldicarb sensitivity of egl-21 mutants."
Reference	"WBPaper00005776"


Anatomy_function : "WBbtf0212"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000019"	Autonomous
Gene	"WBGene00006599"
Involved	"WBbt:0005451"	Sufficient
Remark	"ENTITY:WBtransgene:pkIs1330([hsp-16::gpa-12(Q->L)])|WBbt:0005451(pharyngeal muscle cell)|GO:0006936(muscle contraction) QUALITY:PATO:0000381(decreased frequency)"
Remark	"ENTITY:WBtransgene:pkIs1330([hsp-16::gpa-12(Q->L)])|WBls:0000023(larva)|GO:0040007(growth) QUALITY:PATO:0000297(arrested)"
Remark	"Genotype \"tpa-1(pk1397);pkIs1330[hsp::gpa-12(Q->L)];Ex[myo-2::TPA-1]\""
Remark	"Published_as tpa-1"
Remark	"specific expression of wild-type TPA-1A or TPA-1B in the pharynx in a tpa-1 background results in the inhibition of larval growth after heat shock-induced G12QL expression (pkIs1330[hsp::gpa-12QL]) or treatment with PMA."
Reference	"WBPaper00005783"


Anatomy_function : "WBbtf0213"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000019"	Autonomous
Gene	"WBGene00006599"
Involved	"WBbt:0005451"	Sufficient
Remark	"ENTITY:CHEBI:37537(phorbol 13-acetate 12-myristate)|WBbt:0005451(pharyngeal muscle cell)|GO:0006936(muscle contraction) QUALITY:PATO:0000381(decreased frequency)"
Remark	"ENTITY:CHEBI:37537(phorbol 13-acetate 12-myristate)|WBls:0000023(larva)|GO:0040007(growth) QUALITY:PATO:0000297(arrested)"
Remark	"Genotype \"tpa-1(pk1397);Ex[myo-2::TPA-1]\""
Remark	"Published_as tpa-1"
Remark	"specific expression of wild-type TPA-1A or TPA-1B in the pharynx in a tpa-1 background results in the inhibition of larval growth after heat shock-induced G12QL expression (pkIs1330[hsp::gpa-12QL]) or treatment with PMA."
Reference	"WBPaper00005783"


Anatomy_function : "WBbtf0214"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000019"
Gene	"WBGene00006599"
Not_involved	"WBbt:0007846"	Insufficient
Remark	"ENTITY:WBtransgene:pkIs1330([hsp-16::gpa-12(Q->L)])|WBbt:0005451(pharyngeal muscle cell)|GO:0006936(muscle contraction) QUALITY:PATO:0000381(decreased frequency) NOT"
Remark	"ENTITY:WBtransgene:pkIs1330([hsp-16::gpa-12(Q->L)])|WBls:0000023(larva)|GO:0040007(growth) QUALITY:PATO:0000297(arrested) NOT"
Remark	"Genotype \"tpa-1(pk1397);pkIs1330[hsp::gpa-12(Q->L)];Ex[dpy-7::TPA-1]\""
Remark	"Published_as tpa-1"
Remark	"Transgenic animals carrying tpa-1B cDNA under control of a hypodermal promoter (dpy-7) did not show a growth arrest, but resulted in cuticle defects."
Reference	"WBPaper00005783"


Anatomy_function : "WBbtf0215"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000019"	Autonomous
Gene	"WBGene00006599"
Not_involved	"WBbt:0007846"	Insufficient
Remark	"ENTITY:CHEBI:37537(phorbol 13-acetate 12-myristate)|WBbt:0005451(pharyngeal muscle cell)|GO:0006936(muscle contraction) QUALITY:PATO:0000381(decreased frequency) NOT"
Remark	"ENTITY:CHEBI:37537(phorbol 13-acetate 12-myristate)|WBls:0000023(larva)|GO:0040007(growth) QUALITY:PATO:0000297(arrested) NOT"
Remark	"Genotype \"tpa-1(pk1397);Ex[dpy-7::TPA-1]\""
Remark	"Published_as tpa-1"
Remark	"Transgenic animals carrying tpa-1B cDNA under control of a hypodermal promoter (dpy-7) did not show a growth arrest, but resulted in cuticle defects."
Reference	"WBPaper00005783"


Anatomy_function : "WBbtf0216"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000019"	Autonomous
Gene	"WBGene00001674"
Remark	"ENTITY:WBbt:0005451(pharyngeal muscle cell)|GO:0006936(muscle contraction) QUALITY:PATO:0000381(decreased frequency)"
Remark	"ENTITY:WBls:0000023(larva)|GO:0040007(growth) QUALITY:PATO:0000297(arrested)"
Remark	"Genotype \"Ex[myo-2::gpa-12(Q->L)\""
Remark	"Published_as gpa-12"
Remark	"expression of G12QL from the myo-2 promoter [myo-2::gpa-12(Q->L)] is able to induce a developmental growth arrest."
Reference	"WBPaper00005783"


Anatomy_function : "WBbtf0217"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000106"	Autonomous
Gene	"WBGene00006868"
Involved	"WBbt:0006797"	Necessary
Remark	"ENTITY:WBbt:0006797(oocyte)|GO:0045835(negative regulation of meiosis) QUALITY:PATO:0000468(decreased amount)"
Remark	"ENTITY:WBbt:0007849(hermaphrodite)|GO:0060280(negative regulation of ovulation) QUALITY:PATO:0000468(decreased amount)"
Remark	"Genotype \"rrf-1(pk1417)\""
Remark	"Published_as vab-1"
Remark	"vab-1(RNAi); rrf-1(pk1417) hermaphrodites lay significantly more unfertilized oocytes than rrf-1(pk1417) hermaphrodites. rrf-1 mutants are sensitive to RNAi in the germ line, but resistant to RNAi in the soma."
Reference	"WBPaper00005670"


Anatomy_function : "WBbtf0218"
Phenotype	"WBPhenotype:0000105"
Involved	"WBbt:0006797"	Remark
Involved	"WBbt:0005828"	Remark
Remark	"ENTITY:WBbt:0007849(hermaphrodite)|GO:0005515(protein binding)|MSP(major sperm protein) QUALITY:PATO:0000071(amount)"
Remark	"MSP-FITC binds to oocyte and proximal sheath cell membranes at low nM concentrations in wild-type hermaphrodites and fog-2(q71) females."
Reference	"WBPaper00005670"


Anatomy_function : "WBbtf0219"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000106"	Autonomous
Gene	"WBGene00001163"
Involved	"WBbt:0006797"	Necessary
Remark	"ENTITY:WBbt:0006797(oocyte)|GO:0045835(negative regulation of meiosis) QUALITY:PATO:0000468(decreased amount)"
Remark	"ENTITY:WBbt:0007849(hermaphrodite)|GO:0060280(negative regulation of ovulation) QUALITY:PATO:0000468(decreased amount)"
Remark	"Genotype \"rrf-1(pk1417)\""
Remark	"Published_as efn-2"
Remark	"efn-2(RNAi); rrf-1(pk1417) hermaphrodites lay significantly more unfertilized oocytes than rrf-1(pk1417) hermaphrodites. rrf-1 mutants are sensitive to RNAi in the germ line, but resistant to RNAi in the soma."
Reference	"WBPaper00005670"


Anatomy_function : "WBbtf0220"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001199"	Autonomous
Gene	"WBGene00006868"
Involved	"WBbt:0005828"	Sufficient
Remark	"ENTITY:WBbt:0005828(gonadal sheath cell)|GO:0006939(smooth muscle contraction) QUALITY:PATO:0000468(decreased amount) NOT"
Remark	"Genotype \"rrf-1(pk1417)\""
Remark	"Published_as vab-1"
Remark	"gonadal sheath cell contraction rate in vab-1(RNAi); rrf-1(pk1417) hermaphrodites is similar to that of rrf-1(pk1417) but significantly higher than that of vab-1(RNAi) animals. rrf-1 mutants are sensitive to RNAi in the germ line, but resistant to RNAi in the soma."
Reference	"WBPaper00005670"


Anatomy_function : "WBbtf0221"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001237"	Autonomous
Gene	"WBGene00006770"
Involved	"WBbt:0005237"	Sufficient
Remark	"ENTITY:WBbt:0005237(touch receptor neuron)|GO:0048812(neurite morphogenesis) QUALITY:PATO:0000760(hyperactive)"
Remark	"Genotype \"kyIs192[mec-7::myr::unc-40,str-1::gfp];unc-34(gm104,e951);Ex[mec-7::unc-34]\""
Remark	"Published_as unc-34"
Remark	"unc-34; mec-7::myr::unc-40 animals exhibited partial suppression of the excessive outgrowth phenotype caused by mec-7::myr::unc-40. unc-34 animals bearing both the mec-7::myr::unc-40 and the mec-7::unc-34 transgenes exhibited excessive outgrowth at a level comparable to mec-7::myr::unc-40 in a wild-type background, indicating that unc-34 and myr::unc-40 act in the same cell."
Reference	"WBPaper00005719"


Anatomy_function : "WBbtf0222"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001237"	Autonomous
Gene	"WBGene00000424"
Involved	"WBbt:0005237"	Sufficient
Remark	"ENTITY:WBbt:0005237(touch receptor neuron)|GO:0048812(neurite morphogenesis) QUALITY:PATO:0000760(hyperactive)"
Remark	"Genotype \"kyIs192[mec-7::myr::unc-40,str-1::gfp];ced-10(n1993,n3246);Ex[mec-7::ced-10]\""
Remark	"Published_as ced-10"
Remark	"ced-10; mec-7::myr::unc-40 animals exhibited partial suppression of the excessive outgrowth phenotype caused by mec-7::myr::unc-40. The partial suppression was eliminated in animals expressing mec-7::ced-10."
Reference	"WBPaper00005719"


Anatomy_function : "WBbtf0223"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001237"	Autonomous
Gene	"WBGene00006839"
Involved	"WBbt:0005237"	Sufficient
Remark	"ENTITY:WBbt:0005237(touch receptor neuron)|GO:0048812(neurite morphogenesis) QUALITY:PATO:0000760(hyperactive)"
Remark	"Genotype \"kyIs192[mec-7::myr::unc-40,str-1::gfp];unc-115(ky274,ky275);Ex[mec-7::unc-115]\""
Remark	"Published_as unc-115"
Remark	"unc-115; mec-7::myr::unc-40 animals exhibited partial suppression of the excessive outgrowth phenotype caused by mec-7::myr::unc-40. The partial suppression was eliminated in animals expressing mec-7::unc-115."
Reference	"WBPaper00005719"


Anatomy_function : "WBbtf0224"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000400"
Gene	"WBGene00001981"
Not_involved	"WBbt:0005784"	Unnecessary
Remark	"ENTITY:WBbt:0005175(gonad)|GO:0048513(organ development) QUALITY:PATO:0000460(abnormal) NOT"
Remark	"ENTITY:WBbt:0007854(somatic gonad precursor cell)|GO:0045165(cell fate commitment) QUALITY:PATO:0001507(disrupted) NOT"
Remark	"Genotype \"hnd-1(q740);qEx495[hnd-1(+) myo-3::YFP pes-1::CFP]\""
Remark	"Published_as hnd-1"
Remark	"'germline mosaics', animals that retained the (hnd-1 genomic fragment transgene) array in somatic tissues but failed to transmit it to their progeny; such animals have lost the array in divisions generating the germline blastomere P4. All six germline mosaics had a wild-type gonadal primordium."
Reference	"WBPaper00006002"


Anatomy_function : "WBbtf0225"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000400"	Nonautonomous
Gene	"WBGene00001981"
Involved	"WBbt:0007810"	Sufficient
Remark	"ENTITY:WBbt:0005175(gonad)|GO:0048513(organ development) QUALITY:PATO:0000460(abnormal) NOT"
Remark	"ENTITY:WBbt:0007854(somatic gonad precursor cell)|GO:0045165(cell fate commitment) QUALITY:PATO:0001507(disrupted) NOT"
Remark	"Expression of HND-1::GFP by the hlh-1 promoter rescued the hnd-1 gonadogenesis defects. hlh-1 promoter is active in body muscle and not in SGPs (somatic gonadal precursor cells)."
Remark	"Genotype \"hnd-1(q740); qEx496[hlh-1::hnd-1::gfp]\""
Remark	"Published_as hnd-1"
Reference	"WBPaper00006002"


Anatomy_function : "WBbtf0226"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000400"	Nonautonomous
Gene	"WBGene00001981"
Not_involved	"WBbt:0007854"	Insufficient
Remark	"ENTITY:WBbt:0005175(gonad)|GO:0048513(organ development) QUALITY:PATO:0000460(abnormal)"
Remark	"ENTITY:WBbt:0007854(somatic gonad precursor cell)|GO:0045165(cell fate commitment) QUALITY:PATO:0001507(disrupted)"
Remark	"Genotype \"hnd-1(q740); qEx497[lag-2::hnd-1::gfp]\""
Remark	"HND-1::GFP driven from the lag-2 promoter, which is expressed in the two SGPs (somatic gonadal precursor cells), did not appreciably rescue hnd-1 gonadogenesis defects."
Remark	"Published_as hnd-1"
Reference	"WBPaper00006002"


Anatomy_function : "WBbtf0227"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000637"
Involved	"WBbt:0007855"	Necessary
Remark	"ENTITY:GO:0051093(negative regulation of developmental process)|WBls:0000032(dauer larva) QUALITY:PATO:0000761(hypoactive)"
Remark	"ENTITY:WBbt:0003681(pharynx)|WBls:0000032(dauer larva) QUALITY:PATO:(unconstricted)"
Remark	"Genotype \"Ex[sdf-9p::GFP1, gcy-10::GFP]\""
Remark	"killing XXXL/R cells in L1 larvae by laser microbeam surgery caused about 30% of the operated wild-type animals to become dauer-like larvae resembling those of sdf-9 and having a non-constricted, pumping pharynx."
Reference	"WBPaper00006015"


Anatomy_function : "WBbtf0228"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000643"
Gene	"WBGene00006807"
Involved	"WBbt:0003679"	Necessary
Involved	"WBbt:0003679"	Remark
Remark	"An extrachromosomal array was created that contains the rescuing C17D12 cosmid and two GFP reporters that mark the neuronal and muscle lineages."
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050879(multicellular organismal movement) QUALITY:PATO:0001860(decreased coordination)"
Remark	"Early array loss at AB leads to no rescue in animals."
Remark	"Published_as unc-75"
Reference	"WBPaper00006029"


Anatomy_function : "WBbtf0229"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000643"
Gene	"WBGene00006807"
Not_involved	"WBbt:0007810"	Unnecessary
Not_involved	"WBbt:0007810"	Remark
Remark	"An extrachromosomal array was created that contains the rescuing C17D12 cosmid and two GFP reporters that mark the neuronal and muscle lineages."
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050879(multicellular organismal movement) QUALITY:PATO:0001860(decreased coordination)"
Remark	"Published_as unc-75"
Remark	"animals showing losses at P1 were still rescued."
Reference	"WBPaper00006029"


Anatomy_function : "WBbtf0230"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000005"
Involved	"WBbt:0004617"	Necessary
Involved	"WBbt:0004613"	Necessary
Remark	"ENTITY:WBls:0000041(adult)|WBbt:0007849(hermaphrodite)|GO:0018991(oviposition) QUALITY:PATO:0000760(hyperactive)"
Remark	"Genotype \"vsIs13[modified lin-11::gfp]\""
Remark	"Of 20 VC4/5 ablated animals, six were strongly hyperactive for egg laying. Ablation of all six VC neurons resulted in small adults that produced few eggs."
Reference	"WBPaper00006049"


Anatomy_function : "WBbtf0231"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000005"
Gene	"WBGene00006744"
Involved	"WBbt:0005304"	Sufficient
Remark	"ENTITY:WBls:0000041(adult)|WBbt:0007849(hermaphrodite)|GO:0018991(oviposition) QUALITY:PATO:0000760(hyperactive) NOT"
Remark	"Expression of the unc-4 cDNA using a modified lin-11 promoter that drives expression in six VC neurons rescued the hyperactive egg-laying defect of unc-4 mutants."
Remark	"Genotype \"unc-4; Ex[modified lin-11::unc-4]\""
Remark	"Published_as unc-4"
Reference	"WBPaper00006049"


Anatomy_function : "WBbtf0232"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000005"
Gene	"WBGene00000481"
Involved	"WBbt:0005304"	Sufficient
Remark	"ENTITY:WBls:0000041(adult)|WBbt:0007849(hermaphrodite)|GO:0018991(oviposition) QUALITY:PATO:0000760(hyperactive) NOT"
Remark	"Expression of the cha-1 cDNA using a modified lin-11 promoter that drives expression in six VC neurons rescued the hyperactive egg-laying defect of cha-1 mutants."
Remark	"Genotype \"cha-1; Ex[modified lin-11::cha-1]\""
Remark	"Published_as cha-1"
Reference	"WBPaper00006049"


Anatomy_function : "WBbtf0233"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000005"
Gene	"WBGene00006756"
Involved	"WBbt:0005304"	Sufficient
Remark	"ENTITY:WBls:0000041(adult)|WBbt:0007849(hermaphrodite)|GO:0018991(oviposition) QUALITY:PATO:0000760(hyperactive) NOT"
Remark	"Expression of the unc-17 cDNA using a modified lin-11 promoter that drives expression in six VC neurons rescued the hyperactive egg-laying defect of unc-17 mutants."
Remark	"Genotype \"unc-17; Ex[modified lin-11::unc-17]\""
Remark	"Published_as unc-17"
Reference	"WBPaper00006049"


Anatomy_function : "WBbtf0234"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001272"	Autonomous
Gene	"WBGene00000238"
Involved	"WBbt:0008117"	Sufficient
Remark	"Analyzed 24 mosaic animals in which P4.p contained the array but in which other cells had lost the array, and found that P4.p did not adopt the F (mutant) fate in any case."
Remark	"ENTITY:WBbt:0006892(P4.p)|GO:0001708(cell fate specification) QUALITY:PATO:0001507(disrupted) NOT"
Remark	"Genotype \"unc-29(e1072); ncl-1(e1942); unc-30(e191); bar-1(ga80); gaEx117[F35D3; C33C3; pSC11; pDE204]\""
Remark	"Published_as bar-1"
Reference	"WBPaper00003200"


Anatomy_function : "WBbtf0235"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001272"	Autonomous
Gene	"WBGene00000238"
Involved	"WBbt:0004409"	Remark
Remark	"Published_as bar-1"
Remark	"data not shown."
Reference	"WBPaper00003200"


Anatomy_function : "WBbtf0236"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000633"	Nonautonomous
Gene	"WBGene00000237"
Involved	"WBbt:0006768"	Sufficient
Remark	"ENTITY:WBbt:0004617(VC4)|GO:0048668(collateral sprouting)|WBbt:0006748(vulva) QUALITY:PATO(excessive) NOT"
Remark	"ENTITY:WBbt:0004613(VC5)|GO:0048668(collateral sprouting)|WBbt:0006748(vulva) QUALITY:PATO(excessive) NOT"
Remark	"Genotype \"bam-2; Ex[deltaxbalp:bam-2::gfp]\""
Remark	"Published_as bam-2"
Remark	"The VC branch guidance defects in bam-2 mutants were rescued when bam-2 was expressed in VulF with endogenous promoter elements or the heterologous vulval-specific promoter B0024.1p."
Reference	"WBPaper00006123"


Anatomy_function : "WBbtf0237"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000633"	Nonautonomous
Gene	"WBGene00000237"
Not_involved	"WBbt:0004617"	Insufficient
Not_involved	"WBbt:0004613"	Insufficient
Remark	"ENTITY:WBbt:0004617(VC4)|GO:0048668(collateral sprouting)|WBbt:0006748(vulva) QUALITY:PATO(excessive)"
Remark	"ENTITY:WBbt:0004613(VC5)|GO:0048668(collateral sprouting)|WBbt:0006748(vulva) QUALITY:PATO(excessive)"
Remark	"Genotype \"bam-2; Ex[cat-1:bam-2::gfp]\""
Remark	"Published_as bam-2"
Remark	"The VC branch guidance defects in bam-2 mutants were not rescued when bam-2 was expressed ectopically in VC4 and VC5 by means of the cat-1 promoter."
Reference	"WBPaper00006123"


Anatomy_function : "WBbtf0238"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000885"
Gene	"WBGene00004205"
Involved	"WBbt:0007803"	Sufficient
Remark	"ENTITY:GO:0043652(engulfment of apoptotic cell) QUALITY:PATO:0000468(decreased amount)"
Remark	"Expression of PSR-1 in the psr-1(tm469) mutant under the control of the promoter of the ced-1 gene, which is expressed in cell types acting as engulfing cells but not in dying cells fully rescued the corpse engulfment defect of the psr-1 mutant."
Remark	"Genotype \"psr-1(tm469); Ex[pced-1::psr-1]\""
Remark	"Published_as psr-1"
Reference	"WBPaper00006212"


Anatomy_function : "WBbtf0239"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000201"
Gene	"WBGene00004754"
Involved	"WBbt:0007846"	Sufficient
Remark	"ENTITY:WBbt:0005755(cuticle)|GO:0009058(biosynthetic process) QUALITY:PATO:0000468(decreased amount) NOT"
Remark	"ENTITY:WBls:0000015(elongating embryo)|GO:0010171(body morphogenesis) QUALITY:PATO:0000297(incomplete) NOT"
Remark	"Genotype \"sec-23(ij13); Ex[dpy::sec-23,col-12::GFP]\""
Remark	"Published_as sec-23"
Remark	"sec-23(ij13) homozygotes that carried also the dpy-7::sec-23 gene fusion elongated completely, produced a functional cuticle, and expressed the col-12::GFP reporter. Thus, restoration of zygotic sec-23 function only in the hypodermis was sufficient to rescue the embryonic elongation and cuticle synthesis defects of the sec-23(ij13) mutant."
Reference	"WBPaper00006236"


Anatomy_function : "WBbtf0240"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001612"
Gene	"WBGene00004830"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0031987(locomotion during locomotory behavior)|PATO:0000468(decreased amount)|GO:0042221(response to chemical stimulus)|CHEBI:16236(ethanol) QUALITY:PATO:0000468(decreased amount) NOT"
Remark	"Genotype \"slo-1(js118); Ex[Psnb-1::slo-1]\""
Remark	"Published_as slo-1"
Remark	"expression of slo-1(+) in neurons can fully restore ethanol sensitivity for locomotion to a slo-1(js118) null mutant."
Reference	"WBPaper00006275"


Anatomy_function : "WBbtf0241"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001612"
Gene	"WBGene00004830"
Not_involved	"WBbt:0007810"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0031987(locomotion during locomotory behavior)|PATO:0000468(decreased amount)|GO:0042221(response to chemical stimulus)|CHEBI:16236(ethanol) QUALITY:PATO:0000468(decreased amount)"
Remark	"Genotype \"slo-1(js118); Ex[Pmyo-3::slo-1]\""
Remark	"Published_as slo-1"
Remark	"expression of slo-1(+) in muscle resulted in no significant restoration of ethanol sensitivity for locomotion to a slo-1(js118) null mutant."
Reference	"WBPaper00006275"


Anatomy_function : "WBbtf0242"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001612"
Gene	"WBGene00004830"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0018991(oviposition)|PATO:0000381(decreased frequency)|GO:0042221(response to chemical stimulus)|CHEBI:16236(ethanol) QUALITY:PATO:0000468(decreased amount) NOT"
Remark	"Neuronal expression of slo-1(+) in slo-1(js118) mutant animals partially restored ethanol sensitivity for egg laying."
Remark	"Published_as slo-1"
Reference	"WBPaper00006275"


Anatomy_function : "WBbtf0243"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000643"
Gene	"WBGene00001395"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050881(musculoskeletal movement) QUALITY:PATO:0000468(decreased amount) NOT"
Remark	"Genotype \"fat-3(lg8101); Ex[Punc-119::fat-3]\""
Remark	"Published_as fat-3"
Remark	"fat-3 expressed under the control of the neuronal promoter almost completely rescue the movement defects of fat-3(lg8101) homozygous animals."
Reference	"WBPaper00006282"


Anatomy_function : "WBbtf0244"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000643"
Gene	"WBGene00001395"
Not_involved	"WBbt:0007810"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050881(musculoskeletal movement) QUALITY:PATO:0000468(decreased amount)"
Remark	"Genotype \"fat-3(lg8101); Ex[Pmyo-3::fat-3]\""
Remark	"Published_as fat-3"
Remark	"fat-3 expressed under the control of the muscular promoter did not rescue the movement defects of fat-3(lg8101) homozygous animals."
Reference	"WBPaper00006282"


Anatomy_function : "WBbtf0245"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000643"
Gene	"WBGene00001395"
Not_involved	"WBbt:0005792"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050881(musculoskeletal movement) QUALITY:PATO:0000468(decreased amount)"
Remark	"Genotype \"fat-3(lg8101); Ex[Pelt-2::fat-3]\""
Remark	"Published_as fat-3"
Remark	"fat-3 expressed under the control of the intestinal promoter did not rescue the movement defects of fat-3(lg8101) homozygous animals."
Reference	"WBPaper00006282"


Anatomy_function : "WBbtf0246"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000006"
Gene	"WBGene00001395"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBbt:0007849(hermaphrodite)|GO:0018991(oviposition) QUALITY:PATO:0000468(decreased amount) NOT"
Remark	"Genotype \"fat-3(lg8101)/fat-3(qa1811); Ex[Punc-119::fat-3]\""
Remark	"Published_as fat-3"
Remark	"fat-3 expressed under the control of the neuronal promoter unc-119 completely rescue the egg-laying defect of fat-3(lg8101)/fat-3(qa1181) animals."
Reference	"WBPaper00006282"


Anatomy_function : "WBbtf0247"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000006"
Gene	"WBGene00001395"
Not_involved	"WBbt:0007810"	Insufficient
Remark	"ENTITY:WBbt:0007849(hermaphrodite)|GO:0018991(oviposition) QUALITY:PATO:0000468(decreased amount)"
Remark	"Genotype \"fat-3(lg8101)/fat-3(qa1811); Ex[Pmyo-3::fat-3]\""
Remark	"Published_as fat-3"
Remark	"fat-3 expressed under the control of the muscular promoter myo-3 did not rescue the egg-laying defect of fat-3(lg8101)/fat-3(qa1181) animals."
Reference	"WBPaper00006282"


Anatomy_function : "WBbtf0248"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000017"
Gene	"WBGene00001395"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050881(musculoskeletal movement)|GO:0042221(response to chemical stimulus)|CHEBI:2555(aldicarb) QUALITY:PATO:0000468(decreased amount) NOT"
Remark	"Published_as fat-3"
Remark	"fat-3 expressed in neurons restores normal aldicarb sensitivity to fat-3(lg8101) mutants."
Reference	"WBPaper00006282"


Anatomy_function : "WBbtf0249"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000017"
Gene	"WBGene00001395"
Not_involved	"WBbt:0007810"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050881(musculoskeletal movement)|GO:0042221(response to chemical stimulus)|CHEBI:2555(aldicarb) QUALITY:PATO:0000468(decreased amount)"
Remark	"Published_as fat-3"
Remark	"fat-3 expressed in muscles, does not restore normal aldicarb sensitivity to fat-3(lg8101) mutants."
Reference	"WBPaper00006282"


Anatomy_function : "WBbtf0250"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000195"
Gene	"WBGene00003254"
Involved	"WBbt:0003810"	Necessary
Remark	"ENTITY:WBbt:0006865(DTC)|GO:0016477(cell migration)|PATO:0001233(dorsal to)|WBbt:0005753(seam cell) QUALITY:PATO:0000468(reduced)"
Remark	"Genotype \"mig-23(k180); ncl-1(e1865); Ex[mig-23(+),sur-5::GFP,ncl-1(+)]\""
Remark	"Published_as mig-23"
Remark	"genetic mosaic analysis revealed that MIG-23 is required in the C lineage and NOT required in the AB, EMS and P3 lineages."
Reference	"WBPaper00006309"


Anatomy_function : "WBbtf0251"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000195"
Gene	"WBGene00003254"
Not_involved	"WBbt:0004015"	Unnecessary
Remark	"ENTITY:WBbt:0006865(DTC)|GO:0016477(cell migration)|PATO:0001233(dorsal to)|WBbt:0005753(seam cell) QUALITY:PATO:0000468(reduced) NOT"
Remark	"Published_as mig-23"
Remark	"genetic mosaic analysis revealed that MIG-23 is not required in the AB lineage."
Reference	"WBPaper00006309"


Anatomy_function : "WBbtf0252"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000195"
Gene	"WBGene00003254"
Not_involved	"WBbt:0006876"	Unnecessary
Remark	"ENTITY:WBbt:0006865(DTC)|GO:0016477(cell migration)|PATO:0001233(dorsal to)|WBbt:0005753(seam cell) QUALITY:PATO:0000468(reduced) NOT"
Remark	"Published_as mig-23"
Remark	"genetic mosaic analysis revealed that MIG-23 is not required in the EMS lineage."
Reference	"WBPaper00006309"


Anatomy_function : "WBbtf0253"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000195"	Nonautonomous
Gene	"WBGene00003254"
Involved	"WBbt:0006804"	Sufficient
Remark	"ENTITY:WBbt:0006865(DTC)|GO:0016477(cell migration)|PATO:0001233(dorsal to)|WBbt:0005753(seam cell) QUALITY:PATO:0000468(reduced) NOT"
Remark	"Genotype \"mig-23(k180); Ex[unc-54p::mig-23::GFP]\""
Remark	"Published_as mig-23"
Remark	"When the unc54p::mig-23::GFP transgene was introduced into mig-23 mutants, it rescued the DTC migration defects."
Reference	"WBPaper00006309"


Anatomy_function : "WBbtf0254"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000195"
Gene	"WBGene00003254"
Not_involved	"WBbt:0007846"	Insufficient
Remark	"ENTITY:WBbt:0006865(DTC)|GO:0016477(cell migration)|PATO:0001233(dorsal to)|WBbt:0005753(seam cell) QUALITY:PATO:0000468(reduced)"
Remark	"Genotype \"mig-23(k180); Ex[dpy-7p::mig-23::GFP]\""
Remark	"Published_as mig-23"
Remark	"When the dpy-7::mig-23::GFP transgene was expressed in mig-23 mutants, the fusion gene failed to rescue the DTC migration defects."
Reference	"WBPaper00006309"


Anatomy_function : "WBbtf0255"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000306"	Autonomous
Gene	"WBGene00000553"
Involved	"WBbt:0005662"	Sufficient
Remark	"ENTITY:WBbt:0005662(AFD)|Temperature:25|Transgene:(gcy-8::gfp)|GO:0010467(gene expression) QUALITY:PATO:0000468(decreased amount) NOT"
Remark	"Expression of a cmk-1 cDNA exclusively in the AFD neurons under the ttx-1 promoter fully rescued the gcy-8 expression defects of cmk-1 mutants."
Remark	"Genotype \"cmk-1(oy21);gcy-8::gfp; Ex[ttx-1::cmk-1]\""
Remark	"Published_as cmk-1"
Reference	"WBPaper00006343"


Anatomy_function : "WBbtf0256"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000306"	Autonomous
Gene	"WBGene00006526"
Involved	"WBbt:0005662"	Sufficient
Remark	"ENTITY:WBbt:0005662(AFD)|Temperature:15|Transgene:(gcy-8::gfp)|GO:0010467(gene expression) QUALITY:PATO:0000468(decreased amount) NOT"
Remark	"Expression of a tax-4 cDNA exclusively in the AFD neurons under the ttx-1 promoter fully rescued the gcy-8 expression defects of tax-4 mutants."
Remark	"Genotype \"tax-4(p678);gcy-8::gfp; Ex[ttx-1::tax-4]\""
Remark	"Published_as tax-4"
Reference	"WBPaper00006343"


Anatomy_function : "WBbtf0257"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000999"
Gene	"WBGene00000553"
Involved	"WBbt:0005662"	Sufficient
Remark	"At the culturing temperature of 17C, cmk-1 mutant animals showed a turning ratio less than that of wild type; expression of CMK-1 in the AFD neurons restored wild-type behavior of cmk-1 mutants."
Remark	"ENTITY:WBbt:0007833(organism)|GO:0040040(thermosensory behavior) QUALITY:PATO:0000468(decreased amount) NOT"
Remark	"Genotype \"cmk-1(oy21);Ex[ttx-1::cmk-1]\""
Remark	"Published_as cmk-1"
Reference	"WBPaper00006343"


Anatomy_function : "WBbtf0258"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000999"
Gene	"WBGene00006526"
Involved	"WBbt:0005662"	Sufficient
Remark	"At the culturing temperature of 17C, tax-4 mutant animals showed a turning ratio less than that of wild type; expression of TAX-4 in the AFD neurons restored wild-type behavior of cmk-1 mutants."
Remark	"ENTITY:WBbt:0005662(AFD)|GO:0040040(thermosensory behavior) QUALITY:PATO:0000468(decreased amount) NOT"
Remark	"Genotype \"tax-4(p678);Ex[ttx-1::tax-4]\""
Remark	"Published_as tax-4"
Reference	"WBPaper00006343"


Anatomy_function : "WBbtf0259"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000012"
Gene	"WBGene00000901"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:Genotype:daf-7(e1372)|GO:0043053(dauer entry) QUALITY:PATO:0000468(	decreased amount) NOT"
Remark	"Genotype \"daf-5(e1386);daf-7(e1372);Ex[pF25B3.3::daf-5::gfp]\""
Remark	"Published_as daf-5"
Remark	"pF25B3.3 strongly expressed daf-5::GFP exclusively in nervous system and rescued daf-5 mutants. Similarly punc-14, which expressed daf-5::GFP in nervous system at high level in addition to some non-neuronal expression, also showed strong rescue, transgenic daf-5;daf-7 animals formed dauer constitutively."
Reference	"WBPaper00006391"


Anatomy_function : "WBbtf0260"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000012"
Gene	"WBGene00000901"
Not_involved	"WBbt:0007810"	Insufficient
Remark	"ENTITY:Genotype:daf-7(e1372)|GO:0043053(dauer entry) QUALITY:PATO:0000468(	decreased amount)"
Remark	"Genotype \"daf-5(e1386);daf-7(e1372);Ex[pmyo-3::daf-5::gfp]\""
Remark	"Published_as daf-5"
Remark	"Strong expression of daf-5::GFP from the muscle promoter pmyo-3 did not rescue at all; daf-5;daf-7 transgenic animals did not form dauers consitutively."
Reference	"WBPaper00006391"


Anatomy_function : "WBbtf0261"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000012"
Gene	"WBGene00000901"
Not_involved	"WBbt:0007846"	Insufficient
Remark	"ENTITY:Genotype:daf-7(e1372)|GO:0043053(dauer entry) QUALITY:PATO:0000468(	decreased amount)"
Remark	"Genotype \"daf-5(e1386);daf-7(e1372);Ex[pdpy-7::daf-5::gfp]\""
Remark	"Published_as daf-5"
Remark	"Strong expression of daf-5::GFP from the hypodermal promoter pdpy-7 did not rescue at all; daf-5;daf-7 transgenic animals did not form dauers consitutively."
Reference	"WBPaper00006391"


Anatomy_function : "WBbtf0262"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0004027"
Gene	"WBGene00001052"
Involved	"WBbt:0005237"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0007638(mechanosensory behavior)|GO:0046959(habituation) QUALITY:PATO:0000912(increased rate) NOT"
Remark	"Genotype \"dop-1(ev748);him-5(e1490);Ex[pmec-7:dop-1\""
Remark	"Published_as dop-1"
Remark	"Transgenic animals of dop-1 mutants carrying dop-1(+) coding region under the control of the touch-neuron specific mec-7 promoter did not exhibit the dop-1 precocious habituation phenotype."
Reference	"WBPaper00006389"


Anatomy_function : "WBbtf0263"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000203"
Gene	"WBGene00006543"
Involved	"WBbt:0005672"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0022401(adaptation of signaling pathway)|GO:0042048(olfactory behavior)|CHEBI:15837(isoamylol) QUALITY:PATO:0000468(decreased amount) NOT"
Remark	"Genotype \"sdf-13(ut180);Ex[pgpa-2::tbx-2]\""
Remark	"Published_as sdf-13"
Remark	"Transformants of ut180 mutant transformed with Ce-tbx-2 cDNA connected to gcy-10 or gpa-2 promoters (drive expression in AWC, AWB and I1 neurons, AWC neurons, respectively) restored normal adaption to isoamy alcohol."
Reference	"WBPaper00006381"


Anatomy_function : "WBbtf0264"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000203"
Gene	"WBGene00006543"
Not_involved	"WBbt:0005671"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0022401(adaptation of signaling pathway)|GO:0042048(olfactory behavior)|CHEBI:15837(isoamylol) QUALITY:PATO:0000468(decreased amount)"
Remark	"Genotype \"sdf-13(ut180);Ex[pstr-1::tbx-2]\""
Remark	"Published_as sdf-13"
Remark	"Transformants of ut180 mutant transformed with Ce-tbx-2 cDNA connected to str-1 promoter (drives expression in AWB neurons) did not restore normal adaption to isoamy alcohol."
Reference	"WBPaper00006381"


Anatomy_function : "WBbtf0265"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000306"	Autonomous
Gene	"WBGene00002004"
Involved	"WBbt:0006804"	Necessary
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|GO:0034605(cellular response to heat)|GO:0010628(positive regulation of gene expression)|Gene:hsp-70 QUALITY:PATO:0000468(decreased amount)"
Remark	"Expression of a dominant negative HSF-1 under control of the unc-54 promoter resulted in muscle specific loss of heat shock promoter inducible GFP reporter expression."
Remark	"Genotype \"Ex[pC12C8.1::gfp, punc-54::hsf-1DN]\""
Remark	"Published_as hsf-1"
Reference	"WBPaper00006377"


Anatomy_function : "WBbtf0266"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000306"	Autonomous
Gene	"WBGene00002004"
Involved	"WBbt:0003679"	Necessary
Remark	"ENTITY:WBbt:0003679(neuron)|GO:0034605(cellular response to heat)|GO:0010628(positive regulation of gene expression)|Gene:hsp-70 QUALITY:PATO:0000468(decreased amount)"
Remark	"Expression of a dominant negative HSF-1 under control of the neuronal F25B3.3 promoter resulted in neuron specific loss of heat shock promoter inducible GFP reporter expression."
Remark	"Genotype \"Ex[pC12C8.1::gfp, pF25B3.3::hsf-1DN]\""
Remark	"Published_as hsf-1"
Reference	"WBPaper00006377"


Anatomy_function : "WBbtf0267"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000306"	Autonomous
Gene	"WBGene00002004"
Involved	"WBbt:0005792"	Necessary
Remark	"ENTITY:WBbt:0005792(intestinal cell)|GO:0034605(cellular response to heat)|GO:0010628(positive regulation of gene expression)|Gene:hsp-70 QUALITY:PATO:0000468(decreased amount)"
Remark	"Expression of a dominant negative HSF-1 under control of the intestinal vha-6 promoter resulted in intestinal specific loss of heat shock promoter inducible GFP reporter expression."
Remark	"Genotype \"Ex[pC12C8.1::gfp, pvha-6::hsf-1DN]\""
Remark	"Published_as hsf-1"
Reference	"WBPaper00006377"


Anatomy_function : "WBbtf0268"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000306"	Autonomous
Gene	"WBGene00002004"
Involved	"WBbt:0006804"	Sufficient
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|GO:0010467(gene expression)|Gene:hsp-70 QUALITY:PATO:0000470(increased amount)"
Remark	"Genotype \"Ex[pC12C8.1::gfp, punc-54::hsf-1]\""
Remark	"Overexpression of HSF-1 under control of the unc-54 promoter resulted in muscle specific increase of hsp-70 GFP reporter expression."
Remark	"Published_as hsf-1"
Reference	"WBPaper00006377"


Anatomy_function : "WBbtf0269"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000306"	Autonomous
Gene	"WBGene00002004"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBbt:0003679(neuron)|GO:0010467(gene expression)|Gene:hsp-70 QUALITY:PATO:0000470(increased amount)"
Remark	"Genotype \"Ex[pC12C8.1::gfp, pF25B3.3::hsf-1]\""
Remark	"Overexpression of HSF-1 under control of the neuronal F25B3.3 promoter resulted in neuronal specific increase of hsp-70 GFP reporter expression."
Remark	"Published_as hsf-1"
Reference	"WBPaper00006377"


Anatomy_function : "WBbtf0270"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000306"	Autonomous
Gene	"WBGene00002004"
Involved	"WBbt:0005792"	Sufficient
Remark	"ENTITY:WBbt:0005792(intestinal cell)|GO:0010467(gene expression)|Gene:hsp-70 QUALITY:PATO:0000470(increased amount)"
Remark	"Genotype \"Ex[pC12C8.1::gfp, pvha-6::hsf-1]\""
Remark	"Overexpression of HSF-1 under control of the intestinal vha-6 promoter resulted in intestinal specific increase of hsp-70 GFP reporter expression."
Remark	"Published_as hsf-1"
Reference	"WBPaper00006377"


Anatomy_function : "WBbtf0271"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000039"
Gene	"WBGene00002004"
Involved	"WBbt:0006804"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0010259(multicellular organismal aging) QUALITY:PATO:0000911(decreased rate)"
Remark	"Genotype \"Ex[myo-2::gfp, punc-54::hsf-1]\""
Remark	"Overexpression of HSF-1 in body-wall muscle cells of otherwise wild-type animals resulted in a significant (15%) extension of life span."
Remark	"Published_as hsf-1"
Reference	"WBPaper00006377"


Anatomy_function : "WBbtf0272"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000039"
Gene	"WBGene00002004"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0010259(multicellular organismal aging) QUALITY:PATO:0000911(decreased rate)"
Remark	"Genotype \"Ex[myo-2::gfp, pF25B3.3::hsf-1]\""
Remark	"Overexpression of HSF-1 in neurons of otherwise wild-type animals resulted in a significant (15%) extension of life span."
Remark	"Published_as hsf-1"
Reference	"WBPaper00006377"


Anatomy_function : "WBbtf0273"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000039"
Gene	"WBGene00002004"
Involved	"WBbt:0006804"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|Genotype:age-1(hx546)|GO:0010259(multicellular organismal aging) QUALITY:PATO:0000912(increased rate)"
Remark	"Expression of dominant negative HSF-1 under control of the unc-54 promoter suppressed age-1(hx546) life span by 16%."
Remark	"Genotype \"age-1(hx546);Ex[myo-2::gfp, punc-54::hsf-1DN]\""
Remark	"Published_as hsf-1"
Reference	"WBPaper00006377"


Anatomy_function : "WBbtf0274"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000039"
Gene	"WBGene00002004"
Involved	"WBbt:0003679"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|Genotype:age-1(hx546)|GO:0010259(multicellular organismal aging) QUALITY:PATO:0000912(increased rate)"
Remark	"Expression of dominant negative HSF-1 under control of the neuronal F25B3.3 promoter suppressed age-1(hx546) life span by 13%."
Remark	"Genotype \"age-1(hx546);Ex[myo-2::gfp, pF25B3.3::hsf-1DN]\""
Remark	"Published_as hsf-1"
Reference	"WBPaper00006377"


Anatomy_function : "WBbtf0275"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000565"
Gene	"WBGene00006845"
Involved	"WBbt:0006804"	Sufficient
Involved	"WBbt:0005751"	Sufficient
Remark	"cof-2 gene contains cis-regulartory elements driving moderate reporter expression in muscle. Expression is also observed in coelomocytes but their involvment in unc-122 function was excluded based on other evidence."
Remark	"ENTITY:WBbt:0005740(midbody) QUALITY:PATO:0000404(coiled) NOT"
Remark	"ENTITY:WBbt:0007833(organism)|GO:0040011(locomotion) QUALITY:PATO:0000770(uncoordinated) NOT"
Remark	"Genotype \"unc-122(e2520);Ex[cof-2p::unc-122]\""
Remark	"Published_as unc-122"
Remark	"unc-122 cDNA expressed under control of the cof-2 cis-regulatory elements is capable of rescuing the unc-122 coiling phenotype. cof-2 gene contains cis-regulartory elements driving moderate reporter expression in muscle and in coelomocytes."
Reference	"WBPaper00006427"


Anatomy_function : "WBbtf0276"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000565"
Gene	"WBGene00006845"
Involved	"WBbt:0006804"	Necessary
Remark	"ENTITY:WBbt:0005740(midbody) QUALITY:PATO:0000404(coiled)"
Remark	"ENTITY:WBbt:0007833(organism)|GO:0040011(locomotion) QUALITY:PATO:0000770(uncoordinated)"
Remark	"Genotype \"unc-122(e2520);Ex[unc-122,myo-3::gfp,ttx-3::gfp]\""
Remark	"Published_as unc-122"
Remark	"mosaic animals in which AB cell descendants retained the unc-122-rescuing transgene but not P cell descendants showed coiling mutant phenotype, indicating that loss of unc-122 in muscle cell lineages affects locomotory behavior."
Reference	"WBPaper00006427"


Anatomy_function : "WBbtf0277"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000565"
Gene	"WBGene00006845"
Involved	"WBbt:0006804"	Sufficient
Remark	"ENTITY:WBbt:0005740(midbody) QUALITY:PATO:0000404(coiled) NOT"
Remark	"ENTITY:WBbt:0007833(organism)|GO:0040011(locomotion) QUALITY:PATO:0000770(uncoordinated) NOT"
Remark	"Genotype \"unc-122(e2520);Ex[unc-122,myo-3::gfp,ttx-3::gfp]\""
Remark	"Published_as unc-122"
Remark	"mosaic animals in which P cell descendants retained the unc-122-rescuing transgene but not AB cell descendants showed rescue of the coiling mutant phenotype, indicating that loss of unc-122 in neuronal lineages has no impact on locomotory behavior."
Reference	"WBPaper00006427"


Anatomy_function : "WBbtf0278"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000565"
Gene	"WBGene00006845"
Not_involved	"WBbt:0005751"	Unnecessary
Remark	"Animals in which the coelomocytes were removed still retained the ability to be rescued by the unc-122 rescuing construct."
Remark	"ENTITY:WBbt:0005740(midbody) QUALITY:PATO:0000404(coiled) NOT"
Remark	"ENTITY:WBbt:0007833(organism)|GO:0040011(locomotion) QUALITY:PATO:0000770(uncoordinated) NOT"
Remark	"Genotype \"unc-122(e2520);Ex[unc-122,ttx-3::gfp,punc-122::diphtheria_toxin_A_catalytic_fragment]\""
Remark	"Published_as unc-122"
Reference	"WBPaper00006427"


Anatomy_function : "WBbtf0279"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001398"
Gene	"WBGene00000096"
Involved	"WBbt:0005025"	Sufficient
Involved	"WBbt:0005025"	Remark
Involved	"WBbt:0005023"	Sufficient
Involved	"WBbt:0005023"	Remark
Remark	"ENTITY:WBbt:0005025(RMEL)|GO:0043005(neuron projection) QUALITY:PATO:0000628(mislocalised) NOT"
Remark	"ENTITY:WBbt:0005023(RMER)|GO:0043005(neuron projection) QUALITY:PATO:0000628(mislocalised) NOT"
Remark	"Genotype \"ahr-1(ju145);Ex[punc-25::ahr-1]\""
Remark	"Published_as ahr-1"
Remark	"a functional ahr-1::GFP transgene is expressed in RMEL/R but not in RMED/V."
Remark	"expression of ahr-1 in the four RMEs using a unc-25 promoter fully rescued the RMEL/R cell morphology defects of ahr-1(ju145) and repressed RMED/V the formation and elongation of the longitudinal processes along the nerve cords."
Reference	"WBPaper00006431"


Anatomy_function : "WBbtf0280"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000306"
Gene	"WBGene00000096"
Involved	"WBbt:0005025"	Sufficient
Involved	"WBbt:0005023"	Sufficient
Remark	"ENTITY:WBbt:0005025(RMEL)|GO:0010468(regulation of gene expression)|Gene:lim-6 QUALITY:PATO:0001507(disrupted) NOT"
Remark	"ENTITY:WBbt:0005023(RMER)|GO:0010468(regulation of gene expression)|Gene:lim-6 QUALITY:PATO:0001507(disrupted) NOT"
Remark	"Genotype \"ahr-1(ju145);Ex[punc-25::ahr-1];Ex[plim-6::GFP]\""
Remark	"Published_as ahr-1"
Remark	"expression of ahr-1 in the four RMEs using a unc-25 promoter, in ahr-1(ju145) mutant animals fully restored plim-6::GFP expression in RMEL/R cells and caused ectopic expression of plim-6::GFP in RMED/V cells."
Remark	"expression of ahr-1 in the four RMEs using a unc-25 promoter, in ahr-1(ju145) mutant animals fully restores plim-6::GFP expression in RMEL/R cells and caused ectopic expression of plim-6::GFP in RMED/V cells."
Reference	"WBPaper00006431"


Anatomy_function : "WBbtf0281"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000054"
Gene	"WBGene00000095"
Involved	"WBbt:0003681"	Sufficient
Remark	"ENTITY:WBls:0000023(larva) QUALITY:PATO:0000718(lethal (sensu genetics))"
Remark	"Published_as aha-1"
Remark	"aha-1(ia1) larval lethality can be rescued by specific pharyngeal expression of aha-1."
Reference	"WBPaper00006431"


Anatomy_function : "WBbtf0282"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000019"
Gene	"WBGene00001133"
Involved	"WBbt:0005451"	Sufficient
Remark	"ENTITY:WBbt:0003681(pharynx)|GO:0006936(muscle contraction) QUALITY:PATO:0000911(decreased rate)"
Remark	"Genotype \"eat-2(ad465);Ex[myo-2::eat-2]\""
Remark	"Published_as eat-2"
Remark	"transgene of full-length eat-2 cDNA fused to the pharyngeal muscle-specific myo-2 promoter rescued the slow-pumping phenotype of eat-2 mutants."
Reference	"WBPaper00006439"


Anatomy_function : "WBbtf0283"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000515"
Gene	"WBGene00002003"
Involved	"WBbt:0007846"	Sufficient
Remark	"ENTITY:WBbt:0006976(PVQ)|GO:0048812(neurite morphogenesis) QUALITY:PATO:0000460(abnormal)"
Remark	"ENTITY:WBbt:0006976(PVQ)|GO:0043005(neuron projection) QUALITY:PATO:0001959(defasciculated)"
Remark	"ENTITY:WBbt:0006976(PVQ)|GO:0043005(neuron projection) QUALITY:PATO:0001953(	decussate)"
Remark	"Genotype \"hse-5; Ex[dpy-7::hse-5]\""
Remark	"Published_as hse-5"
Remark	"hse-5 expressed under the control of hypodermis-specific cis-regulatory elements from the dpy-7 gene can rescue the defects of hse-5 mutant midline crossover defects of PVQ axons."
Reference	"WBPaper00006471"


Anatomy_function : "WBbtf0284"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000515"
Gene	"WBGene00002029"
Involved	"WBbt:0007846"	Sufficient
Remark	"ENTITY:WBbt:0006976(PVQ)|GO:0048812(neurite morphogenesis) QUALITY:PATO:0000460(abnormal)"
Remark	"ENTITY:WBbt:0006976(PVQ)|GO:0043005(neuron projection) QUALITY:PATO:0001959(defasciculated)"
Remark	"ENTITY:WBbt:0006976(PVQ)|GO:0043005(neuron projection) QUALITY:PATO:0001953(	decussate)"
Remark	"Genotype \"hst-2; Ex[dpy-7::hst-2]\""
Remark	"Published_as hst-2"
Remark	"hst-2 expressed under the control of hypodermis-specific cis-regulatory elements from the dpy-7 gene can rescue the defects of hst-2 mutant midline crossover defects of PVQ axons."
Reference	"WBPaper00006471"


Anatomy_function : "WBbtf0285"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000515"
Gene	"WBGene00002031"
Not_involved	"WBbt:0007846"	Insufficient
Remark	"ENTITY:WBbt:0006976(PVQ)|GO:0048812(neurite morphogenesis) QUALITY:PATO:0000460(abnormal)"
Remark	"ENTITY:WBbt:0006976(PVQ)|GO:0043005(neuron projection) QUALITY:PATO:0001959(defasciculated)"
Remark	"ENTITY:WBbt:0006976(PVQ)|GO:0043005(neuron projection) QUALITY:PATO:0001953(	decussate)"
Remark	"Genotype \"hst-6; Ex[dpy-7::hst-6]\""
Remark	"Published_as hst-6"
Remark	"hst-6 expressed under the control of hypodermis-specific cis-regulatory elements from the dpy-7 gene does not rescue the defects of hst-6 mutant midline crossover defects of PVQ axons."
Reference	"WBPaper00006471"


Anatomy_function : "WBbtf0286"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000436"
Gene	"WBGene00007750"
Involved	"WBbt:0006767"	Necessary
Involved	"WBbt:0006768"	Necessary
Remark	"ENTITY:WBbt:0004758(HSNL)|GO:0030424(axon)|WBGene00006365(syg-1)|GO:0008104(protein localization) QUALITY:PATO:0001513(diffuse)"
Remark	"Genotype \"lin-11(n566); kyIs288[unc-86::syg-1::gfp,odr-1::rfp]\""
Remark	"In lin-11 mutants, SYG-2::GFP expression was absent from the primary vulval epithelial cells, whereas SYG-2 expression was maintained in other regions such as body wall muscle. SYG-1 was diffusely localized on the HSNL axon in lin-11(n566) mutant animals, providing further evidence that the expression of SYG-2 in the primary vulval epithelial cells correlates with the clustering of SYG-1 and synaptic vesicles in the adjacent HSNL axon."
Remark	"Published_as syg-2"
Reference	"WBPaper00006489"


Anatomy_function : "WBbtf0287"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000847"
Gene	"WBGene00007750"
Involved	"WBbt:0006767"	Necessary
Involved	"WBbt:0006768"	Necessary
Remark	"ENTITY:WBbt:0004758(HSNL)|GO:0030424(axon)|WBGene00004897(snb-1)|GO:0008104(protein localization) QUALITY:PATO:0001632(anterior to) ENTITY:WBbt:0006748(vulva)"
Remark	"Genotype \"lin-11(n566); kyIs235[unc-86::snb-1::yfp,unc-4::lin-10::dsRED,odr-1::dsRED]\""
Remark	"In lin-11 mutants, SYG-2::GFP expression was absent from the primary vulval epithelial cells, whereas SYG-2 expression was maintained in other regions such as body wall muscle. Whilst SNB-1 was abnormally localized anterior to the developing vulva."
Remark	"Published_as syg-2"
Reference	"WBPaper00006489"


Anatomy_function : "WBbtf0288"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000436"
Gene	"WBGene00007750"
Involved	"WBbt:0006767"	Sufficient
Involved	"WBbt:0006768"	Sufficient
Remark	"Because syg-2 is normally expressed in the primary but not the secondary vulval cells, one can infer that normally, syg-2 expression in the primary cells is sufficient to direct SYG-1 localization in HSNL to sites adjacent to the primary cells."
Remark	"ENTITY:WBbt:0004758(HSNL)|GO:0030424(axon)|WBGene00006365(syg-1)|GO:0008104(protein localization) QUALITY:PATO:0001513(diffuse) NOT"
Remark	"Expressing SYG-2 in secondary vulval epithelial cells, using an egl-17 promoter (active in secondary vulval cells), in syg-2(ky673) mutants caused SYG-1 in HSNL to localize to the contact sites between HSNL and the ventral secondary vulval cells instead of the primary cells. These results suggest that SYG-2 expression in the secondary vulval cells is sufficient to attract SYG-1 protein from the HSNL axon."
Remark	"Published_as syg-2"
Reference	"WBPaper00006489"


Anatomy_function : "WBbtf0289"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000847"
Gene	"WBGene00007750"
Involved	"WBbt:0006767"	Sufficient
Involved	"WBbt:0006768"	Sufficient
Remark	"Because syg-2 is normally expressed in the primary and not the secondary vulval cells, one can infer that normally, syg-2 expression in the primary cells is sufficient to cause SNB-1 (containing vesicles) to cluster at the segment of the HSNL axon that contacts primary cells."
Remark	"ENTITY:WBbt:0004758(HSNL)|GO:0030424(axon)|WBGene00004897(snb-1)|GO:0008104(protein localization) QUALITY:PATO:0001632(anterior to) ENTITY:WBbt:0006748(vulva) NOT"
Remark	"In syg-2(ky673);Ex(egl-17::syg-2) animals, synaptic vesicles were clustered at the segment of the HSNL axon that contacted secondary vulval cells."
Remark	"Published_as syg-2"
Reference	"WBPaper00006489"


Anatomy_function : "WBbtf0290"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001237"	Autonomous
Gene	"WBGene00003009"
Involved	"WBbt:0005190"
Remark	"ENTITY:WBbt:0003843(AVL)|GO:0048675(axon extension) QUALITY:PATO:0000628(mislocalised)"
Remark	"Genotype \"lin-23(ot1); Ex[unc-47p::lin-23]\""
Remark	"Published_as lin-23"
Reference	"WBPaper00006497"


Anatomy_function : "WBbtf0291"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001278"	Autonomous
Gene	"WBGene00003889"
Involved	"WBbt:0005660"	Sufficient
Remark	"ocr-2 mosaic expression data not found."
Remark	"ENTITY:WBbt:0005660(ADF)|WBGene00006600(tph-1)|GO:0010467(gene expression) QUALITY:PATO:0001997(present in fewer numbers in organism) NOT"
Remark	"Genotype \"osm-9(yz6);Ex[Pcat-1::osm-9]\""
Remark	"Published_as osm-9"
Remark	"When osm-9(yz6) mutant animals carry a transgene expressed in the ADF neurons (Pcat-1::osm-9, Plin-11::osm-9), tph-1::gfp expression in the ADF neurons is restored, whereas the mutant animals carrying the transgene not expressed in the ADF neurons (Podr-7::osm-9, Posm-10::osm-9, Ptax-2::osm-9) exhibit reduced tph-1::gfp expression similar to their non-transgenic siblings."
Reference	"WBPaper00006505"


Anatomy_function : "WBbtf0292"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001224"
Gene	"WBGene00001184"
Involved	"WBbt:0007846"	Sufficient
Remark	"ENTITY:WBbt:0003679(neuron)|GO:0048675(axon extension) QUALITY:PATO:0001997(	reduced) NOT"
Remark	"ENTITY:WBbt:0003679(neuron)|GO:0007411(axon guidance) QUALITY:PATO:0001511(defective) NOT"
Remark	"Expression of a wild-type egl-15 cDNA under control of the heterologous, hypodermis-specific dpy-7 promoter can rescue the axon extension and guidance defects of egl-15 null mutants."
Remark	"Genotype \"egl-15(n1456); Ex[pdpy-7::egl-15(5A)cDNA]\""
Remark	"Published_as egl-15"
Reference	"WBPaper00013448"


Anatomy_function : "WBbtf0293"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001224"
Gene	"WBGene00001184"
Not_involved	"WBbt:0003679"	Insufficient
Remark	"ENTITY:WBbt:0003679(neuron)|GO:0048675(axon extension) QUALITY:PATO:0001997(	reduced)"
Remark	"ENTITY:WBbt:0003679(neuron)|GO:0007411(axon guidance) QUALITY:PATO:0001511(defective)"
Remark	"Expression of a wild-type egl-15 cDNA under control of the panneuronal F25B3.3 promoter does not rescue the axon extension and guidance defects of egl-15 null mutants."
Remark	"Genotype \"egl-15(n1456); Ex[pF25B3.3::egl-15(5A)cDNA]\""
Remark	"Published_as egl-15"
Reference	"WBPaper00013448"


Anatomy_function : "WBbtf0294"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001224"
Gene	"WBGene00002335"
Involved	"WBbt:0007846"	Sufficient
Remark	"ENTITY:WBbt:0003679(neuron)|GO:0048675(axon extension) QUALITY:PATO:0001997(	reduced) NOT"
Remark	"Expression of a let-60 cDNA constitutively activated by a G13E mutation and expressed under the control of the hypodermis-specific dpy-7 promoter completely rescues the lethality and axon extension defects of egl-15 null mutants."
Remark	"Genotype \"egl-15(n1456); otEx1271[pdpy-7::let-60G13E;pceh-22::gfp]\""
Remark	"Published_as let-60"
Reference	"WBPaper00013448"


Anatomy_function : "WBbtf0295"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000012"	Nonautonomous
Gene	"WBGene00000905"
Involved	"WBbt:0007846"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0055115(diapause) QUALITY:PATO:0000760(hyperactive) NOT"
Remark	"ENTITY:WBbt:0006865(DTC)|GO:0016477(cell migration) QUALITY:PATO:0000692(heterochronic) NOT"
Remark	"ENTITY:WBbt:0007833(organism)|GO:0000003(reproduction) QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"daf-9(dh6); dhEx66[daf-9::gfp]\""
Remark	"Mosaics arise spontaneously from transgenic lines of daf-9(dh6) containing extrachromosamal array of genomic daf-9::gfp (dhEx66). Mosaics expressing daf-9 in the hypodermis (but not XXX cells) bypassed diapause, had normal gonadal development and were fertile."
Remark	"Published_as daf-9"
Reference	"WBPaper00013396"


Anatomy_function : "WBbtf0296"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000012"
Gene	"WBGene00000905"
Not_involved	"WBbt:0007855"	Unnecessary
Remark	"AB-P1+ mosaics derived from daf-9 transgenic animals, which do not express daf-9 in XXX cells, reached adulthood, implying that expression of daf-9 in XXX cells is not absolutely required for reproductive growth."
Remark	"ENTITY:WBbt:0007833(organism)|GO:0055115(diapause) QUALITY:PATO:0000760(hyperactive) NOT"
Remark	"ENTITY:WBbt:0006865(DTC)|GO:0016477(cell migration) QUALITY:PATO:0000692(heterochronic) NOT"
Remark	"ENTITY:WBbt:0007833(organism)|GO:0000003(reproduction) QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"daf-9(dh6) ncl-1(e1865); dhEx107[daf-9::gfp, sur-5::gfp, ncl-1(+)]\""
Remark	"Published_as daf-9"
Reference	"WBPaper00013396"


Anatomy_function : "WBbtf0297"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000012"
Gene	"WBGene00000905"
Involved	"WBbt:0007846"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0055115(diapause) QUALITY:PATO:0000760(hyperactive) NOT"
Remark	"ENTITY:WBbt:0006865(DTC)|GO:0016477(cell migration) QUALITY:PATO:0000692(heterochronic) NOT"
Remark	"ENTITY:WBbt:0007833(organism)|GO:0000003(reproduction) QUALITY:PATO:0001997(reduced) NOT"
Remark	"ENTITY:WBbt:0005772(intestine) QUALITY:PATO:0000327(dark) NOT"
Remark	"Genotype \"daf-9(dh6); dhEx217[dpy-7::daf-9::gfp]\""
Remark	"Published_as daf-9"
Remark	"gfp fusions to daf-9 cDNA driven by dpy-7 promoter restored daf-9(dh6) and daf-9(rh50) to near wild-type function. Transgenically rescued animals bypassed diapause, had normal light intestines, complete gonadal reflexion and large broods."
Reference	"WBPaper00013396"


Anatomy_function : "WBbtf0298"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000012"
Gene	"WBGene00000905"
Involved	"WBbt:0007846"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0055115(diapause) QUALITY:PATO:0000760(hyperactive) NOT"
Remark	"ENTITY:WBbt:0006865(DTC)|GO:0016477(cell migration) QUALITY:PATO:0000692(heterochronic) NOT"
Remark	"ENTITY:WBbt:0007833(organism)|GO:0000003(reproduction) QUALITY:PATO:0001997(reduced) NOT"
Remark	"ENTITY:WBbt:0005772(intestine) QUALITY:PATO:0000327(dark) NOT"
Remark	"Genotype \"daf-9(dh6); dhEx207[col-3::daf-9::gfp]\""
Remark	"Published_as daf-9"
Remark	"gfp fusions to daf-9 cDNA driven by col-3 promoter restored daf-9(dh6) and daf-9(rh50) to near wild-type function. Transgenically rescued animals bypassed diapause, had normal light intestines, complete gonadal reflexion and large broods."
Reference	"WBPaper00013396"


Anatomy_function : "WBbtf0299"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000012"
Gene	"WBGene00000905"
Involved	"WBbt:0007846"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0055115(diapause) QUALITY:PATO:0000760(hyperactive) NOT"
Remark	"ENTITY:WBbt:0006865(DTC)|GO:0016477(cell migration) QUALITY:PATO:0000692(heterochronic) NOT"
Remark	"ENTITY:WBbt:0007833(organism)|GO:0000003(reproduction) QUALITY:PATO:0001997(reduced) NOT"
Remark	"ENTITY:WBbt:0005772(intestine) QUALITY:PATO:0000327(dark) NOT"
Remark	"Genotype \"daf-9(dh6); dhEx294[wrt-1::daf-9::gfp]\""
Remark	"Published_as daf-9"
Remark	"gfp fusions to daf-9 cDNA driven by wrt-1 promoter restored daf-9(dh6) and daf-9(rh50) to near wild-type function. Transgenically rescued animals bypassed diapause, had normal light intestines, complete gonadal reflexion and large broods."
Reference	"WBPaper00013396"


Anatomy_function : "WBbtf0300"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000012"
Gene	"WBGene00000905"
Not_involved	"WBbt:0005237"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0055115(diapause) QUALITY:PATO:0000760(hyperactive) NOT"
Remark	"ENTITY:WBbt:0006865(DTC)|GO:0016477(cell migration) QUALITY:PATO:0000692(heterochronic) NOT"
Remark	"ENTITY:WBbt:0007833(organism)|GO:0000003(reproduction) QUALITY:PATO:0001997(reduced) NOT"
Remark	"Expression of daf-9 in touch neurons with the mec-7 promoter failed to rescue daf-9 mutant Daf-c and Mig phenotypes."
Remark	"Genotype \"daf-9(dh6); dhEx176[mec-7::daf-9::gfp]\""
Remark	"Published_as daf-9"
Reference	"WBPaper00013396"


Anatomy_function : "WBbtf0301"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000012"
Gene	"WBGene00000905"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0055115(diapause) QUALITY:PATO:0000760(hyperactive) NOT"
Remark	"ENTITY:WBbt:0006865(DTC)|GO:0016477(cell migration) QUALITY:PATO:0000692(heterochronic) NOT"
Remark	"ENTITY:WBbt:0007833(organism)|GO:0000003(reproduction) QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"daf-9(e1406); dhEx256[F25B3.3::daf-9::gfp]\""
Remark	"Pan-neuronal expression of daf-9 using the F25B3.3 promoter also rescued Daf-c and Mig phenotypes, but much less effectively."
Remark	"Published_as daf-9"
Reference	"WBPaper00013396"


Anatomy_function : "WBbtf0302"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000012"
Gene	"WBGene00000905"
Involved	"WBbt:0007855"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0055115(diapause) QUALITY:PATO:0000760(hyperactive) NOT"
Remark	"ENTITY:WBbt:0006865(DTC)|GO:0016477(cell migration) QUALITY:PATO:0000692(heterochronic) NOT"
Remark	"ENTITY:WBbt:0007833(organism)|GO:0000003(reproduction) QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"daf-9(e1406); dhEx354[sdf-9::daf-9::gfp]\""
Remark	"Published_as daf-9"
Remark	"daf-9 expression under a sdf-9 promoter which is expressed in the XXX cells can rescue the Daf-c and Mig phenotypes of daf-9(e1406)."
Reference	"WBPaper00013396"


Anatomy_function : "WBbtf0303"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000012"	Nonautonomous
Gene	"WBGene00000905"
Involved	"WBbt:0007846"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0055115(diapause) QUALITY:PATO:0000760(hyperactive) NOT"
Remark	"ENTITY:WBbt:0007833(organism)|GO:0000003(reproduction) QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"daf-9(e1406); Ex[dpy-7p::daf-9cDNA::GFP]\""
Remark	"Published_as daf-9"
Remark	"Restoration of daf-9 activity in the hypodermis alone was sufficient to prevent dauer arrest of daf-9(e1406) mutant animals; these transgenic animals developed into reproductive adults with the same growth rate as animals carrying a daf-9 transgene driven by its own promoter."
Reference	"WBPaper00006519"


Anatomy_function : "WBbtf0304"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000012"	Nonautonomous
Gene	"WBGene00000905"
Involved	"WBbt:0007855"	Sufficient
Involved	"WBbt:0007855"	Remark
Remark	"At 20 deg C, daf-9 expression in the two XXXL/R cells was sufficient to prevent dauer arrest of daf-9(e1406) mutant animals. Nevertheless, 5-20% of daf-9(e1406) animals that expressed daf-9 in the XXXL/R cells arrested as dauers at 25 deg C."
Remark	"ENTITY:WBbt:0007833(organism)|GO:0055115(diapause) QUALITY:PATO:0000760(hyperactive) NOT"
Remark	"ENTITY:WBbt:0007833(organism)|GO:0000003(reproduction) QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"daf-9(e1406); Ex[sdf-9p::daf-9cDNA::GFP]\""
Remark	"Published_as daf-9"
Remark	"incomplete."
Reference	"WBPaper00006519"


Anatomy_function : "WBbtf0305"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000012"	Nonautonomous
Gene	"WBGene00000905"
Involved	"WBbt:0006816"	Sufficient
Involved	"WBbt:0006816"	Remark
Remark	"ENTITY:WBbt:0007833(organism)|GO:0055115(diapause) QUALITY:PATO:0000760(hyperactive) NOT"
Remark	"ENTITY:WBbt:0007833(organism)|GO:0000003(reproduction) QUALITY:PATO:0001997(reduced) NOT"
Remark	"Ectopic daf-9 activity in the ciliated sensory neurons was sufficient to prevent dauer arrest of the majority of daf-9(e1406) mutant animals; only a small fraction of transgenic animals arrested as partial dauers."
Remark	"Genotype \"daf-9(e1406); Ex[che-2p::daf-9cDNA::GFP]\""
Remark	"Published_as daf-9"
Remark	"incomplete."
Reference	"WBPaper00006519"


Anatomy_function : "WBbtf0306"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000690"	Nonautonomous
Gene	"WBGene00000905"
Involved	"WBbt:0007846"	Sufficient
Remark	"ENTITY:WBbt:0006865(DTC)|GO:0016477(cell migration) QUALITY:PATO:0000692(heterochronic) NOT"
Remark	"Normal gonadal migration was observed in daf-9(e1406) mutant animals when daf-9 was expressed exclusively in the hypodermis."
Remark	"Published_as daf-9"
Reference	"WBPaper00006519"


Anatomy_function : "WBbtf0307"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000690"	Nonautonomous
Gene	"WBGene00000905"
Involved	"WBbt:0006816"	Sufficient
Involved	"WBbt:0006816"	Remark
Remark	"ENTITY:WBbt:0006865(DTC)|GO:0016477(cell migration) QUALITY:PATO:0000692(heterochronic) NOT"
Remark	"Ectopic daf-9 activity in the ciliated sensory neurons was partially sufficient to prevent a gonad migration defect of daf-9(e1406) mutant animals; only 30% of transgenic animals did not display a gonadal migration defect."
Remark	"Published_as daf-9"
Remark	"incomplete."
Reference	"WBPaper00006519"


Anatomy_function : "WBbtf0308"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000690"	Nonautonomous
Gene	"WBGene00000905"
Involved	"WBbt:0007855"	Sufficient
Remark	"ENTITY:WBbt:0006865(DTC)|GO:0016477(cell migration) QUALITY:PATO:0000692(heterochronic) NOT"
Remark	"Normal gonadal migration was observed in daf-9(e1406) mutant animals when daf-9 was expressed exclusively in the XXXL/R cells."
Remark	"Published_as daf-9"
Reference	"WBPaper00006519"


Anatomy_function : "WBbtf0309"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001010"
Gene	"WBGene00001184"
Involved	"WBbt:0007846"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050878(regulation of body fluid levels) QUALITY:PATO:0001507(disrupted)"
Remark	"Genotype \"clr-1(e1745ts); egl-15(n1783); Ex[pdyp-7::egl-15]\""
Remark	"Published_as egl-15"
Remark	"When authors expressed EGL-15 from either of two hypodermal promoters, Pdpy-7 and Prol-6, they observed robust rescue of egl-15 mutant phenotypes, including the Suppressor of clr-1 Clear phenotype."
Reference	"WBPaper00024207"


Anatomy_function : "WBbtf0310"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001010"
Gene	"WBGene00001184"
Not_involved	"WBbt:0006804"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050878(regulation of body fluid levels) QUALITY:PATO:0001507(disrupted) NOT"
Remark	"Expression of EGL-15 in all body wall muscles from the unc-54 promoter failed to show any rescue activity of the Suppressor of clr-1 Clear phenotype."
Remark	"Genotype \"clr-1(e1745ts); egl-15(n1783); Ex[punc-54::egl-15]\""
Remark	"Published_as egl-15"
Reference	"WBPaper00024207"


Anatomy_function : "WBbtf0311"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001010"
Gene	"WBGene00000548"
Not_involved	"WBbt:0006804"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050878(regulation of body fluid levels) QUALITY:PATO:0001507(disrupted)"
Remark	"Expression of CLR-1 in all body wall muscles from the unc-54 promoter failed to show any rescue activity of clr-1(e1745ts) mutant phenotype."
Remark	"Genotype \"clr-1(e1745ts); Ex[punc-54::clr-1]\""
Remark	"Published_as clr-1"
Reference	"WBPaper00024207"


Anatomy_function : "WBbtf0312"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001010"
Gene	"WBGene00000548"
Involved	"WBbt:0007846"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050878(regulation of body fluid levels) QUALITY:PATO:0001507(disrupted) NOT"
Remark	"Genotype \"clr-1(e1745ts); Ex[pdpy-7::clr-1]\""
Remark	"Hypodermal expression of CLR-1 with a dpy-7 promoter shows robust rescue activity."
Remark	"Published_as clr-1"
Reference	"WBPaper00024207"


Anatomy_function : "WBbtf0313"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001010"
Gene	"WBGene00000548"
Involved	"WBbt:0007846"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050878(regulation of body fluid levels) QUALITY:PATO:0001507(disrupted) NOT"
Remark	"Genotype \"clr-1(e1745ts); Ex[prol-6::clr-1]\""
Remark	"Hypodermal expression of CLR-1 with a rol-6 promoter shows robust rescue activity."
Remark	"Published_as clr-1"
Reference	"WBPaper00024207"


Anatomy_function : "WBbtf0314"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001010"
Gene	"WBGene00003401"
Involved	"WBbt:0006874"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050878(regulation of body fluid levels) QUALITY:PATO:0001507(disrupted)"
Remark	"Genotype \"clr-1(e1745ts); mpk-1 ncl-1 unc-36; sDp3\""
Remark	"Mosaic animals with sDp3 losses in AB descendants when shifted to the restrictive temperature displayed the Clr phenotype, suggesting that loss of mpk-1 activity in the AB lineage is not sufficient to suppress the Clr phenotype. Therefore, mpk-1(+) activity within P1 descendants can function to prevent the Soc phenotype."
Remark	"Published_as mpk-1"
Reference	"WBPaper00024207"


Anatomy_function : "WBbtf0315"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001010"
Gene	"WBGene00003401"
Involved	"WBbt:0004015"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050878(regulation of body fluid levels) QUALITY:PATO:0001507(disrupted)"
Remark	"Mosaic animals with sDp3 losses in P1 descendants when shifted to the restrictive temperature displayed the Clr phenotype, suggesting that loss of mpk-1 activity in the P1 lineage is also not sufficient to suppress the Clr phenotype. Therefore, mpk-1(+) activity within the AB lineage can function to prevent the Soc phenotype."
Remark	"Published_as mpk-1"
Reference	"WBPaper00024207"


Anatomy_function : "WBbtf0316"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000054"
Gene	"WBGene00002881"
Involved	"WBbt:0006874"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|WBls:0000023(larva)|GO:0040007(growth) QUALITY:PATO:0000297(arrested) NOT"
Remark	"Genotype \"dpy-17 let-756 ncl-1 unc-36; sDp3\""
Remark	"Published_as let-756"
Remark	"We first screened dpy-17 let-756 ncl-1 unc-36; sDp3 animals for either Unc non-Dpy or Dpy non-Unc mosaic animals. Unc non-Dpy animals were identified as expected, and the vast majority of these animals had losses in either AB, AB.p, or descendants in the AB.p lineage. Besides being Unc, these mosaic animals were completely wild type, suggesting that lack of let-756(+) expression in the AB lineage is not essential for viability."
Reference	"WBPaper00024207"


Anatomy_function : "WBbtf0317"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000054"
Gene	"WBGene00002881"
Involved	"WBbt:0006874"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|WBls:0000023(larva)|GO:0040007(growth) QUALITY:PATO:0000297(arrested)"
Remark	"Genotype \"dpy-17 let-756 ncl-1 unc-36; sDp3\""
Remark	"Published_as let-756"
Remark	"We screened dpy-17 let-756 ncl-1 unc-36; sDp3 animals for mosaic animals. Dpy non-Unc animals were extremely rare, and the few Dpy non-Unc animals identified turned out to result from the breakdown of the free duplication. This striking finding suggests that the cellular focus of let-756 is not easily separable from that of dpy-17. DPY-17 is thought to be required in the P1 lineage."
Reference	"WBPaper00024207"


Anatomy_function : "WBbtf0318"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000412"
Gene	"WBGene00001709"
Involved	"WBbt:0005665"	Sufficient
Involved	"WBbt:0005661"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050919(negative chemotaxis)|CHEBI:37868(octanol) QUALITY:PATO:0001997(reduced) NOT"
Remark	"Expression of the srb-6::Ce-grk-2 transgene restored response to octanol in a dose-dependent manner. The srb-6 promoter was used to express Ce-GRK-2 in two of the chemosensory neurons that detect octanol, ASH and ADL."
Remark	"Genotype \"grk-2(rt97); Ex[psrb-6::grk-2]\""
Remark	"Published_as grk-2"
Reference	"WBPaper00013467"


Anatomy_function : "WBbtf0319"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000412"
Gene	"WBGene00001709"
Involved	"WBbt:0005665"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050919(negative chemotaxis)|CHEBI:37868(octanol) QUALITY:PATO:0001997(reduced) NOT"
Remark	"Expression of Ce-grk-2 in ASH neurons using the osm-10 promoter also partially restored octanol response in Ce-grk-2 mutant animals."
Remark	"Genotype \"grk-2(rt97); Ex[posm-10::grk-2]\""
Remark	"Published_as grk-2"
Reference	"WBPaper00013467"


Anatomy_function : "WBbtf0320"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000412"
Gene	"WBGene00001709"
Not_involved	"WBbt:0007804"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050919(negative chemotaxis)|CHEBI:37868(octanol) QUALITY:PATO:0001997(reduced)"
Remark	"Genotype \"grk-2(rt97); Ex[pglr-1::grk-2]\""
Remark	"Published_as grk-2"
Remark	"The glr-1::Ce-grk-2 transgene, expressed at either low or high concentrations, had no effect on octanol response. The glr-1 promoter drives expression in 17 classes of neurons, including the command interneurons but not in the chemosensory neurons."
Reference	"WBPaper00013467"


Anatomy_function : "WBbtf0321"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000876"
Gene	"WBGene00016329"
Involved	"WBbt:0007846"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050879(multicellular organismal movement)|GO:0006972(hyperosmotic response)|CHEBI:26710(sodium chloride) QUALITY:PATO:0000470(increased) NOT"
Remark	"Genotype \"osr-1(rm1); Ex[Pdyp-7::osr-1::gfp]\""
Remark	"Published_as osr-1"
Remark	"expression of osr-1 cDNA under the hypodermal promoter (Pdpy-7) was able to rescue all the osr-1(rm1) phenotypes [mutants show motility in 500 mM NaCl, but not transgenic animals]."
Reference	"WBPaper00013472"


Anatomy_function : "WBbtf0322"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000876"
Gene	"WBGene00016329"
Not_involved	"WBbt:0005792"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050879(multicellular organismal movement)|GO:0006972(hyperosmotic response)|CHEBI:26710(sodium chloride) QUALITY:PATO:0000470(increased)"
Remark	"Genotype \"osr-1(rm1); Ex[Pvha-6::osr-1::gfp]\""
Remark	"Published_as osr-1"
Remark	"expression of osr-1 cDNA under the intestinal promoter (Pvha-6) was unable to rescue any of the osr-1(rm1) phenotypes [mutants show motility in 500 mM NaCl, so do transgenic animals]."
Reference	"WBPaper00013472"


Anatomy_function : "WBbtf0323"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000876"
Gene	"WBGene00016329"
Not_involved	"WBbt:0005334"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050879(multicellular organismal movement)|GO:0006972(hyperosmotic response)|CHEBI:26710(sodium chloride) QUALITY:PATO:0000470(increased)"
Remark	"Genotype \"osr-1(rm1); Ex[PF25B3.3::osr-1::gfp]\""
Remark	"Published_as osr-1"
Remark	"expression of osr-1 cDNA under the pan-neuronal promoter (PF25B3.3) was unable to rescue any of the osr-1(rm1) phenotypes [mutants show motility in 500 mM NaCl, so do transgenic animals]."
Reference	"WBPaper00013472"


Anatomy_function : "WBbtf0324"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000876"
Gene	"WBGene00016329"
Involved	"WBbt:0007846"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0016265(death)|GO:0006972(hyperosmotic response)|CHEBI:26710(sodium chloride) QUALITY:PATO:0001997(decreased) NOT"
Remark	"Published_as osr-1"
Remark	"expression of osr-1 cDNA under the hypodermal promoter (Pdpy-7) was able to rescue all the osr-1(rm1) phenotypes [mutants can survive in 500 mM NaCl, but not transgenic animals]."
Reference	"WBPaper00013472"


Anatomy_function : "WBbtf0325"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000876"
Gene	"WBGene00016329"
Not_involved	"WBbt:0005792"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0016265(death)|GO:0006972(hyperosmotic response)|CHEBI:26710(sodium chloride) QUALITY:PATO:0001997(decreased)"
Remark	"Published_as osr-1"
Remark	"expression of osr-1 cDNA under the intestinal promoter (Pvha-6) was unable to rescue any of the osr-1(rm1) phenotypes [mutants can survive in 500 mM NaCl, so do transgenic animals]."
Reference	"WBPaper00013472"


Anatomy_function : "WBbtf0326"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000876"
Gene	"WBGene00016329"
Not_involved	"WBbt:0003679"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0016265(death)|GO:0006972(hyperosmotic response)|CHEBI:26710(sodium chloride) QUALITY:PATO:0001997(decreased)"
Remark	"Published_as osr-1"
Remark	"expression of osr-1 cDNA under the pan-neuronal promoter (PF25B3.5) was unable to rescue any of the osr-1(rm1) phenotypes [mutants can survive in 500 mM NaCl, so do transgenic animals]."
Reference	"WBPaper00013472"


Anatomy_function : "WBbtf0327"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001453"
Gene	"WBGene00016329"
Involved	"WBbt:0007846"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050919(negative chemotaxis)|GO:0006972(hyperosmotic response) QUALITY:PATO:0001997(decreased) NOT"
Remark	"Published_as osr-1"
Remark	"expression of osr-1 cDNA under the hypodermal promoter (Pdpy-7) was able to rescue all the osr-1(rm1) phenotypes [mutants fail to avoid regions of 4M NaCl or 8M fructose, but transgenic animals do]."
Reference	"WBPaper00013472"


Anatomy_function : "WBbtf0328"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001453"
Gene	"WBGene00016329"
Not_involved	"WBbt:0005792"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050919(negative chemotaxis)|GO:0006972(hyperosmotic response) QUALITY:PATO:0001997(decreased)"
Remark	"Published_as osr-1"
Remark	"expression of osr-1 cDNA under the intestinal promoter (Pvha-6) was unable to rescue any of osr-1(rm1) phenotypes [mutants fail to avoid regions of 4M NaCl or 8M fructose, so as transgenic animals]."
Reference	"WBPaper00013472"


Anatomy_function : "WBbtf0329"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001453"
Gene	"WBGene00016329"
Not_involved	"WBbt:0003679"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050919(negative chemotaxis)|GO:0006972(hyperosmotic response) QUALITY:PATO:0001997(decreased)"
Remark	"Published_as osr-1"
Remark	"expression of osr-1 cDNA under the pan-neuronal promoter (PF25b3.3) was unable to rescue any of osr-1(rm1) phenotypes [mutants fail to avoid regions of 4M NaCl or 8M fructose, so as transgenic animals]."
Reference	"WBPaper00013472"


Anatomy_function : "WBbtf0330"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000083"
Gene	"WBGene00003831"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0048589(developmental growth)|WBls:0000035(L3 larva) QUALITY:PATO:0000297(arrested) NOT"
Remark	"Genotype \"nuo-1(ua1); uaEx17[Punc-119::nuo-1(+)]\""
Remark	"Over 90 percent of the homozygous nuo-1(ua1) progeny of LB77 uaEx17[Punc-119::nuo-1(+)], which expresses nuo-1 in the nervous system, were able to develop to the L4 or the adult stages."
Remark	"Published_as nuo-1"
Reference	"WBPaper00013500"


Anatomy_function : "WBbtf0331"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000083"
Gene	"WBGene00003831"
Not_involved	"WBbt:0007810"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0048589(developmental growth)|WBls:0000035(L3 larva) QUALITY:PATO:0000297(arrested)"
Remark	"Genotype \"nuo-1(ua1); Ex[Punc-54::nuo-1(+)]\""
Remark	"Published_as nuo-1"
Remark	"Transformation of LB77 with the Punc-54::nuo-1(+) construct did not affect the nuo-1(ua1) L3 arrest phenotype."
Reference	"WBPaper00013500"


Anatomy_function : "WBbtf0332"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000083"
Gene	"WBGene00003831"
Not_involved	"WBbt:0005784"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0048589(developmental growth)|WBls:0000035(L3 larva) QUALITY:PATO:0000297(arrested)"
Remark	"Genotype \"nuo-1(ua1); Ex[Ppie-1::nuo-1(+)]\""
Remark	"Published_as nuo-1"
Remark	"Transformation of LB77 with the Ppie-1::nuo-1(+) construct did not affect the nuo-1(ua1) L3 arrest phenotype."
Reference	"WBPaper00013500"


Anatomy_function : "WBbtf0333"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000127"
Gene	"WBGene00003831"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0048589(developmental growth)|WBls:0000032(dauer larva) QUALITY:PATO:0000297(arrested) NOT"
Remark	"Genotype \"nuo-1(ua1); uaEx17[Punc-119::nuo-1(+)]\""
Remark	"Once entered into the dauer stage, three-quarters of the animals (homozygous nuo-1(ua1) progeny of LB77 uaEx17[Punc-119::nuo-1(+)], which expresses nuo-1 in the nervous system) could exit dauer and develop into L4 or adult worms."
Remark	"Published_as nuo-1"
Reference	"WBPaper00013500"


Anatomy_function : "WBbtf0334"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000127"
Gene	"WBGene00003831"
Not_involved	"WBbt:0007810"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0048589(developmental growth)|WBls:0000032(dauer larva) QUALITY:PATO:0000297(arrested)"
Remark	"Genotype \"nuo-1(ua1); Ex[Punc-54::nuo-1(+)]\""
Remark	"Published_as nuo-1"
Remark	"Transformation of LB77 with the Punc-54::nuo-1(+) construct did not allow nuo-1(ua1) animals to exit dauer in response to more favorable conditions."
Reference	"WBPaper00013500"


Anatomy_function : "WBbtf0335"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000127"
Gene	"WBGene00003831"
Not_involved	"WBbt:0005784"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0048589(developmental growth)|WBls:0000032(dauer larva) QUALITY:PATO:0000297(arrested)"
Remark	"Genotype \"nuo-1(ua1); Ex[Ppie-1::nuo-1(+)]\""
Remark	"Published_as nuo-1"
Remark	"Transformation of LB77 with the Ppie-1::nuo-1(+) construct did not allow nuo-1(ua1) animals to exit dauer in response to more favorable conditions."
Reference	"WBPaper00013500"


Anatomy_function : "WBbtf0336"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000127"
Gene	"WBGene00003831"
Not_involved	"WBbt:0005451"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0048589(developmental growth)|WBls:0000032(dauer larva) QUALITY:PATO:0000297(arrested)"
Remark	"Genotype \"nuo-1(ua1); Ex[Pmyo-2::nuo-1(+)]\""
Remark	"Published_as nuo-1"
Remark	"Transformation of LB77 with the Pmyo-2::nuo-1(+) construct did not allow nuo-1(ua1) animals to exit dauer in response to more favorable conditions."
Reference	"WBPaper00013500"


Anatomy_function : "WBbtf0337"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000083"
Gene	"WBGene00003831"
Involved	"WBbt:0005451"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0048589(developmental growth)|WBls:0000035(L3 larva) QUALITY:PATO:0000297(arrested) NOT"
Remark	"Genotype \"nuo-1(ua1); Ex[Pmyo-2::nuo-1(+)]\""
Remark	"Introduction of the Pmyo-2::nuo-1(+) construct leads to nuo-1 expression in the pharynx and resulted in partial complementation of the L3 larval arrest. Between 10 and 30 percent of the homozygous nuo-1(ua1) progeny were able to progress to the L4 stage."
Remark	"Published_as nuo-1"
Reference	"WBPaper00013500"


Anatomy_function : "WBbtf0338"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000102"
Gene	"WBGene00001499"
Involved	"WBbt:0005190"	Sufficient
Remark	"ENTITY:WBbt:0005190(GABAergic neuron)|GO:0031594(neuromuscular junction)|GO:0008021(synaptic vesicle) QUALITY:PATO:0000628(mislocalized) NOT"
Remark	"Expressing FSN-1 cDNA in GABAergic motoneurons in fsn-1-null animals rescued the defects (some vesicle pools are 2-5-fold larger than normal, whereas some regions lack vesicle pools) in GABAergic NMJs."
Remark	"Genotype \"fsn-1(hp1);juIs1; Ex[Punc-25::fsn-1]\""
Remark	"Published_as fsn-1"
Reference	"WBPaper00024212"


Anatomy_function : "WBbtf0339"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000102"
Gene	"WBGene00001499"
Not_involved	"WBbt:0006804"	Insufficient
Remark	"ENTITY:WBbt:0005190(GABAergic neuron)|GO:0031594(neuromuscular junction)|GO:0008021(synaptic vesicle) QUALITY:PATO:0000628(mislocalized)"
Remark	"Expressing FSN-1 cDNA in body wall muscles in fsn-1-null animals failed to rescue the defects (some vesicle pools are 2-5-fold larger than normal, whereas some regions lack vesicle pools) in GABAergic NMJs."
Remark	"Genotype \"fsn-1(hp1);juIs1; Ex[Pmyo-3::fsn-1]\""
Remark	"Published_as fsn-1"
Reference	"WBPaper00024212"


Anatomy_function : "WBbtf0340"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000102"
Gene	"WBGene00001499"
Involved	"WBbt:0004015"	Sufficient
Remark	"ENTITY:WBbt:0005190(GABAergic neuron)|GO:0031594(neuromuscular junction)|GO:0008021(synaptic vesicle) QUALITY:PATO:0000628(mislocalized) NOT"
Remark	"Eight out of eight mosaic animals expressing FSN-1(+) only in the AB lineage (not in P1 lineage) were wild-type for juIs1 synaptic marker."
Remark	"Genotype \"fsn-1(hp1);juIs1; Ex[sur-5::GFP, fsn-1(+)]\""
Remark	"Published_as fsn-1"
Reference	"WBPaper00024212"


Anatomy_function : "WBbtf0341"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000102"
Gene	"WBGene00001499"
Involved	"WBbt:0004015"	Necessary
Remark	"All twelve animals that express FSN-1(+) only in the P1 lineage (not in AB lineage) displayed fsn-1-like juIs1 defects."
Remark	"ENTITY:WBbt:0005190(GABAergic neuron)|GO:0031594(neuromuscular junction)|GO:0008021(synaptic vesicle) QUALITY:PATO:0000628(mislocalized)"
Remark	"Genotype \"fsn-1(hp1);juIs1; Ex[sur-5::GFP, fsn-1(+)]\""
Remark	"Published_as fsn-1"
Reference	"WBPaper00024212"


Anatomy_function : "WBbtf0342"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000384"	Autonomous
Gene	"WBGene00000548"
Involved	"WBbt:0005237"	Sufficient
Remark	"ENTITY:WBbt:0003832(AVM)|GO:0007411(axon guidance) QUALITY:PATO:0001233(dorsal) NOT"
Remark	"Genotype \"clr-1; slt-1; cyEx[mec-7::clr-1]\""
Remark	"Published_as clr-1"
Remark	"mec-7::clr-1 rescued the effect of the clr-1 mutation in a clr-1; slt-1 double mutant (clr-1 mutations suppress a defect in AVM axon ventral guidance caused by slt-1 mutations)."
Reference	"WBPaper00024195"


Anatomy_function : "WBbtf0343"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001291"
Gene	"WBGene00001555"
Involved	"WBbt:0003927"	Sufficient
Involved	"WBbt:0004096"	Sufficient
Involved	"WBbt:0006846"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0035176(social behavior)|GO:0007631(feeding behavior) QUALITY:PATO:0001630(dispersed) NOT"
Remark	"Genotype \"gcy-35; npr-1; Ex[gcy-32::gcy-35::gfp]\""
Remark	"Published_as gcy-35"
Remark	"pgcy-32::gcy-35::gfp construct restored strong aggregation and bordering behaviors to gcy-35;npr-1 animals. The gcy-32 promoter is expressed exclusively in the AQR, PQR, and URX neurons."
Reference	"WBPaper00024217"


Anatomy_function : "WBbtf0344"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001291"
Gene	"WBGene00001555"
Involved	"WBbt:0006846"	Sufficient
Involved	"WBbt:0006817"	Sufficient
Involved	"WBbt:0004086"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0035176(social behavior)|GO:0007631(feeding behavior) QUALITY:PATO:0001630(dispersed) NOT"
Remark	"Genotype \"gcy-35; npr-1; Ex[flp-8::gcy-35::gfp]\""
Remark	"Published_as gcy-35"
Remark	"pflp-8::gcy-35::gfp construct restored strong aggregation and bordering behaviors to gcy-35;npr-1 animals. The flp-8 promoter is expressed in the URX, AUA, and PVM neurons."
Reference	"WBPaper00024217"


Anatomy_function : "WBbtf0345"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001291"
Gene	"WBGene00001556"
Involved	"WBbt:0003927"	Sufficient
Involved	"WBbt:0004096"	Sufficient
Involved	"WBbt:0006846"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0035176(social behavior)|GO:0007631(feeding behavior) QUALITY:PATO:0001630(dispersed) NOT"
Remark	"Genotype \"gcy-36; npr-1; Ex[gcy-32::gcy-36::gfp]\""
Remark	"Published_as gcy-36"
Remark	"pgcy-32::gcy-36::gfp construct restored aggregation and bordering behaviors to gcy-36;npr-1 animals. The gcy-32 promoter is expressed exclusively in the AQR, PQR, and URX neurons."
Reference	"WBPaper00024217"


Anatomy_function : "WBbtf0346"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001291"
Gene	"WBGene00001556"
Involved	"WBbt:0006846"	Sufficient
Involved	"WBbt:0006817"	Sufficient
Involved	"WBbt:0004086"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0035176(social behavior)|GO:0007631(feeding behavior) QUALITY:PATO:0001630(dispersed) NOT"
Remark	"Genotype \"gcy-36; npr-1; Ex[flp-8::gcy-36::gfp]\""
Remark	"Published_as gcy-36"
Remark	"pflp-8::gcy-36::gfp construct restored aggregation and bordering behaviors to gcy-36;npr-1 animals. The flp-8 promoter is expressed in the URX, AUA, and PVM neurons."
Reference	"WBPaper00024217"


Anatomy_function : "WBbtf0347"
Assay	"Blastomere_isolation"
Phenotype	"WBPhenotype:0000306"
Not_involved	"WBbt:0004458"	Insufficient
Remark	"ENTITY:WBbt:0004458(MS)|GO:0010467(gene expression)|WBGene00003623(nhr-25) QUALITY:PATO:0000462(absent)"
Remark	"Genotype \"qtIs9[nhr-25::YFP]\""
Remark	"Using a laser to ablate all other cells, partial embryos resulting from isolated wild-type MS blastomeres failed to show significant nhr-25::YFP."
Reference	"WBPaper00034727"


Anatomy_function : "WBbtf0348"
Assay	"Blastomere_isolation"
Phenotype	"WBPhenotype:0000306"
Involved	"WBbt:0003810"	Sufficient
Remark	"ENTITY:WBbt:0003810(C)|GO:0010467(gene expression)|WBGene00003623(nhr-25) QUALITY:PATO:0000467(present)"
Remark	"Genotype \"qtIs9[nhr-25::YFP]\""
Remark	"Using a laser to ablate all other cells, partial embryos resulting from isolated wild-type C blastomeres generated nhr-25::YFP descendants."
Reference	"WBPaper00034727"


Anatomy_function : "WBbtf0349"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000389"	Autonomous
Gene	"WBGene00001249"
Involved	"WBbt:0005784"	Necessary
Remark	"ENTITY:WBbt:0006798(sperm)|GO:0009566(fertilization) QUALITY:PATO:0001511(defective)"
Remark	"ENTITY:WBbt:0006798(sperm)|GO:0031143(pseudopodium)|GO:0048513(organ development) QUALITY:PATO:0000460(defective)"
Remark	"ENTITY:WBbt:0006798(sperm)|GO:0048870(cell motility) QUALITY:PATO:0001511(defective)"
Remark	"Genotype \"elt-1(ok1002); Ex[elt-1(+) rol-6(su1006)]\""
Remark	"Published_as elt-1"
Remark	"loss of the elt-1 transgene in the primordial germ line stem cells Z2 and/or Z3 during development, or silencing of the transgene in the germ line, resulted in sterility caused by sperm-specific defects."
Reference	"WBPaper00034714"


Anatomy_function : "WBbtf0350"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000389"	Autonomous
Gene	"WBGene00001249"
Involved	"WBbt:0005784"	Sufficient
Remark	"ENTITY:WBbt:0006798(sperm)|GO:0009566(fertilization) QUALITY:PATO:0001511(defective) NOT"
Remark	"ENTITY:WBbt:0006798(sperm)|GO:0009566(fertilization) QUALITY:PATO:0001511(defective) NOT"
Remark	"ENTITY:WBbt:0006798(sperm)|GO:0031143(pseudopodium)|GO:0048513(organ development) QUALITY:PATO:0000460(defective) NOT"
Remark	"ENTITY:WBbt:0006798(sperm)|GO:0048870(cell motility) QUALITY:PATO:0001511(defective) NOT"
Remark	"Published_as elt-1"
Remark	"RNAi of elt-1 caused variable penetrance of sperm sterility defects since sperm genes as a group appear particularly refractory to inactivation by this technique."
Reference	"WBPaper00034714"


Anatomy_function : "WBbtf0351"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001503"	Nonautonomous
Gene	"WBGene00006980"
Involved	"WBbt:0004070"	Sufficient
Remark	"ENTITY:WBls:000006(young adult)|WBbt:0006976(PVQ)|GO:0030424(axon)|GO:0007413(axonal fasciculation) QUALITY:PATO:0000460(aberrant) NOT"
Remark	"Genotype \"zig-3(tm924); Ex[gcy-1::zig-3]\""
Remark	"Published_as zig-3"
Remark	"expression of zig-3 under control of the gcy-1 promoter, which is active in PVT, the gut, and a few head neurons, rescues the zig-3 mutant phenotype."
Reference	"WBPaper00035166"


Anatomy_function : "WBbtf0352"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001503"	Nonautonomous
Gene	"WBGene00006980"
Involved	"WBbt:0006804"	Sufficient
Remark	"ENTITY:WBls:000006(young adult)|WBbt:0006976(PVQ)|GO:0030424(axon)|GO:0007413(axonal fasciculation) QUALITY:PATO:0000460(aberrant) NOT"
Remark	"Genotype \"zig-3(tm924); Ex[myo-3::zig-3]\""
Remark	"Published_as zig-3"
Remark	"expression of zig-3 under control of the myo-3 promoter, which is exclusively active in body wall muscle cells that abut the ventral nerve cord, we observe full rescue of the zig-3 mutant phenotype."
Reference	"WBPaper00035166"


Anatomy_function : "WBbtf0353"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001503"	Nonautonomous
Gene	"WBGene00006980"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBls:000006(young adult)|WBbt:0006976(PVQ)|GO:0030424(axon)|GO:0007413(axonal fasciculation) QUALITY:PATO:0000460(aberrant) NOT"
Remark	"Genotype \"zig-3(tm924); Ex[unc-14::zig-3]\""
Remark	"Published_as zig-3"
Remark	"expression of zig-3 under control of the unc-14 promoter, which is active in all neurons, rescues the zig-3 mutant phenotype."
Reference	"WBPaper00035166"


Anatomy_function : "WBbtf0354"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001503"	Nonautonomous
Gene	"WBGene00006980"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBls:000006(young adult)|WBbt:0006976(PVQ)|GO:0030424(axon)|GO:0007413(axonal fasciculation) QUALITY:PATO:0000460(aberrant) NOT"
Remark	"Genotype \"zig-3(tm924); Ex[dpy-7::zig-3]\""
Remark	"Published_as zig-3"
Remark	"expression of zig-3 under control of the dpy-7 promoter, which is active exclusively in hypodermal cells that underlie the ventral nerve cord, rescues the zig-3 mutant phenotype."
Reference	"WBPaper00035166"


Anatomy_function : "WBbtf0355"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001503"	Nonautonomous
Gene	"WBGene00006980"
Not_involved	"WBbt:0006976"	Insufficient
Remark	"ENTITY:WBls:000006(young adult)|WBbt:0006976(PVQ)|GO:0030424(axon)|GO:0007413(axonal fasciculation) QUALITY:PATO:0000460(aberrant)"
Remark	"Genotype \"zig-3(tm924); Ex[sra-6::zig-3]\""
Remark	"Published_as zig-3"
Remark	"expression of zig-3 under control of the sra-6 promoter, which is active only in PVQ neurons in the ventral nerve cord, does not rescue the zig-3 mutant phenotype."
Reference	"WBPaper00035166"


Anatomy_function : "WBbtf0356"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001503"
Involved	"WBbt:0004070"	Necessary
Remark	"ENTITY:WBls:000006(young adult)|WBbt:0006976(PVQ)|GO:0030424(axon)|GO:0007413(axonal fasciculation) QUALITY:PATO:0000460(aberrant)"
Remark	"postembryonic (early L1 stage) laser ablation of PVT phenocopies the (PVQ) axon maintenance defects observed in zig-3 and zig-4 mutant animals."
Reference	"WBPaper00035166"


Anatomy_function : "WBbtf0357"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001714"
Not_involved	"WBbt:0003904"	Unnecessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0006935(chemotaxis)|CHEBI:26710(sodium chloride) QUALITY:PATO:0000461(normal)"
Remark	"ablation of ASEL had no apparent effect on the relationship between temporal change of NaCl concentration (dC/dT) and probability of pirouette."
Reference	"WBPaper00033096"


Anatomy_function : "WBbtf0358"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001462"
Not_involved	"WBbt:0003904"	Unnecessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0006935(chemotaxis)|CHEBI:26710(sodium chloride) QUALITY:PATO:0000461(normal)"
Remark	"ablation of ASEL had no apparent effect on NaCl chemotaxis."
Reference	"WBPaper00033096"


Anatomy_function : "WBbtf0359"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0004017"
Not_involved	"WBbt:0003904"	Unnecessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0006935(chemotaxis)|CHEBI:26710(sodium chloride) QUALITY:PATO:0000461(normal)"
Remark	"ablation of ASEL had no apparent effect on NaCl chemotaxis weathervane response, assayed by the relationship between NaCl gradient in normal direction and average curving rate."
Reference	"WBPaper00033096"


Anatomy_function : "WBbtf0360"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001714"
Involved	"WBbt:0003903"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0006935(chemotaxis)|CHEBI:26710(sodium chloride) QUALITY:PATO:0000460(abnormal)"
Remark	"ablation of ASER caused partial impairment of the pirouette response, assayed by the relationship between temporal change of NaCl concentration (dC/dT) and probability of pirouette."
Reference	"WBPaper00033096"


Anatomy_function : "WBbtf0361"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001462"
Involved	"WBbt:0003903"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0006935(chemotaxis)|CHEBI:26710(sodium chloride) QUALITY:PATO:0000460(abnormal)"
Remark	"ablation of ASER caused poor NaCl chemotaxis."
Reference	"WBPaper00033096"


Anatomy_function : "WBbtf0362"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0004017"
Involved	"WBbt:0003903"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0006935(chemotaxis)|CHEBI:26710(sodium chloride) QUALITY:PATO:0000460(abnormal)"
Remark	"ablation of ASER partial impairment of NaCl chemotaxis weathervane response, assayed by the relationship between NaCl gradient in normal direction and average curving rate."
Reference	"WBPaper00033096"


Anatomy_function : "WBbtf0363"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001714"
Involved	"WBbt:0005663"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0006935(chemotaxis)|CHEBI:26710(sodium chloride) QUALITY:PATO:0000460(abnormal)"
Remark	"ablation of ASEL on top of ASER caused almost complete abolishment of the pirouette response, assayed by the relationship between temporal change of NaCl concentration (dC/dT) and probability of pirouette."
Reference	"WBPaper00033096"


Anatomy_function : "WBbtf0364"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001462"
Involved	"WBbt:0005663"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0006935(chemotaxis)|CHEBI:26710(sodium chloride) QUALITY:PATO:0000460(abnormal)"
Remark	"ablation of ASEL on top of ASER causes almost complete abolishment of NaCl chemotaxis."
Reference	"WBPaper00033096"


Anatomy_function : "WBbtf0365"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0004017"
Involved	"WBbt:0005663"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0006935(chemotaxis)|CHEBI:26710(sodium chloride) QUALITY:PATO:0000460(abnormal)"
Remark	"ablation of ASEL on top of ASER causes almost complete abolishment of NaCl chemotaxis weathervane response, assayed by the relationship between NaCl gradient in normal direction and average curving rate."
Reference	"WBPaper00033096"


Anatomy_function : "WBbtf0366"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001714"
Not_involved	"WBbt:0006833"	Unnecessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0006935(chemotaxis)|CHEBI:26710(sodium chloride) QUALITY:PATO:0000461(normal)"
Remark	"killing RIA did not affect the relationship between temporal change of NaCl concentration (dC/dT) and probability of pirouette."
Reference	"WBPaper00033096"


Anatomy_function : "WBbtf0367"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001462"
Not_involved	"WBbt:0006812"	Unnecessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0006935(chemotaxis)|CHEBI:26710(sodium chloride) QUALITY:PATO:0000461(normal)"
Remark	"killing the primary interneuron AIA did not cause discernible effect on NaCl chemotaxis."
Reference	"WBPaper00033096"


Anatomy_function : "WBbtf0368"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0004017"
Not_involved	"WBbt:0006833"	Unnecessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0006935(chemotaxis)|CHEBI:26710(sodium chloride) QUALITY:PATO:0000461(normal)"
Remark	"killing RIA did not affect NaCl chemotaxis weathervane response, assayed by the relationship between NaCl gradient in normal direction and average curving rate."
Reference	"WBPaper00033096"


Anatomy_function : "WBbtf0369"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001714"
Not_involved	"WBbt:0006839"	Unnecessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0006935(chemotaxis)|CHEBI:26710(sodium chloride) QUALITY:PATO:0000461(normal)"
Remark	"killing RIV did not affect the relationship between temporal change of NaCl concentration (dC/dT) and probability of pirouette."
Reference	"WBPaper00033096"


Anatomy_function : "WBbtf0370"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001462"
Not_involved	"WBbt:0006813"	Unnecessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0006935(chemotaxis)|CHEBI:26710(sodium chloride) QUALITY:PATO:0000461(normal)"
Remark	"killing the primary interneuron AIB did not cause discernible effect on NaCl chemotaxis."
Reference	"WBPaper00033096"


Anatomy_function : "WBbtf0371"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0004017"
Not_involved	"WBbt:0006839"	Unnecessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0006935(chemotaxis)|CHEBI:26710(sodium chloride) QUALITY:PATO:0000461(normal)"
Remark	"killing RIV did not affect NaCl chemotaxis weathervane response, assayed by the relationship between NaCl gradient in normal direction and average curving rate."
Reference	"WBPaper00033096"


Anatomy_function : "WBbtf0372"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001462"
Not_involved	"WBbt:0006833"	Unnecessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0006935(chemotaxis)|CHEBI:26710(sodium chloride) QUALITY:PATO:0000461(normal)"
Remark	"killing RIA did not affect NaCl chemotaxis."
Reference	"WBPaper00033096"


Anatomy_function : "WBbtf0373"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001462"
Not_involved	"WBbt:0005413"	Unnecessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0006935(chemotaxis)|CHEBI:26710(sodium chloride) QUALITY:PATO:0000461(normal)"
Remark	"killing the primary interneuron AIY did not cause discernible effect on NaCl chemotaxis."
Reference	"WBPaper00033096"


Anatomy_function : "WBbtf0374"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001462"
Not_involved	"WBbt:0006839"	Unnecessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0006935(chemotaxis)|CHEBI:26710(sodium chloride) QUALITY:PATO:0000461(normal)"
Remark	"killing RIV did not affect NaCl chemotaxis."
Reference	"WBPaper00033096"


Anatomy_function : "WBbtf0375"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001714"
Involved	"WBbt:0005836"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0006935(chemotaxis)|CHEBI:26710(sodium chloride) QUALITY:PATO:0000460(abnormal)"
Remark	"when AIZ neurons were ablated, a severe impairment, similar in extent to ASE ablation, of the pirouette response was observed, assayed by the relationship between temporal change of NaCl concentration (dC/dT) and probability of pirouette."
Reference	"WBPaper00033096"


Anatomy_function : "WBbtf0376"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001462"
Involved	"WBbt:0005836"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0006935(chemotaxis)|CHEBI:26710(sodium chloride) QUALITY:PATO:0000460(abnormal)"
Remark	"when AIZ neurons were ablated, a severe impairment, similar in extent to ASE ablation, of NaCl chemotaxis was observed."
Reference	"WBPaper00033096"


Anatomy_function : "WBbtf0377"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0004017"
Involved	"WBbt:0005836"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0006935(chemotaxis)|CHEBI:26710(sodium chloride) QUALITY:PATO:0000460(abnormal)"
Remark	"when AIZ neurons were ablated, a severe impairment was observed, similar in extent to ASE ablation, of NaCl chemotaxis weathervane response, assayed by the relationship between NaCl gradient in normal direction and average curving rate."
Reference	"WBPaper00033096"


Anatomy_function : "WBbtf0378"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000464"
Gene	"WBGene00015964"
Involved	"WBbt:0006846"	Sufficient
Involved	"WBbt:0003927"	Sufficient
Involved	"WBbt:0004096"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0006935(chemotaxis)|CHEBI:15379(oxygen)|CHEBI:16526(CO2) QUALITY:PATO:0001997(reduced) NOT"
Remark	"Expressing the HW (Hawaiian CB4856) allele of glb-5 in XQTL:HW animals under the gcy-36 promoter, which is selectively expressed in the URX, AQR, and PQR neurons, was sufficient for HW-like behavior, ie, animals showed a transient increase in turning upon a (1 percent CO2 + 20 percent O2) to (0 percent CO2 + 21 percent O2) shift and reduced turning upon the converse shift."
Remark	"Genotype \"XQTL:HW; Ex[pgcy-36::glb-5(HW)]\""
Remark	"Published_as glb-5"
Remark	"XQTL:HW is a strain with nearly pure N2 DNA except for the QTL region on chromosome X"
Reference	"WBPaper00032998"


Anatomy_function : "WBbtf0379"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000464"
Involved	"WBbt:0006846"	Necessary
Involved	"WBbt:0003927"	Necessary
Involved	"WBbt:0004096"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0006935(chemotaxis)|CHEBI:15379(oxygen)|CHEBI:16526(CO2) QUALITY:PATO:0001997(reduced)"
Remark	"Genotype \"VQTL:HW; XQTL:HW; qaIs2241\""
Remark	"Tested in a strain in which the URX, AQR, and PQR neurons are selectively killed by the BH3 protein egl-1, URX, AQR, and PQR were essential for the O2 and O2/CO2 (turning) responses in the VQTL::HW; XQTL::HW background."
Remark	"VQTL:HW; XQTL:HW is a strain with nearly pure N2 DNA except for the QTL region on chromosome V and X"
Reference	"WBPaper00032998"


Anatomy_function : "WBbtf0380"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001764"
Gene	"WBGene00015964"
Involved	"WBbt:0006846"	Sufficient
Involved	"WBbt:0003927"	Sufficient
Involved	"WBbt:0004096"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0006935(chemotaxis)|CHEBI:15379(oxygen)|CHEBI:16526(CO2) QUALITY:PATO:0001997(reduced) NOT"
Remark	"Expressing the HW (Hawaiian CB4856) allele of glb-5 in XQTL:HW animals under the gcy-36 promoter, which is selectively expressed in the URX, AQR, and PQR neurons, was sufficient for HW-like behavior, ie, animals showed a transient increase in turning upon a (1 percent CO2 + 20 percent O2) to (0 percent CO2 + 21 percent O2) shift and reduced turning upon the converse shift."
Remark	"Genotype \"XQTL:HW; Ex[pgcy-36::glb-5(HW)]\""
Remark	"Published_as glb-5"
Remark	"XQTL:HW is a strain with nearly pure N2 DNA except for the QTL region on chromosome X"
Reference	"WBPaper00032998"


Anatomy_function : "WBbtf0381"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000551"
Gene	"WBGene00015964"
Involved	"WBbt:0006846"	Sufficient
Involved	"WBbt:0003927"	Sufficient
Involved	"WBbt:0004096"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0006935(chemotaxis)|CHEBI:15379(oxygen)|CHEBI:16526(CO2) QUALITY:PATO:0001997(reduced) NOT"
Remark	"Expressing the HW (Hawaiian CB4856) allele of glb-5 in XQTL:HW animals under the gcy-36 promoter, which is selectively expressed in the URX, AQR, and PQR neurons, was sufficient for HW-like behavior, ie, animals showed a transient increase in turning upon a (1 percent CO2 + 20 percent O2) to (0 percent CO2 + 21 percent O2) shift and reduced turning upon the converse shift."
Remark	"Genotype \"XQTL:HW; Ex[pgcy-36::glb-5(HW)]\""
Remark	"Published_as glb-5"
Remark	"XQTL:HW is a strain with nearly pure N2 DNA except for the QTL region on chromosome X"
Reference	"WBPaper00032998"


Anatomy_function : "WBbtf0382"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0001764"
Involved	"WBbt:0006846"	Necessary
Involved	"WBbt:0003927"	Necessary
Involved	"WBbt:0004096"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0006935(chemotaxis)|CHEBI:15379(oxygen)|CHEBI:16526(CO2) QUALITY:PATO:0001997(reduced)"
Remark	"Genotype \"VQTL:HW; XQTL:HW; qaIs2241\""
Remark	"Tested in a strain in which the URX, AQR, and PQR neurons are selectively killed by the BH3 protein egl-1, URX, AQR, and PQR were essential for the O2 and O2/CO2 (turning) responses in the VQTL::HW; XQTL::HW background."
Remark	"VQTL:HW; XQTL:HW is a strain with nearly pure N2 DNA except for the QTL region on chromosome V and X"
Reference	"WBPaper00032998"


Anatomy_function : "WBbtf0383"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000551"
Involved	"WBbt:0006846"	Necessary
Involved	"WBbt:0003927"	Necessary
Involved	"WBbt:0004096"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0006935(chemotaxis)|CHEBI:15379(oxygen)|CHEBI:16526(CO2) QUALITY:PATO:0001997(reduced)"
Remark	"Genotype \"VQTL:HW; XQTL:HW; qaIs2241\""
Remark	"Tested in a strain in which the URX, AQR, and PQR neurons are selectively killed by the BH3 protein egl-1, URX, AQR, and PQR were essential for the O2 and O2/CO2 (turning) responses in the VQTL::HW; XQTL::HW background."
Remark	"VQTL:HW; XQTL:HW is a strain with nearly pure N2 DNA except for the QTL region on chromosome V and X"
Reference	"WBPaper00032998"


Anatomy_function : "WBbtf0384"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000660"
Gene	"WBGene00015964"
Involved	"WBbt:0006846"	Sufficient
Involved	"WBbt:0003927"	Sufficient
Involved	"WBbt:0004096"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0007631(feeding behavior) QUALITY:PATO:0001629(aggregated) NOT"
Remark	"Genotype \"XQTL:HW; Ex[pgcy-36::glb-5(HW)]\""
Remark	"Published_as glb-5"
Remark	"XQTL:HW is a strain with nearly pure N2 DNA except for the QTL region on chromosome X"
Remark	"aggregation (but not bordering) of the glb-5(N2) strain was suppressed by expressing glb-5(HW) under the promoter expressed in URX, AQR, and PQR neurons."
Reference	"WBPaper00032998"


Anatomy_function : "WBbtf0385"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0001524"
Involved	"WBbt:0005670"	Necessary
Remark	"ENTITY:WBls:0000024(L1 larva)|GO:(organism quiescence)|PATO:0000077(response to)|CHEBI:16583(diacetyl) QUALITY:PATO:0000470(increased) NOT"
Remark	"Genotype \"odr-7(ky4)\""
Remark	"odr-7(ky4) mutant, which lacks a transcription factor required to specify AWA neurons. Fewer odr-7 than N2 worms entered quiescence, suggesting that AWA neurons promote entry into diacetyl-induced L1 arrest."
Reference	"WBPaper00036288"


Anatomy_function : "WBbtf0386"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000081"
Involved	"WBbt:0005670"	Necessary
Remark	"ENTITY:WBls:0000024(L1 larva)|GO:(organism quiescence)|PATO:0000077(response to)|CHEBI:16583(diacetyl) QUALITY:PATO:0000470(increased) NOT"
Remark	"Genotype \"odr-7(ky4)\""
Remark	"odr-7(ky4) mutant, which lacks a transcription factor required to specify AWA neurons. Fewer odr-7 than N2 worms entered quiescence, suggesting that AWA neurons promote entry into diacetyl-induced L1 arrest."
Reference	"WBPaper00036288"


Anatomy_function : "WBbtf0387"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0001524"
Involved	"WBbt:0005671"	Necessary
Remark	"ENTITY:WBls:0000024(L1 larva)|GO:(organism quiescence)|PATO:0000077(response to)|CHEBI:16583(diacetyl) QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"lim-4(ky403)\""
Remark	"Significantly more L1 lim-4(ky403) mutants (which lack AWB neurons) entered arrest (diacetyl-induced quiescence)."
Reference	"WBPaper00036288"


Anatomy_function : "WBbtf0388"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000081"
Involved	"WBbt:0005671"	Necessary
Remark	"ENTITY:WBls:0000024(L1 larva)|GO:(organism quiescence)|PATO:0000077(response to)|CHEBI:16583(diacetyl) QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"lim-4(ky403)\""
Remark	"Significantly more L1 lim-4(ky403) mutants (which lack AWB neurons) entered arrest (diacetyl-induced quiescence)."
Reference	"WBPaper00036288"


Anatomy_function : "WBbtf0389"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0001524"
Involved	"WBbt:0005672"	Necessary
Remark	"ENTITY:WBls:0000024(L1 larva)|GO:(organism quiescence)|PATO:0000077(response to)|CHEBI:16583(diacetyl) QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"ceh-36(?)\""
Remark	"Significantly more L1 ceh-36 mutants (which lack AWC neurons) entered arrest (diacetyl-induced quiescence)."
Reference	"WBPaper00036288"


Anatomy_function : "WBbtf0390"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000081"
Involved	"WBbt:0005672"	Necessary
Remark	"ENTITY:WBls:0000024(L1 larva)|GO:(organism quiescence)|PATO:0000077(response to)|CHEBI:16583(diacetyl) QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"ceh-36(?)\""
Remark	"Significantly more L1 ceh-36 mutants (which lack AWC neurons) entered arrest (diacetyl-induced quiescence)."
Reference	"WBPaper00036288"


Anatomy_function : "WBbtf0391"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000216"	Autonomous
Gene	"WBGene00003595"
Involved	"WBbt:0005978"	Sufficient
Involved	"WBbt:0005978"	Necessary
Involved	"WBbt:0005978"	Remark
Remark	"ENTITY:WBbt:0008407(ABaraappaaa)|GO:0001708(cell fate specification)|GO:0009855(determination of bilateral asymmetry)|WBbt:0003664(MI)|WBbt:0003701(e1D)"
Remark	"Genotype \"ngn-1(n1921); nEx1638[ngn-1(+), sur-5::gfp, unc-119::gfp]\""
Remark	"Published_as ngn-1"
Remark	"We further examined the 36 animals of Class IV, in which ABaraappaaa was transformed into an e3D-like cell that had lost the array. We determined the cell division at which the array had been mitotically lost by scoring the presence or absence of the array in cells that shared a precursor cell with ABaraappaaa at some point of their lineage history. We identified 10 animals that had an extra e3D-like cell and had lost the array at the cell division of ABaraapp (Fig. 3E). This observation indicates that the presence of a functional ngn-1 gene in ABaraapp is insufficient to generate an MI neuron and thus that to generate MI a functional ngn-1 gene is necessary at or later than the stage of ABaraappa, the MI grandmother cell. By contrast, we identified no animals that had lost the array at the next cell division, that of the MI grandmother cell, ABaraappa (Fig. 3E). This result suggests that in all animals in which the array was present in the MI grandmother cell, ABaraappaaa differentiated as normal into an MI neuron whether the array was (Class I animals) or was not (Class II animals) transmitted to the presumptive MI neuron. Thus, the presence of the array in the MI grandmother cell was sufficient to rescue the MI transformation of ngn-1(n1921) mutants. Together, these findings indicate that the presence of the ngn-1 wild-type gene in the MI grandmother cell is both necessary and sufficient to generate an MI neuron and establish left-right asymmetry in the cell lineage."
Reference	"WBPaper00037739"


Anatomy_function : "WBbtf0392"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000216"	Autonomous
Gene	"WBGene00000457"
Involved	"WBbt:0006153"	Sufficient
Involved	"WBbt:0006153"	Necessary
Involved	"WBbt:0006153"	Remark
Remark	"ENTITY:WBbt:0008407(ABaraappaaa)|GO:0001708(cell fate specification)|GO:0009855(determination of bilateral asymmetry)|WBbt:0003664(MI)|WBbt:0003701(e1D)"
Remark	"Genotype \"ceh-36(n5333) lin-15AB(n765); nEx1703[ceh-36(+), sur-5::gfp, unc-119::gfp, lin-15AB(+)]\""
Remark	"Published_as ceh-36"
Remark	"We further examined the 28 animals of Class IV, in which ABaraappaaa was transformed into an e3D-like cell that had lost the array and determined the cell division at which the array had been mitotically lost. We identified eight animals that had an extra e3D-like cell and had lost the array at the cell division of ABaraap. By contrast, we identified no animals that had lost the array at the next cell division, that of the MI great grandmother cell, ABaraapp. Together, these findings indicate that the presence of the ceh-36 wild-type gene in the MI great grandmother cell is both necessary and sufficient to rescue the MI transformation defect of ceh-36(n5333)."
Reference	"WBPaper00037739"


Anatomy_function : "WBbtf0393"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000012"	Nonautonomous
Gene	"WBGene00010671"
Involved	"WBbt:0007855"	Sufficient
Remark	"ENTITY:WBls:0000032(dauer larva)|GO:0032502(development) QUALITY:PATO:0000380(increased frequency) NOT"
Remark	"Genotype \"eak-7;akt-1;Ex[eak-4p::EAK-7::GFP]\""
Remark	"Published_as eak-7"
Remark	"XXX cell-specific (eak-4 promoter driven) expression of EAK-7::GFP rescues the dauer arrest phenotype of eak-7;akt-1 mutants."
Reference	"WBPaper00036472"


Anatomy_function : "WBbtf0394"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000012"	Nonautonomous
Gene	"WBGene00010671"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBls:0000032(dauer larva)|GO:0032502(development) QUALITY:PATO:0000380(increased frequency) NOT"
Remark	"Genotype \"eak-7;akt-1;Ex[ric-19p::EAK-7::GFP]\""
Remark	"Published_as eak-7"
Remark	"neuron-specific ric-19 promoter-driven expression of EAK-7::GFP rescues the dauer arrest phenotype of eak-7;akt-1 mutants."
Reference	"WBPaper00036472"


Anatomy_function : "WBbtf0395"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000012"
Gene	"WBGene00010671"
Not_involved	"WBbt:0005792"	Insufficient
Remark	"ENTITY:WBls:0000032(dauer larva)|GO:0032502(development) QUALITY:PATO:0000380(increased frequency)"
Remark	"Genotype \"eak-7;akt-1;Ex[ges-1p::EAK-7::GFP]\""
Remark	"Published_as eak-7"
Remark	"intestinal cell-specific (ges-1 promoter driven) expression of EAK-7::GFP does not rescue the dauer arrest phenotypeof eak-7;akt-1 mutants."
Reference	"WBPaper00036472"


Anatomy_function : "WBbtf0396"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000039"	Nonautonomous
Gene	"WBGene00010671"
Involved	"WBbt:0007855"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0008340(determination of adult life span) QUALITY:PATO:0001333(temporally extended) NOT"
Remark	"Genotype \"eak-7;akt-1;Ex[eak-4p::EAK-7::GFP]\""
Remark	"Published_as eak-7"
Remark	"XXX cell-specific (eak-4 promoter driven) expression of EAK-7::GFP rescues the life span extension phenotype of eak-7;akt-1 mutants."
Reference	"WBPaper00036472"


Anatomy_function : "WBbtf0397"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000039"	Nonautonomous
Gene	"WBGene00010671"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0008340(determination of adult life span) QUALITY:PATO:0001333(temporally extended) NOT"
Remark	"Genotype \"eak-7;akt-1;Ex[ric-19p::EAK-7::GFP]\""
Remark	"Published_as eak-7"
Remark	"neuron-specific (ric-19 promoter driven) expression of EAK-7::GFP rescues the life span extension phenotype of eak-7;akt-1 mutants."
Reference	"WBPaper00036472"


Anatomy_function : "WBbtf0398"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000039"	Nonautonomous
Gene	"WBGene00010671"
Involved	"WBbt:0005792"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0008340(determination of adult life span) QUALITY:PATO:0001333(temporally extended) NOT"
Remark	"Genotype \"eak-7;akt-1;Ex[ges-1p::EAK-7::GFP]\""
Remark	"Published_as eak-7"
Remark	"intestine-specific (ges-1 promoter driven) expression of EAK-7::GFP rescues the life span extension phenotype of eak-7;akt-1 mutants."
Reference	"WBPaper00036472"


Anatomy_function : "WBbtf0399"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000633"	Autonomous
Gene	"WBGene00016611"
Involved	"WBbt:0006831"	Sufficient
Remark	"ENTITY:WBbt:0006831(PVD)|(tertiary)|GO:0044307(dendritic branch)|GO:0048856(anatomical structure development) QUALITY:PATO:0000584(hypertrophy) NOT"
Remark	"Genotype \"bicd-1(ok2731); otIs138[ser2prom3::GFP];Ex[ser2prom3p::bicd-1]\""
Remark	"Published_as bicd-1"
Remark	"Selective expression of BICD-1 in PVD neurons (using ser2prom3 promoter, which is also active in OLL neurons) partially rescued the enhanced-branching phenotype in three out of four independent transgenic lines, whereas exclusively expressing BICD-1 in muscle cells (using a myo-3 promoter) only weakly rescued the enhanced-branching phenotype in one out of three independent transgenic lines."
Reference	"WBPaper00037977"


Anatomy_function : "WBbtf0400"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000633"
Gene	"WBGene00016611"
Involved	"WBbt:0005994"	Sufficient
Remark	"ENTITY:WBbt:0006831(PVD)|(tertiary)|GO:0044307(dendritic branch)|GO:0048856(anatomical structure development) QUALITY:PATO:0000584(hypertrophy) NOT"
Remark	"Genotype \"bicd-1(ok2731); otIs138[ser2prom3::GFP];Ex[bicd-1(+);myo-3prom::RFP;mec-7prom::GFP]\""
Remark	"Published_as bicd-1"
Remark	"genetic mosaic analyses revealed that animals that retained wild-type bicd-1 in the AB.p lineage (which gives rise to the PVD neurons) but not the P1 lineage (which gives rise to 94 out of 95 body wall muscles) exhibited partial rescue of the enhanced-branching bicd-1(ok2731) mutant phenotype."
Reference	"WBPaper00037977"


Anatomy_function : "WBbtf0401"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000273"
Gene	"WBGene00001187"
Involved	"WBbt:0003679"	Sufficient
Involved	"WBbt:0003675"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:(movement in liquid) QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"egl-19(n582); Ex[egl-19(+) sur-5::GFP]\""
Remark	"Published_as egl-19"
Remark	"Reduced locomotion of egl-19(n582) was partially restored by neuronal EGL-19 transgene, but was either unaffected (in liquid) or very slightly improved by muscle EGL-19 transgene. However, locomotion was only fully rescued when EGL-19 transgene was present in both neurons and muscles."
Reference	"WBPaper00038056"


Anatomy_function : "WBbtf0402"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000646"
Gene	"WBGene00001187"
Involved	"WBbt:0003679"	Sufficient
Involved	"WBbt:0003675"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0040011(locomotion)|PATO:0000008(velocity) QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"egl-19(n582); Ex[egl-19(+) sur-5::GFP]\""
Remark	"Published_as egl-19"
Remark	"Reduced locomotion of egl-19(n582) was partially restored by neuronal EGL-19 transgene, but was either unaffected (in liquid) or very slightly improved by muscle EGL-19 transgene. However, locomotion was only fully rescued when EGL-19 transgene was present in both neurons and muscles."
Reference	"WBPaper00038056"


Anatomy_function : "WBbtf0403"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001315"
Gene	"WBGene00001187"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|GO:0045760(activation of action potential)|PATO:0000044(frequency) QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"egl-19(n582); Ex[egl-19(+) sur-5::GFP]\""
Remark	"Published_as egl-19"
Remark	"we compared the kinetics and frequency of spontaneous action potentials in egl-19 (n582) mutants that carried a functional EGL-19 transgene in different tissues by mosaic analyses and tissue-specific rescue. When the transgene was present in both neurons and muscles, the frequency and duration of the action potentials were fully restored. When the transgene was present in neurons alone, only the frequency of action potentials was rescued, suggesting that frequency was strictly regulated through a neuronal role of L-VGCC/EGL-19."
Reference	"WBPaper00038056"


Anatomy_function : "WBbtf0404"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001315"
Gene	"WBGene00001187"
Not_involved	"WBbt:0003679"	Insufficient
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|GO:0045760(activation of action potential)|PATO:0001309(duration) QUALITY:PATO:0000573(long)"
Remark	"Genotype \"egl-19(n582); Ex[egl-19(+) sur-5::GFP]\""
Remark	"Published_as egl-19"
Remark	"we compared the kinetics and frequency of spontaneous action potentials in egl-19 (n582) mutants that carried a functional EGL-19 transgene in different tissues by mosaic analyses and tissue-specific rescue. When the transgene was present in both neurons and muscles, the frequency and duration of the action potentials were fully restored. When the transgene was present in neurons alone, the duration of action potentials was not rescued (remains longer than WT)."
Reference	"WBPaper00038056"


Anatomy_function : "WBbtf0405"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001315"
Gene	"WBGene00001187"
Not_involved	"WBbt:0003679"	Insufficient
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|GO:(resting membrane potential) QUALITY:PATO:0001475(high)"
Remark	"Genotype \"egl-19(n582); Ex[egl-19(+) sur-5::GFP]\""
Remark	"Published_as egl-19"
Remark	"we compared action potentials in egl-19 (n582) mutants that carried a functional EGL-19 transgene in different tissues by mosaic analyses and tissue-specific rescue. When the transgene was present in both neurons and muscles, the wild-type level of resting membrane potentials was fully restored. When the transgene was present in neurons alone, the resting potential was not affected, higher than that of wild type."
Reference	"WBPaper00038056"


Anatomy_function : "WBbtf0406"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001315"
Gene	"WBGene00001187"
Involved	"WBbt:0006804"	Sufficient
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|GO:(resting membrane potential) QUALITY:PATO:0001475(high) NOT"
Remark	"Genotype \"egl-19(n582); Ex[Pmyo-3-egl-19 Podr-1::GFP]\""
Remark	"Published_as egl-19"
Remark	"we compared action potentials in egl-19 (n582) mutants that carried a functional EGL-19 transgene in different tissues by mosaic analyses and tissue-specific rescue. When the transgene was present in both neurons and muscles, the wild-type level of resting membrane potentials was fully restored. We used an alternative strategy where we expressed EGL-19 minigene by a body wall muscle-specific promoter in egl-19(n582) mutants. In these animals, the resting membrane potential was fully restored."
Reference	"WBPaper00038056"


Anatomy_function : "WBbtf0407"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001315"
Gene	"WBGene00001187"
Not_involved	"WBbt:0006804"	Insufficient
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|GO:0045760(activation of action potential)|PATO:0000044(frequency) QUALITY:PATO:0001997(reduced)"
Remark	"Genotype \"egl-19(n582); Ex[Pmyo-3-egl-19 Podr-1::GFP]\""
Remark	"Published_as egl-19"
Remark	"we compared the kinetics and frequency of spontaneous action potentials in egl-19 (n582) mutants that carried a functional EGL-19 transgene in different tissues by mosaic analyses and tissue-specific rescue. When the transgene was present in both neurons and muscles, the frequency and duration of the action potentials were fully restored. We used an alternative strategy where we expressed EGL-19 minigene by a body wall muscle-specific promoter in egl-19(n582) mutants. In these animals, the action potential frequency remains reduced."
Reference	"WBPaper00038056"


Anatomy_function : "WBbtf0408"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001315"
Gene	"WBGene00001187"
Involved	"WBbt:0006804"	Sufficient
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|GO:0045760(activation of action potential)|PATO:0001309(duration) QUALITY:PATO:0000573(long) NOT"
Remark	"Genotype \"egl-19(n582); Ex[Pmyo-3-egl-19 Podr-1::GFP]\""
Remark	"Published_as egl-19"
Remark	"we compared the kinetics and frequency of spontaneous action potentials in egl-19 (n582) mutants that carried a functional EGL-19 transgene in different tissues by mosaic analyses and tissue-specific rescue. When the transgene was present in both neurons and muscles, the frequency and duration of the action potentials were fully restored. We used an alternative strategy where we expressed EGL-19 minigene by a body wall muscle-specific promoter in egl-19(n582) mutants. In these animals, the duration of action potential was partially restored."
Reference	"WBPaper00038056"


Anatomy_function : "WBbtf0409"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000107"
Gene	"WBGene00007772"
Not_involved	"WBbt:0005784"	Insufficient
Remark	"ENTITY:WBbt:0007849(hermaphrodite)|GO:0030728(ovulation) QUALITY:PATO:0000694(premature)"
Remark	"Genotype \"rrf-1(pk1417)\""
Remark	"Published_as egrh-1"
Remark	"we examined the effect of egrh-1(RNAi) in an rrf-1(pk1417) mutant background. rrf-1(pk1417) mutants are specifically resistant to RNAi in the soma but remain sensitive to RNAi in the germline. We found that egrh-1(RNAi) was less effective in rrf-1(pk1417) than in a wild-type background. Indeed, rrf-1(pk1417); egrh-1(RNAi) animals exhibited only a slight increase in the frequency of oocyte defects when compared with untreated rrf-1(pk1417) mutants. Thus, we conclude that egrh-1 functions in the soma."
Reference	"WBPaper00037082"


Anatomy_function : "WBbtf0410"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000107"
Gene	"WBGene00007772"
Involved	"WBbt:0005785"	Necessary
Involved	"WBbt:0005792"	Necessary
Remark	"ENTITY:WBbt:0007849(hermaphrodite)|GO:0030728(ovulation) QUALITY:PATO:0000694(premature)"
Remark	"Genotype \"egrh-1(tm1736); CuEx531[egrh-1(+) sur-5::gfp]\""
Remark	"Published_as egrh-1"
Remark	"We next examined the phenotype of egrh-1(tm1736) animals that were mosaic for a rescuing transgene. We generated the strain egrh-1(tm1736); cuEx531 containing the egrh-1(+) cosmid C27C12 and the cell autonomous marker for somatic cells sur-5::gfp. We first identified animals that specifically lost this transgene in the EMS blastomere, which is the precursor of the somatic gonad and gut but not the germline, and 95% of these animals exhibited abnormal and distal oocytes. Thus, egrh-1 function is required in somatic tissues derived from EMS. We next identified mosaic animals that lost the transgene only in MS or E, the descendants of EMS that give rise to the somatic gonad or gut, respectively. Loss in either MS or E resulted in the egrh-1 phenotype, strongly suggesting that egrh-1 function is required in both the somatic gonad and the gut for normal oocyte development."
Reference	"WBPaper00037082"


Anatomy_function : "WBbtf0411"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000107"
Gene	"WBGene00007772"
Involved	"WBbt:0005792"	Sufficient
Remark	"ENTITY:WBbt:0007849(hermaphrodite)|GO:0030728(ovulation) QUALITY:PATO:0000694(premature) NOT"
Remark	"Genotype \"egrh-1(tm1736); Ex[ges-1::egrh-1]\""
Remark	"Published_as egrh-1"
Remark	"We next expressed egrh-1 in the E lineage using the ges-1 promoter and asked if gut expression is sufficient to rescue egrh1 mutants. egrh-1 expression in the E lineage partially rescued the formation of abnormal and distal oocytes in both egrh-1 mutant hermaphrodites and egrh-1 mutant females."
Reference	"WBPaper00037082"


Anatomy_function : "WBbtf0412"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001930"	Autonomous
Gene	"WBGene00016539"
Involved	"WBbt:0006804"	Sufficient
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|GO:0031253(membrane extension) QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"madd-2(tr103); Ex[myo-3p::MADD-2A]\""
Remark	"Published_as madd-2"
Remark	"To test whether madd-2 functions cell autonomously, we expressed MADD-2 in either all BWMs (by using the myo-3 promoter) or only the distal BWMs (by using the him-4 promoter) of tr103 mutants and observed complete rescue of the muscle arm extension defects."
Reference	"WBPaper00036485"


Anatomy_function : "WBbtf0413"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001930"
Gene	"WBGene00016539"
Not_involved	"WBbt:0003679"	Insufficient
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|GO:0031253(membrane extension) QUALITY:PATO:0001997(reduced)"
Remark	"Genotype \"madd-2(tr103); Ex[unc-119p::MADD-2A]\""
Remark	"Published_as madd-2"
Remark	"To test whether madd-2 functions cell autonomously, we expressed MADD-2 in either all BWMs (by using the myo-3 promoter) or only the distal BWMs (by using the him-4 promoter) of tr103 mutants and observed complete rescue of the muscle arm extension defects. By contrast, neuronal expression of MADD-2 failed to rescue the muscle arm extension defects of the madd-2 null mutant."
Reference	"WBPaper00036485"


Anatomy_function : "WBbtf0414"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001652"	Autonomous
Gene	"WBGene00000380"
Involved	"WBbt:0004522"	Necessary
Remark	"ENTITY:WBbt:0004522(anchor cell)|PATO:0002103(infiltrating)|GO:0005604(basement membrane) QUALITY:PATO:0000468(reduced)"
Remark	"Genotype \"rde-1(ne219); fos-1a>RDE-1;rrf-3(pk1426)\""
Remark	"Published_as cct-5"
Remark	"we used a C. elegans strain in which only uterine tissue, including the AC, is sensitive to RNAi. RNAi depletions targeting cct-5 gene, which showed transgene localization in the AC, blocked invasion. Because uterine cells do not contribute to AC invasion, an AC invasion defect in this background indicates that the gene functions in the AC."
Reference	"WBPaper00036215"


Anatomy_function : "WBbtf0415"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001652"	Autonomous
Gene	"WBGene00020391"
Involved	"WBbt:0004522"	Necessary
Remark	"ENTITY:WBbt:0004522(anchor cell)|PATO:0002103(infiltrating)|GO:0005604(basement membrane) QUALITY:PATO:0000468(reduced)"
Remark	"Genotype \"rde-1(ne219); fos-1a>RDE-1;rrf-3(pk1426)\""
Remark	"Published_as cct-7"
Remark	"we used a C. elegans strain in which only uterine tissue, including the AC, is sensitive to RNAi. RNAi depletions targeting cct-7 gene, which showed transgene localization in the AC, blocked invasion. Because uterine cells do not contribute to AC invasion, an AC invasion defect in this background indicates that the gene functions in the AC."
Reference	"WBPaper00036215"


Anatomy_function : "WBbtf0416"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001652"	Autonomous
Gene	"WBGene00001834"
Involved	"WBbt:0004522"	Necessary
Remark	"ENTITY:WBbt:0004522(anchor cell)|PATO:0002103(infiltrating)|GO:0005604(basement membrane) QUALITY:PATO:0000468(reduced)"
Remark	"Genotype \"rde-1(ne219); fos-1a>RDE-1;rrf-3(pk1426)\""
Remark	"Published_as hda-1"
Remark	"we used a C. elegans strain in which only uterine tissue, including the AC, is sensitive to RNAi. RNAi depletions targeting hda-1 gene, which showed transgene localization in the AC, blocked invasion. Because uterine cells do not contribute to AC invasion, an AC invasion defect in this background indicates that the gene functions in the AC."
Reference	"WBPaper00036215"


Anatomy_function : "WBbtf0417"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001652"	Autonomous
Gene	"WBGene00003218"
Involved	"WBbt:0004522"	Necessary
Remark	"ENTITY:WBbt:0004522(anchor cell)|PATO:0002103(infiltrating)|GO:0005604(basement membrane) QUALITY:PATO:0000468(reduced)"
Remark	"Genotype \"rde-1(ne219); fos-1a>RDE-1;rrf-3(pk1426)\""
Remark	"Published_as mep-1"
Remark	"we used a C. elegans strain in which only uterine tissue, including the AC, is sensitive to RNAi. RNAi depletions targeting mep-1 gene, which showed transgene localization in the AC, blocked invasion. Because uterine cells do not contribute to AC invasion, an AC invasion defect in this background indicates that the gene functions in the AC."
Reference	"WBPaper00036215"


Anatomy_function : "WBbtf0418"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001652"	Autonomous
Gene	"WBGene00001345"
Involved	"WBbt:0004522"	Necessary
Remark	"ENTITY:WBbt:0004522(anchor cell)|PATO:0002103(infiltrating)|GO:0005604(basement membrane) QUALITY:PATO:0000468(reduced)"
Remark	"Genotype \"rde-1(ne219); fos-1a>RDE-1;rrf-3(pk1426)\""
Remark	"Published_as fos-1a"
Remark	"we used a C. elegans strain in which only uterine tissue, including the AC, is sensitive to RNAi. RNAi depletions targeting fos-1a gene, which showed transgene localization in the AC, blocked invasion. Because uterine cells do not contribute to AC invasion, an AC invasion defect in this background indicates that the gene functions in the AC."
Reference	"WBPaper00036215"


Anatomy_function : "WBbtf0419"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001652"	Autonomous
Gene	"WBGene00016739"
Involved	"WBbt:0004522"	Necessary
Remark	"ENTITY:WBbt:0004522(anchor cell)|PATO:0002103(infiltrating)|GO:0005604(basement membrane) QUALITY:PATO:0000468(reduced)"
Remark	"Genotype \"rde-1(ne219); fos-1a>RDE-1;rrf-3(pk1426)\""
Remark	"Published_as C48A7.2"
Remark	"we used a C. elegans strain in which only uterine tissue, including the AC, is sensitive to RNAi. RNAi depletions targeting C48A7.2 gene, which showed transgene localization in the AC, blocked invasion. Because uterine cells do not contribute to AC invasion, an AC invasion defect in this background indicates that the gene functions in the AC."
Reference	"WBPaper00036215"


Anatomy_function : "WBbtf0420"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001652"	Autonomous
Gene	"WBGene00012230"
Involved	"WBbt:0004522"	Necessary
Remark	"ENTITY:WBbt:0004522(anchor cell)|PATO:0002103(infiltrating)|GO:0005604(basement membrane) QUALITY:PATO:0000468(reduced)"
Remark	"Genotype \"rde-1(ne219); fos-1a>RDE-1;rrf-3(pk1426)\""
Remark	"Published_as cacn-1"
Remark	"we used a C. elegans strain in which only uterine tissue, including the AC, is sensitive to RNAi. RNAi depletions targeting cacn-1 gene, which showed transgene localization in the AC, blocked invasion. Because uterine cells do not contribute to AC invasion, an AC invasion defect in this background indicates that the gene functions in the AC."
Reference	"WBPaper00036215"


Anatomy_function : "WBbtf0421"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001652"	Autonomous
Gene	"WBGene00009223"
Involved	"WBbt:0004522"	Necessary
Remark	"ENTITY:WBbt:0004522(anchor cell)|PATO:0002103(infiltrating)|GO:0005604(basement membrane) QUALITY:PATO:0000468(reduced)"
Remark	"Genotype \"rde-1(ne219); fos-1a>RDE-1;rrf-3(pk1426)\""
Remark	"Published_as F28F8.5"
Remark	"we used a C. elegans strain in which only uterine tissue, including the AC, is sensitive to RNAi. RNAi depletions targeting F28F8.5 gene, which showed transgene localization in the AC, blocked invasion. Because uterine cells do not contribute to AC invasion, an AC invasion defect in this background indicates that the gene functions in the AC."
Reference	"WBPaper00036215"


Anatomy_function : "WBbtf0422"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001652"	Autonomous
Gene	"WBGene00020600"
Involved	"WBbt:0004522"	Necessary
Remark	"ENTITY:WBbt:0004522(anchor cell)|PATO:0002103(infiltrating)|GO:0005604(basement membrane) QUALITY:PATO:0000468(reduced)"
Remark	"Genotype \"rde-1(ne219); fos-1a>RDE-1;rrf-3(pk1426)\""
Remark	"Published_as T20B12.1"
Remark	"we used a C. elegans strain in which only uterine tissue, including the AC, is sensitive to RNAi. RNAi depletions targeting T20B12.1 gene, which showed transgene localization in the AC, blocked invasion. Because uterine cells do not contribute to AC invasion, an AC invasion defect in this background indicates that the gene functions in the AC."
Reference	"WBPaper00036215"


Anatomy_function : "WBbtf0423"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001652"	Autonomous
Gene	"WBGene00003048"
Involved	"WBbt:0004522"	Necessary
Remark	"ENTITY:WBbt:0004522(anchor cell)|PATO:0002103(infiltrating)|GO:0005604(basement membrane) QUALITY:PATO:0000468(reduced)"
Remark	"Genotype \"rde-1(ne219); fos-1a>RDE-1;rrf-3(pk1426)\""
Remark	"Published_as lit-1"
Remark	"we used a C. elegans strain in which only uterine tissue, including the AC, is sensitive to RNAi. RNAi depletions targeting lit-1 gene, which showed transgene localization in the AC, blocked invasion. Because uterine cells do not contribute to AC invasion, an AC invasion defect in this background indicates that the gene functions in the AC."
Reference	"WBPaper00036215"


Anatomy_function : "WBbtf0424"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001652"	Autonomous
Gene	"WBGene00021097"
Involved	"WBbt:0004522"	Necessary
Remark	"ENTITY:WBbt:0004522(anchor cell)|PATO:0002103(infiltrating)|GO:0005604(basement membrane) QUALITY:PATO:0000468(reduced)"
Remark	"Genotype \"rde-1(ne219); fos-1a>RDE-1;rrf-3(pk1426)\""
Remark	"Published_as cdc-37"
Remark	"we used a C. elegans strain in which only uterine tissue, including the AC, is sensitive to RNAi. RNAi depletions targeting cdc-37 gene, which showed transgene localization in the AC, blocked invasion. Because uterine cells do not contribute to AC invasion, an AC invasion defect in this background indicates that the gene functions in the AC."
Reference	"WBPaper00036215"


Anatomy_function : "WBbtf0425"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001652"	Autonomous
Gene	"WBGene00020190"
Involved	"WBbt:0004522"	Necessary
Remark	"ENTITY:WBbt:0004522(anchor cell)|PATO:0002103(infiltrating)|GO:0005604(basement membrane) QUALITY:PATO:0000468(reduced)"
Remark	"Genotype \"rde-1(ne219); fos-1a>RDE-1;rrf-3(pk1426)\""
Remark	"Published_as T03F1.8"
Remark	"we used a C. elegans strain in which only uterine tissue, including the AC, is sensitive to RNAi. RNAi depletions targeting T03F1.8 gene, which showed transgene localization in the AC, blocked invasion. Because uterine cells do not contribute to AC invasion, an AC invasion defect in this background indicates that the gene functions in the AC."
Reference	"WBPaper00036215"


Anatomy_function : "WBbtf0426"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001652"
Gene	"WBGene00006796"
Not_involved	"WBbt:0007815"	Unnecessary
Remark	"ENTITY:WBbt:0004522(anchor cell)|PATO:0002103(infiltrating)|GO:0005604(basement membrane) QUALITY:PATO:0000468(reduced) NOT"
Remark	"Genotype \"rde-1(ne219); fos-1a>RDE-1;rrf-3(pk1426)\""
Remark	"Published_as unc-62"
Remark	"we used a C. elegans strain in which only uterine tissue, including the AC, is sensitive to RNAi. RNAi depletions targeting unc-62 gene, which were not expressed in the AC, showed normal invasion."
Reference	"WBPaper00036215"


Anatomy_function : "WBbtf0427"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001652"
Gene	"WBGene00001824"
Not_involved	"WBbt:0007815"	Unnecessary
Remark	"ENTITY:WBbt:0004522(anchor cell)|PATO:0002103(infiltrating)|GO:0005604(basement membrane) QUALITY:PATO:0000468(reduced) NOT"
Remark	"Genotype \"rde-1(ne219); fos-1a>RDE-1;rrf-3(pk1426)\""
Remark	"Published_as hbl-1"
Remark	"we used a C. elegans strain in which only uterine tissue, including the AC, is sensitive to RNAi. RNAi depletions targeting hbl-1 gene, which were not expressed in the AC, showed normal invasion."
Reference	"WBPaper00036215"


Anatomy_function : "WBbtf0428"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001225"	Autonomous
Gene	"WBGene00022473"
Involved	"WBbt:0008409"	Sufficient
Involved	"WBbt:0008409"	Necessary
Involved	"WBbt:0008409"	Remark
Remark	"ENTITY:WBbt:0008410(phasmid socket cell)|GO:0045165(cell fate commitment) QUALITY:PATO:0000468(reduced)"
Remark	"Genotype \"bet-1(os46); Ex[scm::bet-1::gfp]\""
Remark	"Published_as bet-1"
Remark	"To examine whether BET-1 functions cell-autonomously, we performed a mosaic analysis. Genetic mosaics were generated by the spontaneous loss of an extrachromosomal array containing scm::bet-1::gfp during embryogenesis in bet-1 mutants. When BET1::GFP was expressed in the T, but not the neighboring V6, lineage, the Psa phenotype was usually rescued, but expression in the V6, but not the T, lineage did not rescue it. Therefore, BET-1 functions cell-autonomously."
Reference	"WBPaper00036007"


Anatomy_function : "WBbtf0429"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000892"	Autonomous
Gene	"WBGene00000871"
Involved	"WBbt:0005784"	Necessary
Remark	"ENTITY:WBbt:0007849(hermaphrodite)|WBbt:0005784(germline)|GO:0008283(cell proliferation) QUALITY:PATO:0001997(reduced)"
Remark	"Published_as cye-1"
Remark	"we restricted cye-1 RNAi to the germline using rrf-1 mutants, which are defective for somatic but not germline RNAi; this mutant therefore permitted CYE-1 depletion in young larvae without affecting somatic divisions. However, cye-1 RNAi treatment initiated in rrf-1 first stage larvae (L1s) again resulted in typical distal germline defects."
Reference	"WBPaper00038281"


Anatomy_function : "WBbtf0430"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000892"	Autonomous
Gene	"WBGene00000871"
Involved	"WBbt:0005784"	Necessary
Remark	"ENTITY:WBbt:0007849(hermaphrodite)|WBbt:0005784(germline)|GO:0008283(cell proliferation) QUALITY:PATO:0001997(reduced)"
Remark	"Genotype \"cye-1(eh10); qIs134[cye-1(+) Psur-5::GFGP]\""
Remark	"Published_as cye-1"
Remark	"a genomic cye-1 transgene, qIs134, generated using a method predicted to allow expression in somatic cells but not germ cells. Consistent with that prediction, CYE-1 protein was detected in somatic but not germ cells of cye-1(0); qIs134 embryos and qIs134 rescued cye-1(0) somatic defects. However, germlines in these somatically rescued cye-1(0); qIs134 animals were smaller than normal, with abnormally enlarged distal germ cells, as seen previously in cye-1 null mutants."
Reference	"WBPaper00038281"


Anatomy_function : "WBbtf0431"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001765"
Gene	"WBGene00006525"
Involved	"WBbt:0005662"	Sufficient
Involved	"WBbt:0006825"	Sufficient
Involved	"WBbt:0005663"	Sufficient
Involved	"WBbt:0003927"	Sufficient
Involved	"WBbt:0004096"	Sufficient
Involved	"WBbt:0006846"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050919(negative chemotaxis)|CHEBI:16526(carbon dioxide) QUALITY:PATO:0001997(reduced) NOT"
Remark	"Expressing full-length tax-2 cDNA in the AFD, BAG, ASE, and AQR, PQR and URX neurons rescues CO2 avoidance in tax-2(p694) mutants."
Remark	"Genotype \"tax-2(p694); Ex[pgcy-8::tax-2 pflp-17::tax-2 pflp-6ASE-specific::tax-2 pgcy-32::tax-2]\""
Remark	"Published_as tax-2"
Reference	"WBPaper00038260"


Anatomy_function : "WBbtf0432"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0001765"
Involved	"WBbt:0005662"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050919(negative chemotaxis)|CHEBI:16526(carbon dioxide) QUALITY:PATO:0001997(reduced)"
Remark	"Genotype \"ttx-1(p767)\""
Remark	"Specification of the AFD neurons requires the otd/Otx homeodomain transcription factor ttx-1, which is expressed only in AFD. ttx-1 mutants had a strong CO2 avoidance defect off food, and a weaker defect on food."
Reference	"WBPaper00038260"


Anatomy_function : "WBbtf0433"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0001765"
Involved	"WBbt:0006825"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050919(negative chemotaxis)|CHEBI:16526(carbon dioxide) QUALITY:PATO:0001997(reduced)"
Remark	"Genotype \"ttx-1(p767); Ex[pgcy-33::egl-1]\""
Remark	"To ablate BAG we expressed the egl-1 programmed cell death activator from a BAG-specific gcy-33 promoter. Surprisingly, the CO2 avoidance of BAG-ablated animals was not significantly different from wild-type, both on and off food. We asked if combined genetic ablation of AFD and BAG causes a synthetic CO2 avoidance phenotype. Ablating the BAG neurons disrupted the residual CO2 avoidance of ttx-1(p767) mutants on food."
Reference	"WBPaper00038260"


Anatomy_function : "WBbtf0434"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000551"
Involved	"WBbt:0006825"	Necessary
Involved	"WBbt:0005662"	Necessary
Remark	"Coablation of AFD and BAG abolished the suppression of reversals and omega turns following a fall in CO2. These data suggest that together BAG and AFD act to suppress reversals and omega turns when CO2 decreases."
Remark	"ENTITY:WBbt:0007833(organism)|GO:0040011(locomotion)|GO:0035178(turning)|CHEBI:16526(carbon dioxide) QUALITY:PATO:0000460(abnormal)"
Remark	"Genotype \"ttx-1(p767); Ex[pgcy-33::egl-1]\""
Reference	"WBPaper00038260"


Anatomy_function : "WBbtf0435"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001983"
Gene	"WBGene00003807"
Involved	"WBbt:0006842"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0060756(foraging behavior)|GO:0035641(locomotory exploration behavior) QUALITY:PATO:0000470(increased) NOT"
Remark	"Genotype \"Ex[flp-21::LoxStopLox::npr-1(N2)]; Ex[ncs-1::nCre]\""
Remark	"Published_as npr-1"
Remark	"Specific transgenic expression of the N2 npr-1 allele in its essential site of action, the RMG motor neurons, sharply reduced the bacterial lawn leaving rate of HW (Hawaiin CB4856) animals"
Reference	"WBPaper00038234"


Anatomy_function : "WBbtf0436"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001983"
Gene	"WBGene00006475"
Involved	"WBbt:0005668"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0060756(foraging behavior)|GO:0035641(locomotory exploration behavior) QUALITY:PATO:0000470(increased) NOT"
Remark	"Genotype \"Ex[Psra-9::tyra-3b]\""
Remark	"Published_as tyra-3"
Remark	"expression of tyra-3 in ASK or BAG sensory neurons in worms of Hawaiin background significantly reduced leaving from bacterial lawn."
Reference	"WBPaper00038234"


Anatomy_function : "WBbtf0437"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001983"
Gene	"WBGene00006475"
Involved	"WBbt:0006825"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0060756(foraging behavior)|GO:0035641(locomotory exploration behavior) QUALITY:PATO:0000470(increased) NOT"
Remark	"Genotype \"Ex[Pflp-17::tyra-3b]\""
Remark	"Published_as tyra-3"
Remark	"expression of tyra-3 in ASK or BAG sensory neurons in worms of Hawaiin background significantly reduced leaving from bacterial lawn."
Reference	"WBPaper00038234"


Anatomy_function : "WBbtf0438"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001983"
Gene	"WBGene00006475"
Not_involved	"WBbt:0005244"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0060756(foraging behavior)|GO:0035641(locomotory exploration behavior) QUALITY:PATO:0000470(increased)"
Remark	"Genotype \"Ex[Pdat-1::tyra-3b]\""
Remark	"Published_as tyra-3"
Remark	"expression of tyra-3 in CEP or ADL sensory neurons in worms of Hawaiin background did not significantly reduce leaving from bacterial lawn."
Reference	"WBPaper00038234"


Anatomy_function : "WBbtf0439"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001983"
Gene	"WBGene00006475"
Not_involved	"WBbt:0005661"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0060756(foraging behavior)|GO:0035641(locomotory exploration behavior) QUALITY:PATO:0000470(increased)"
Remark	"Genotype \"Ex[Psri-51::tyra-3b]\""
Remark	"Published_as tyra-3"
Remark	"expression of tyra-3 in CEP or ADL sensory neurons in worms of Hawaiin background did not significantly reduce leaving from bacterial lawn."
Reference	"WBPaper00038234"


Anatomy_function : "WBbtf0440"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001983"
Involved	"WBbt:0005668"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0060756(foraging behavior)|GO:0035641(locomotory exploration behavior) QUALITY:PATO:0000470(increased) NOT"
Remark	"Killing the ASK neurons reduced the leaving rate of Hawaiin animals, indicating that ASK can promote leaving. The ablation resembled the effect of the ASK::tyra-3 transgene, suggesting that tyra-3 reduces ASK activity. In agreement with this idea, killing the ASK neurons in a strain with the N2 high-activity tyra-3 allele did not reduce their leaving rates further."
Reference	"WBPaper00038234"


Anatomy_function : "WBbtf0441"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001983"
Involved	"WBbt:0006825"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0060756(foraging behavior)|GO:0035641(locomotory exploration behavior) QUALITY:PATO:0001997(reduced) NOT"
Remark	"Killing the BAG neurons increased leaving rates in the strain with the N2 tyra-3 allele, demonstrating that BAG neurons prevent leaving. However, killing BAG had no effect in the strain with the Hawaiin tyra-3 allele, suggesting that BAG activity is already low in this strain under the assay conditions."
Reference	"WBPaper00038234"


Anatomy_function : "WBbtf0442"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001652"
Gene	"WBGene00003930"
Involved	"WBbt:0004522"	Necessary
Remark	"Blocking invasion in animals expressing a dominant negative form of the C. elegans integrin specifically in the anchor cell (zmp-1>HA-beta-tail; HA, haemagglutinin) also resulted in a failure to generate a basement membrane gap."
Remark	"ENTITY:WBbt:0004522(anchor cell)|WBbt:0007831(vulval cell)|GO:0005604(basement membrane)|GO:0022411(cellular component disassembly) QUALITY:PATO:0001997(reduced)"
Remark	"Genotype \"qyIs15[zmp-1>HA-beta-tail]\""
Remark	"Published_as pat-3"
Reference	"WBPaper00038447"


Anatomy_function : "WBbtf0443"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001652"
Involved	"WBbt:0004522"	Necessary
Remark	"ENTITY:WBbt:0004522(anchor cell)|WBbt:0007831(vulval cell)|GO:0005604(basement membrane)|GO:0022411(cellular component disassembly) QUALITY:PATO:0001997(reduced)"
Remark	"When the anchor cell was ablated just before invasion, the basement membrane remained completely intact through the L4 stage."
Reference	"WBPaper00038447"


Anatomy_function : "WBbtf0444"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001652"
Not_involved	"WBbt:0006781"	Unnecessary
Remark	"ENTITY:WBbt:0004522(anchor cell)|WBbt:0007831(vulval cell)|GO:0005604(basement membrane)|GO:0022411(cellular component disassembly) QUALITY:PATO:0000461(normal)"
Remark	"Removal of the dorsal uterine cells and their descendants did not alter the expansion or positioning of the basement membrane gap."
Reference	"WBPaper00038447"


Anatomy_function : "WBbtf0445"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001652"
Involved	"WBbt:0006780"	Necessary
Remark	"ENTITY:WBbt:0004522(anchor cell)|WBbt:0007831(vulval cell)|GO:0005604(basement membrane)|GO:0022411(cellular component disassembly) QUALITY:PATO:0000600(increased width)"
Remark	"laser ablation of the ventral uterine cells (at L2/L3 molt) perturbed gap formation. Surprisingly, this alteration resulted in basement membrane gap boundaries overexpanding in nearly 20% of operated animals. Thus, the ventral uterine cell descendants restrict basement membrane gap expansion."
Reference	"WBPaper00038447"


Anatomy_function : "WBbtf0446"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001652"
Involved	"WBbt:0008112"	Necessary
Involved	"WBbt:0008117"	Necessary
Involved	"WBbt:0008121"	Necessary
Involved	"WBbt:0008129"	Necessary
Involved	"WBbt:0008133"	Necessary
Remark	"ENTITY:WBbt:0004522(anchor cell)|WBbt:0007831(vulval cell)|GO:0005604(basement membrane)|GO:0022411(cellular component disassembly) QUALITY:PATO:0001997(reduced)"
Remark	"To further examine the role of the vulval cells in promoting basement membrane gap expansion, we reduced the number of VPCs by laser ablating all VPCs except the innermost P6.p descendants P6.pa and P6.pp, a treatment that does not interfere with anchor cell invasion and results in the isolated development of primary-fated vulF cells. This reduction of the number and invagination of VPCs decreased the expansion of the basement membrane gap."
Reference	"WBPaper00038447"


Anatomy_function : "WBbtf0447"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001652"
Gene	"WBGene00002081"
Not_involved	"WBbt:0004522"	Unnecessary
Not_involved	"WBbt:0006781"	Unnecessary
Not_involved	"WBbt:0006780"	Unnecessary
Remark	"ENTITY:WBbt:0004522(anchor cell)|WBbt:0007831(vulval cell)|GO:0005604(basement membrane)|GO:0022411(cellular component disassembly) QUALITY:PATO:0000461(normal)"
Remark	"Genotype \"qyIs103[fos-1a>RDE-1];rde-1(ne219);rrf-3(pk1426)\""
Remark	"Published_as ina-1"
Remark	"RNAi-targeted depletion of ina-1 in the uterine tissue (fos-1a>rde-1 strain) did not significantly alter basement membrane gap positioning."
Reference	"WBPaper00038447"


Anatomy_function : "WBbtf0448"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001652"
Gene	"WBGene00003929"
Not_involved	"WBbt:0004522"	Unnecessary
Not_involved	"WBbt:0006781"	Unnecessary
Not_involved	"WBbt:0006780"	Unnecessary
Remark	"ENTITY:WBbt:0004522(anchor cell)|WBbt:0007831(vulval cell)|GO:0005604(basement membrane)|GO:0022411(cellular component disassembly) QUALITY:PATO:0000461(normal)"
Remark	"Genotype \"qyIs103[fos-1a>RDE-1];rde-1(ne219);rrf-3(pk1426)\""
Remark	"Published_as pat-2"
Remark	"RNAi-targeted depletion of pat-2 in the uterine tissue (fos-1a>rde-1 strain) did not significantly alter basement membrane gap positioning."
Reference	"WBPaper00038447"


Anatomy_function : "WBbtf0449"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001652"
Gene	"WBGene00003930"
Not_involved	"WBbt:0004522"	Unnecessary
Not_involved	"WBbt:0006781"	Unnecessary
Not_involved	"WBbt:0006780"	Unnecessary
Remark	"ENTITY:WBbt:0004522(anchor cell)|WBbt:0007831(vulval cell)|GO:0005604(basement membrane)|GO:0022411(cellular component disassembly) QUALITY:PATO:0000461(normal)"
Remark	"Genotype \"qyIs103[fos-1a>RDE-1];rde-1(ne219);rrf-3(pk1426)\""
Remark	"Published_as pat-3"
Remark	"RNAi-targeted depletion of pat-3 in the uterine tissue (fos-1a>rde-1 strain) did not significantly alter basement membrane gap positioning."
Reference	"WBPaper00038447"


Anatomy_function : "WBbtf0450"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001652"
Gene	"WBGene00002081"
Involved	"WBbt:0007809"	Necessary
Remark	"ENTITY:WBbt:0004522(anchor cell)|WBbt:0007831(vulval cell)|GO:0005604(basement membrane)|GO:0022411(cellular component disassembly) QUALITY:PATO:0000600(increased width)"
Remark	"Genotype \"qyIs138[unc-62>RDE-1];rde-1(ne219);rrf-3(pk1426)\""
Remark	"Published_as ina-1"
Remark	"RNAi-targeted knockdown of ina-1 in the vulval tissue (unc-62>rde-1 strain), however, caused an basement membrane gap over expansion defect, similar to ina-1(gm39) mutants."
Reference	"WBPaper00038447"


Anatomy_function : "WBbtf0451"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001652"
Gene	"WBGene00003930"
Involved	"WBbt:0007809"	Necessary
Remark	"ENTITY:WBbt:0004522(anchor cell)|WBbt:0007831(vulval cell)|GO:0005604(basement membrane)|GO:0022411(cellular component disassembly) QUALITY:PATO:0000600(increased width)"
Remark	"Genotype \"qyIs138[unc-62>RDE-1];rde-1(ne219);rrf-3(pk1426)\""
Remark	"Published_as pat-3"
Remark	"RNAi-targeted knockdown of pat-3 in the vulval tissue (unc-62>rde-1 strain), however, caused an basement membrane gap over expansion defect, similar to ina-1(gm39) mutants."
Reference	"WBPaper00038447"


Anatomy_function : "WBbtf0452"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001652"
Gene	"WBGene00003929"
Not_involved	"WBbt:0007809"	Unnecessary
Remark	"ENTITY:WBbt:0004522(anchor cell)|WBbt:0007831(vulval cell)|GO:0005604(basement membrane)|GO:0022411(cellular component disassembly) QUALITY:PATO:0000461(normal)"
Remark	"Genotype \"qyIs138[unc-62>RDE-1];rde-1(ne219);rrf-3(pk1426)\""
Remark	"No defects in basement membrane gap formation were observed after RNAi depletion of pat-2 in the vulval tissue."
Remark	"Published_as pat-2"
Reference	"WBPaper00038447"


Anatomy_function : "WBbtf0453"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001652"
Gene	"WBGene00006882"
Involved	"WBbt:0007809"	Necessary
Remark	"ENTITY:WBbt:0004522(anchor cell)|WBbt:0007831(vulval cell)|GO:0005604(basement membrane)|GO:0022411(cellular component disassembly) QUALITY:PATO:0000600(increased width)"
Remark	"Genotype \"qyIs138[unc-62>RDE-1];rde-1(ne219);rrf-3(pk1426)\""
Remark	"Published_as vab-19"
Remark	"Similar to integrin function, vulval- and uterine-specific RNAi-mediated knockdown of vab-19 suggested that vab-19 functions within the vulval cells."
Reference	"WBPaper00038447"


Anatomy_function : "WBbtf0454"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001652"
Gene	"WBGene00006882"
Not_involved	"WBbt:0004522"	Unnecessary
Not_involved	"WBbt:0006780"	Unnecessary
Not_involved	"WBbt:0006781"	Unnecessary
Remark	"ENTITY:WBbt:0004522(anchor cell)|WBbt:0007831(vulval cell)|GO:0005604(basement membrane)|GO:0022411(cellular component disassembly) QUALITY:PATO:0000461(normal)"
Remark	"Genotype \"qyIs103[fos-1a>RDE-1];rde-1(ne219);rrf-3(pk1426)\""
Remark	"Published_as vab-19"
Remark	"Similar to integrin function, vulval- and uterine-specific RNAi-mediated knockdown of vab-19 suggested that vab-19 functions within the vulval cells."
Reference	"WBPaper00038447"


Anatomy_function : "WBbtf0455"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001661"	Autonomous
Gene	"WBGene00006831"
Involved	"WBbt:0005672"	Sufficient
Remark	"ENTITY:WBbt:0005672(AWC)|GO:0007368(left-right asymmetry)|GO:0001708(cell fate specification) QUALITY:PATO:0000461(normal)"
Remark	"Expression of unc-104 in AWC from the ord-3 promoter significatly rescued the enhancement of 2AWC-ON frequency from 91% to 39% in tir-1(ky388ts); unc-104(e1265) double mutants."
Remark	"Genotype \"tir-1(ky388ts); unc-104(e1265); odr-3p::unc-104\""
Remark	"Published_as unc-104"
Reference	"WBPaper00039901"


Anatomy_function : "WBbtf0456"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001661"	Autonomous
Gene	"WBGene00006831"
Involved	"WBbt:0005832"	Sufficient
Involved	"WBbt:0005832"	Necessary
Remark	"ENTITY:WBbt:0005832(AWC-ON)|GO:0001708(cell fate specification) QUALITY:PATO:0000380(increased frequency)"
Remark	"Genotype \"unc-104(e1265); Ex[unc-104p::unc-104 odr-1p::DsRed]\""
Remark	"Published_as unc-104"
Remark	"Spontaneous loss of the extrachromosomal array (unc-104p::unc-104) in one of the two AWC neurons resulted in mosaic animals in which one of the two AWC neurons expressed the transgene and therefore had unc-104 activity; this cell could be identified by expression of the DsRed marker. In the majority of these mosaic animals, the unc-104(+) AWC neuron became AWC-ON and the unc-104(-) AWC neuron became AWC-OFF."
Reference	"WBPaper00039901"


Anatomy_function : "WBbtf0457"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001661"	Nonautonomous
Gene	"WBGene00006831"
Involved	"WBbt:0005832"	Sufficient
Involved	"WBbt:0005832"	Necessary
Remark	"ENTITY:WBbt:0005833(AWC-OFF)|GO:0001708(cell fate specification) QUALITY:PATO:0000380(increased frequency)"
Remark	"Genotype \"unc-104(e1265); Ex[unc-104p::unc-104 odr-1p::DsRed]\""
Remark	"Published_as unc-104"
Remark	"Spontaneous loss of the extrachromosomal array (unc-104p::unc-104) in one of the two AWC neurons resulted in mosaic animals in which one of the two AWC neurons expressed the transgene and therefore had unc-104 activity; this cell could be identified by expression of the DsRed marker. In the majority of these mosaic animals, the unc-104(+) AWC neuron became AWC-ON and the unc-104(-) AWC neuron became AWC-OFF."
Reference	"WBPaper00039901"


Anatomy_function : "WBbtf0458"
Assay	"Blastomere_isolation"
Phenotype	"WBPhenotype:0000436"
Involved	"WBbt:0006876"	Sufficient
Remark	"ENTITY:WBbt:0006873(Psub2)|WP:CE24910(GPR-1)|GO:0008104(protein localization) QUALITY:PATO:0000628(ectopic)"
Remark	"We combined two pairs of P2-EMS cells expressing mCherry::GPR-1 in an antiparallel orientation and found that ectopic P2-EMS contacts (contacts between non-sister P2-EMS cells) and endogenous P2-EMS contacts (contacts between sister P2-EMS cells) recruited indistinguishable levels of protein."
Reference	"WBPaper00040172"


Anatomy_function : "WBbtf0459"
Assay	"Blastomere_isolation"
Phenotype	"WBPhenotype:0000436"
Gene	"WBGene00003219"
Involved	"WBbt:0006876"	Necessary
Remark	"ENTITY:WBbt:0006873(Psub2)|WP:CE24910(GPR-1)|GO:0008104(protein localization) QUALITY:PATO:0000628(ectopic) NOT"
Remark	"Genotype \"mes-1(bn7)\""
Remark	"Published_as mes-1"
Remark	"the ectopic P2-EMS contacts can recruit GPR-1 as endogenous P2-EMS contacts do, and hence that cell-cell contact can enrich GPR-1 at a cortical site. This appears to depend on MES-1 signaling specifically at the P2-EMS contact, as control recombinations between P2-EMS pairs and the other two cells of the four-cell stage - ABa and ABp - referred to as ABx here, and contacts with P2-EMS pairs that lack MES-1 failed to accumulate similar levels of mCherry::GPR-1."
Reference	"WBPaper00040172"


Anatomy_function : "WBbtf0460"
Assay	"Blastomere_isolation"
Phenotype	"WBPhenotype:0000760"
Involved	"WBbt:0006876"	Sufficient
Remark	"ENTITY:WBbt:0006873(Psub2)|GO:0000132(mitotic spindle orientation) QUALITY:PATO:0000628(ectopic)"
Remark	"We combined two pairs of P2-EMS cells in an antiparallel orientation and noticed that spindle orientation in P2 depended on specific cell contacts."
Reference	"WBPaper00040172"


Anatomy_function : "WBbtf0461"
Assay	"Blastomere_isolation"
Phenotype	"WBPhenotype:0000760"
Gene	"WBGene00003219"
Involved	"WBbt:0006876"	Necessary
Remark	"ENTITY:WBbt:0006873(Psub2)|GO:0000132(mitotic spindle orientation) QUALITY:PATO:0000628(ectopic) NOT"
Remark	"Genotype \"mes-1(bn7)\""
Remark	"Published_as mes-1"
Remark	"We combined two pairs of P2-EMS cells in an antiparallel orientation and noticed that spindle orientation in P2 depended on specific cell contacts and MES-1."
Reference	"WBPaper00040172"


Anatomy_function : "WBbtf0462"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000743"	Autonomous
Gene	"WBGene00004323"
Involved	"WBbt:0006804"	Sufficient
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|GO:0016246(RNA interference) QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"pmyo-2::hp-gfp; rde-1(-); pmyo-3::rde-1(+)\""
Remark	"Published_as rde-1"
Remark	"in rde-1(-) mutant animals, expression of dsRNA in the pharynx that targets gfp, silenced gfp gene expression in anterior body-wall muscle cells only when gfp and rde-1(+) were coexpressed in body-wall muscle cells."
Reference	"WBPaper00040276"


Anatomy_function : "WBbtf0463"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000743"	Nonautonomous
Gene	"WBGene00004326"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|GO:0016246(RNA interference) QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"Prgef-1::unc-22ds; rde-4(-); Prgef-1::rde-1(+)\""
Remark	"Published_as rde-4"
Remark	"We rescued RNAi pathway mutants only in neurons of animals that contain the neur::u22ds transgene and measured silencing of the target gene unc-22 in mutant muscle cells. We detected unc-22 silencing in rde-4(−) animals that expressed rde-4(+) in neurons. Consistent with silencing due to mobile RNAs, SID-1 was required for the observed silencing."
Reference	"WBPaper00040276"


Anatomy_function : "WBbtf0464"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000743"	Nonautonomous
Gene	"WBGene00003499"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|GO:0016246(RNA interference) QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"Prgef-1::unc-22ds; mut-2(-); Prgef-1::mut-2(+)\""
Remark	"Published_as mut-2"
Remark	"We rescued RNAi pathway mutants only in neurons of animals that contain the neur::u22ds transgene and measured silencing of the target gene unc-22 in mutant muscle cells. We detected unc-22 silencing in mut-2(−) animals that expressed mut-2(+) in neurons, and this silencing was due to mobile RNA because it required SID-1."
Reference	"WBPaper00040276"


Anatomy_function : "WBbtf0465"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000743"	Nonautonomous
Gene	"WBGene00004326"
Involved	"WBbt:0006804"	Sufficient
Remark	"ENTITY:WBbt:0005792(intestinal cell)|GO:0016246(RNA interference) QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"sur-5::gfp; rde-4(-); Pmyo-3::rde-4(+)\""
Remark	"Published_as rde-4"
Remark	"We generated rde-4(&minus;); sur-5::gfp animals and moved a representative transgene that expresses rde-4 in bwm cells (bwm::rde-4(+)) into these animals. Significant silencing (P < 0.05) was detected in tissues other than muscle in the resultant mosaic animals and was most easily observed in the prominent gut nuclei. Consistent with silencing due to mobile RNAs, SID-1 was required for the observed silencing of gut nuclei."
Reference	"WBPaper00040276"


Anatomy_function : "WBbtf0466"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000743"	Nonautonomous
Gene	"WBGene00003499"
Involved	"WBbt:0006804"	Sufficient
Remark	"ENTITY:WBbt:0005792(intestinal cell)|GO:0016246(RNA interference) QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"sur-5::gfp; mut-2(-); Pmyo-3::mut-2(+)\""
Remark	"Moving a representative transgene that expressed mut-2(+) in bwm cells (bwm::mut-2(+)) into mut-2(&minus;); sur-5::gfp animals resulted in the silencing of GFP expression in the gut. The observed silencing was dependent on SID-1, showing that mobile RNA triggered the silencing in mut-2(&minus;) gut cells."
Remark	"Published_as mut-2"
Reference	"WBPaper00040276"


Anatomy_function : "WBbtf0467"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000540"	Nonautonomous
Gene	"WBGene00009958"
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|GO:0042995(cell projection)|GO:0006935(chemotaxis) QUALITY:PATO:0000628(ectopic)"
Remark	"Genotype \"madd-4(tr185); Ex[ceh-23::MADD-4]\""
Remark	"Published_as madd-4"
Reference	"WBPaper00040335"


Anatomy_function : "WBbtf0468"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000572"	Autonomous
Gene	"WBGene00000913"
Involved	"WBbt:0005413"	Sufficient
Involved	"WBbt:0005413"	Necessary
Remark	"ENTITY:WBbt:0005413(AIY)|GO:0043005(neurite)|GO:0031175(neurite outgrowth) QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"daf-18(mg198); Ex[pdaf-18:: daf-18 cDNA]\""
Remark	"Published_as daf-18"
Remark	"We analyzed daf-18(mg198) mosaic animals retaining the rescuing array in a subset of cells. We observed that mosaic animals retaining the array in AIY were rescued, whereas animals that did not retain the array in AIY, but retained it in other cells, such as postsynaptic partner RIA, were not rescued for the neurite length phenotype in AIY (P<0.001). These mosaic data suggest that DAF-18 acts cell-autonomously in AIY."
Reference	"WBPaper00040402"


Anatomy_function : "WBbtf0469"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000572"	Autonomous
Gene	"WBGene00000913"
Involved	"WBbt:0005413"	Necessary
Remark	"ENTITY:WBbt:0005413(AIY)|GO:0043005(neurite)|GO:0031175(neurite outgrowth) QUALITY:PATO:0001997(reduced)"
Remark	"Genotype \"daf-18(mg198); Ex[pdaf-18:: daf-18 cDNA]\""
Remark	"Published_as daf-18"
Remark	"We analyzed daf-18(mg198) mosaic animals retaining the rescuing array in a subset of cells. We observed that mosaic animals retaining the array in AIY were rescued, whereas animals that did not retain the array in AIY, but retained it in other cells, such as postsynaptic partner RIA, were not rescued for the neurite length phenotype in AIY (P<0.001). These mosaic data suggest that DAF-18 acts cell-autonomously in AIY."
Reference	"WBPaper00040402"


Anatomy_function : "WBbtf0470"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000572"	Autonomous
Gene	"WBGene00000913"
Involved	"WBbt:0005413"	Sufficient
Remark	"ENTITY:WBbt:0005413(AIY)|GO:0043005(neurite)|GO:0031175(neurite outgrowth) QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"daf-18(mg198); Ex[pttx-3g:: daf-18]\""
Remark	"Published_as daf-18"
Remark	"To examine further the role of DAF-18 in AIY, we generated transgenic animals that expressed a daf-18 cDNA from the AIY-specific promoter ttx-3g. When we examined daf-18(mg198) animals expressing this construct, we observed that they were rescued for the neurite length defect in AIY. These results indicate that expression of DAF-18 specifically in AIY is sufficient to rescue the neurite length defects seen in daf18(mg198) mutants."
Reference	"WBPaper00040402"


Anatomy_function : "WBbtf0471"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000572"	Autonomous
Gene	"WBGene00000912"
Involved	"WBbt:0005413"	Sufficient
Remark	"ENTITY:WBbt:0005413(AIY)|GO:0043005(neurite)|GO:0031175(neurite outgrowth) QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"daf-16(mgDf47); Ex[R13H8 daf-16AB(+)]\""
Remark	"Published_as daf-16"
Remark	"We then examined whether DAF-16B acted cell-autonomously to rescue AIY neurite outgrowth. To achieve this, we conducted mosaic analysis using cosmid R13H8 (which contains the complete A and B DAF-16 isoforms, but not D or F isoforms) in daf16(mgDF47) mutant animals. Examination of mosaic animals revealed that animals retaining the array in AIY were rescued for the neurite outgrowth phenotype. Conversely, animals that did not retain the array in AIY, but retained it in other cells, were not rescued for the neurite outgrowth phenotype in AIY."
Reference	"WBPaper00040402"


Anatomy_function : "WBbtf0472"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000572"	Autonomous
Gene	"WBGene00000912"
Involved	"WBbt:0005413"	Necessary
Remark	"ENTITY:WBbt:0005413(AIY)|GO:0043005(neurite)|GO:0031175(neurite outgrowth) QUALITY:PATO:0001997(reduced)"
Remark	"Genotype \"daf-16(mgDf47); Ex[R13H8 daf-16AB(+)]\""
Remark	"Published_as daf-16"
Remark	"We then examined whether DAF-16B acted cell-autonomously to rescue AIY neurite outgrowth. To achieve this, we conducted mosaic analysis using cosmid R13H8 (which contains the complete A and B DAF-16 isoforms, but not D or F isoforms) in daf16(mgDF47) mutant animals. Examination of mosaic animals revealed that animals retaining the array in AIY were rescued for the neurite outgrowth phenotype. Conversely, animals that did not retain the array in AIY, but retained it in other cells, were not rescued for the neurite outgrowth phenotype in AIY."
Reference	"WBPaper00040402"


Anatomy_function : "WBbtf0473"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001512"	Autonomous
Gene	"WBGene00001883"
Involved	"WBbt:0006636"	Sufficient
Involved	"WBbt:0006636"	Necessary
Remark	"ENTITY:WBbt:0008407(ABaraappaaa)|GO:0001708(cell fate specification)|GO:0009855(determination of bilateral asymmetry)|WBbt:0003664(MI)|WBbt:0003701(e1D)"
Remark	"QUALITY:PATO:0001507(interrupted)"
Remark	"Genotype \"Ex[his-9(H113D) sur-5::gfp unc-119::gfp]\""
Remark	"Published_as his-9"
Remark	"We generated animals carrying an extrachromosomal array containing the his-9(H113D) transgene marked with cell-autonomous gfp reporters sur-5::gfp and unc-119::gfp. We observed that none of the 45 animals in which the array loss had occurred at or prior to the division of ABaraapp showed MI transformation. By contrast, of 686 animals in which the his-9(H113D) array was present in the postmitotic ABaraappaaa cell, 293 animals (43%) displayed MI transformation, suggesting that his-9 gain-of-function activity acts cell-autonomously to cause MI transformation. In addition, we identified 38 animals in which the array had been lost at the cell division of either ABaraappa or ABaraappaa. Three of these thirty-eight animals (3%) showed MI transformation. This low fraction of MI transformation compared to that of the animals in which the array was present in the postmitotic ABaraappaaa cell (43%) likely reflects two groups among the 38 animals, one in which the array had been lost at the ABaraappa division and another in which the array loss had occurred at the ABaraappaa division. Together these observations suggest that the presence of the his-9(H113D) transgene in ABaraappaa, the MI mother cell, is sufficient to cause MI transformation. We concluded that his-9 gain-of-function activity cell-autonomously acts in the MI mother cell to cause MI transformation."
Reference	"WBPaper00040574"


Anatomy_function : "WBbtf0474"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000127"
Gene	"WBGene00001996"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBls:0000032(dauer larva)|GO:0043054(dauer exit)"
Remark	"QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"hpl-2(tm1489); daf-2(e1370); Ex[Prab-3::hpl-2]\""
Remark	"Published_as hpl-2"
Remark	"To establish in which tissue HPL-2 acts to influence dauer development, we carried out tissue-specific rescue experiments on hpl-2;daf-2(e1370) animals raised at 22&deg;C. While at this temperature all daf-2 animals reenter the reproductive cycle after 7 days, less than 1% of the double hpl-2;daf-2 mutants ever exit the dauer stage. Expression of hpl-2 under the control of the pan neuronal rab-3 promoter allowed more than 30% of hpl-2;daf-2(e1370) mutant animals to exit the dauer stage."
Reference	"WBPaper00040560"


Anatomy_function : "WBbtf0475"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000127"
Gene	"WBGene00001996"
Involved	"WBbt:0005792"	Sufficient
Remark	"ENTITY:WBls:0000032(dauer larva)|GO:0043054(dauer exit)"
Remark	"QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"hpl-2(tm1489); daf-2(e1370); Ex[Pges-1::hpl-2]\""
Remark	"Published_as hpl-2"
Remark	"To establish in which tissue HPL-2 acts to influence dauer development, we carried out tissue-specific rescue experiments on hpl-2;daf-2(e1370) animals raised at 22&deg;C. While at this temperature all daf-2 animals reenter the reproductive cycle after 7 days, less than 1% of the double hpl-2;daf-2 mutants ever exit the dauer stage. Expression of hpl-2 under the control of the intestinal ges-1 promoter allowed more than 30% of hpl-2;daf-2(e1370) mutant animals to exit the dauer stage."
Reference	"WBPaper00040560"


Anatomy_function : "WBbtf0476"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000127"
Gene	"WBGene00001996"
Not_involved	"WBbt:0007809"	Insufficient
Remark	"ENTITY:WBls:0000032(dauer larva)|GO:0043054(dauer exit)"
Remark	"QUALITY:PATO:0001997(reduced)"
Remark	"Genotype \"hpl-2(tm1489); daf-2(e1370); Ex[Plin-31::hpl-2]\""
Remark	"Published_as hpl-2"
Remark	"To establish in which tissue HPL-2 acts to influence dauer development, we carried out tissue-specific rescue experiments on hpl-2;daf-2(e1370) animals raised at 22&deg;C. While at this temperature all daf-2 animals reenter the reproductive cycle after 7 days, less than 1% of the double hpl-2;daf-2 mutants ever exit the dauer stage. Expression of hpl-2 under the control of the lin-31 promoter, which is expressed in vulval precursor cells, failed to promote rescue."
Reference	"WBPaper00040560"


Anatomy_function : "WBbtf0477"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000724"	Autonomous
Gene	"WBGene00000241"
Involved	"WBbt:0005661"	Sufficient
Involved	"WBbt:0005665"	Sufficient
Involved	"WBbt:0005670"	Sufficient
Involved	"WBbt:0005660"	Sufficient
Involved	"WBbt:0006753"	Sufficient
Remark	"ENTITY:WBbt:0005661(ADL)|GO:0046903(secretion)|WP:CE25720(DAF-28)|GO:0005159(insulin-like growth factor)"
Remark	"QUALITY:PATO:0001589(enhanced) NOT"
Remark	"Expression of bbs-1 under the promoter of ocr-2, which drives expression in ADL in addition to a few other sensory neurons, abrogated the enhanced secretion of bbs-1 mutant animals (assayed by ADL-expressed, tagged insulin accumulation in coelomocytes)."
Remark	"Genotype \"bbs-1(ok1111); Ex[Psrh-220::DAF-28::mCherry]; Ex[Pocr-2::bbs-1]\""
Remark	"Published_as bbs-1"
Reference	"WBPaper00040543"


Anatomy_function : "WBbtf0478"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000724"	Autonomous
Gene	"WBGene00000241"
Not_involved	"WBbt:0005672"	Insufficient
Not_involved	"WBbt:0005666"	Insufficient
Not_involved	"WBbt:0005662"	Insufficient
Not_involved	"WBbt:0005664"	Insufficient
Not_involved	"WBbt:0005667"	Insufficient
Not_involved	"WBbt:0005668"	Insufficient
Not_involved	"WBbt:0006825"	Insufficient
Not_involved	"WBbt:0006846"	Insufficient
Not_involved	"WBbt:0005663"	Insufficient
Remark	"By contrast, use of the tax-4 promoter to drive expression in numerous sensory neurons excluding ADL had no effect on the secretion phenotype of bbs-1 mutants (assayed by ADL-expressed, tagged insulin accumulation in coelomocytes)."
Remark	"ENTITY:WBbt:0005661(ADL)|GO:0046903(secretion)|WP:CE25720(DAF-28)|GO:0005159(insulin-like growth factor)"
Remark	"QUALITY:PATO:0001589(enhanced)"
Remark	"Genotype \"bbs-1(ok1111); Ex[Psrh-220::DAF-28::mCherry]; Ex[Ptax-4::bbs-1]\""
Remark	"Published_as bbs-1"
Reference	"WBPaper00040543"


Anatomy_function : "WBbtf0479"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000724"	Autonomous
Gene	"WBGene00000241"
Involved	"WBbt:0005661"	Sufficient
Remark	"ENTITY:WBbt:0005661(ADL)|GO:0046903(secretion)|WP:CE25720(DAF-28)|GO:0005159(insulin-like growth factor)"
Remark	"QUALITY:PATO:0001589(enhanced) NOT"
Remark	"Expression exclusively in ADL neurons (with srh-220 promoter) showed partial but highly significant reduction in the enhanced insulin secretion of bbs-1 mutants (assayed by ADL-expressed, tagged insulin accumulation in coelomocytes), suggesting that the BBSome regulates secretion at least partially cell autonomously."
Remark	"Genotype \"bbs-1(ok1111); [Psrh-220::DAF-28::mCherry]; Ex[Psrh-220::bbs-1]\""
Remark	"Published_as bbs-1"
Reference	"WBPaper00040543"


Anatomy_function : "WBbtf0480"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000724"	Autonomous
Gene	"WBGene00003892"
Involved	"WBbt:0005661"	Sufficient
Remark	"ENTITY:WBbt:0005661(ADL)|GO:0046903(secretion)|WP:CE25720(DAF-28)|GO:0005159(insulin-like growth factor)"
Remark	"QUALITY:PATO:0001589(enhanced) NOT"
Remark	"Genotype \"bbs-7(n1606); [Psrh-220::DAF-28::mCherry]; Ex[Psrh-220::bbs-7]\""
Remark	"Published_as bbs-7"
Remark	"When a functional bbs-7 cDNA was expressed in a bbs-7 mutant: two independently generated transgenic lines showed partial but highly significant reductions of the enhanced insulin secretion (assayed by ADL-expressed, tagged insulin accumulation in coelomocytes) of bbs-7 mutants when expressed exclusively in ADL."
Reference	"WBPaper00040543"


Anatomy_function : "WBbtf0481"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001996"	Autonomous
Gene	"WBGene00000870"
Involved	"WBbt:0005792"	Sufficient
Remark	"ENTITY:WBls:0000024(L1 larva)|WBbt:0005792(intestinal cell)|GO:0070314(cell cycle quiescence)"
Remark	"QUALITY:PATO:0001997(reduced)"
Remark	"Expression of cyd-1/cdk-4 combination from the intestine-specific elt-2 promoter prevented the normal cell cycle arrest in the intestine of late embryonic and starved L1 animals. Expression of CYD-1 alone was sufficient to trigger nuclear division and DNA replication, whereas CDK expression alone did not induce an apparent cell cycle response."
Remark	"Genotype \"heEx346[Pelt-2::CYD-1; Pelt-2::CDK-4::Venus; Pmyo-2::TdTomato]\""
Remark	"Published_as cyd-1"
Reference	"WBPaper00040426"


Anatomy_function : "WBbtf0482"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001996"	Autonomous
Gene	"WBGene00000871"
Involved	"WBbt:0005792"	Sufficient
Remark	"ENTITY:WBls:0000024(L1 larva)|WBbt:0005792(intestinal cell)|GO:0070314(cell cycle quiescence)"
Remark	"QUALITY:PATO:0001997(reduced)"
Remark	"Expression of cye-1/cdk-2 combination from the intestine-specific elt-2 promoter prevented the normal cell cycle arrest in the intestine of late embryonic and starved L1 animals. Expression of CYE-1 alone was sufficient to trigger nuclear division and DNA replication, whereas CDK expression alone did not induce an apparent cell cycle response."
Remark	"Genotype \"heEx288[Pelt-2::CYE-1; Pelt-2::CDK-2AF::Venus;Pmyo-2::GFP]\""
Remark	"Published_as cye-1"
Reference	"WBPaper00040426"


Anatomy_function : "WBbtf0483"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000806"	Autonomous
Gene	"WBGene00003915"
Involved	"WBbt:0005784"	Necessary
Remark	"ENTITY:WBls:0000057(adult hermaphrodite)|WBbt:0005784(germline)|GO:0007281(germ cell development)"
Remark	"QUALITY:PATO:0000460(defective)"
Remark	"Genotype \"rrf-1(pk1417)\""
Remark	"Published_as pan-1"
Remark	"germline-specific RNAi (using rrf-1 mutant worms) of pan-1 resulted in sterile F1 progeny that have empty gonads or gonads with abnormal oocytes."
Reference	"WBPaper00040830"


Anatomy_function : "WBbtf0484"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000638"
Gene	"WBGene00003915"
Not_involved	"WBbt:0005784"	Unnecessary
Remark	"ENTITY:WBls:0000023(larva)|WBbt:0005755(cuticle)|GO:0042303(molting cycle)"
Remark	"QUALITY:PATO:0000460(defective) NOT"
Remark	"Genotype \"rrf-1(pk1417)\""
Remark	"Published_as pan-1"
Remark	"germline-specific RNAi (using rrf-1 mutant worms) of pan-1 resulted in sterile F1 progeny that bypassed larval arrest (molting defects)."
Reference	"WBPaper00040830"


Anatomy_function : "WBbtf0485"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000625"	Autonomous
Gene	"WBGene00019347"
Involved	"WBbt:0005278"	Sufficient
Remark	"ENTITY:WBbt:0004857(DA9)|GO:0048786(presynaptic active zone)|GO:0007528(neuromuscular junction development)"
Remark	"QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"mbl-1(tm1563); Ex[Punc-4c::mbl-1]\""
Remark	"Published_as mbl-1"
Remark	"We expressed a genomic fragment including most of the mbl-1 ORF under the control of promoters that express in neurons including DA9, and scored rescue of the DA9 synaptic phenotype in mbl-1(tm1563) mutant animals. Punc-4c, a truncated version of the unc-4 promoter, drives expression in only the DA-type motorneurons. Expression of the mbl-1 genomic fragment under the control of the unc-4c promoter rescues the DA9 synaptic defect,"
Reference	"WBPaper00040749"


Anatomy_function : "WBbtf0486"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000625"	Autonomous
Gene	"WBGene00019347"
Involved	"WBbt:0004857"	Sufficient
Involved	"WBbt:0004645"	Sufficient
Remark	"ENTITY:WBbt:0004857(DA9)|GO:0048786(presynaptic active zone)|GO:0007528(neuromuscular junction development)"
Remark	"QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"mbl-1(tm1563); Ex[Pmig-13::mbl-1]\""
Remark	"Published_as mbl-1"
Remark	"We expressed a genomic fragment including most of the mbl-1 ORF under the control of promoters that express in neurons including DA9, and scored rescue of the DA9 synaptic phenotype in mbl-1(tm1563) mutant animals. The mig-13 promoter is expressed in DA9, VA12 and other anterior DA neurons and is expressed beginning at embryonic stages. When we used Pmig-13 to drive expression of the mbl-1 genomic fragment, we found that it also significantly restores the correct number of synapses to the dorsal axon in DA9."
Reference	"WBPaper00040749"


Anatomy_function : "WBbtf0487"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000625"
Gene	"WBGene00019347"
Not_involved	"WBbt:0006804"	Insufficient
Remark	"ENTITY:WBbt:0004857(DA9)|GO:0048786(presynaptic active zone)|GO:0007528(neuromuscular junction development)"
Remark	"QUALITY:PATO:0001997(reduced)"
Remark	"Genotype \"mbl-1(tm1563); Ex[Phlh-1::mbl-1]\""
Remark	"Published_as mbl-1"
Remark	"We expressed a genomic fragment including most of the mbl-1 ORF under the control of promoters that express in body wall muscles (Phlh-1) and scored rescue of the DA9 synaptic phenotype in mbl-1(tm1563) mutant animals. Expression of mbl-1 in muscle failed to rescue the DA9 synaptic defect."
Reference	"WBPaper00040749"


Anatomy_function : "WBbtf0488"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000625"
Gene	"WBGene00019347"
Involved	"WBbt:0004857"	Sufficient
Involved	"WBbt:0004645"	Sufficient
Remark	"ENTITY:WBbt:0004857(DA9)|GO:0048786(presynaptic active zone)"
Remark	"QUALITY:PATO:0000628(ectopic) NOT"
Remark	"Expression of the mbl-1 genomic fragment under the control of the Pmig-13 promoters can rescue or partially rescue the appearance of ectopic dendritic puncta in mbl-1(tm1563)."
Remark	"Genotype \"mbl-1(tm1563); Ex[Pmig-13::mbl-1]\""
Remark	"Published_as mbl-1"
Reference	"WBPaper00040749"


Anatomy_function : "WBbtf0489"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000625"
Gene	"WBGene00019347"
Involved	"WBbt:0005278"	Sufficient
Remark	"ENTITY:WBbt:0004857(DA9)|GO:0048786(presynaptic active zone)"
Remark	"QUALITY:PATO:0000628(ectopic) NOT"
Remark	"Expression of the mbl-1 genomic fragment under the control of the Pmig-13 promoters can rescue or partially rescue the appearance of ectopic dendritic puncta in mbl-1(tm1563)."
Remark	"Genotype \"mbl-1(tm1563); Ex[Punc-4c::mbl-1]\""
Remark	"Published_as mbl-1"
Reference	"WBPaper00040749"


Anatomy_function : "WBbtf0490"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000615"
Gene	"WBGene00001130"
Involved	"WBbt:0005671"	Necessary
Involved	"WBbt:0005665"	Necessary
Remark	"ENTITY:WBbt:0005671(AWB)|GO:0060170(cilium membrane)"
Remark	"QUALITY:PATO:0001602(expanded)"
Remark	"Genotype \"sru-38p::dyn-1(RNAi)\""
Remark	"Knock-down of dyn-1 function using cell-specific RNAi (sru-38p::dyn-1RNAi) caused abnormal cilium morphology in AWB."
Remark	"Published_as dyn-1"
Reference	"WBPaper00040829"


Anatomy_function : "WBbtf0491"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000615"
Gene	"WBGene00004268"
Involved	"WBbt:0005671"	Necessary
Involved	"WBbt:0005665"	Necessary
Remark	"ENTITY:WBbt:0005671(AWB)|GO:0060170(cilium membrane)"
Remark	"QUALITY:PATO:0001602(expanded)"
Remark	"Genotype \"sru-38p::rab-5(RNAi)\""
Remark	"Knock-down of rab-5 function using cell-specific RNAi (sru-38p::rab-5 RNAi) caused abnormal cilium morphology in AWB."
Remark	"Published_as rab-5"
Reference	"WBPaper00040829"


Anatomy_function : "WBbtf0492"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000059"
Gene	"WBGene00025707"
Not_involved	"WBbt:0005784"	Unnecessary
Remark	"C. briggsae Cbr-puf-2(nm66) mutant animals arrest at an early larval stage. But nm66 homozygote animals that carry a wild-type Cbr-puf-2 transgene (CP113) develop into fertile adults. Since germline transgene silencing is a known phenomenon in C. elegans, CP113 was probably a somatic-rescued but germline-null Cbr-puf-2 mutant."
Remark	"ENTITY:NCBITaxon:6238(C. briggsae)|WBls:0000023(larva)|GO:0040007(growth)"
Remark	"QUALITY:PATO:0000297(arrested) NOT"
Remark	"Genotype \"Cbr-unc-119(nm67); Cbr-puf-2(nm66); Is[Cbr-unc119(+) Cbr-puf-2(+)]\""
Remark	"Published_as Cbr-puf-2"
Reference	"WBPaper00040859"


Anatomy_function : "WBbtf0493"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000102"	Autonomous
Gene	"WBGene00003243"
Involved	"WBbt:0005413"	Sufficient
Remark	"ENTITY:WBbt:0005413(AIY)|GO:0008021(synaptic vesicle)|GO:0097091(synaptic vesicle clustering)"
Remark	"QUALITY:PATO:0001997(reduced) NOT"
Remark	"Expression of this rescuing fosmid in mig-10(ct41) mutant animals resulted in robust rescue of the AIY synaptic vesicle clustering defect (Fig. 4 H). To examine where MIG-10 functions to direct AIY synaptic vesicle clustering, we took advantage of the mitotic instability of the transgene arrays and analyzed mig-10(ct41) mosaic animals retaining the rescuing fosmid array in subsets of cells (Fig. 4 H; Yochem and Herman, 2003). We observed that mosaic animals retaining the array in AIY were rescued for the AIY presynaptic defect, whereas animals that did not retain the array in AIY, but retained it in other cells, such as postsynaptic partner RIA, did not show any detectable rescue of the AIY presynaptic defect (Fig. 4 H)."
Remark	"Genotype \"mig-10(ct41); Ex[mig-10(+) Pttx-3::rfp Pglr-3::rfp]\""
Remark	"Published_as mig-10"
Reference	"WBPaper00041162"


Anatomy_function : "WBbtf0494"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000102"	Autonomous
Gene	"WBGene00003243"
Not_involved	"WBbt:0006833"	Insufficient
Remark	"ENTITY:WBbt:0005413(AIY)|GO:0008021(synaptic vesicle)|GO:0097091(synaptic vesicle clustering)"
Remark	"QUALITY:PATO:0001997(reduced)"
Remark	"Expression of this rescuing fosmid in mig-10(ct41) mutant animals resulted in robust rescue of the AIY synaptic vesicle clustering defect (Fig. 4 H). To examine where MIG-10 functions to direct AIY synaptic vesicle clustering, we took advantage of the mitotic instability of the transgene arrays and analyzed mig-10(ct41) mosaic animals retaining the rescuing fosmid array in subsets of cells (Fig. 4 H; Yochem and Herman, 2003). We observed that mosaic animals retaining the array in AIY were rescued for the AIY presynaptic defect, whereas animals that did not retain the array in AIY, but retained it in other cells, such as postsynaptic partner RIA, did not show any detectable rescue of the AIY presynaptic defect (Fig. 4 H)."
Remark	"Genotype \"mig-10(ct41); Ex[mig-10(+) Pttx-3::rfp Pglr-3::rfp]\""
Remark	"Published_as mig-10"
Reference	"WBPaper00041162"


Anatomy_function : "WBbtf0495"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000102"	Autonomous
Gene	"WBGene00006776"
Involved	"WBbt:0005413"	Sufficient
Remark	"ENTITY:WBbt:0005413(AIY)|GO:0008021(synaptic vesicle)|GO:0097091(synaptic vesicle clustering)"
Remark	"QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"unc-40(e271); wyEx800 [Pttx-3::mCherry Pglr-3::mCherry Punc-40::unc-40]\""
Remark	"Published_as unc-40"
Remark	"To identify the cell(s) in which unc-40 functions to direct AIY-RIA innervation, we analyzed unc-40 mosaic animals that retain an unstable rescuing array in subsets of cells (8). Interestingly, only when the array was retained in the AIY interneuron did we observe significant rescue of the AIY presynaptic patterning defects. Retention in the RIA interneuron resulted in rescue of the RIA axon guidance defect but not of the AIY presynaptic phenotype (reduction of a synaptic vesicle marker mCherry::RAB-3, in zone 2)."
Reference	"WBPaper00031068"


Anatomy_function : "WBbtf0496"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000102"	Autonomous
Gene	"WBGene00006776"
Involved	"WBbt:0005413"	Sufficient
Remark	"ENTITY:WBbt:0005413(AIY)|GO:0008021(synaptic vesicle)|GO:0097091(synaptic vesicle clustering)"
Remark	"QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"unc-40(n324);wyEx1474[Pttx-3::mCherry, Pcex-1::mCherry, Punc-40::unc-40]\""
Remark	"Published_as unc-40"
Remark	"To identify the cell(s) in which unc-40 functions to direct AIY-RIA innervation, we analyzed unc-40 mosaic animals that retain an unstable rescuing array in subsets of cells (8). Interestingly, only when the array was retained in the AIY interneuron did we observe significant rescue of the AIY presynaptic patterning defects. Retention of the array in the closely related interneuron RIB or RIM (RIB/RIM) did not result in rescue (reduction of a synaptic vesicle marker mCherry::RAB-3, in zone 2)."
Reference	"WBPaper00031068"


Anatomy_function : "WBbtf0497"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000102"	Autonomous
Gene	"WBGene00006776"
Not_involved	"WBbt:0006833"	Insufficient
Remark	"ENTITY:WBbt:0005413(AIY)|GO:0008021(synaptic vesicle)|GO:0097091(synaptic vesicle clustering)"
Remark	"QUALITY:PATO:0001997(reduced)"
Remark	"Genotype \"unc-40(e271); wyEx800 [Pttx-3::mCherry Pglr-3::mCherry Punc-40::unc-40]\""
Remark	"Published_as unc-40"
Remark	"To identify the cell(s) in which unc-40 functions to direct AIY-RIA innervation, we analyzed unc-40 mosaic animals that retain an unstable rescuing array in subsets of cells (8). Interestingly, only when the array was retained in the AIY interneuron did we observe significant rescue of the AIY presynaptic patterning defects. Retention in the RIA interneuron resulted in rescue of the RIA axon guidance defect but not of the AIY presynaptic phenotype (reduction of a synaptic vesicle marker mCherry::RAB-3, in zone 2)."
Reference	"WBPaper00031068"


Anatomy_function : "WBbtf0498"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000102"	Autonomous
Gene	"WBGene00006776"
Not_involved	"WBbt:0005834"	Insufficient
Remark	"ENTITY:WBbt:0005413(AIY)|GO:0008021(synaptic vesicle)|GO:0097091(synaptic vesicle clustering)"
Remark	"QUALITY:PATO:0001997(reduced)"
Remark	"Genotype \"unc-40(n324);wyEx1474[Pttx-3::mCherry, Pcex-1::mCherry, Punc-40::unc-40]\""
Remark	"Published_as unc-40"
Remark	"To identify the cell(s) in which unc-40 functions to direct AIY-RIA innervation, we analyzed unc-40 mosaic animals that retain an unstable rescuing array in subsets of cells (8). Interestingly, only when the array was retained in the AIY interneuron did we observe significant rescue of the AIY presynaptic patterning defects. Retention of the array in the closely related interneuron RIB or RIM (RIB/RIM) did not result in rescue (reduction of a synaptic vesicle marker mCherry::RAB-3, in zone 2)."
Reference	"WBPaper00031068"


Anatomy_function : "WBbtf0499"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000847"	Autonomous
Gene	"WBGene00006776"
Involved	"WBbt:0005413"	Sufficient
Remark	"ENTITY:WBbt:0005413(AIY)|GO:0048786(presynaptic active zone)|GO:0097105(presynaptic membrane assembly)"
Remark	"QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"unc-40(e271); wyEx800 [Pttx-3::mCherry Pglr-3::mCherry Punc-40::unc-40]\""
Remark	"Published_as unc-40"
Remark	"To identify the cell(s) in which unc-40 functions to direct AIY-RIA innervation, we analyzed unc-40 mosaic animals that retain an unstable rescuing array in subsets of cells (8). Interestingly, only when the array was retained in the AIY interneuron did we observe significant rescue of the AIY presynaptic patterning defects. Retention in the RIA interneuron resulted in rescue of the RIA axon guidance defect but not of the AIY presynaptic phenotype (reduction of active zone markers ELKS-1::YP and SYD-2::GFP, in zone 2)."
Reference	"WBPaper00031068"


Anatomy_function : "WBbtf0500"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000847"	Autonomous
Gene	"WBGene00006776"
Not_involved	"WBbt:0006833"	Insufficient
Remark	"ENTITY:WBbt:0005413(AIY)|GO:0048786(presynaptic active zone)|GO:0097105(presynaptic membrane assembly)"
Remark	"QUALITY:PATO:0001997(reduced)"
Remark	"Genotype \"unc-40(e271); wyEx800 [Pttx-3::mCherry Pglr-3::mCherry Punc-40::unc-40]\""
Remark	"Published_as unc-40"
Remark	"To identify the cell(s) in which unc-40 functions to direct AIY-RIA innervation, we analyzed unc-40 mosaic animals that retain an unstable rescuing array in subsets of cells (8). Interestingly, only when the array was retained in the AIY interneuron did we observe significant rescue of the AIY presynaptic patterning defects. Retention in the RIA interneuron resulted in rescue of the RIA axon guidance defect but not of the AIY presynaptic phenotype (reduction of active zone markers ELKS-1::YP and SYD-2::GFP, in zone 2)."
Reference	"WBPaper00031068"


Anatomy_function : "WBbtf0501"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000847"	Autonomous
Gene	"WBGene00006776"
Involved	"WBbt:0005413"	Sufficient
Remark	"ENTITY:WBbt:0005413(AIY)|GO:0048786(presynaptic active zone)|GO:0097105(presynaptic membrane assembly)"
Remark	"QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"unc-40(n324);wyEx1474[Pttx-3::mCherry, Pcex-1::mCherry, Punc-40::unc-40]\""
Remark	"Published_as unc-40"
Remark	"To identify the cell(s) in which unc-40 functions to direct AIY-RIA innervation, we analyzed unc-40 mosaic animals that retain an unstable rescuing array in subsets of cells (8). Interestingly, only when the array was retained in the AIY interneuron did we observe significant rescue of the AIY presynaptic patterning defects. Retention of the array in the closely related interneuron RIB or RIM (RIB/RIM) did not result in rescue. (reduction of active zone markers ELKS-1::YP and SYD-2::GFP, in zone 2)."
Reference	"WBPaper00031068"


Anatomy_function : "WBbtf0502"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000847"	Autonomous
Gene	"WBGene00006776"
Not_involved	"WBbt:0005834"	Insufficient
Remark	"ENTITY:WBbt:0005413(AIY)|GO:0048786(presynaptic active zone)|GO:0097105(presynaptic membrane assembly)"
Remark	"QUALITY:PATO:0001997(reduced)"
Remark	"Genotype \"unc-40(n324);wyEx1474[Pttx-3::mCherry, Pcex-1::mCherry, Punc-40::unc-40]\""
Remark	"Published_as unc-40"
Remark	"To identify the cell(s) in which unc-40 functions to direct AIY-RIA innervation, we analyzed unc-40 mosaic animals that retain an unstable rescuing array in subsets of cells (8). Interestingly, only when the array was retained in the AIY interneuron did we observe significant rescue of the AIY presynaptic patterning defects. Retention of the array in the closely related interneuron RIB or RIM (RIB/RIM) did not result in rescue. (reduction of active zone markers ELKS-1::YP and SYD-2::GFP, in zone 2)."
Reference	"WBPaper00031068"


Anatomy_function : "WBbtf0503"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000384"	Autonomous
Gene	"WBGene00006776"
Not_involved	"WBbt:0005413"	Insufficient
Remark	"ENTITY:WBbt:0006833(RIA)|GO:0030424(axon)|GO:0007411(axon guidance)"
Remark	"QUALITY:PATO:0001997(reduced)"
Remark	"Genotype \"unc-40(e271); wyEx800 [Pttx-3::mCherry Pglr-3::mCherry Punc-40::unc-40]\""
Remark	"Published_as unc-40"
Remark	"To identify the cell(s) in which unc-40 functions to direct AIY-RIA innervation, we analyzed unc-40 mosaic animals that retain an unstable rescuing array in subsets of cells (8). Retention in the AIY neuron did not result in rescue of the RIA axon guidance defect (RIA processes fail to extend ventrally to create the loop that is innervated by AIY in zone 2)."
Reference	"WBPaper00031068"


Anatomy_function : "WBbtf0504"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000616"	Nonautonomous
Gene	"WBGene00006746"
Involved	"WBbt:0004925"	Sufficient
Involved	"WBbt:0004923"	Sufficient
Remark	"ENTITY:WBbt:0005413(AIY)|WBbt:0006833(RIA)|GO:0045202(synapse)|GO:0050808(synapse development)"
Remark	"QUALITY:PATO:0001507(disrupted) NOT"
Remark	"Genotype \"unc-6(ev400); wyEx1126[Punc-6::unc-6, Phlh-17::mCherry]\""
Remark	"Mosaic analysis using an unc-6 rescuing construct showed that expression of UNC-6 (netrin) by VCSCs (ventral cephalic sheath cells), but not by DCSCs (dordal cephalic sheath cells), regulates the pattern of AIY presynapses."
Remark	"Published_as unc-6"
Reference	"WBPaper00031068"


Anatomy_function : "WBbtf0505"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000616"	Nonautonomous
Gene	"WBGene00006746"
Not_involved	"WBbt:0004929"	Insufficient
Not_involved	"WBbt:0004927"	Insufficient
Remark	"ENTITY:WBbt:0005413(AIY)|WBbt:0006833(RIA)|GO:0045202(synapse)|GO:0050808(synapse development)"
Remark	"QUALITY:PATO:0001507(disrupted)"
Remark	"Genotype \"unc-6(ev400); wyEx1126[Punc-6::unc-6, Phlh-17::mCherry]\""
Remark	"Mosaic analysis using an unc-6 rescuing construct showed that expression of UNC-6 (netrin) by VCSCs (ventral cephalic sheath cells), but not by DCSCs (dordal cephalic sheath cells), regulates the pattern of AIY presynapses."
Remark	"Published_as unc-6"
Reference	"WBPaper00031068"


Anatomy_function : "WBbtf0506"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000682"	Autonomous
Gene	"WBGene00001483"
Involved	"WBbt:0005784"	Necessary
Remark	"ENTITY:WBbt:0007849(hermaphrodite)|WBbt:0006798(sperm)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0001511(defective)"
Remark	"Genetic mosaics were scored in a fog-3 null mutant strain carrying an extrachromosomal array that harbored wild-type fog-3 and an ubiquitously expressed GFP marker. Only mosaic animals that lost the array in P4 (germline founder cell) showed sterile phenotype."
Remark	"Published_as fog-3"
Reference	"WBPaper00041299"


Anatomy_function : "WBbtf0507"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001661"	Autonomous
Gene	"WBGene00003299"
Involved	"WBbt:0005832"	Sufficient
Remark	"ENTITY:WBbt:0005832(AWC-ON)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0002051(increased occurrence)"
Remark	"Genotype \"Ex[odr-3p::mir-71 odr-1p::DsRed]\""
Remark	"Mosaic animals were generated by random and spontaneous mitotic loss of an unstable transgene expressing the mir-71(OE) construct odr-3p::mir-71 and a mosaic marker odr1p::DsRed that showed which AWC cells retained the transgene.  When the mir-71(OE) transgene was retained in only one of the two AWC neurons, the mir-71(OE) AWC neuron became AWCON and wildtype AWC neuron became AWCOFF in the majority of these mosaic animals."
Remark	"Published_as mir-71"
Reference	"WBPaper00041411"


Anatomy_function : "WBbtf0508"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001661"
Gene	"WBGene00003822"
Involved	"WBbt:0005672"	Sufficient
Involved	"WBbt:0005671"	Sufficient
Remark	"ENTITY:WBbt:0005832(AWC-ON)|GO:0009855(determination of bilateral asymmetry)"
Remark	"QUALITY:PATO:0002051(increased occurrence) NOT"
Remark	"Genotype \"nsy-1(n397); Ex[odr-3::NSY-1]\""
Remark	"Published_as nsy-1"
Remark	"To ask whether NSY-1 expression in AWC is sufficient to rescue nsy-1 mutants, we placed the nsy-1 cDNA under the control of the odr-3 promoter. This promoter drives strong expression in both AWC neurons, weak expression in the AWB neurons, and variable expression in AWA, ADF, and ASH neurons. The odr-3::NSY-1 transgene rescued the 2 AWCON asymmetry defect of nsy-1 mutants and occasionally caused a gain-of-function (2 AWCOFF) phenotype, supporting the hypothesis that NSY-1 acts in the AWC neurons to mediate AWC asymmetry."
Reference	"WBPaper00004669"


Anatomy_function : "WBbtf0509"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001661"
Gene	"WBGene00006779"
Involved	"WBbt:0005672"	Sufficient
Involved	"WBbt:0005671"	Sufficient
Remark	"ENTITY:WBbt:0005832(AWC-ON)|GO:0009855(determination of bilateral asymmetry)"
Remark	"QUALITY:PATO:0002051(increased occurrence) NOT"
Remark	"Genotype \"unc-43(n1186), Ex[odr-3::unc-43]\""
Remark	"Published_as unc-43"
Remark	"Since the CaMKII homolog unc-43 has a similar phenotype to nsy-1, we asked whether it could also function in AWC neurons. An unc-43 cDNA (Rongo and Kaplan, 1999) under the control of the odr-3 promoter rescued the 2 AWCON str-2::GFP phenotype of an unc-43 mutant and occasionally caused a gain-of-function (2 AWCOFF) phenotype (Table 1), consistent with the possibility that unc-43 acts in the AWC neurons."
Reference	"WBPaper00004669"


Anatomy_function : "WBbtf0510"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001661"
Gene	"WBGene00003822"
Involved	"WBbt:0005672"	Necessary
Remark	"Because the odr-3 promoter is reproducibly expressed in both AWC and AWB neurons, it is possible that nsy-1 expression in AWB rescues AWC cell fate. To rule out this possibility, we examined mosaic animals that expressed odr-3::NSY-1 in the AWB neurons but not the AWC neurons. Mosaic animals arose through the random loss of extrachromosomal arrays containing both odr-3::NSY-1 and the marker odr-1::RFP in a nsy-1 mutant background. str-2::GFP asymmetry was rescued when the arrays were present in AWC neurons, but not when they were present only in AWB neurons."
Remark	"ENTITY:WBbt:0005832(AWC-ON)|GO:0009855(determination of bilateral asymmetry)"
Remark	"QUALITY:PATO:0002051(increased occurrence)"
Remark	"Genotype \"nsy-1(n397); Ex[odr-3::NSY-1 elt-2::GFP odr-1::RFP]\""
Remark	"Published_as nsy-1"
Reference	"WBPaper00004669"


Anatomy_function : "WBbtf0511"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001661"
Gene	"WBGene00006779"
Involved	"WBbt:0005672"	Necessary
Remark	"Because the odr-3 promoter is reproducibly expressed in both AWC and AWB neurons, it is possible that unc-43 expression in AWB rescues AWC cell fate. To rule out this possibility, we examined mosaic animals that expressed odr-3::UNC-43 in the AWB neurons but not the AWC neurons. Mosaic animals arose through the random loss of extrachromosomal arrays containing both odr-3::UNC-43 and the marker odr-1::RFP in a unc-43 mutant background. str-2::GFP asymmetry was rescued when the arrays were present in AWC neurons, but not when they were present only in AWB neurons."
Remark	"ENTITY:WBbt:0005832(AWC-ON)|GO:0009855(determination of bilateral asymmetry)"
Remark	"QUALITY:PATO:0002051(increased occurrence)"
Remark	"Genotype \"unc-43(n1186); Ex[odr-3::UNC-43 elt-2::GFP odr-1::RFP]\""
Remark	"Published_as unc-43"
Reference	"WBPaper00004669"


Anatomy_function : "WBbtf0512"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001661"	Autonomous
Gene	"WBGene00006779"
Involved	"WBbt:0005833"	Necessary
Remark	"ENTITY:WBbt:0005833(AWC-OFF)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0002052(decreased occurence)"
Remark	"Genotype \"unc-43(n1186); Is[str-2::GFP]; Ex[odr-3::UNC-43 elt-2::GFP odr-1::RFP]\""
Remark	"Mosaic analysis was conducted with unc-43(lf) animals bearing a transgenic extra-chromosomal array of odr-3::UNC-43 and odr-1::RFP. The odr-1 promoter drives expression in the AWB and AWC neurons. Mosaic animals with one RFP AWC neuron were identified in two transgenic lines. Both lines exhibited two major classes of mosaics (Table 1): animals in which str-2::GFP was only expressed in the mutant, non-RFP-expressing cell and animals in which both the mutant and wild-type cells expressed str-2::GFP. These are the two classes expected if unc-43 were acting to execute the AWCOFF cell fate, but not to coordinate the two AWC fates via cell interaction and feedback."
Remark	"Published_as unc-43"
Reference	"WBPaper00004669"


Anatomy_function : "WBbtf0513"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001661"	Autonomous
Gene	"WBGene00006779"
Involved	"WBbt:0005833"	Sufficient
Remark	"ENTITY:WBbt:0005833(AWC-OFF)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0002052(decreased occurence)"
Remark	"Genotype \"Is[str-2::GFP]; Ex[odr-3::UNC-43(GF) odr-1::RFP\""
Remark	"Mosaic analysis was also performed with a wild-type strain bearing a transgenic extrachromosomal array of odr-3::UNC-43(GF) and odr-1::RFP. All three lines yielded two major classes of mosaics. Animals in one class of mosaics expressed str-2::GFP in the wild-type cell but not in the gain-of-function, RFP cell, and animals in the second class did not express str-2::GFP in either cell. These are the classes expected if unc-43 were acting to execute the AWCOFF cell fate, but not to coordinate the fates of the two AWC cells via cell interaction."
Remark	"Published_as unc-43"
Reference	"WBPaper00004669"


Anatomy_function : "WBbtf0514"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001661"	Nonautonomous
Gene	"WBGene00003299"
Involved	"WBbt:0005832"	Sufficient
Remark	"ENTITY:WBbt:0005833(AWC-OFF)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0002051(increased occurrence)"
Remark	"Genotype \"Ex[odr-3p::mir-71 odr-1p::DsRed]\""
Remark	"Mosaic animals were generated by random and spontaneous mitotic loss of an unstable transgene expressing the mir-71(OE) construct odr-3p::mir-71 and a mosaic marker odr1p::DsRed that showed which AWC cells retained the transgene.  When the mir-71(OE) transgene was retained in only one of the two AWC neurons, the mir-71(OE) AWC neuron became AWCON and wildtype AWC neuron became AWCOFF in the majority of these mosaic animals."
Remark	"Published_as mir-71"
Reference	"WBPaper00041411"


Anatomy_function : "WBbtf0515"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001661"	Autonomous
Involved	"WBbt:0005672"	Sufficient
Remark	"ENTITY:WBbt:0005672(AWC)|GO:0009855(determination of bilateral asymmetry)"
Remark	"QUALITY:PATO:0001507(disrupted) NOT"
Remark	"Genotype \"Is[str-2::gfp]; sek-1(km4); Ex[odr-3p::sek-1]\""
Remark	"To determine whether sek-1 expression in AWC neurons, or in an another cell type, is required for asymmetrical str-2 expression, sek-1 cDNA was expressed under the control of the odr-3 promoter, which drives expression in the AWC neurons. For transgenic sek-1(km4) mutants harboring the odr-3p::sek-1 transgene, most animals showed str-2 expression only in one AWC neuron, but not in both. Thus, SEK-1 acts within the AWC neurons to determine asymmetric expression of str-2."
Reference	"WBPaper00005102"


Anatomy_function : "WBbtf0516"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001661"	Autonomous
Involved	"WBbt:0005672"	Sufficient
Remark	"ENTITY:WBbt:0005672(AWC)|GO:0009855(determination of bilateral asymmetry)"
Remark	"QUALITY:PATO:0001507(disrupted)"
Remark	"Genotype \"Is[str-2::gfp]; Ex[odr-3p::sek-1(STDD)]\""
Remark	"We generated sek-1(STDD) mutants, in which both Ser 204 and Thr 208 were replaced with Asp. The sek-1(STDD) mutants are predicted to have constitutively active kinase activity. When an odr-3p::sek-1(STDD) transgene was introduced into N2 wild-type animals, most animals had no str-2 expression in either of the AWC neurons, the opposite phenotype of sek-1(km4)."
Reference	"WBPaper00005102"


Anatomy_function : "WBbtf0517"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001661"	Autonomous
Involved	"WBbt:0005672"	Sufficient
Remark	"ENTITY:WBbt:0005672(AWC)|GO:0009855(determination of bilateral asymmetry)"
Remark	"QUALITY:PATO:0001507(disrupted) NOT"
Remark	"Genotype \"Is[str-2::gfp]; tir-1(ky388); Ex[odr-3::tir-1::DsRed]\""
Remark	"To confirm the identification of F13B10.1 as nsy-2/tir-1 and determine the site of gene action, we generated an odr-3 tir-1 DsRed transgene that drives expression of a tagged tir-1a cDNA strongly in AWC neurons and weakly in four other classes of sensory neurons (the tir-1a cDNA affected by the ky388 mutation was used in all molecular studies). The transgene rescued the str-2 expression defect in tir-1(ky388) mutant when injected at 5 ng/microL, resulting in a high percentage of animals with the wild-type 1 AWCON phenotype. This result suggests that tir-1 acts in AWC to affect asymmetric odorant receptor expression."
Reference	"WBPaper00024676"


Anatomy_function : "WBbtf0518"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001661"	Autonomous
Involved	"WBbt:0005833"	Sufficient
Remark	"Although the rescue of tir-1 using the odr-3 promoter suggests a site of action in AWC, it does not distinguish whether the protein acts in the AWCON cell, the AWCOFF cell, or both. These possibilities can be distinguished in mosaic animals in which tir-1 activity is altered in only one of the two AWC neurons. The partial penetrance of tir-1 mutations was problematic for mosaic analysis, so the gain-of-function phenotype of tir-1 overexpression was used. The single DsRed-expressing AWC cell did not express str-2 GFP in 95% of the animals, a percentage consistent with a cell-autonomous repression of str-2 GFP by the odr-3::tir-1 transgene in that neuron. The AWC neuron in the mosaics that did not express DsRed should be genotypically wild-type. Approximately 40% of the AWC cells that lacked DsRed fluorescence expressed str-2 GFP."
Remark	"ENTITY:WBbt:0005833(AWC-OFF)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0002051(increased occurrence)"
Remark	"Genotype \"Is[str-2::gfp]; Ex[odr-3::tir-1::DsRed]\""
Reference	"WBPaper00024676"


Anatomy_function : "WBbtf0519"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001661"
Gene	"WBGene00021415"
Involved	"WBbt:0005672"	Sufficient
Remark	"ENTITY:WBbt:0005832(AWC-ON)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0002052(decreased occurrence) NOT"
Remark	"Genotype \"nsy-4(ky616); Is[str-2::GFP]; Ex[odr-3::nsy-4, odr-1::dsRed]\""
Remark	"Published_as nsy-4"
Remark	"To ask whether expression of nsy-4 in AWC could be sufficient for phenotypic rescue, nsy-4 cDNAs were expressed under control of the AWC-selective odr-3 promoter and introduced into nsy-4 mutants. These transgenes partially rescued str-2 expression in nsy-4 animals, suggesting that nsy-4 expression in AWC can drive the AWCON receptor choice."
Reference	"WBPaper00028384"


Anatomy_function : "WBbtf0520"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001661"
Gene	"WBGene00021415"
Not_involved	"WBbt:0005413"	Insufficient
Remark	"ENTITY:WBbt:0005832(AWC-ON)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0002052(decreased occurrence)"
Remark	"Genotype \"nsy-4(ky616); Is[str-2::GFP]; Ex[ttx-3::nsy-4, odr-1::dsRed]\""
Remark	"Published_as nsy-4"
Remark	"The ttx-3 promoter drives expression in the interneuron AIY, a primary synaptic partner of AWC. Expression of nsy-4 under the ttx-3 promoter failed to rescue nsy-4 and had no effect in a wild-type background."
Reference	"WBPaper00028384"


Anatomy_function : "WBbtf0521"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001661"	Autonomous
Gene	"WBGene00021415"
Involved	"WBbt:0005832"	Necessary
Remark	"ENTITY:WBbt:0005832(AWC-ON)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0002052(decreased occurrence) NOT"
Remark	"Genotype \"nsy-4(ky616); Is[str-2::GFP]; Ex[odr-3::nsy-4, odr-1::dsRed]\""
Remark	"Mosaic analysis was conducted in nsy-4(ky616);str2::GFP animals using unstable extrachromosomal arrays of odr-3::nsy-4 and the AWC marker odr-1::dsRed. Mosaic animals were recognized by loss of dsRed in one of the two AWC neurons, and expression of str-2::GFP was scored in the wild-type (dsRed+) and mutant (dsRed2) AWC cell. In one major class of mosaic animals, the cell expressing dsRed became AWCON, and the mutant cell became AWCOFF. In the second significant class of mosaic animals, both cells became AWCOFF. The first class suggests that nsy-4 acts primarily cell-autonomously in AWCON to promote AWCON receptor choice and is consistent with a function in signal reception. The second class can be explained by incomplete rescue from the extrachromosomal arrays."
Remark	"Published_as nsy-4"
Reference	"WBPaper00028384"


Anatomy_function : "WBbtf0522"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001661"	Autonomous
Gene	"WBGene00021415"
Involved	"WBbt:0005832"	Sufficient
Remark	"ENTITY:WBbt:0005832(AWC-ON)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0002051(increased occurrence)"
Remark	"Genotype \"Is[str-2::GFP]; Ex[odr-3::nsy-4(OE), odr-1::dsRed]\""
Remark	"Published_as nsy-4"
Remark	"We analyzed mosaic animals in lines that overexpressed odr-3::nsy-4 in a wild-type background [odr-3::nsy-4(OE)]. In animals in which only one of the 2 AWC neurons expressed odr-3::nsy-4, that neuron became AWCON significantly more than 50% of the time. This result supports and confirms the nsy-4 loss-of-function mosaics by indicating that nsy-4 overexpression in AWC has a cell-autonomous ability to promote AWCON receptor choice."
Reference	"WBPaper00028384"


Anatomy_function : "WBbtf0523"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001661"	Nonautonomous
Gene	"WBGene00021415"
Involved	"WBbt:0005832"	Sufficient
Remark	"ENTITY:WBbt:0005833(AWC-OFF)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0002051(increased occurrence)"
Remark	"Genotype \"Is[str-2::GFP]; Ex[odr-3::nsy-4(OE), odr-1::dsRed]\""
Remark	"Published_as nsy-4"
Remark	"We analyzed mosaic animals in lines that overexpressed odr-3::nsy-4 in a wild-type background [odr-3::nsy-4(OE)]. In animals in which only one of the 2 AWC neurons expressed odr-3::nsy-4, that neuron became AWCON significantly more than 50% of the time. Strikingly, the wild-type AWC neuron in these mosaic lines was also affected: instead of becoming AWCON in 50% of the animals, the wild-type neuron almost always became AWCOFF. Thus, overexpression of nsy-4 in 1 AWC neuron had a nonautonomous effect on the other, wild-type AWC neuron."
Reference	"WBPaper00028384"


Anatomy_function : "WBbtf0524"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001661"	Autonomous
Gene	"WBGene00002141"
Involved	"WBbt:0005672"	Sufficient
Remark	"ENTITY:WBbt:0005672(AWC)|GO:0009855(determination of bilateral asymmetry)"
Remark	"QUALITY:PATO:0001507(disrupted) NOT"
Remark	"Genotype \"nsy-5(ky634); Is[str-2::GFP]; Ex[odr-3::nsy-5]\""
Remark	"Published_as nsy-5"
Remark	"We expressed nsy-5 cDNAs under different promoters in nsy-5 mutant background. Only transgenes (ord-3::nsy-5 or tax-4::nsy-5) expressed in AWC neurons were able to rescue nsy-5 mutants, suggesting that one important site of nsy-5 action is AWC."
Reference	"WBPaper00029404"


Anatomy_function : "WBbtf0525"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001661"
Gene	"WBGene00002141"
Involved	"WBbt:0005672"	Sufficient
Involved	"WBbt:0005665"	Sufficient
Involved	"WBbt:0005662"	Sufficient
Remark	"ENTITY:WBbt:0005672(AWC)|GO:0009855(determination of bilateral asymmetry)"
Remark	"QUALITY:PATO:0001507(disrupted) NOT"
Remark	"Genotype \"nsy-5(ky634); Is[str-2::GFP]; Ex[odr-3::nsy-5; sra-6::nsy-5; gcy-8::nsy-5]\""
Remark	"Published_as nsy-5"
Remark	"We expressed nsy-5 cDNAs under different promoters in nsy-5 mutant background. Only transgenes (ord-3::nsy-5 or tax-4::nsy-5) expressed in AWC neurons were able to rescue nsy-5 mutants, suggesting that one important site of nsy-5 action is AWC. However, expression of nsy-5 in other neurons modified the rescue in AWC neurons. Simultaneous nsy-5 expression from odr-3 (AWC) and sra-6 (ASH) promoters led to a strong gain-of-function 2 AWCON phenotype not observed with either promoter alone. This enhancement was suppressed when nsy-5 was simultaneously expressed from odr-3 (AWC), sra-6 (ASH), and gcy-8 (AFD) promoters."
Reference	"WBPaper00029404"


Anatomy_function : "WBbtf0526"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001661"
Gene	"WBGene00002141"
Involved	"WBbt:0005672"	Sufficient
Involved	"WBbt:0005665"	Sufficient
Involved	"WBbt:0005662"	Sufficient
Remark	"ENTITY:WBbt:0005672(AWC)|GO:0009855(determination of bilateral asymmetry)"
Remark	"QUALITY:PATO:0001507(disrupted)"
Remark	"Genotype \"Is[str-2::GFP]; Ex[odr-3::nsy-5; sra-6::nsy-5; gcy-8::nsy-5]\""
Remark	"Published_as nsy-5"
Remark	"The AWC-ASH-AFD interaction was also observed when nsy-5 transgenes were expressed in a wild-type background. At the low DNA concentrations used to make these transgenic lines, no appreciable gain-of-function phenotypes were generated by introducing individual transgenes into wild-type strains. However, expression of nsy-5 in both AWC and ASH generated a strong 2 AWCON gain-of-function phenotype that was suppressed by coexpression of nsy-5 in AFD or AWB."
Reference	"WBPaper00029404"


Anatomy_function : "WBbtf0527"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001661"
Gene	"WBGene00002141"
Involved	"WBbt:0005672"	Sufficient
Involved	"WBbt:0005665"	Sufficient
Involved	"WBbt:0005671"	Sufficient
Remark	"ENTITY:WBbt:0005672(AWC)|GO:0009855(determination of bilateral asymmetry)"
Remark	"QUALITY:PATO:0001507(disrupted)"
Remark	"Genotype \"Is[str-2::GFP]; Ex[odr-3::nsy-5; sra-6::nsy-5; str-1::nsy-5]\""
Remark	"Published_as nsy-5"
Remark	"The AWC-ASH-AFD interaction was also observed when nsy-5 transgenes were expressed in a wild-type background. At the low DNA concentrations used to make these transgenic lines, no appreciable gain-of-function phenotypes were generated by introducing individual transgenes into wild-type strains. However, expression of nsy-5 in both AWC and ASH generated a strong 2 AWCON gain-of-function phenotype that was suppressed by coexpression of nsy-5 in AFD or AWB."
Reference	"WBPaper00029404"


Anatomy_function : "WBbtf0528"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001661"	Autonomous
Gene	"WBGene00002141"
Involved	"WBbt:0005832"	Sufficient
Involved	"WBbt:0005832"	Necessary
Remark	"ENTITY:WBbt:0005832(AWC-ON)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0001507(disrupted)"
Remark	"Genotype \"nsy-5(ky634): Is[str-2::GFP]; Ex[nsy-5(genomic) odr-1::DsRed]\""
Remark	"Published_as nsy-5"
Remark	"To further refine the site of nsy-5 action, mosaic animals in which nsy-5 activity differed between the two AWC neurons were used to ask whether nsy-5 acts in the future AWCON cell, the future AWCOFF cell, or both. Mosaic animals were generated by random loss of an unstable transgene with the nsy-5 genomic clone and an odr-1::DsRed marker (expressed in AWC and AWB) that showed which cells retained the transgenic array. Spontaneous loss of the extrachromosomal array resulted in mosaic animals in which one of the two AWC neurons expressed DsRed fluorescence and nsy-5 activity. In the majority of these mosaic animals, the nsy-5+ AWC neuron expressed str-2::GFP and the nsy-5- AWC neuron did not."
Reference	"WBPaper00029404"


Anatomy_function : "WBbtf0529"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001661"	Nonautonomous
Gene	"WBGene00002141"
Involved	"WBbt:0005832"	Sufficient
Involved	"WBbt:0005832"	Necessary
Remark	"ENTITY:WBbt:0005833(AWC-OFF)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0001507(disrupted)"
Remark	"Genotype \"nsy-5(ky634): Is[str-2::GFP]; Ex[nsy-5(genomic) odr-1::DsRed]\""
Remark	"Published_as nsy-5"
Remark	"To further refine the site of nsy-5 action, mosaic animals in which nsy-5 activity differed between the two AWC neurons were used to ask whether nsy-5 acts in the future AWCON cell, the future AWCOFF cell, or both. Mosaic animals were generated by random loss of an unstable transgene with the nsy-5 genomic clone and an odr-1::DsRed marker (expressed in AWC and AWB) that showed which cells retained the transgenic array. Spontaneous loss of the extrachromosomal array resulted in mosaic animals in which one of the two AWC neurons expressed DsRed fluorescence and nsy-5 activity. In the majority of these mosaic animals, the nsy-5+ AWC neuron expressed str-2::GFP and the nsy-5- AWC neuron did not."
Reference	"WBPaper00029404"


Anatomy_function : "WBbtf0530"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001661"	Autonomous
Gene	"WBGene00002141"
Involved	"WBbt:0005832"	Sufficient
Remark	"ENTITY:WBbt:0005832(AWC-ON)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0001507(disrupted)"
Remark	"Genotype \"Is[str-2::GFP]; Ex[nsy-5(OE) odr-1::DsRed]\""
Remark	"Mosaic analysis was also conducted in transgenic lines in which nsy-5 was overexpressed in a wild-type background, resulting in a 2 AWCON phenotype. When the transgene was retained in only one of the AWC neurons, the nsy-5(OE) neuron expressed str2::GFP over 80% of the time, suggesting that nsy-5 has a cell-autonomous ability to promote the AWCON receptor choice."
Remark	"Published_as nsy-5"
Reference	"WBPaper00029404"


Anatomy_function : "WBbtf0531"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001661"	Nonautonomous
Gene	"WBGene00002141"
Involved	"WBbt:0005832"	Sufficient
Remark	"ENTITY:WBbt:0005833(AWC-OFF)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0001507(disrupted)"
Remark	"Genotype \"Is[str-2::GFP]; Ex[nsy-5(OE) odr-1::DsRed]\""
Remark	"Mosaic analysis was also conducted in transgenic lines in which nsy-5 was overexpressed in a wild-type background, resulting in a 2 AWCON phenotype. When the transgene was retained in only one of the AWC neurons, the nsy-5(OE) neuron expressed str2::GFP over 80% of the time, suggesting that nsy-5 has a cell-autonomous ability to promote the AWCON receptor choice. The DsRed-negative AWC neuron in these mosaic animals, which should have a wildtype genotype, nearly always became AWCOFF. This result suggests that the decision of one AWC neuron to become AWCON due to nsy-5 overexpression was sensed by the wild-type AWC neuron, which then became AWCOFF."
Remark	"Published_as nsy-5"
Reference	"WBPaper00029404"


Anatomy_function : "WBbtf0532"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001661"	Nonautonomous
Gene	"WBGene00002141"
Involved	"WBbt:0006581"	Necessary
Remark	"ENTITY:WBbt:0005672(AWC)|GO:0009855(determination of bilateral asymmetry)"
Remark	"QUALITY:PATO:0001507(disrupted)"
Remark	"Genotype \"nsy-5(ky634): Is[str-2::GFP]; Ex[nsy-5(genomic) odr-1::DsRed]\""
Remark	"Published_as nsy-5"
Remark	"Several classes of mosaic animals indicated that nsy-5 rescue is not entirely cell autonomous to AWCON. First, in a minor but significant class of mosaic animals, a nsy-5 mutant AWC neuron became AWCON, suggesting nonautonomous rescue of AWC. Second, mosaic animals that lost the array in the AWBR lineage (ABpra) but retained it in both AWC neurons had a significant bias in left-right asymmetry, such that 71% of the AWCR neurons became AWCON. This result suggests that nsy-5-expressing cells in the ABpra lineage affect communication between the two AWC neurons."
Reference	"WBPaper00029404"


Anatomy_function : "WBbtf0533"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001661"	Nonautonomous
Gene	"WBGene00002141"
Involved	"WBbt:0006571"	Sufficient
Involved	"WBbt:0006451"	Sufficient
Remark	"ENTITY:WBbt:0005672(AWC)|GO:0009855(determination of bilateral asymmetry)"
Remark	"QUALITY:PATO:0001507(disrupted)"
Remark	"Genotype \"Is[str-2::GFP]; Ex[nsy-5(OE) odr-1::DsRed]\""
Remark	"Published_as nsy-5"
Remark	"The effect of the nsy-5-overexpressing transgene in the wild-type background was largely dependent on the genotype of the AWC neurons. However, a rare class of mosaics in which nsy-5 was overexpressed in both AWB lineages but not in either AWC had an unexpected 2 AWCOFF loss-of-function phenotype. These mosaics indicate that overexpression of nsy-5 in cells related to AWB can cause a dominant disruptive effect on AWC signaling."
Reference	"WBPaper00029404"


Anatomy_function : "WBbtf0534"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001661"
Gene	"WBGene00007260"
Involved	"WBbt:0005672"	Sufficient
Remark	"ENTITY:WBbt:0005832(AWC-ON)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0002052(decreased occurrence) NOT"
Remark	"Expression of olrn-1 cDNAs under the AWC-selective odr-3 promoter rescued the 2AWCOFF phenotypes of olrn1(ky626) mutants."
Remark	"Genotype \"olrn-1(ky626); Is[str-2::GFP]; Ex[odr-3::olrn-1b]\""
Remark	"Published_as olrn-1"
Reference	"WBPaper00031175"


Anatomy_function : "WBbtf0535"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001661"
Gene	"WBGene00007260"
Involved	"WBbt:0005672"	Sufficient
Remark	"ENTITY:WBbt:0005832(AWC-ON)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0002051(increased occurrence)"
Remark	"Expression of olrn-1 cDNAs under the AWC-selective odr-3 promoter rescued the 2AWCOFF phenotypes of olrn-1(ky626) mutants. Additionally, overexpression of olrn-1b in a wild-type background caused a 2AWCON phenotype."
Remark	"Genotype \"Is[str-2::GFP]; Ex[odr-3::olrn-1b(OE)]\""
Remark	"Published_as olrn-1"
Reference	"WBPaper00031175"


Anatomy_function : "WBbtf0536"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001661"	Autonomous
Gene	"WBGene00007260"
Involved	"WBbt:0005832"	Sufficient
Remark	"ENTITY:WBbt:0005832(AWC-ON)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0002052(decreased occurrence) NOT"
Remark	"Genotype \"olrn-1(ky626); Is[str-2::GFP]; Ex[odr-3::olrn-1b odr-1::DsRed]\""
Remark	"Published_as olrn-1"
Remark	"To understand how the (AWC-ON/AWC-OFF) decision is made, we used genetic mosaic analysis to examine animals in which the two AWCs had different levels of olrn-1 gene activity. In an olrn-1 mutant background, most mosaic animals with a single rescued AWC had the wild-type, asymmetric phenotype: the rescued cell became AWCON and the mutant cell became AWCOFF. This result suggests that olrn-1 acts cell autonomously in the future AWCON cell to induce its identity."
Reference	"WBPaper00031175"


Anatomy_function : "WBbtf0537"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001661"	Nonautonomous
Gene	"WBGene00007260"
Involved	"WBbt:0005832"	Sufficient
Remark	"ENTITY:WBbt:0005833(AWC-OFF)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0002051(increased occurrence)"
Remark	"Genotype \"Is[str-2::GFP]; Ex[odr-3::olrn-1b odr-1::DsRed]\""
Remark	"Published_as olrn-1"
Remark	"To understand how the (AWC-ON/AWC-OFF) decision is made, we used genetic mosaic analysis to examine animals in which the two AWCs had different levels of olrn-1 gene activity. In wild-type animals overexpressing odr-3::olrn-1 transgenes, most animals that lost the transgene in one AWC also had a wild-type asymmetric AWC phenotype. In these animals, the cell overexpressing olrn-1 nearly always became AWCON, and the wild-type contralateral cell nearly always became AWCOFF."
Reference	"WBPaper00031175"


Anatomy_function : "WBbtf0538"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001661"	Nonautonomous
Gene	"WBGene00007260"
Involved	"WBbt:0005832"	Sufficient
Remark	"ENTITY:WBbt:0005833(AWC-OFF)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0002051(increased occurrence)"
Remark	"Genotype \"nsy-4(ky616); Is[str-2::GFP]; Ex[odr-3::olrn-1b odr-1::DsRed]\""
Remark	"Published_as olrn-1"
Remark	"To understand how the (AWC-ON/AWC-OFF) decision is made, we used genetic mosaic analysis to examine animals in which the two AWCs had different levels of olrn-1 gene activity. To separate cell-intrinsic functions of olrn-1 from possible network functions, we generated mosaics overexpressing OLRN-1 in one AWC in nsy-4 mutants. In these experiments,olrn-1(OE) behaved exactly as it did in the wild-type background, specifically converting the olrn-1-expressing neuron to AWCON. These results suggest that olrn-1 functions independently of, and most likely downstream of nsy-4 in AWCON."
Reference	"WBPaper00031175"


Anatomy_function : "WBbtf0539"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001661"	Autonomous
Gene	"WBGene00007260"
Involved	"WBbt:0005832"	Sufficient
Remark	"ENTITY:ENTITY:WBbt:0005832(AWC-ON)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0002051(increased occurrence)"
Remark	"Genotype \"nsy-4(ky616); Is[str-2::GFP]; Ex[odr-3::olrn-1b odr-1::DsRed]\""
Remark	"Published_as olrn-1"
Remark	"To understand how the (AWC-ON/AWC-OFF) decision is made, we used genetic mosaic analysis to examine animals in which the two AWCs had different levels of olrn-1 gene activity. To separate cell-intrinsic functions of olrn-1 from possible network functions, we generated mosaics overexpressing OLRN-1 in one AWC in nsy-4 mutants. In these experiments,olrn-1(OE) behaved exactly as it did in the wild-type background, specifically converting the olrn-1-expressing neuron to AWCON. These results suggest that olrn-1 functions independently of, and most likely downstream of nsy-4 in AWCON."
Reference	"WBPaper00031175"


Anatomy_function : "WBbtf0540"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001661"	Autonomous
Gene	"WBGene00007260"
Involved	"WBbt:0005832"	Sufficient
Remark	"ENTITY:ENTITY:WBbt:0005832(AWC-ON)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0002051(increased occurrence)"
Remark	"Genotype \"Is[str-2::GFP]; Ex[odr-3::olrn-1b odr-1::DsRed]\""
Remark	"Published_as olrn-1"
Remark	"To understand how the (AWC-ON/AWC-OFF) decision is made, we used genetic mosaic analysis to examine animals in which the two AWCs had different levels of olrn-1 gene activity. In wild-type animals overexpressing odr-3::olrn-1 transgenes, most animals that lost the transgene in one AWC also had a wild-type asymmetric AWC phenotype. In these animals, the cell overexpressing olrn-1 nearly always became AWCON, and the wild-type contralateral cell nearly always became AWCOFF."
Reference	"WBPaper00031175"


Anatomy_function : "WBbtf0541"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001661"	Autonomous
Gene	"WBGene00007260"
Involved	"WBbt:0005832"	Sufficient
Remark	"ENTITY:ENTITY:WBbt:0005832(AWC-ON)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0002051(increased occurrence)"
Remark	"Genotype \"nsy-5(ky634); Is[str-2::GFP]; Ex[odr-3::olrn-1b odr-1::DsRed]\""
Remark	"Published_as olrn-1"
Remark	"To understand how the (AWC-ON/AWC-OFF) decision is made, we used genetic mosaic analysis to examine animals in which the two AWCs had different levels of olrn-1 gene activity. To separate cell-intrinsic functions of olrn-1 from possible network functions, we generated mosaics overexpressing OLRN-1 in one AWC in nsy-5 mutants. In these experiments,olrn-1(OE) behaved exactly as it did in the wild-type background, specifically converting the olrn-1-expressing neuron to AWCON. These results suggest that olrn-1 functions independently of, and most likely downstream of nsy-5 in AWCON."
Reference	"WBPaper00031175"


Anatomy_function : "WBbtf0542"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001661"	Nonautonomous
Gene	"WBGene00007260"
Involved	"WBbt:0005832"	Sufficient
Remark	"ENTITY:WBbt:0005833(AWC-OFF)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0002051(increased occurrence)"
Remark	"Genotype \"nsy-5(ky634); Is[str-2::GFP]; Ex[odr-3::olrn-1b odr-1::DsRed]\""
Remark	"Published_as olrn-1"
Remark	"To understand how the (AWC-ON/AWC-OFF) decision is made, we used genetic mosaic analysis to examine animals in which the two AWCs had different levels of olrn-1 gene activity. To separate cell-intrinsic functions of olrn-1 from possible network functions, we generated mosaics overexpressing OLRN-1 in one AWC in nsy-5 mutants. In these experiments,olrn-1(OE) behaved exactly as it did in the wild-type background, specifically converting the olrn-1-expressing neuron to AWCON. These results suggest that olrn-1 functions independently of, and most likely downstream of nsy-5 in AWCON."
Reference	"WBPaper00031175"


Anatomy_function : "WBbtf0543"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001661"	Autonomous
Gene	"WBGene00006772"
Involved	"WBbt:0005672"	Sufficient
Remark	"ENTITY:WBbt:0005672(AWC)|GO:0009855(determination of bilateral asymmetry)"
Remark	"QUALITY:PATO:0001507(disrupted) NOT"
Remark	"Genotype \"unc-36(e251); Is[str-2::GFP]; Ex[odr-3::unc-36]\""
Remark	"Published_as unc-36"
Remark	"Similar rescue and mosaic overexpression experiments were conducted with the calcium channel genes unc-36 (alpha2 delta subunit) and unc-2 (CaV2 alpha1 subunit). Expression of either gene under the AWC-selective odr-3 promoter rescued AWC asymmetry of the corresponding mutant. Thus, the calcium channels are likely to function within AWC neurons."
Reference	"WBPaper00031175"


Anatomy_function : "WBbtf0544"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001661"	Autonomous
Gene	"WBGene00006742"
Involved	"WBbt:0005672"	Sufficient
Remark	"ENTITY:WBbt:0005672(AWC)|GO:0009855(determination of bilateral asymmetry)"
Remark	"QUALITY:PATO:0001507(disrupted) NOT"
Remark	"Genotype \"unc-2(lj1); Is[str-2::GFP]; Ex[odr-3::unc-2]\""
Remark	"Published_as unc-2"
Remark	"Similar rescue and mosaic overexpression experiments were conducted with the calcium channel genes unc-36 (alpha2 delta subunit) and unc-2 (CaV2 alpha1 subunit). Expression of either gene under the AWC-selective odr-3 promoter rescued AWC asymmetry of the corresponding mutant. Thus, the calcium channels are likely to function within AWC neurons."
Reference	"WBPaper00031175"


Anatomy_function : "WBbtf0545"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001661"	Autonomous
Gene	"WBGene00006772"
Involved	"WBbt:0005833"	Sufficient
Remark	"ENTITY:WBbt:0005833(AWC-OFF)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0002052(decreased occurrence) NOT"
Remark	"For both unc-36 and unc-2, mosaic animals with a single rescued AWC had the wild-type asymmetric phenotype: the rescued cell always became AWCOFF, and the mutant cell always became AWCON. This result was substantially different from the result with downstream kinases such as unc-43, where a single rescued AWC randomly became AWCON or AWCOFF, and the mutant cell always became AWCON. The difference suggests that unc-36 and unc-2 influence the coordinated AWCON/ AWCOFF decision."
Remark	"Genotype \"unc-36(e251); Is[str-2::GFP]; Ex[odr-3::unc-36]\""
Remark	"Published_as unc-36"
Reference	"WBPaper00031175"


Anatomy_function : "WBbtf0546"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001661"	Nonautonomous
Gene	"WBGene00006772"
Involved	"WBbt:0005832"	Sufficient
Remark	"ENTITY:WBbt:0005832(AWC-ON)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0002051(increased occurrence) NOT"
Remark	"For both unc-36 and unc-2, mosaic animals with a single rescued AWC had the wild-type asymmetric phenotype: the rescued cell always became AWCOFF, and the mutant cell always became AWCON. This result was substantially different from the result with downstream kinases such as unc-43, where a single rescued AWC randomly became AWCON or AWCOFF, and the mutant cell always became AWCON. The difference suggests that unc-36 and unc-2 influence the coordinated AWCON/ AWCOFF decision."
Remark	"Genotype \"unc-36(e251); Is[str-2::GFP]; Ex[odr-3::unc-36]\""
Remark	"Published_as unc-36"
Reference	"WBPaper00031175"


Anatomy_function : "WBbtf0547"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001661"	Autonomous
Gene	"WBGene00006742"
Involved	"WBbt:0005833"	Sufficient
Remark	"ENTITY:WBbt:0005833(AWC-OFF)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0002052(decreased occurrence) NOT"
Remark	"For both unc-36 and unc-2, mosaic animals with a single rescued AWC had the wild-type asymmetric phenotype: the rescued cell always became AWCOFF, and the mutant cell always became AWCON. This result was substantially different from the result with downstream kinases such as unc-43, where a single rescued AWC randomly became AWCON or AWCOFF, and the mutant cell always became AWCON. The difference suggests that unc-36 and unc-2 influence the coordinated AWCON/ AWCOFF decision."
Remark	"Genotype \"unc-2(lj1); Is[str-2::GFP]; Ex[odr-3::unc-2]\""
Remark	"Published_as unc-2"
Reference	"WBPaper00031175"


Anatomy_function : "WBbtf0548"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000717"
Gene	"WBGene00000195"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0030968(endoplasmic reticulum unfolded protein response)|WBGene00000024(abu-1)|WBGene00000030(abu-7)|WBGene00000031(abu-8)|WBGene00004174(abu-14)|WBGene00004099(abu-15)|GO:0010467(gene expression)"
Remark	"QUALITY:PATO:0000470(increased) NOT"
Remark	"Genotype \"arr-1(ok401); Ex[pVS4(Punc-119::arr-1::gfp)]\""
Remark	"Published_as arr-1"
Remark	"We found that five abu genes were upregulated in arr-1 (ok401) animals when exposed to P. aeruginosa. The upregulation of abu genes was rescued by ARR-1 expression in the nervous system, indicating that neural ARR-1 regulates this non-canonical UPR pathway."
Reference	"WBPaper00041568"


Anatomy_function : "WBbtf0549"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001014"
Gene	"WBGene00000195"
Involved	"WBbt:0003679"	Sufficient
Remark	"ARR-1::GFP expressed under the regulation of a pan neuronal promoter unc-119 also fully rescued the ERP phenotype of arr-1(ok401) animals. Native or pan neuronal expression of ARR-1 also rescued the reduced accumulation of P. aeruginosa phenotype exhibited by arr-1(ok401) animals."
Remark	"ENTITY:WBbt:0007833(organism)|GO:0042742(defense response to bacterium)|NEWT:287(Pseudomonas aeruginosa)"
Remark	"QUALITY:PATO:0000470(increased) NOT"
Remark	"Genotype \"arr-1(ok401); Ex[pVS4(Punc-119::arr-1::gfp)]\""
Remark	"Published_as arr-1"
Reference	"WBPaper00041568"


Anatomy_function : "WBbtf0550"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001661"	Nonautonomous
Gene	"WBGene00006742"
Involved	"WBbt:0005833"	Sufficient
Remark	"ENTITY:WBbt:0005832(AWC-ON)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0002051(increased occurrence)"
Remark	"For both unc-36 and unc-2, mosaic animals with a single rescued AWC had the wild-type asymmetric phenotype: the rescued cell always became AWCOFF, and the mutant cell always became AWCON. This result was substantially different from the result with downstream kinases such as unc-43, where a single rescued AWC randomly became AWCON or AWCOFF, and the mutant cell always became AWCON. The difference suggests that unc-36 and unc-2 influence the coordinated AWCON/ AWCOFF decision. The rescue of the unc-2 mutant cell in these mosaics is particularly informative. unc-2 has an incompletely penetrant phenotype; in unc-2 controls, 33% of animals have one AWCOFF neuron, and 4% have two AWCOFF neurons, so in total approximately 20% of all unc-2 mutant AWCs became AWCOFF. In unc-2 mosaics with one rescued AWC, fewer than 5% of the unc-2(-) AWCs became AWCOFF, indicating that the unc-2(-) AWC neuron was affected by the rescued AWC on the contralateral side."
Remark	"Genotype \"unc-2(lj1); Is[str-2::GFP]; Ex[odr-3::unc-2]\""
Remark	"Published_as unc-2"
Reference	"WBPaper00031175"


Anatomy_function : "WBbtf0551"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001014"
Gene	"WBGene00000195"
Not_involved	"WBbt:0005665"	Insufficient
Not_involved	"WBbt:0005666"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0042742(defense response to bacterium)|NEWT:287(Pseudomonas aeruginosa)"
Remark	"QUALITY:PATO:0000470(increased)"
Remark	"Genotype \"arr-1(ok401); Ex[pVS5(Psra-6::arr-1::gfp)]\""
Remark	"Published_as arr-1"
Remark	"no differences in survival or bacterial accumulation were observed between arr-1(ok401) and arr-1(ok401) animals expressing ARR-1 under the regulation of the sra-6 promoter, which drives ARR-1 expression to neurons ASH and ASI."
Reference	"WBPaper00041568"


Anatomy_function : "WBbtf0552"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000717"
Gene	"WBGene00000195"
Not_involved	"WBbt:0005665"	Insufficient
Not_involved	"WBbt:0005666"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0030968(endoplasmic reticulum unfolded protein response)|WBGene00000024(abu-1)|WBGene00000030(abu-7)|WBGene00000031(abu-8)|WBGene00004174(abu-14)|WBGene00004099(abu-15)|GO:0010467(gene expression)"
Remark	"QUALITY:PATO:0000470(increased)"
Remark	"Genotype \"arr-1(ok401); Ex[pVS5(Psra-6::arr-1::gfp)]\""
Remark	"Neither did the expression of ARR-1 (under the regulation of the sra-6 promoter) further enhance the upregulation of abu genes in arr-1(ok401) animals,"
Remark	"Published_as arr-1"
Reference	"WBPaper00041568"


Anatomy_function : "WBbtf0553"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001014"
Gene	"WBGene00000195"
Involved	"WBbt:0003927"	Sufficient
Involved	"WBbt:0004096"	Sufficient
Involved	"WBbt:0006846"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0042742(defense response to bacterium)|NEWT:287(Pseudomonas aeruginosa)"
Remark	"QUALITY:PATO:0000470(increased) NOT"
Remark	"Genotype \"arr-1(ok401); Ex[pVS6(Pgcy-32::arr-1::gfp)]\""
Remark	"Published_as arr-1"
Remark	"the ERP phenotype of arr-1(ok401) was partially rescued by expression of ARR-1 under the control of the gcy-32 promoter, which drives its expression to AQR, PQR, and URX neurons."
Reference	"WBPaper00041568"


Anatomy_function : "WBbtf0554"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000717"
Gene	"WBGene00000195"
Involved	"WBbt:0003927"	Sufficient
Involved	"WBbt:0004096"	Sufficient
Involved	"WBbt:0006846"	Sufficient
Remark	"ARR-1 expression (under the control of gcy-32 promoter) in arr-1(ok401) animals rescued the up regulation of only 1 out of 5 abu genes, suggesting that ARR-1 function in AQR, PQR, and URX neurons only plays a small role in the control of abu genes."
Remark	"ENTITY:WBbt:0007833(organism)|GO:0030968(endoplasmic reticulum unfolded protein response)|WBGene00004174(abu-14)|GO:0010467(gene expression)"
Remark	"QUALITY:PATO:0000470(increased) NOT"
Remark	"Genotype \"arr-1(ok401); Ex[pVS6(Pgcy-32::arr-1::gfp)]\""
Remark	"Published_as arr-1"
Reference	"WBPaper00041568"


Anatomy_function : "WBbtf0555"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001014"
Gene	"WBGene00000195"
Involved	"WBbt:0005660"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0042742(defense response to bacterium)|NEWT:287(Pseudomonas aeruginosa)"
Remark	"QUALITY:PATO:0000470(increased) NOT"
Remark	"Genotype \"arr-1(ok401); Ex[pVS7(Psrh-142::arr-1::gfp)]\""
Remark	"Published_as arr-1"
Remark	"We found that while ARR-1 expression under the regulation of the srh-142 promoter, which drives ARR-1 expression to ADF neurons, slightly rescued the extended lifespan of arr-1(ok401) animals (Fig. 5A), it rescued the ERP phenotype of arr-1(ok401) animals more strongly."
Reference	"WBPaper00041568"


Anatomy_function : "WBbtf0556"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000717"
Gene	"WBGene00000195"
Involved	"WBbt:0005660"	Sufficient
Remark	"ARR-1 expression in ADF neurons also partially rescued the enhanced expression of abu genes."
Remark	"ENTITY:WBbt:0007833(organism)|GO:0030968(endoplasmic reticulum unfolded protein response)|WBGene00000024(abu-1)|WBGene00000030(abu-7)|WBGene00004174(abu-14)|GO:0010467(gene expression)"
Remark	"QUALITY:PATO:0000470(increased) NOT"
Remark	"Genotype \"arr-1(ok401); Ex[pVS7(Psrh-142::arr-1::gfp)]\""
Remark	"Published_as arr-1"
Reference	"WBPaper00041568"


Anatomy_function : "WBbtf0557"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001014"
Gene	"WBGene00000195"
Involved	"WBbt:0005662"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0042742(defense response to bacterium)|NEWT:287(Pseudomonas aeruginosa)"
Remark	"QUALITY:PATO:0000470(increased) NOT"
Remark	"Genotype \"arr-1(ok401); Ex[pVS(Pgcy-8::arr-1::gfp)]\""
Remark	"Published_as arr-1"
Remark	"We found that while ARR-1 activity driven to AFD neurons by the gcy-8 promoter had no effect on the extended lifespan of arr-1(ok401) animals (Fig. 6A), it strongly rescued their ERP phenotype."
Reference	"WBPaper00041568"


Anatomy_function : "WBbtf0558"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001014"
Gene	"WBGene00000195"
Involved	"WBbt:0005662"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0030968(endoplasmic reticulum unfolded protein response)|WBGene00000024(abu-1)|WBGene00000030(abu-7)|WBGene00000031(abu-8)|WBGene00004174(abu-14)|WBGene00004099(abu-15)|GO:0010467(gene expression)"
Remark	"QUALITY:PATO:0000470(increased) NOT"
Remark	"Genotype \"arr-1(ok401); Ex[pVS(Pgcy-8::arr-1::gfp)]\""
Remark	"In addition, ARR-1 activity in AFD neurons strongly rescued the enhanced expression of abu genes."
Remark	"Published_as arr-1"
Reference	"WBPaper00041568"


Anatomy_function : "WBbtf0559"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001661"	Autonomous
Gene	"WBGene00044508"
Involved	"WBbt:0005672"	Sufficient
Remark	"ENTITY:WBbt:0005672(AWC)|GO:0009855(determination of bilateral asymmetry)"
Remark	"QUALITY:PATO:0001507(disrupted)"
Remark	"Genotype \"nsy-7(tm3080); Ex[podr-3::C18F3.4]\""
Remark	"Published_as nsy-7"
Remark	"When expressed in both AWC neurons of nsy-7 (tm3080) mutants under the AWC-selective odr-3 promoter, C18F3.4 cDNAs caused an overexpression phenotype opposite to the nsy-7 mutant phenotype. Both AWCs in these transgenic animals expressed str-2 and not srsx-3, exhibiting the properties of AWCON cells (Fig. 2C). These results suggest that C18F3.4 functions in AWC to regulate expression of str-2 and srsx-3 and confer the AWCON identity."
Reference	"WBPaper00032896"


Anatomy_function : "WBbtf0560"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001661"	Autonomous
Gene	"WBGene00006526"
Involved	"WBbt:0005672"	Sufficient
Remark	"ENTITY:WBbt:0005672(AWC)|WBGene00022408(srsx-3)|GO:0010467(gene expression)"
Remark	"QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"tax-4(ky791); kyIs408[srsx-3::GFP; str-2::dsRed; elt-2::GFP]; kyEx3447[odr-3::TAX-4; elt-2::mCherry]\""
Remark	"Published_as tax-4"
Remark	"To ask where tax-4 acts to regulate srsx-3 expression, we expressed the tax-4 cDNA in AWC or ASI in a tax-4(ky791) mutant background. AWC-selective expression of TAX-4 rescued the srsx-3 expression defect of tax-4(ky791) mutants, but ASI expression did not."
Reference	"WBPaper00037048"


Anatomy_function : "WBbtf0561"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001661"
Gene	"WBGene00006526"
Not_involved	"WBbt:0005666"	Insufficient
Remark	"ENTITY:WBbt:0005672(AWC)|WBGene00022408(srsx-3)|GO:0010467(gene expression)"
Remark	"QUALITY:PATO:0001997(reduced)"
Remark	"Genotype \"tax-4(ky791); kyIs408[srsx-3::GFP; str-2::dsRed; elt-2::GFP]; kyEx3443 [str-3::TAX-4; elt-2::mCherry]\""
Remark	"Published_as tax-4"
Remark	"To ask where tax-4 acts to regulate srsx-3 expression, we expressed the tax-4 cDNA in AWC or ASI in a tax-4(ky791) mutant background. AWC-selective expression of TAX-4 rescued the srsx-3 expression defect of tax-4(ky791) mutants, but ASI expression did not."
Reference	"WBPaper00037048"


Anatomy_function : "WBbtf0562"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001661"	Autonomous
Gene	"WBGene00000897"
Involved	"WBbt:0005672"	Sufficient
Remark	"ENTITY:WBbt:0005672(AWC)|WBGene00022408(srsx-3)|GO:0010467(gene expression)"
Remark	"QUALITY:PATO:0001997(reduced) NOT"
Remark	"Expression of DAF-1 in AWC rescued the srsx-3 expression defect of daf-1(m40) mutants, suggesting that TGF-beta signals directly to AWC to maintain receptor gene expression."
Remark	"Genotype \"daf-1(m40); kyIs408[srsx-3::GFP; str-2::dsRed; elt-2::GFP]; kyEx3180[odr-3::DAF-1; elt-2::mCherry]\""
Remark	"Published_as daf-1"
Reference	"WBPaper00037048"


Anatomy_function : "WBbtf0563"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001661"	Autonomous
Gene	"WBGene00018786"
Involved	"WBbt:0005672"	Sufficient
Remark	"ENTITY:WBbt:0005672(AWC)|WBGene00022408(srsx-3)|GO:0010467(gene expression)"
Remark	"QUALITY:PATO:0001997(reduced)"
Remark	"Expression of DAF-1 in AWC rescued the srsx-3 expression defect of daf-1(m40) High-copy odr-3::hmbx-1 transgenes repressed srsx-3 in wild-type and tm1274 backgrounds."
Remark	"Genotype \"Ex[odr-3::hmbx-1]\""
Remark	"Published_as hmbx-1"
Reference	"WBPaper00037048"


Anatomy_function : "WBbtf0564"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001661"	Nonautonomous
Gene	"WBGene00018786"
Involved	"WBbt:0005118"	Sufficient
Involved	"WBbt:0005663"	Sufficient
Involved	"WBbt:0007807"	Sufficient
Involved	"WBbt:0007808"	Sufficient
Involved	"WBbt:0005664"	Sufficient
Involved	"WBbt:0005660"	Sufficient
Involved	"WBbt:0005661"	Sufficient
Involved	"WBbt:0005665"	Sufficient
Involved	"WBbt:0005666"	Sufficient
Involved	"WBbt:0005667"	Sufficient
Involved	"WBbt:0005668"	Sufficient
Remark	"ENTITY:WBbt:0005832(AWC-ON)|WBGene00022408(srsx-3)|GO:0010467(gene expression)"
Remark	"QUALITY:PATO:0000628(ectopic)"
Remark	"Expression of hmbx-1 under the osm-3 promoter, which drives expression in 26 chemosensory neurons but not in AWC (Tabish et al. 1995), resulted in ectopic expression of srsx-3 in AWC-ON in some animals."
Remark	"Genotype \"kyIs408[srsx-3::GFP; str-2::dsRed; elt-2::GFP]; kyEx3390[osm-3::HMBX-1;elt-2::mCherry]\""
Remark	"Published_as hmbx-1"
Reference	"WBPaper00037048"


Anatomy_function : "WBbtf0565"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001739"
Gene	"WBGene00011908"
Not_involved	"WBbt:0007846"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|WBls:0000041(adult)|GO:0007568(aging)|PATO:0000050(life span)"
Remark	"QUALITY:PATO:0000499(decreased duration)"
Remark	"Genotype \"pash-1(mj100); Ex[col-10::pash-1::gfp::unc-54]\""
Remark	"Published_as pash-1"
Remark	"We generated transgenes placing expression of PASH-1:GFP under control of various tissue-specific promoters. Rescue constructs expressed in the hypodermis, pharyngeal muscle, or gut did not increase lifespan."
Reference	"WBPaper00041677"


Anatomy_function : "WBbtf0566"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001739"
Gene	"WBGene00011908"
Not_involved	"WBbt:0005451"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|WBls:0000041(adult)|GO:0007568(aging)|PATO:0000050(life span)"
Remark	"QUALITY:PATO:0000499(decreased duration)"
Remark	"Genotype \"pash-1(mj100); Ex[myo-2::pash-1::gfp::unc-54]\""
Remark	"Published_as pash-1"
Remark	"We generated transgenes placing expression of PASH-1:GFP under control of various tissue-specific promoters. Rescue constructs expressed in the hypodermis, pharyngeal muscle, or gut did not increase lifespan."
Reference	"WBPaper00041677"


Anatomy_function : "WBbtf0567"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001739"
Gene	"WBGene00011908"
Not_involved	"WBbt:0005792"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|WBls:0000041(adult)|GO:0007568(aging)|PATO:0000050(life span)"
Remark	"QUALITY:PATO:0000499(decreased duration)"
Remark	"Genotype \"pash-1(mj100); Ex[ges-1::pash-1::gfp::unc-54]\""
Remark	"Published_as pash-1"
Remark	"We generated transgenes placing expression of PASH-1:GFP under control of various tissue-specific promoters. Rescue constructs expressed in the hypodermis, pharyngeal muscle, or gut did not increase lifespan."
Reference	"WBPaper00041677"


Anatomy_function : "WBbtf0568"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001739"
Gene	"WBGene00011908"
Involved	"WBbt:0006804"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|WBls:0000041(adult)|GO:0007568(aging)|PATO:0000050(life span)"
Remark	"QUALITY:PATO:0000499(decreased duration) NOT"
Remark	"Genotype \"pash-1(mj100); Ex[myo-3::pash-1::gfp::unc-54]\""
Remark	"Published_as pash-1"
Remark	"We generated transgenes placing expression of PASH-1:GFP under control of various tissue-specific promoters. Rescue constructs expressed in the hypodermis, pharyngeal muscle, or gut did not increase lifespan, while rescue constructs expressed in body wall muscle had a marginal effect."
Reference	"WBPaper00041677"


Anatomy_function : "WBbtf0569"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001739"
Gene	"WBGene00011908"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|WBls:0000041(adult)|GO:0007568(aging)|PATO:0000050(life span)"
Remark	"QUALITY:PATO:0000499(decreased duration) NOT"
Remark	"Genotype \"pash-1(mj100); Ex[sng-1::pash-1::gfp]\""
Remark	"Published_as pash-1"
Remark	"We generated transgenes placing expression of PASH-1:GFP under control of various tissue-specific promoters. ... Expression of PASH-1::GFP specifically in neurons significantly increased lifespan."
Reference	"WBPaper00041677"


Anatomy_function : "WBbtf0570"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001739"
Gene	"WBGene00011908"
Involved	"WBbt:0007846"	Sufficient
Involved	"WBbt:0006804"	Sufficient
Involved	"WBbt:0005451"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|WBls:0000041(adult)|GO:0007568(aging)|PATO:0000050(life span)"
Remark	"QUALITY:PATO:0000499(decreased duration) NOT"
Remark	"Genotype \"pash-1(mj100); Ex[col-10::pash-1::gfp::unc-54 myo-2::pash-1::gfp::unc-54 myo-3::pash-1::gfp::unc-54]\""
Remark	"Published_as pash-1"
Remark	"We generated transgenes placing expression of PASH-1:GFP under control of various tissue-specific promoters. ... a transgene expressed in both hypodermis and muscle is sufficient to increase lifespan, although to a reduced extend compared with neuronal rescue."
Reference	"WBPaper00041677"


Anatomy_function : "WBbtf0571"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001661"	Autonomous
Gene	"WBGene00000248"
Involved	"WBbt:0005672"	Sufficient
Remark	"ENTITY:WBbt:0005672(AWC)|GO:0007368(left-right asymmetry)|GO:0001708(cell fate specification)|GO:0042493(response to drug)|CHEBI:34892(Nocodazole)"
Remark	"QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"ben-1(e1880); Ex[odr-3p::ben-1]\""
Remark	"Loss-of-function mutations in ben-1, which encodes a beta-tubulin, confer resistance to benzimidazoles such as nocodazole and benomyl (Driscoll et al., 1989). To determine whether the 2AWCON phenotype is due to disruption of microtubules, we examined the effect of nocodazole on ben-1 mutants. ben-1(e1880) mutants showed wild-type expression of str-2, and treatment of ben-1(e1880) mutant embryos with nocodazole did not cause a 2AWCON phenotype (Table 1, rows d and e). However, expression of wild-type ben-1 gene primarily in AWC using an odr-3 promoter (Roayaie et al., 1998) restored the susceptibility of ben-1(e1880) mutants to nocodazole in the generation of 2AWCON phenotype."
Remark	"Published_as ben-1"
Reference	"WBPaper00039901"


Anatomy_function : "WBbtf0572"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000005"
Gene	"WBGene00006830"
Involved	"WBbt:0007810"	Sufficient
Remark	"ENTITY:WBbt:0007849(hermaphrodite)|WBls:0000041(adult)|GO:0018991(oviposition)|WBbt:0005821(vulval muscle)|GO:0006936(muscle contraction)"
Remark	"QUALITY:PATO:0000760(hyperactive) NOT"
Remark	"Genotype \"unc-103(sy673, e1597dm); Ex[myo-3::unc-103e]\""
Remark	"Published_as unc-103"
Remark	"We found that re-expression of the vulval muscle-expressed E isoform of ERG in vulval muscle using the muscle-specific myo-3 promoter fully rescued the hyperactive egg-laying defect of ERG-null mutants."
Reference	"WBPaper00041908"


Anatomy_function : "WBbtf0573"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000005"
Gene	"WBGene00006830"
Not_involved	"WBbt:0006830"
Remark	"ENTITY:WBbt:0007849(hermaphrodite)|WBls:0000041(adult)|GO:0018991(oviposition)|WBbt:0005821(vulval muscle)|GO:0006936(muscle contraction)"
Remark	"QUALITY:PATO:0000760(hyperactive)"
Remark	"Genotype \"unc-103(sy673, e1597dm); Ex[tph-1::unc-103f]\""
Remark	"Published_as unc-103"
Reference	"WBPaper00041908"


Anatomy_function : "WBbtf0574"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000005"
Gene	"WBGene00006830"
Involved	"WBbt:0007810"	Necessary
Remark	"ENTITY:WBbt:0007849(hermaphrodite)|WBls:0000041(adult)|GO:0018991(oviposition)|WBbt:0005821(vulval muscle)|GO:0006936(muscle contraction)"
Remark	"QUALITY:PATO:0000760(hyperactive)"
Remark	"Expression of DN-ERG in muscle caused hyperactive egg-laying."
Remark	"Genotype \"Ex[myo-3::unc-103(dn)]\""
Remark	"Published_as unc-103"
Reference	"WBPaper00041908"


Anatomy_function : "WBbtf0575"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000005"
Gene	"WBGene00006830"
Involved	"WBbt:0006830"	Necessary
Remark	"ENTITY:WBbt:0007849(hermaphrodite)|WBls:0000041(adult)|GO:0018991(oviposition)|WBbt:0005821(vulval muscle)|GO:0006936(muscle contraction)"
Remark	"QUALITY:PATO:0000760(hyperactive)"
Remark	"Expression of DN-ERG in the HSN caused a significant reduction in the number of unlaid eggs, suggesting that ERG does regulate the electrical excitability of the HSN. However, this phenotype was weaker than that seen for muscle-specific inactivation of ERG."
Remark	"Genotype \"Ex[tph-1::unc-103(dn)]\""
Remark	"Published_as unc-103"
Reference	"WBPaper00041908"


Anatomy_function : "WBbtf0576"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000005"
Gene	"WBGene00001648"
Not_involved	"WBbt:0006830"	Unnecessary
Remark	"ENTITY:WBbt:0007849(hermaphrodite)|WBls:0000041(adult)|GO:0018991(oviposition)|WBbt:0005821(vulval muscle)|GO:0006936(muscle contraction)"
Remark	"QUALITY:PATO:0000760(hyperactive)"
Remark	"Genotype \"goa-1(n363); egl-1\""
Remark	"Published_as goa-1"
Remark	"To determine whether lack of Goa-1 in the vulva muscles is sufficient to cause hyperactive egg laying, we examined the egg laying behavior of goa-1;egl-1 double mutants. Mutations in the egl-1 gene cause the HSN neurons to die. Because the goa-1(n363);egl-1 mutants continue to lay eggs hyperactively, we conclude that goa-1 in the vulva muscles to inhibit egg laying."
Reference	"WBPaper00002141"


Anatomy_function : "WBbtf0577"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0001066"
Involved	"WBbt:0006830"	Necessary
Remark	"By tracking the behavior of animals lacking both HSNs, we found that elimination of the HSNs did not qualitatively alter the pattern of egg laying: eggs were still laid in clusters, and the intervals between clusters and between egg-laying events within a cluster were still exponentially distributed. However, HSN ablation did cause a substantial lengthening of the inactive phase, which led to a slower overall rate of egg laying."
Remark	"ENTITY:WBbt:0007849(hermaphrodite)|WBls:0000041(adult)|GO:0018991(oviposition)"
Remark	"QUALITY:PATO:PATO:0000381(infrequent)"
Remark	"Genotype \"egl-1(n986)\""
Reference	"WBPaper00003151"


Anatomy_function : "WBbtf0578"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001066"
Involved	"WBbt:0006830"	Necessary
Remark	"By tracking the behavior of animals lacking both HSNs, we found that elimination of the HSNs did not qualitatively alter the pattern of egg laying: eggs were still laid in clusters, and the intervals between clusters and between egg-laying events within a cluster were still exponentially distributed. However, HSN ablation did cause a substantial lengthening of the inactive phase, which led to a slower overall rate of egg laying."
Remark	"ENTITY:WBbt:0007849(hermaphrodite)|WBls:0000041(adult)|GO:0018991(oviposition)"
Remark	"QUALITY:PATO:PATO:0000381(low frequency)"
Reference	"WBPaper00003151"


Anatomy_function : "WBbtf0579"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001858"
Not_involved	"WBbt:0006834"	Unnecessary
Remark	"By contrast, mock-ablated and RIC-ablated animals showed a normal backing response and had no defects in the suppression of head oscillations in response to anterior touch."
Remark	"ENTITY:WBbt:0007833(organism)|GO:0009612(response to mechanical stimulus)|PATO:0002052(decreased occurrence)|WBbt:0005739(head)|GO:0050881(movement)|GO:0014703(oscillatory muscle contraction)"
Remark	"QUALITY:PATO:0002052(decreased occurrence) NOT"
Reference	"WBPaper00025096"


Anatomy_function : "WBbtf0580"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001858"
Involved	"WBbt:0005842"	Necessary
Remark	"AVA-ablated animals back in response to anterior touch, but backing is uncoordinated (Chalfie et al., 1985). We found that head oscillations were not suppressed in response to anterior touch in AVA-ablated animals, suggesting that the gap junctions between the RIM and AVA neurons are important in linking the touch response to the suppression of head oscillations."
Remark	"ENTITY:WBbt:0007833(organism)|GO:0009612(response to mechanical stimulus)|PATO:0002052(decreased occurrence)|WBbt:0005739(head)|GO:0050881(movement)|GO:0014703(oscillatory muscle contraction)"
Remark	"QUALITY:PATO:0002052(decreased occurrence)"
Reference	"WBPaper00025096"


Anatomy_function : "WBbtf0581"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001858"
Not_involved	"WBbt:0006819"	Unnecessary
Remark	"By contrast, AVE-ablated animals showed a normal backing response and normally suppressed head oscillation in response to anterior touch."
Remark	"ENTITY:WBbt:0007833(organism)|GO:0009612(response to mechanical stimulus)|PATO:0002052(decreased occurrence)|WBbt:0005739(head)|GO:0050881(movement)|GO:0014703(oscillatory muscle contraction)"
Remark	"QUALITY:PATO:0002052(decreased occurrence) NOT"
Reference	"WBPaper00025096"


Anatomy_function : "WBbtf0582"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000315"
Involved	"WBbt:0005835"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0009612(response to mechanical stimulus)|PATO:0002052(decreased occurrence)|GO:0043057(backward movement"
Remark	"QUALITY:PATO:0002052(decreased occurrence)"
Remark	"We found that animals in which the tyraminergic RIMs were ablated had an impaired backing minergic RIMs were ablated had an impaired backing."
Reference	"WBPaper00025096"


Anatomy_function : "WBbtf0583"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000315"
Not_involved	"WBbt:0006834"	Unnecessary
Remark	"By contrast, mock-ablated and RIC-ablated animals showed a normal backing response."
Remark	"ENTITY:WBbt:0007833(organism)|GO:0009612(response to mechanical stimulus)|PATO:0002052(decreased occurrence)|GO:0043057(backward movement"
Remark	"QUALITY:PATO:0002052(decreased occurrence) NOT"
Reference	"WBPaper00025096"


Anatomy_function : "WBbtf0584"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001858"
Involved	"WBbt:0005835"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0009612(response to mechanical stimulus)|PATO:0002052(decreased occurrence)|WBbt:0005739(head)|GO:0050881(movement)|GO:0014703(oscillatory muscle contraction)"
Remark	"QUALITY:PATO:0002052(decreased occurrence)"
Remark	"We found that animals in which the tyraminergic RIMs were ablated had an impaired backing response to anterior touch and failed to suppress head oscillations."
Reference	"WBPaper00025096"


Anatomy_function : "WBbtf0585"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001858"
Involved	"WBbt:0006818"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0009612(response to mechanical stimulus)|PATO:0002052(decreased occurrence)|WBbt:0005739(head)|GO:0050881(movement)|GO:0014703(oscillatory muscle contraction)"
Remark	"QUALITY:PATO:0002052(decreased occurrence)"
Remark	"To test the role of the AVD neurons in coupling the touch response to the suppression of head oscillations, we ablated the AVD neurons. Five of seven AVD-ablated animals failed to suppress head oscillations in response to anterior touch."
Reference	"WBPaper00025096"


Anatomy_function : "WBbtf0586"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000203"
Gene	"WBGene00000195"
Involved	"WBbt:0005672"	Sufficient
Involved	"WBbt:0005670"	Sufficient
Involved	"WBbt:0005671"	Sufficient
Involved	"WBbt:0005665"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0006935(chemotaxis)|CHEBI:15837(isoamyl alcohol)|GO:0023058(adaptation)"
Remark	"QUALITY:PATO:0000460(defective)"
Remark	"Genotype \"arr-1(ok401); Ex[ODR-3::ARR-1] \""
Remark	"Published_as arr-1"
Remark	"To determine whether the defects in adaptation in arr-1(ok401) animals were because of the loss of ARR-1 in the chemosensory neurons, 2.7 kb of the odr-3 promoter was used to drive expression of wild-type ARR-1 (ODR-3::WT) or C-terminally truncated ARR-1 (ODR-3::1-368) in the AWC neurons of arr-1(ok401) null mutants. These transgenic strains were then tested for their ability to adapt to isoamyl alcohol in both the standard adaptation and time course chemotaxis assays. The arr-1(ok401) adaptation defect was fully rescued in both transgenic strains."
Reference	"WBPaper00025173"


Anatomy_function : "WBbtf0587"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001629"
Gene	"WBGene00004776"
Involved	"WBbt:0007810"	Sufficient
Remark	"ENTITY:WBbt:0007849(hermaphrodite)|WBls:0000041(adult)|GO:0018991(oviposition)|WBbt:0005821(vulval muscle)|GO:0006936(muscle contraction)|GO:0042493(response to drug)|CHEBI:28790(serotonin)"
Remark	"QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"ser-1(ok345);Ex[Pmyo-3::ser-1]\""
Remark	"Published_as ser-1"
Remark	"We found the Pmyo-3::ser-1(+) transgene partially restored 5-HT-dependent egg laying to ser-1(ok345) animals."
Reference	"WBPaper00028900"


Anatomy_function : "WBbtf0588"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001629"
Gene	"WBGene00004776"
Involved	"WBbt:0005821"	Necessary
Remark	"A wild-type ser-1 transgene with the same3.4kB promoter that failed to express gfp in the vulval muscles also failed to rescue the egg-laying defects of the ser-1 mutant animals."
Remark	"ENTITY:WBbt:0007849(hermaphrodite)|WBls:0000041(adult)|GO:0018991(oviposition)|WBbt:0005821(vulval muscle)|GO:0006936(muscle contraction)|GO:0042493(response to drug)|CHEBI:28790(serotonin)"
Remark	"QUALITY:PATO:0001997(reduced)"
Remark	"Published_as ser-1"
Reference	"WBPaper00028900"


Anatomy_function : "WBbtf0589"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000005"
Gene	"WBGene00003839"
Remark	"ENTITY:WBbt:0007849(hermaphrodite)|WBls:0000041(adult)|GO:0018991(oviposition)|WBbt:0005821(vulval muscle)|GO:0006936(muscle contraction)"
Remark	"QUALITY:PATO:0000760(hyperactive) NOT"
Remark	"Genotype \"ocr-2(vs29);Ex[OCR-2::gfp]\""
Remark	"Published_as ocr-2"
Remark	"We transformed ocr-2(vs29) animals with an extrachromosomal transgene that expresses full-length OCR-2 fused to GFP under the control of the ocr-2 promoter and 3-prime regulatory regions. We found that animals expressing OCR-2::GFP in the uv1/utse cells were rescued for the premature egg-laying defect caused by ocr-2(vs29), while mosaic animals lacking expression in the uv1/utse cells but retaining expression in other cells were not rescued."
Reference	"WBPaper00028739"


Anatomy_function : "WBbtf0590"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000005"
Gene	"WBGene00003839"
Remark	"ENTITY:WBbt:0007849(hermaphrodite)|WBls:0000041(adult)|GO:0018991(oviposition)|WBbt:0005821(vulval muscle)|GO:0006936(muscle contraction)"
Remark	"QUALITY:PATO:0000760(hyperactive)"
Remark	"Genotype \"ocr-2(vs29);Ex[OCR-2::gfp]\""
Remark	"Published_as ocr-2"
Remark	"We transformed ocr-2(vs29) animals with an extrachromosomal transgene that expresses full-length OCR-2 fused to GFP under the control of the ocr-2 promoter and 3-prime regulatory regions. We found that animals expressing OCR-2::GFP in the uv1/utse cells were rescued for the premature egg-laying defect caused by ocr-2(vs29), while mosaic animals lacking expression in the uv1/utse cells but retaining expression in other cells were not rescued."
Reference	"WBPaper00028739"


Anatomy_function : "WBbtf0591"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001314"	Autonomous
Gene	"WBGene00003001"
Involved	"WBbt:0006918"	Sufficient
Involved	"WBbt:0006918"	Necessary
Remark	"ENTITY:WBbt:0006918(vm2)|GO:0036194(muscle arm)|GO:0048858(cell projection morphagenesis)"
Remark	"QUALITY:PATO:PATO:0000462(absent)"
Remark	"Genotype \"lin-12(wy750); Ex[lin-12::SL2::mCherry]\""
Remark	"Published_as lin-12"
Remark	"To further understand whether lin-12 is required in the vulval epithelial cells or vm2, we injected this [lin-12::SL2::mCherry fosmid] construct into the lin-12(wy750) mutant and analyzed mosaic animals in which expression of this transgene was lost in some of the tissues. ... whereas the muscle arm defect was never rescued in any of the examined animals (>50) lacking lin-12 expression in the vm2 cell."
Remark	"To further understand whether lin-12 is required in the vulval epithelial cells or vm2, we injected this [lin-12::SL2::mCherry fosmid] construct into the lin-12(wy750) mutant and analyzed mosaic animals in which expression of this transgene was lost in some of the tissues. Forty-five of 48 animals with lin-12 expressed in the vm2 cells (vm2+) showed a rescued, wild-type muscle arms."
Reference	"WBPaper00042187"


Anatomy_function : "WBbtf0592"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001314"
Gene	"WBGene00003001"
Not_involved	"WBbt:0007831"	Insufficient
Not_involved	"WBbt:0007831"	Unnecessary
Remark	"ENTITY:WBbt:0006918(vm2)|GO:0036194(muscle arm)|GO:0048858(cell projection morphagenesis)"
Remark	"QUALITY:PATO:PATO:0000462(absent)"
Remark	"Genotype \"lin-12(wy750); Ex[lin-12::SL2::mCherry]\""
Remark	"Published_as lin-12"
Remark	"To further understand whether lin-12 is required in the vulval epithelial cells or vm2, we injected this [lin-12::SL2::mCherry fosmid] construct into the lin-12(wy750) mutant and analyzed mosaic animals in which expression of this transgene was lost in some of the tissues. [...] On the contrary, lin-12 expression in vulval epithelial cells was not correlated with the rescue of the muscle arm defects."
Reference	"WBPaper00042187"


Anatomy_function : "WBbtf0593"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001314"	Nonautonomous
Gene	"WBGene00000168"
Involved	"WBbt:0006917"	Sufficient
Remark	"Cell-specific expression of apx-1 in vm1 muscle cells rescued the muscle arm defects of apx-1(wy755) mutants."
Remark	"ENTITY:WBbt:0006918(vm2)|GO:0036194(muscle arm)|GO:0048858(cell projection morphagenesis)"
Remark	"QUALITY:PATO:PATO:0000462(absent) NOT"
Remark	"Genotype \"apx-1(wy755); Ex[egl-15::apx-1 cDNA]\""
Remark	"Published_as apx-1"
Reference	"WBPaper00042187"


Anatomy_function : "WBbtf0594"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001314"	Nonautonomous
Gene	"WBGene00000168"
Involved	"WBbt:0007831"	Sufficient
Remark	"Cell-specific expression of apx-1 in secondary vulval epithelial cells [with an egl-17 promoter] rescued the muscle arm defects of apx-1(wy755) mutants."
Remark	"ENTITY:WBbt:0006918(vm2)|GO:0036194(muscle arm)|GO:0048858(cell projection morphagenesis)"
Remark	"QUALITY:PATO:PATO:0000462(absent) NOT"
Remark	"Genotype \"apx-1(wy755); Ex[egl-17::apx-1 cDNA]\""
Remark	"Published_as apx-1"
Reference	"WBPaper00042187"


Anatomy_function : "WBbtf0595"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001314"	Autonomous
Gene	"WBGene00004769"
Involved	"WBbt:0005821"	Sufficient
Remark	"ENTITY:WBbt:0006918(vm2)|GO:0036194(muscle arm)|GO:0048858(cell projection morphagenesis)"
Remark	"QUALITY:PATO:PATO:0000462(absent) NOT"
Remark	"Genotype \"sel-12(wy760); Ex[unc-103e::sel-12 cDNA]\""
Remark	"Published_as sel-12"
Remark	"To understand where sel-12 was required, we performed cell-specific rescue experiments. We found that expression of sel-12 in vulval muscle cells [with the unc-103e promoter] completely rescued the vm2 muscle arm phenotype of sel-12(wy760)."
Reference	"WBPaper00042187"


Anatomy_function : "WBbtf0596"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001314"
Gene	"WBGene00002245"
Involved	"WBbt:0005821"	Sufficient
Remark	"ENTITY:WBbt:0006918(vm2)|GO:0036194(muscle arm)|GO:0048858(cell projection morphagenesis)"
Remark	"QUALITY:PATO:PATO:0000462(absent)"
Remark	"Genotype \"Ex[unc-103e::dnLag-1]\""
Remark	"Published_as lag-1"
Remark	"specific expression of a dominant-negative lag-1 construct in the vulval muscles phenocopied the muscle arm defects observed in lin-12(wy750), apx-1(wy750) and sel-12(wy760) mutants, suggesting that the canonical LIN-12/Notch pathway is likely involved by controlling the transcription of downstream genes."
Reference	"WBPaper00042187"


Anatomy_function : "WBbtf0597"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001314"	Autonomous
Gene	"WBGene00006776"
Involved	"WBbt:0005821"	Sufficient
Remark	"ENTITY:WBbt:0006918(vm2)|GO:0036194(muscle arm)|GO:0048858(cell projection morphagenesis)"
Remark	"QUALITY:PATO:PATO:0000462(absent) NOT"
Remark	"Genotype \"unc-40(e271); Ex[unc-103e::unc-40::GFP]\""
Remark	"Published_as unc-40"
Remark	"unc-40(n324) null mutants showed specific vulval muscle arm defects with largely normal vulval muscle morphology. These defects were strongly rescued by expressing unc-40 specifically in vulval muscles [with the unc-103e promoter] in mutants."
Reference	"WBPaper00042187"


Anatomy_function : "WBbtf0598"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001314"	Autonomous
Gene	"WBGene00016539"
Involved	"WBbt:0005821"	Sufficient
Remark	"ENTITY:WBbt:0006918(vm2)|GO:0036194(muscle arm)|GO:0048858(cell projection morphagenesis)"
Remark	"QUALITY:PATO:PATO:0000462(absent) NOT"
Remark	"Genotype \"madd-2(ok2226); Ex[unc-103e::madd-2::GFP]\""
Remark	"Published_as madd-2"
Remark	"madd-2(ok2226) null mutants showed specific vulval muscle arm defects with largely normal vulval muscle morphology. These defects were strongly rescued by expressing madd-2 specifically in vulval muscles [with the unc-103e promoter] in mutants."
Reference	"WBPaper00042187"


Anatomy_function : "WBbtf0599"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000812"	Nonautonomous
Gene	"WBGene00003704"
Involved	"WBbt:0005792"	Sufficient
Remark	"ENTITY:WBbt:0007849(hermaphrodite)|WBbt:0005784(germ line)|GO:0048468(cell development)"
Remark	"QUALITY:PATO:0001997(reduced) NOT"
Remark	"Published_as nhr-114"
Remark	"To test whether nhr-114 intestinal expression supports germline development and fertility, we generated animals expressing an epitope-tagged, RNAi-insensitive nhr-114 transgene in the intestines(EV441). Next, we reduced endogenous nhr-114 by injection-mediated RNAi in EV441, leaving the RNAi-insensitive nhr-114 transgene as the only source of nhr-114 activity. In this case, recovered fully fertile animals on an OP50 diet (84%, n = 511), suggesting that somatic NHR-114 activity in the intestine might be sufficient to prevent GSC division defects and sterility."
Reference	"WBPaper00042194"


Anatomy_function : "WBbtf0600"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000812"	Nonautonomous
Gene	"WBGene00003704"
Involved	"WBbt:0008378"	Sufficient
Remark	"A significant number of fertile rrf-1(pk1417); nhr-114(RNAi) animals were recovered), indicating that preservation of somatic nhr-114 activity promotes fertility."
Remark	"ENTITY:WBbt:0007849(hermaphrodite)|WBbt:0005784(germ line)|GO:0048468(cell development)"
Remark	"QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"rrf-1(pk1417); nhr-114(RNAi)\""
Remark	"Published_as nhr-114"
Reference	"WBPaper00042194"


Anatomy_function : "WBbtf0601"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000384"	Autonomous
Gene	"WBGene00004140"
Involved	"WBbt:0003679"	Sufficient
Involved	"WBbt:0003679"	Necessary
Remark	"ENTITY:WBbt:0003832(AVM)|GO:0030424(axon)|GO:0007411(axon guidance)"
Remark	"QUALITY:PATO:0000460(defective)"
Remark	"Genotype \"ebax-1(ju699); unc-6(ev400); Ex[Pebax-1::EBAX-1]\""
Remark	"Published_as ebax-1"
Remark	"We performed mosaic analysis in unc-6; ebax-1 double mutants coexpressing a rescuing transgene Pebax-1::EBAX-1 and a coinjection marker Psur-5::SUR-5::mCherry that labels nuclei of cells carrying the transgene. We then identi&amp;#64257;ed animals speci&amp;#64257;cally losing the transgenes either in the AB lineage-derived cells (mainly neurons) or in the P1 lineage-derived cells (mainly nonneuronal cells) and scored them for AVM guidance defects. AB-loss animals showed the same severity of axon guidance defects as ebax-1; unc-6 double mutant animals. In contrast, the guidance defects in P1-loss animals were rescued by neuron-restricted expression of EBAX-1."
Reference	"WBPaper00044158"


Anatomy_function : "WBbtf0602"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000384"	Autonomous
Gene	"WBGene00004140"
Involved	"WBbt:0003679"	Sufficient
Involved	"WBbt:0003679"	Necessary
Remark	"ENTITY:WBbt:0003832(AVM)|GO:0030424(axon)|GO:0007411(axon guidance)"
Remark	"QUALITY:PATO:0000460(defective)"
Remark	"Genotype \"ebax-1(ju699); unc-40(e1430); Ex[Pebax-1::EBAX-1]\""
Remark	"Published_as ebax-1"
Remark	"We performed mosaic analysis in unc-40; ebax-1 double mutants coexpressing a rescuing transgene Pebax-1::EBAX-1 and a coinjection marker Psur-5::SUR-5::mCherry that labels nuclei of cells carrying the transgene. We then identi&amp;#64257;ed animals speci&amp;#64257;cally losing the transgenes either in the AB lineage-derived cells (mainly neurons) or in the P1 lineage-derived cells (mainly nonneuronal cells) and scored them for AVM guidance defects. AB-loss animals showed the same severity of axon guidance defects as ebax-1; unc-40 double mutant animals. In contrast, the guidance defects in P1-loss animals were rescued by neuron-restricted expression of EBAX-1."
Reference	"WBPaper00044158"


Anatomy_function : "WBbtf0603"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000384"
Gene	"WBGene00000915"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBbt:0003832(AVM)|GO:0030424(axon)|GO:0007411(axon guidance)"
Remark	"QUALITY:PATO:0000460(defective) NOT"
Remark	"Genotype \"daf-21; unc-6(ev400); Ex[Prgef-1::DAF-21]\""
Remark	"Published_as daf-21"
Remark	"daf-21 mutants showed synergistic enhancement of AVM guidance defects in the unc-6 mutant background. The enhanced defects in unc-6; daf-21 mutants were rescued by expression of DAF-21 in neurons."
Reference	"WBPaper00044158"


Anatomy_function : "WBbtf0604"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000384"	Autonomous
Gene	"WBGene00000915"
Involved	"WBbt:0005237"	Sufficient
Remark	"ENTITY:WBbt:0003832(AVM)|GO:0030424(axon)|GO:0007411(axon guidance)"
Remark	"QUALITY:PATO:0000460(defective) NOT"
Remark	"Genotype \"daf-21; unc-6(ev400); Ex[Pmec-7::DAF-21]\""
Remark	"Published_as daf-21"
Remark	"daf-21 mutants showed synergistic enhancement of AVM guidance defects in the unc-6 mutant background. The enhanced defects in unc-6; daf-21 mutants were rescued by expression of DAF-21 in touch neurons."
Reference	"WBPaper00044158"


Anatomy_function : "WBbtf0605"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000384"
Gene	"WBGene00000915"
Not_involved	"WBbt:0007810"	Insufficient
Remark	"ENTITY:WBbt:0003832(AVM)|GO:0030424(axon)|GO:0007411(axon guidance)"
Remark	"QUALITY:PATO:0000460(defective)"
Remark	"Genotype \"daf-21; unc-6(ev400); Ex[Pmyo-3::DAF-21]\""
Remark	"Published_as daf-21"
Remark	"daf-21 mutants showed synergistic enhancement of AVM guidance defects in the unc-6 mutant background. The enhanced defects in unc-6; daf-21 mutants were not rescued by expression of DAF-21 in muscles."
Reference	"WBPaper00044158"


Anatomy_function : "WBbtf0606"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000730"	Autonomous
Gene	"WBGene00012735"
Involved	"WBbt:0006598"	Necessary
Remark	"ENTITY:WBbt:0006122(MSpaaaaap)|GO:0006915(apoptotic cell death)"
Remark	"QUALITY:PATO:0000467(present) NOT"
Remark	"Genotype \"sptf-3(n4850);Ex[sptf-3-rescuing sur-5::gfp unc-119::gfp] \""
Remark	"Published_as sptf-3"
Remark	"We generated sptf-3(n4850) mutants carrying an extrachromosomal array containing an sptf-3-rescuing transgene marked with the cell-autonomous GFP reporters sur-5::gfp and unc-119::gfp. We observed 56 mosaic animals that were not rescued for the defect in M4 sister cell death but that carried the array with the sptf-3-rescuing transgene. Among these 56 animals, we found two animals that retained the array in the blastomere MSpa, the great-great-great-grandmother of the M4 sister (MSpaaaaap), but did not find any animals that retained the array in the blastomere MSpaa, the great-great-grandmother of the M4 sister, indicating that sptf-3 is required at or later than the stage of the blastomere MSpaa and seems to function cell autonomously to promote the death of the M4 sister."
Reference	"WBPaper00043906"


Anatomy_function : "WBbtf0607"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001652"	Autonomous
Gene	"WBGene00006794"
Involved	"WBbt:0004522"	Sufficient
Remark	"ENTITY:WBbt:0004522(anchor cell)|GO:0005604(basement membrane)|GO:0022411(cellular component disassembly)"
Remark	"QUALITY:PATO:0002052(decreased occurrence) NOT"
Remark	"Genotype \"qyIs224[cdh-3 > GFP::Cbrunc-60]\""
Remark	"Published_as unc-60"
Remark	"To determine if ADF/cofilin functions within the AC, we generated a construct in which the unc-60 (ADF/cofilin) transcript from the related nematode Caenorhabditis briggsae was expressed specifically in the AC. cdh-3>GFP::Cbrunc-60 restored invasion in animals treated with C. elegans unc-60a RNAi."
Reference	"WBPaper00045029"


Anatomy_function : "WBbtf0608"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000901"	Nonautonomous
Gene	"WBGene00000936"
Involved	"WBbt:0004467"	Sufficient
Remark	"ENTITY:WBbt:0003712(g1)|GO:0009653(morphogenesis)"
Remark	"QUALITY:PATO:0000460(defective) NOT"
Remark	"Genotype \"dbl-1(ev580); cuEx611[phat-3::yfp Pser-7b::dbl-1 rol-6d]\""
Remark	"Published_as dbl-1"
Remark	"We hypothesize that DBL-1 is expressed and secreted from M4 to affect gland cell morphology. To test this hypothesis, we asked if expressing dbl-1 in the M4 cell using the ser-7b promoter would rescue gland cell defects of dbl-1 and ceh-28 mutants. The ser-7b promoter is active exclusively in M4, and we have previously shown it remains active in ceh-28 mutants. ser-7b::dbl-1 partially rescued gland cell defects in both dbl-1 and ceh-28 mutants."
Reference	"WBPaper00045065"


Anatomy_function : "WBbtf0609"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000850"
Gene	"WBGene00003929"
Involved	"WBbt:0005406"	Necessary
Involved	"WBbt:0003832"	Necessary
Remark	"ENTITY:WBbt:0005739(head)|GO:0050975(sensory perception of touch)"
Remark	"QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"pat-2(ok2148);uEx829(pat-2p::pat-2, pCFJ90, mec-3p::rfp)\""
Remark	"Published_as pat-2"
Remark	"To circumvent the embryonic lethality associated with the complete loss of the focal adhesion genes, we tested touch sensitivity in animals that were mosaic for null alleles. Loss of pat-2/alpha-integrin in the anterior TRNs (the two ALM cells and the AVM cell) yielded animals that were partially insensitive to anterior touch."
Reference	"WBPaper00045249"


Anatomy_function : "WBbtf0610"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000850"
Gene	"WBGene00003930"
Involved	"WBbt:0005406"	Necessary
Involved	"WBbt:0003832"	Necessary
Remark	"ENTITY:WBbt:0005739(head)|GO:0050975(sensory perception of touch)"
Remark	"QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"pat-3(st564); uEx826(pat-3p::pat-3, pCFJ90, mec-3p::rfp)\""
Remark	"Published_as pat-3"
Remark	"To circumvent the embryonic lethality associated with the complete loss of the focal adhesion genes, we tested touch sensitivity in animals that were mosaic for null alleles. Loss of pat-3/beta-integrin in the anterior TRNs (the two ALM cells and the AVM cell) yielded animals that were partially insensitive to anterior touch."
Reference	"WBPaper00045249"


Anatomy_function : "WBbtf0611"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000850"
Gene	"WBGene00006826"
Involved	"WBbt:0005406"	Necessary
Involved	"WBbt:0003832"	Necessary
Remark	"ENTITY:WBbt:0005739(head)|GO:0050975(sensory perception of touch)"
Remark	"QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"unc-97(ra115)dpy-8(e130); uEx832(unc-97p::unc-97, pCFJ90, mec-3p::rfp)\""
Remark	"Published_as unc-97"
Remark	"To circumvent the embryonic lethality associated with the complete loss of the focal adhesion genes, we tested touch sensitivity in animals that were mosaic for null alleles. Loss of unc-97/PINCH in the anterior TRNs (the two ALM cells and the AVM cell) yielded animals that were partially insensitive to anterior touch."
Reference	"WBPaper00045249"


Anatomy_function : "WBbtf0612"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000850"
Gene	"WBGene00006836"
Involved	"WBbt:0005406"	Necessary
Involved	"WBbt:0003832"	Necessary
Remark	"ENTITY:WBbt:0005739(head)|GO:0050975(sensory perception of touch)"
Remark	"QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"unc-112(gk1); uEx824(unc-112p::unc-112, pCFJ90, mec-3p::rfp)\""
Remark	"Published_as unc-112"
Remark	"To circumvent the embryonic lethality associated with the complete loss of the focal adhesion genes, we tested touch sensitivity in animals that were mosaic for null alleles. Loss of unc-112/Mig-2 in the anterior TRNs (the two ALM cells and the AVM cell) yielded animals that were partially insensitive to anterior touch."
Reference	"WBPaper00045249"


Anatomy_function : "WBbtf0613"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000850"
Gene	"WBGene00006870"
Involved	"WBbt:0005406"	Necessary
Involved	"WBbt:0003832"	Necessary
Remark	"ENTITY:WBbt:0005739(head)|GO:0050975(sensory perception of touch)"
Remark	"QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"pat-6(st561); uEx827(pat-6p::pat-6, pCFJ90, mec-3p::rfp)\""
Remark	"Published_as pax-6"
Remark	"To circumvent the embryonic lethality associated with the complete loss of the focal adhesion genes, we tested touch sensitivity in animals that were mosaic for null alleles. Loss of pax-6/actopaxin in the anterior TRNs (the two ALM cells and the AVM cell) yielded animals that were partially insensitive to anterior touch."
Reference	"WBPaper00045249"


Anatomy_function : "WBbtf0614"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000850"
Gene	"WBGene00000102"
Involved	"WBbt:0005237"	Sufficient
Remark	"ENTITY:WBbt:0005739(head)|GO:0050975(sensory perception of touch)"
Remark	"QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"akt-1(ok525)V; uEx891(mec-17p::gfp, mec-17p::akt-1a, pCFJ90)\""
Remark	"Published_as akt-1"
Remark	"TRN-specific expression of akt-1(+) restored the anterior touch sensitivity of akt-1 animals (from 2.6 +/- 0.3 responses to 4.0 +/- 0.3responses, N >= 3, p<0.0001), indicating that the pathway was active in the TRNs."
Reference	"WBPaper00045249"


Anatomy_function : "WBbtf0615"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000850"
Involved	"WBbt:0004467"	Necessary
Involved	"WBbt:0004740"	Necessary
Remark	"ENTITY:WBbt:0005739(head)|GO:0050975(sensory perception of touch)"
Remark	"QUALITY:PATO:0001997(reduced)"
Remark	"Laser ablation of both the M4 and I5 neurons in late L4 stage animals resulted in adults whose anterior touch sensitivity mimicked the loss of ins-10 within 24 h of ablation, but whose posterior touch sensitivity did not change (data not shown). Ablation of either cell alone resulted in little or no reduction of anterior touch sensitivity compared with controls."
Reference	"WBPaper00045249"


Anatomy_function : "WBbtf0616"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000850"
Gene	"WBGene00000912"
Involved	"WBbt:0005237"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050975(sensory perception of touch)|WBbt:0005739(head)|GO:0051931(regulation of sensory perception)|PATO:0000033(concentration)|CHEBI:26710(NaCl)"
Remark	"QUALITY:PATO:0001997(reduced) NOT"
Remark	"Expressing daf-16a but not daf-16b in the TRNs of daf-16 animals caused them to reduce anterior touch sensitivity on high salt."
Remark	"Genotype \"daf-16(mgDf50)I; uEx894(mec-17p::gfp, mec-3p::daf-16a, pCFJ90)\""
Remark	"Published_as daf-16"
Reference	"WBPaper00045249"


Anatomy_function : "WBbtf0617"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000850"
Involved	"WBbt:0005663"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050975(sensory perception of touch)|WBbt:0005739(head)"
Remark	"QUALITY:PATO:0001997(reduced)"
Remark	"Genotype \"che-1(ot151) otIs114 I\""
Remark	"che-1 animals, which lack both ASE cells, have reduced anterior touch sensitivity that can be restored by TRN::pdk-1(gf), suggesting that INS-22 from the ASE cells regulates TRN touch sensitivity."
Reference	"WBPaper00045249"


Anatomy_function : "WBbtf0618"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001038"	Autonomous
Involved	"WBbt:0005784"	Sufficient
Remark	"ENTITY:WBbt:0005784(germ line)|GO:0008283(cell proliferation)"
Remark	"QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"kin-10(ok1751);glp-1(ar202gf); ugEx27[kin-10::FLAG]\""
Remark	"To determine in which tissue KIN-10 functions to inhibit the proliferative fate, we performed mosaic analysis using kin-10(ok1751); glp-1(ar202gf); ugEx27[kin-10::FLAG] animals. In mosaic gonads that have no expression in the somatic gonad (including the DTC), expression in the germline is suf&amp;#64257;cient to suppress the tumorous phenotype of the kin-10(ok1751); glp-1(ar202gf) double mutant."
Reference	"WBPaper00045273"


Anatomy_function : "WBbtf0619"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001038"
Gene	"WBGene00002196"
Involved	"WBbt:0005784"	Sufficient
Remark	"ENTITY:WBbt:0005784(germ line)|GO:0008283(cell proliferation)"
Remark	"QUALITY:PATO:0001997(reduced)"
Remark	"Genotype \"kin-10(ok1751);glp-1(ar202gf); ugEx27[kin-10::FLAG]\""
Remark	"Published_as kin-10"
Remark	"To determine in which tissue KIN-10 functions to inhibit the proliferative fate, we performed mosaic analysis using kin-10(ok1751); glp-1(ar202gf); ugEx27[kin-10::FLAG] animals. In mosaic gonads that have no expression in the somatic gonad (including the DTC), expression in the germline is suf&amp;#64257;cient to suppress the tumorous phenotype of the kin-10(ok1751); glp-1(ar202gf) double mutant."
Reference	"WBPaper00045273"


Anatomy_function : "WBbtf0620"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001739"
Gene	"WBGene00000912"
Involved	"WBbt:0005792"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|WBls:0000041(adult)|GO:0010259(multicellular organismal aging)"
Remark	"QUALITY:PATO:0000499(decreased duration) NOT"
Remark	"Genotype \"daf-2(e1370); daf-16(mu86); Ex[Pges-1::daf-16]\""
Remark	"Published_as daf-16"
Remark	"To test the idea that age-related loss of axon regeneration are separately regulated, we attempted to decouple the two phenotypes using daf-16(-) mosaic animals. We found that intestine::daf-16 animals did exhibit increased lifespan compared to controls."
Reference	"WBPaper00044735"


Anatomy_function : "WBbtf0621"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001911"
Gene	"WBGene00000912"
Not_involved	"WBbt:0005792"	Insufficient
Remark	"ENTITY:PATO:0000308(old)|WBls:0000041(adult)|WBbt:0007849(hermaphrodite)|WBbt:0005190(GABAergic neuron)|GO:0030424(axon)|GO:0031099(regeneration)"
Remark	"QUALITY:PATO:0001997(decreased number)"
Remark	"Genotype \"daf-2(e1370); daf-16(mu86); Ex[Pges-1::daf-16]\""
Remark	"Published_as daf-16"
Remark	"To test the idea that age-related loss of axon regeneration and lifespan are separately regulated, we attempted to decouple the two phenotypes using daf-16(-) mosaic animals. However, 5-day adult intestine::daf-16 animals showed a low level of axon regeneration that was similar to wild-type."
Reference	"WBPaper00044735"


Anatomy_function : "WBbtf0622"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001739"
Gene	"WBGene00000912"
Not_involved	"WBbt:0003679"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|WBls:0000041(adult)|GO:0010259(multicellular organismal aging)"
Remark	"QUALITY:PATO:0000499(decreased duration)"
Remark	"Genotype \"daf-2(e1370); daf-16(mu86); Ex[Prgef-1::daf-16]\""
Remark	"Published_as daf-16"
Remark	"We expressed wild-type daf-16 under the control of the pan-neuronal promoter Prgef-1 in daf-2(-); daf-16(-) mutants. In these animals, daf-16 is expressed only in neurons, where it is active due to the lack of daf-2. Neuronal-specific expression of daf-16 had no effect on lifespan."
Reference	"WBPaper00044735"


Anatomy_function : "WBbtf0623"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001911"
Gene	"WBGene00000912"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:PATO:0000308(old)|WBls:0000041(adult)|WBbt:0007849(hermaphrodite)|WBbt:0005190(GABAergic neuron)|GO:0030424(axon)|GO:0031099(regeneration)"
Remark	"QUALITY:PATO:0001997(decreased number) NOT"
Remark	"Genotype \"daf-2(e1370); daf-16(mu86); Ex[Prgef-1::daf-16]\""
Remark	"Published_as daf-16"
Remark	"We expressed wild-type daf-16 under the control of the pan-neuronal promoter Prgef-1 in daf-2(-); daf-16(-) mutants. In these animals, daf-16 is expressed only in neurons, where it is active due to the lack of daf-2. However, aged neuron:daf-16 animals had improved axon regeneration compared to controls, even though they did not live any longer."
Reference	"WBPaper00044735"


Anatomy_function : "WBbtf0624"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001911"	Autonomous
Gene	"WBGene00000913"
Involved	"WBbt:0005190"	Sufficient
Remark	"ENTITY:PATO:0000308(old)|WBls:0000041(adult)|WBbt:0007849(hermaphrodite)|WBbt:0005190(GABAergic neuron)|GO:0030424(axon)|GO:0031099(regeneration)"
Remark	"QUALITY:PATO:0000470(increased number) NOT"
Remark	"Genotype \"daf-18(mg198); Ex[Punc-47::daf-18cDNA]\""
Remark	"Published_as daf-18"
Remark	"We found that GABA-specific daf-18 expression (driven by the unc-47 [vesicular GABA transporter] promoter) inhibits regeneration in aged daf-18(-) mutants."
Reference	"WBPaper00044735"


Anatomy_function : "WBbtf0625"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000753"	Nonautonomous
Gene	"WBGene00000912"
Involved	"WBbt:0007846"	Sufficient
Remark	"ENTITY:WBls:0000035(L3 larva Ce)|WBbt:0007809(VPC)|GO:0051301(cell division)|WBbt:0006748(vulva)|GO:0048513(organ development)|GO:0042594(starvation response)"
Remark	"QUALITY:PATO:0002052(decreased occurrence) NOT"
Remark	"Genotype \"daf-16(mu86); qyEx292[col-12::GFP::daf-16]\""
Remark	"Only GFP::DAF-16 expression from a hypodermis-specific promoter (col-12) significantly rescued the daf-16(mu86) phenotype (reduced VPC cell division arrest upon starvation)."
Remark	"Published_as daf-16"
Reference	"WBPaper00045403"


Anatomy_function : "WBbtf0626"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000753"
Gene	"WBGene00000912"
Not_involved	"WBbt:0003679"	Insufficient
Remark	"ENTITY:WBls:0000035(L3 larva Ce)|WBbt:0007809(VPC)|GO:0051301(cell division)|WBbt:0006748(vulva)|GO:0048513(organ development)|GO:0042594(starvation response)"
Remark	"QUALITY:PATO:0002052(decreased occurrence)"
Remark	"GFP::DAF-16 expressed from tissue-specific promoters for neurons (unc-119) failed to rescue the daf-16(mu86) bypass (reduced VPC cell division arrest upon starvation) phenotype."
Remark	"Genotype \"daf-16(mu86); qyEx262[unc-119::GFP::daf-16]\""
Remark	"Published_as daf-16"
Reference	"WBPaper00045403"


Anatomy_function : "WBbtf0627"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000753"
Gene	"WBGene00000912"
Not_involved	"WBbt:0003679"	Insufficient
Remark	"ENTITY:WBls:0000035(L3 larva Ce)|WBbt:0007809(VPC)|GO:0051301(cell division)|WBbt:0006748(vulva)|GO:0048513(organ development)|GO:0042594(starvation response)"
Remark	"QUALITY:PATO:0002052(decreased occurrence)"
Remark	"GFP::DAF-16 expressed from tissue-specific promoters for neurons (unc-115) failed to rescue the daf-16(mu86) bypass (reduced VPC cell division arrest upon starvation) phenotype."
Remark	"Genotype \"daf-16(mu86); qyEx268[unc-115::GFP::daf-16]\""
Remark	"Published_as daf-16"
Reference	"WBPaper00045403"


Anatomy_function : "WBbtf0628"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000753"
Gene	"WBGene00000912"
Not_involved	"WBbt:0007810"	Insufficient
Remark	"ENTITY:WBls:0000035(L3 larva Ce)|WBbt:0007809(VPC)|GO:0051301(cell division)|WBbt:0006748(vulva)|GO:0048513(organ development)|GO:0042594(starvation response)"
Remark	"QUALITY:PATO:0002052(decreased occurrence)"
Remark	"GFP::DAF-16 expressed from tissue-specific promoters for muscles (myo-3) failed to rescue the daf-16(mu86) bypass (reduced VPC cell division arrest upon starvation) phenotype."
Remark	"Genotype \"daf-16(mu86); qyEx264[myo-3::GFP::daf-16]\""
Remark	"Published_as daf-16"
Reference	"WBPaper00045403"


Anatomy_function : "WBbtf0629"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000753"
Gene	"WBGene00000912"
Not_involved	"WBbt:0005792"	Insufficient
Remark	"ENTITY:WBls:0000035(L3 larva Ce)|WBbt:0007809(VPC)|GO:0051301(cell division)|WBbt:0006748(vulva)|GO:0048513(organ development)|GO:0042594(starvation response)"
Remark	"QUALITY:PATO:0002052(decreased occurrence)"
Remark	"GFP::DAF-16 expressed from tissue-specific promoters for intestine (ges-1) failed to rescue the daf-16(mu86) bypass (reduced VPC cell division arrest upon starvation) phenotype."
Remark	"Genotype \"daf-16(mu86); qyEx267[ges-1::GFP::daf-16]\""
Remark	"Published_as daf-16"
Reference	"WBPaper00045403"


Anatomy_function : "WBbtf0630"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000753"
Gene	"WBGene00000912"
Not_involved	"WBbt:0005792"	Unnecessary
Remark	"ENTITY:WBls:0000035(L3 larva Ce)|WBbt:0007809(VPC)|GO:0051301(cell division)|WBbt:0006748(vulva)|GO:0048513(organ development)|GO:0042594(starvation response)"
Remark	"QUALITY:PATO:0000297(arrested)"
Remark	"Genotype \"rde-1(ne219); nhx-2::rde-1\""
Remark	"Published_as daf-16"
Remark	"We carried out tissue-specific RNAi of daf-16. Targeted reduction of daf-16 in the intestine did not alter sensitivity to the removal from food."
Remark	"strain name VP303"
Reference	"WBPaper00045403"


Anatomy_function : "WBbtf0631"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000753"
Gene	"WBGene00000912"
Not_involved	"WBbt:0006804"	Unnecessary
Remark	"ENTITY:WBls:0000035(L3 larva Ce)|WBbt:0007809(VPC)|GO:0051301(cell division)|WBbt:0006748(vulva)|GO:0048513(organ development)|GO:0042594(starvation response)"
Remark	"QUALITY:PATO:0000297(arrested)"
Remark	"Genotype \"rde-1(ne219); hlh-1::rde-1\""
Remark	"Published_as daf-16"
Remark	"We carried out tissue-specific RNAi of daf-16. Targeted reduction of daf-16 in muscle did not alter sensitivity to the removal from food."
Remark	"strain name NR350"
Reference	"WBPaper00045403"


Anatomy_function : "WBbtf0632"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000753"
Gene	"WBGene00000912"
Involved	"WBbt:0007846"	Necessary
Remark	"ENTITY:WBls:0000035(L3 larva Ce)|WBbt:0007809(VPC)|GO:0051301(cell division)|WBbt:0006748(vulva)|GO:0048513(organ development)|GO:0042594(starvation response)"
Remark	"QUALITY:PATO:0000297(arrested) NOT"
Remark	"Genotype \"rde-1(ne219); lin-26::rde-1\""
Remark	"Published_as daf-16"
Remark	"We carried out tissue-specific RNAi of daf-16. Reducing daf-16 specifically in the hypodermis reproduced the phenotype of systemic loss of daf-16 (altered sensitivity to the removal from food)."
Remark	"strain name NR222"
Reference	"WBPaper00045403"


Anatomy_function : "WBbtf0633"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001661"	Autonomous
Gene	"WBGene00000995"
Involved	"WBbt:0005833"	Sufficient
Remark	"ENTITY:WBbt:0005833(AWC-OFF)|GO:0048664(neuron fate determination)|"
Remark	"GO:0035545(determination of left/right symmetry in nervous system)"
Remark	"QUALITY:PATO:0002052(decreased occurrence) NOT"
Remark	"Genotype \"die-1(w34); kyIs140(str-2p::GFP; vyEx1462[die-1::YFP ord-1p::DsRed])\""
Remark	"Published_as die-1"
Remark	"We generated transgenic die-1(w34)-null mutants that carry an extrachromosomal array containing the rescuing die-1 fosmid reporter and the AWCL/AWCR-expressed odr-1 promoter::DsRed marker. We scored expression of the AWC-ON marker str-2promoter::GFP, contained on a separate, chromosomally integrated array. We found that the presence of the die-1 array in an AWC neuron results in an increased probability of the AWC-OFF state compared with AWC neurons that have lost the array."
Reference	"WBPaper00044621"


Anatomy_function : "WBbtf0634"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001661"	Autonomous
Gene	"WBGene00000995"
Involved	"WBbt:0005833"	Sufficient
Remark	"ENTITY:WBbt:0005833(AWC-OFF)|GO:0048664(neuron fate determination)|"
Remark	"GO:0035545(determination of left/right symmetry in nervous system)"
Remark	"QUALITY:PATO:0002052(decreased occurrence) NOT"
Remark	"Genotype \"die-1(w34); kyIs140(str-2p::GFP; vyEx1462[die-1::YFP ord-1p::DsRed])\""
Remark	"Published_as die-1"
Remark	"We generated transgenic die-1(w34)-null mutants that carry an extrachromosomal array containing the rescuing die-1 fosmid reporter and the AWCL/AWCR-expressed odr-1 promoter::DsRed marker. We scored expression of the AWC-ON marker str-2promoter::GFP, contained on a separate, chromosomally integrated array. We found that the presence of the die-1 array in an AWC neuron results in an increased probability of the AWC-OFF state compared with AWC neurons that have lost the array. Furthermore, we specifically examined animals that contain die-1(+)gene activity on a rescuing array (as assessed with the expression of the odr-1 marker) in one AWC neuron but not the contralateral homolog. We found that in these animals, the presence of the die-1 array tracks with the adoption of the AWC-OFF phenotype."
Reference	"WBPaper00044621"


Anatomy_function : "WBbtf0635"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000469"	Nonautonomous
Gene	"WBGene00000396"
Not_involved	"WBbt:0003927"	Unnecessary
Remark	"ENTITY:WBbt:0008598(Q cell)|WBbt:0003927(AQR)|GO:0016477(cell migration)"
Remark	"QUALITY:PATO:0002052(decreased occurrence)"
Remark	"Genotype \"cdh-4(lq56); Is[gcy-32::cfp]; Ex[cdh-4(+)]\""
Remark	"Published_as cdh-4"
Remark	"To test the functional requirement of cdh-4 in the Q cells, we performed a mosaic analysis using the cdh-4::gfp fosmid transgene. A stably-integrated gcy-32::cfp transgene was used to score the positions of AQR and PQR, and an unstable extrachromosomal array containing rescuing cdh-4::gfp and gcy-32::yfp was used to generate genetic mosaics of cdh-4(+) activity in the cdh-4(lq56) mutant. The cdh-4::gfp extrachromosomal array rescued AQR and PQR defects in cdh-4(lq56) mutants, indicating that it supplies cdh-4(+)activity. We next screened for mosaic animals in which the cdh-4::gfp extrachromosomal array was specifically lost in either AQR or PQR but retained in the other and in the URX neurons using gcy-32::cfp expression. The positions of AQR or PQR that lost the array were then determined by gcy-32::yfp. In such mosaic animals, AQR and PQR migration defects were not significantly different from non-mosiac, rescued animal."
Reference	"WBPaper00045414"


Anatomy_function : "WBbtf0636"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000469"	Nonautonomous
Gene	"WBGene00000396"
Not_involved	"WBbt:0004096"	Unnecessary
Remark	"ENTITY:WBbt:0008598(Q cell)| WBbt:0004096(PQR)|GO:0016477(cell migration)"
Remark	"QUALITY:PATO:0002052(decreased occurrence)"
Remark	"Genotype \"cdh-4(lq56); Is[gcy-32::cfp]; Ex[cdh-4(+)]\""
Remark	"Published_as cdh-4"
Remark	"To test the functional requirement of cdh-4 in the Q cells, we performed a mosaic analysis using the cdh-4::gfp fosmid transgene. A stably-integrated gcy-32::cfp transgene was used to score the positions of AQR and PQR, and an unstable extrachromosomal array containing rescuing cdh-4::gfp and gcy-32::yfp was used to generate genetic mosaics of cdh-4(+) activity in the cdh-4(lq56) mutant. The cdh-4::gfp extrachromosomal array rescued AQR and PQR defects in cdh-4(lq56) mutants, indicating that it supplies cdh-4(+)activity. We next screened for mosaic animals in which the cdh-4::gfp extrachromosomal array was specifically lost in either AQR or PQR but retained in the other and in the URX neurons using gcy-32::cfp expression. The positions of AQR or PQR that lost the array were then determined by gcy-32::yfp. In such mosaic animals, AQR and PQR migration defects were not significantly different from non-mosiac, rescued animal."
Reference	"WBPaper00045414"


Anatomy_function : "WBbtf0637"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000648"
Involved	"WBbt:0008189"	Necessary
Involved	"WBbt:0005784"	Necessary
Involved	"WBbt:0008202"	Necessary
Remark	"ENTITY:WBbt:0007850(male)|GO:0034609(spicule insertion)"
Remark	"QUALITY:PATO:0000502(delayed)"
Remark	"The mature gonad consists of the germ line, seminal vesicle and vas deferens. We measured the initial insertion time and refractory period of males that had different cellular constituents of their gonad laser-ablated. We found that males lacking all of these structures required longer time to commence mating."
Reference	"WBPaper00045365"


Anatomy_function : "WBbtf0638"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000648"
Involved	"WBbt:0005784"	Necessary
Remark	"ENTITY:WBbt:0007850(male)|GO:0034609(spicule insertion)"
Remark	"QUALITY:PATO:0000502(delayed)"
Remark	"We next asked if the somatic gonad, consisting of the seminal vesicle (the storage area of mature sperm) and the vas deferens (a tubular seminal fluid-producing conduit for sperm movement), was sufficient to promote the initial mating drive, or if the germ line was also required. We found that germ line-ablated males behaviorally resembled the gonad-ablated males, indicating that the germ line is required for the gonad to promote mating."
Reference	"WBPaper00045365"


Anatomy_function : "WBbtf0639"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000648"
Not_involved	"WBbt:0005062"	Unnecessary
Remark	"ENTITY:WBbt:0007850(male)|GO:0034609(spicule insertion)"
Remark	"QUALITY:PATO:0000502(delayed) NOT"
Remark	"Removal of the linker cell late in development prevents the mature vas deferens from connecting to the cloacal opening (Sulston et al., 1980). The somatic gonad and germ line are still functional and sperm moves from the seminal vesicle, but are retained in the vas deferens upon spicule insertion. Interestingly, the operation did not affect the initial mating drive."
Reference	"WBPaper00045365"


Anatomy_function : "WBbtf0640"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000648"
Involved	"WBbt:0007805"	Necessary
Involved	"WBbt:0006862"	Necessary
Remark	"ENTITY:WBbt:0007850(male)|GO:0060179(male mating behavior)|REENTRY|POST|GO:0007620(copulation)"
Remark	"QUALITY:PATO:0000694(premature)"
Remark	"Unlike the larval SPD and SPV-ablated males, spicule tip cut adult males did not display variable mating defects. Both the mock-cut control and operated males displayed normal initial response times to hermaphrodites, but interestingly, the spicule tips-cut males displayed a significantly shorter refractory period than control males."
Reference	"WBPaper00045365"


Anatomy_function : "WBbtf0641"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0004013"
Involved	"WBbt:0007805"	Necessary
Involved	"WBbt:0006862"	Necessary
Remark	"Although spicule tips-cut males lacking functional SPV and SPD could insert their spicules, many of the males were defective in ejaculation."
Remark	"ENTITY:WBbt:0007850(male)|GO:0042713(sperm ejaculation)"
Remark	"QUALITY:PATO:0002052(decreased occurrence)"
Reference	"WBPaper00045365"


Anatomy_function : "WBbtf0642"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000648"
Involved	"WBbt:0007805"
Involved	"WBbt:0006862"
Remark	"ENTITY:WBbt:0007850(male)|GO:0060179(male mating behavior)|WBbt:0008441(vas deferens valve cell)|GO:0060401(cytosolic calcium ion transport)|GO:0007320(insemination)"
Remark	"QUALITY:PATO:0002052(decreased occurrence)"
Reference	"WBPaper00045365"


Anatomy_function : "WBbtf0643"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001226"	Autonomous
Gene	"WBGene00004121"
Involved	"WBbt:0005490"	Sufficient
Remark	"ENTITY: WBbt:0005490(PLM)|GO:0007409(axonogenesis)"
Remark	"QUALITY:PATO:0002052(decreased occurrence) NOT"
Remark	"Genotype \"ptrn-1(tm5597);Ex[Punc-86::ptrn-1]\""
Remark	"Published_as ptrn-1"
Remark	"The defective PLM commissure extension observed in the ptrn-1(tm5597) mutant was fully rescued by ptrn-1a cDNA expressed in the PLM neuron, indicating that the role for PTRN-1 in commissure formation is cell-autonomous."
Reference	"WBPaper00044913"


Anatomy_function : "WBbtf0644"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000102"	Autonomous
Gene	"WBGene00004121"
Involved	"WBbt:0005490"	Sufficient
Remark	"ENTITY: WBbt:0005490(PLM)|GO:0008021(synaptic vesicle)|GO:0097091(synaptic vesicle clustering)"
Remark	"QUALITY:PATO:0002052(decreased occurrence) NOT"
Remark	"Genotype \"ptrn-1(tm5597);Ex[Punc-86::ptrn-1a::yfp]\""
Remark	"Published_as ptrn-1"
Remark	"To determine whether the requirement for ptrn-1 in SV localization is cell-autonomous, we used two different promoters to drive ptrn-1a::yfp cDNA expression in the PLM neuron of the ptrn-1 mutants. Both constructs rescued the defects in mCherry::RAB-3 localization, indicating that PTRN-1 functions cell autonomously in the PLM neuron to promote proper SV localization."
Reference	"WBPaper00044913"


Anatomy_function : "WBbtf0645"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000102"	Autonomous
Gene	"WBGene00004121"
Involved	"WBbt:0005490"	Sufficient
Remark	"ENTITY: WBbt:0005490(PLM)|GO:0008021(synaptic vesicle)|GO:0097091(synaptic vesicle clustering)"
Remark	"QUALITY:PATO:0002052(decreased occurrence) NOT"
Remark	"Genotype \"ptrn-1(wy560);Ex[Pmec-3::ptrn-1a::yfp]\""
Remark	"Published_as ptrn-1"
Remark	"To determine whether the requirement for ptrn-1 in SV localization is cell-autonomous, we used two different promoters to drive ptrn-1a::yfp cDNA expression in the PLM neuron of the ptrn-1 mutants. Both constructs rescued the defects in mCherry::RAB-3 localization, indicating that PTRN-1 functions cell autonomously in the PLM neuron to promote proper SV localization."
Reference	"WBPaper00044913"


Anatomy_function : "WBbtf0646"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000039"
Gene	"WBGene00012929"
Involved	"WBbt:0005784"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|WBls:0000041(adult)|GO:0007568(aging)"
Remark	"QUALITY:PATO:0000911(decreased rate)"
Remark	"Published_as rsks-1"
Remark	"Using these tissue-specific RNAi tools, we identified the tissues in which rsks-1 RNAi synergistically extended the lifespan of daf-2 animals. Knockdown of rsks-1 in the daf-2 single mutant extended the mean lifespan by 54%. Germline-specific rsks-1 RNAi extended the daf-2 lifespan by 41%."
Reference	"WBPaper00044638"


Anatomy_function : "WBbtf0647"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000039"
Gene	"WBGene00012929"
Involved	"WBbt:0007846"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|WBls:0000041(adult)|GO:0007568(aging)"
Remark	"QUALITY:PATO:0000911(decreased rate)"
Remark	"Published_as rsks-1"
Remark	"Using these tissue-specific RNAi tools, we identified the tissues in which rsks-1 RNAi synergistically extended the lifespan of daf-2 animals. Knockdown of rsks-1 in the daf-2 single mutant extended the mean lifespan by 54%. Hypodermis-specific rsks-1 RNAi extended the daf-2 lifespan by 39%."
Reference	"WBPaper00044638"


Anatomy_function : "WBbtf0648"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000039"
Gene	"WBGene00012929"
Involved	"WBbt:0005792"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|WBls:0000041(adult)|GO:0007568(aging)"
Remark	"QUALITY:PATO:0000911(decreased rate)"
Remark	"Published_as rsks-1"
Remark	"Using these tissue-specific RNAi tools, we identified the tissues in which rsks-1 RNAi synergistically extended the lifespan of daf-2 animals. Knockdown of rsks-1 in the daf-2 single mutant extended the mean lifespan by 54%. Intestine-specific rsks-1 RNAi in daf-2 caused a moderate lifespan extension of 21%."
Reference	"WBPaper00044638"


Anatomy_function : "WBbtf0649"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000039"
Gene	"WBGene00012929"
Not_involved	"WBbt:0006804"	Unnecessary
Remark	"ENTITY:WBbt:0007833(organism)|WBls:0000041(adult)|GO:0007568(aging)"
Remark	"QUALITY:PATO:0000911(decreased rate) NOT"
Remark	"Published_as rsks-1"
Remark	"Using these tissue-specific RNAi tools, we identified the tissues in which rsks-1 RNAi synergistically extended the lifespan of daf-2 animals. Knockdown of rsks-1 in the daf-2 single mutant extended the mean lifespan by 54%. Body wall muscle-specific rsks-1 RNAi did not extend daf-2 lifespan significantly."
Reference	"WBPaper00044638"


Anatomy_function : "WBbtf0650"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000039"
Gene	"WBGene00000912"
Involved	"WBbt:0005784"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|WBls:0000041(adult)|GO:0007568(aging)"
Remark	"QUALITY:PATO:0000911(decreased rate) NOT"
Remark	"Published_as daf-16"
Remark	"We tested the tissue-specific involvement of the key suppressors of daf-2 rsks-1, including daf-16. Knockdown of daf-16 by RNAi in daf-2 rsks-1 suppressed the mean lifespan by 69%. Upon inhibition of these genes in the germline, the synergistic longevity was significantly suppressed by daf-16 RNAi(49%)."
Reference	"WBPaper00044638"


Anatomy_function : "WBbtf0651"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000039"
Gene	"WBGene00000912"
Involved	"WBbt:0005792"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|WBls:0000041(adult)|GO:0007568(aging)"
Remark	"QUALITY:PATO:0000911(decreased rate) NOT"
Remark	"Published_as daf-16"
Remark	"We tested the tissue-specific involvement of the key suppressors of daf-2 rsks-1, including daf-16. Knockdown of daf-16 by RNAi in daf-2 rsks-1 suppressed the mean lifespan by 69%. Intestine-specific knockdown of daf-16 significantly suppressed daf-2 rsks-1 lifespan by 50%."
Reference	"WBPaper00044638"


Anatomy_function : "WBbtf0652"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000039"
Gene	"WBGene00000912"
Involved	"WBbt:0007846"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|WBls:0000041(adult)|GO:0007568(aging)"
Remark	"QUALITY:PATO:0000911(decreased rate) NOT"
Remark	"Published_as daf-16"
Remark	"We tested the tissue-specific involvement of the key suppressors of daf-2 rsks-1, including daf-16. Knockdown of daf-16 by RNAi in daf-2 rsks-1 suppressed the mean lifespan by 69%. Additionally, inhibition of daf-16 in the hypodermis also significantly decreased the daf-2 rsks-1 lifespan by 63%."
Reference	"WBPaper00044638"


Anatomy_function : "WBbtf0653"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000039"
Gene	"WBGene00000912"
Not_involved	"WBbt:0006804"	Unnecessary
Remark	"ENTITY:WBbt:0007833(organism)|WBls:0000041(adult)|GO:0007568(aging)"
Remark	"QUALITY:PATO:0000911(decreased rate)"
Remark	"Published_as daf-16"
Remark	"We tested the tissue-specific involvement of the key suppressors of daf-2 rsks-1, including daf-16. Knockdown of daf-16 by RNAi in daf-2 rsks-1 suppressed the mean lifespan by 69%. In the body wall muscle, knockdown of daf-16 had little effect on longevity."
Reference	"WBPaper00044638"


Anatomy_function : "WBbtf0654"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000039"
Gene	"WBGene00020142"
Involved	"WBbt:0005784"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|WBls:0000041(adult)|GO:0007568(aging)"
Remark	"QUALITY:PATO:0000911(decreased rate) NOT"
Remark	"Published_as aak-2"
Remark	"We tested the tissue-specific involvement of the key suppressors of daf-2 rsks-1, including aak-2. Knockdown of aak-2 by RNAi in daf-2 rsks-1 suppressed the mean lifespan by 58%. Upon inhibition in the germline, the synergistic longevity was significantly suppressed by aak-2 RNAi(58%)."
Reference	"WBPaper00044638"


Anatomy_function : "WBbtf0655"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000039"
Gene	"WBGene00020142"
Involved	"WBbt:0005792"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|WBls:0000041(adult)|GO:0007568(aging)"
Remark	"QUALITY:PATO:0000911(decreased rate) NOT"
Remark	"Published_as aak-2"
Remark	"We tested the tissue-specific involvement of the key suppressors of daf-2 rsks-1, including aak-2. Knockdown of daf-16 by RNAi in daf-2 rsks-1 suppressed the mean lifespan by 58%. Intestine-specific knockdown of aak-2 significantly suppressed daf-2 rsks-1 lifespan by 39%."
Reference	"WBPaper00044638"


Anatomy_function : "WBbtf0656"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000039"
Gene	"WBGene00002004"
Involved	"WBbt:0005792"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|WBls:0000041(adult)|GO:0007568(aging)"
Remark	"QUALITY:PATO:0000911(decreased rate) NOT"
Remark	"Published_as hsf-1"
Remark	"We tested the tissue-specific involvement of the key suppressors of daf-2 rsks-1, including hsf-1. Knockdown of hsf-1 by RNAi in daf-2 rsks-1 suppressed the mean lifespan by 72%. Intestine-specific knockdown of hsf-1 significantly suppressed daf-2 rsks-1 lifespan by 69%."
Reference	"WBPaper00044638"


Anatomy_function : "WBbtf0657"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000039"
Gene	"WBGene00002004"
Not_involved	"WBbt:0006804"	Unnecessary
Remark	"ENTITY:WBbt:0007833(organism)|WBls:0000041(adult)|GO:0007568(aging)"
Remark	"QUALITY:PATO:0000911(decreased rate)"
Remark	"Published_as hsf-1"
Remark	"We tested the tissue-specific involvement of the key suppressors of daf-2 rsks-1, including hsf-1. Knockdown of hsf-1 by RNAi in daf-2 rsks-1 suppressed the mean lifespan by 72%. In the body wall muscle, knockdown of hsf-1 had little effect on longevity."
Reference	"WBPaper00044638"


Anatomy_function : "WBbtf0658"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000039"
Gene	"WBGene00020142"
Not_involved	"WBbt:0006804"	Unnecessary
Remark	"ENTITY:WBbt:0007833(organism)|WBls:0000041(adult)|GO:0007568(aging)"
Remark	"QUALITY:PATO:0000911(decreased rate)"
Remark	"Published_as aak-2"
Remark	"We tested the tissue-specific involvement of the key suppressors of daf-2 rsks-1, including aak-2. Knockdown of aak-2 by RNAi in daf-2 rsks-1 suppressed the mean lifespan by 58%. In the body wall muscle, knockdown of aak-2 had little effect on longevity."
Reference	"WBPaper00044638"


Anatomy_function : "WBbtf0659"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000113"	Autonomous
Gene	"WBGene00004095"
Involved	"WBbt:0005304"	Sufficient
Remark	"ENTITY:WBbt:0005304(VC neuron)|WBGene00006744(unc-4)|GO:0016458(gene silencing)"
Remark	"QUALIFY:PATO:0002052(deceased occurrence) NOT"
Remark	"Genotype \"pqe-1(u825); uIs45[unc-4p::GFP]; Ex[lin-11p::pes-10p::pqe-1a]\""
Remark	"Mutation of pqe-1 results in ectopic unc-4 promoter expression in all six VC neurons. Since expression of the pqe-1a isoform from the VC-expressed promoter lin-11p::pes-10p, which contains a 500 bp lin-11 enhancer and a pes-10 basal promoter, prevented the ectopic unc-4 expression, PQE-1 acts cell-autonomously and does not require the exonuclease domain."
Remark	"Published_as pqe-1"
Reference	"WBPaper00044613"


Anatomy_function : "WBbtf0660"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000113"	Autonomous
Gene	"WBGene00004095"
Involved	"WBbt:0005304"	Sufficient
Remark	"ENTITY:WBbt:0005304(VC neuron)|WBGene00006744(unc-4)|GO:0016458(gene silencing)"
Remark	"QUALITY:PATO:0002052(deceased occurrence) NOT"
Remark	"Genotype \"pqe-1(u825); uIs45[unc-4p::GFP]; Ex[ida-1p::pqe-1a]\""
Remark	"Mutation of pqe-1 results in ectopic unc-4 promoter expression in all six VC neurons. Since expression of the pqe-1a isoform from the VC-expressed promoter lin-11p::pes-10p, which contains a 500 bp lin-11 enhancer and a pes-10 basal promoter, prevented the ectopic unc-4 expression, PQE-1 acts cell-autonomously and does not require the exonuclease domain. Because lin-11p::pes-10p is also expressed in secondary vulval cells, uterine pi cell progeny, and the spermatheca, we repeated the rescue experiments by expressing pqe-1a(+) from the ida-1 promoter, which is expressed in many neurons but only overlaps with the expression pattern of lin-11p::pes-10p in the VC cells. We obtained similar result."
Remark	"Published_as pqe-1"
Reference	"WBPaper00044613"


Anatomy_function : "WBbtf0661"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000113"	Autonomous
Gene	"WBGene00004095"
Involved	"WBbt:0005304"	Necessary
Remark	"ENTITY:WBbt:0005304(VC neuron)|WBGene00006744(unc-4)|GO:0016458(gene silencing)"
Remark	"QUALIFY:PATO:0002052(deceased occurrence)"
Remark	"Genotype \"pqe-1(u825); uIs45[unc-4p::GFP]; Ex[pqe-1(+)]\""
Remark	"Mutation of pqe-1 results in ectopic unc-4 promoter expression in all six VC neurons. To rule out the possible non-cell autonomous interactions among the VC neurons, which synapses on one another, we also performed mosaic analyses on pqe-1(u825); uIs45 animals with an extragenic pqe-1(+) array. In the 15 mosaic animals we examined, all VC1-3 and VC6 cells lacking the rescuing array expressed GFP strongly, suggesting that pqe-1 acts cell autonomously."
Remark	"Published_as pqe-1"
Reference	"WBPaper00044613"


Anatomy_function : "WBbtf0662"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000113"	Autonomous
Gene	"WBGene00011636"
Involved	"WBbt:0005304"	Sufficient
Remark	"ENTITY:WBbt:0005304(VC neuron)|WBGene00006744(unc-4)|GO:0016458(gene silencing)"
Remark	"QUALIFY:PATO:0002052(deceased occurrence) NOT"
Remark	"Genotype \"cec-3(u830); uIs45[unc-4p::GFP]; Ex[lin-11p::pes-10p::cec-3]\""
Remark	"Mutation of cec-3 results in ectopic unc-4 promoter expression in all six VC neurons. , CEC-3 expression in VC neurons restored the normal unc-4 promoter expression pattern, indicating that it acts cell-autonomously in the VC neurons."
Remark	"Published_as cec-3"
Reference	"WBPaper00044613"


Anatomy_function : "WBbtf0663"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000113"	Autonomous
Gene	"WBGene00011636"
Involved	"WBbt:0005304"	Necessary
Remark	"ENTITY:WBbt:0005304(VC neuron)|WBGene00006744(unc-4)|GO:0016458(gene silencing)"
Remark	"QUALIFY:PATO:0002052(deceased occurrence)"
Remark	"Mutation of cec-3 results in ectopic unc-4 promoter expression in all six VC neurons. , CEC-3 expression in VC neurons restored the normal unc-4 promoter expression pattern. Mosaic analysis confirmed the cec-3 cell autonomy in individual VC cells (data not shown)."
Remark	"Published_as cec-3"
Reference	"WBPaper00044613"


Anatomy_function : "WBbtf0664"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000113"	Autonomous
Gene	"WBGene00002335"
Involved	"WBbt:0005304"	Sufficient
Remark	"ENTITY:WBbt:0004617(VC4)|WBbt:0004613(VC5)|WBGene00006744(unc-4)|GO:0006351(transcription, DNA-templated)"
Remark	"QUALIFY:PATO:0002052(deceased occurrence) NOT"
Remark	"Genotype \"let-60(n2021); uIs45[unc-4p::GFP]; Ex[lin-11p::pes-10p::let-60(+)]\""
Remark	"Published_as let-60"
Remark	"let-60/RAS and lin-45/RAF mutant, which lack downstream effectors of EGFR, also failed to express unc-4 in vulval VC neurons. Importantly, unc-4 expression in VC4 and VC5 neurons was restored in animals with hypomorphic alleles of let-60 and lin-45 by VC-specific expression of the respective wild-type gene, indicating that the EGFR/RAS/RAF signaling cascade functions cell-autonomously in VC neurons."
Reference	"WBPaper00044613"


Anatomy_function : "WBbtf0665"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000113"	Autonomous
Gene	"WBGene00003030"
Involved	"WBbt:0005304"	Sufficient
Remark	"ENTITY:WBbt:0004617(VC4)|WBbt:0004613(VC5)|WBGene00006744(unc-4)|GO:0006351(transcription, DNA-templated)"
Remark	"QUALIFY:PATO:0002052(deceased occurrence) NOT"
Remark	"Genotype \"lin-45(n2018); uIs45[unc-4p::GFP]; Ex[lin-11p::pes-10p::lin-45(+)]\""
Remark	"Published_as lin-45"
Remark	"let-60/RAS and lin-45/RAF mutant, which lack downstream effectors of EGFR, also failed to express unc-4 in vulval VC neurons. Importantly, unc-4 expression in VC4 and VC5 neurons was restored in animals with hypomorphic alleles of let-60 and lin-45 by VC-specific expression of the respective wild-type gene, indicating that the EGFR/RAS/RAF signaling cascade functions cell-autonomously in VC neurons."
Reference	"WBPaper00044613"


Anatomy_function : "WBbtf0666"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000113"
Involved	"WBbt:0006768"	Necessary
Remark	"ENTITY:WBbt:0004617(VC4)|WBbt:0004613(VC5)|WBGene00006744(unc-4)|GO:0006351(transcription, DNA-templated)"
Remark	"QUALIFY:PATO:0002052(deceased occurrence)"
Remark	"Genotype \"uIs45[unc-4p::GFP]\""
Remark	"laser ablation of vulF cells caused the loss of unc-4 expression in the VC4 and VC5 neurons, suggesting that vulF cells are responsible for releasing EGF that activates unc-4."
Reference	"WBPaper00044613"


Anatomy_function : "WBbtf0667"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000113"
Involved	"WBbt:0006768"	Necessary
Remark	"ENTITY:WBbt:0004617(VC4)|WBbt:0004613(VC5)|WBGene00006744(unc-4)|GO:0006351(transcription, DNA-templated)"
Remark	"QUALIFY:PATO:0002052(deceased occurrence)"
Remark	"Genotype \"lin-12(n137); uIs45[unc-4p::GFP]\""
Remark	"Laser ablation of vulF cells caused the loss of unc-4 expression in the VC4 and VC5 neurons, suggesting that vulF cells are responsible for releasing EGF that activates unc-4. To further confirm the importance of vulF cells in inducing unc-4, we examined lin-12d mutants, in which all the six vulval precursor cells adopt the secondary vulval cell fate and the primary lineage progeny vulF cells are not generate. The strong lin-12d allele n137 caused a multivulva phenotype but had no unc-4 expression in any VC cells."
Reference	"WBPaper00044613"


Anatomy_function : "WBbtf0668"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000113"
Involved	"WBbt:0006768"	Necessary
Remark	"ENTITY:WBbt:0004617(VC4)|WBbt:0004613(VC5)|WBGene00006744(unc-4)|GO:0006351(transcription, DNA-templated)"
Remark	"QUALIFY:PATO:0002052(deceased occurrence)"
Remark	"Genotype \"lin-12(n302); uIs45[unc-4p::GFP]\""
Remark	"Laser ablation of vulF cells caused the loss of unc-4 expression in the VC4 and VC5 neurons, suggesting that vulF cells are responsible for releasing EGF that activates unc-4. To further confirm the importance of vulF cells in inducing unc-4, we examined lin-12d mutants, in which all the six vulval precursor cells adopt the secondary vulval cell fate and the primary lineage progeny vulF cells are not generate. The weaker lin-12d allele n302 resulted in a vulvaless phenotype and the elimination of unc-4 expression in VC4 and VC5 neurons."
Reference	"WBPaper00044613"


Anatomy_function : "WBbtf0669"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000113"	Autonomous
Gene	"WBGene00003000"
Involved	"WBbt:0005304"	Sufficient
Remark	"ENTITY:WBbt:0004617(VC4)|WBbt:0004613(VC5)|WBGene00006744(unc-4)|GO:0006351(transcription, DNA-templated)"
Remark	"QUALIFY:PATO:0002052(deceased occurrence) NOT"
Remark	"Genotype \"lin-11(n389); uIs45[unc-4p::GFP]; ida-1p::lin-11(+)\""
Remark	"Mutation of lin-11, which encodes a LIM homeodomain protein, eliminated uIs45 expression in VC4 and VC5. Expression of lin-11(+) using lin-11p::pes-10p, which is active in VC neurons but transiently expressed in the developing vulval cells, mainly the vulC and vulD cells but not the vulF cells, produced a normal unc-4 expression pattern in lin-11 mutants. We obtained a similar rescue using the ida-1 promoter, which is expressed in many neurons, including the VC neurons, but not vulval cells."
Remark	"Published_as lin-11"
Reference	"WBPaper00044613"


Anatomy_function : "WBbtf0670"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0004028"
Gene	"WBGene00020506"
Not_involved	"WBbt:0006746"	Unnecessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0040011(locomotion)|PATO:0000304(decreased speed)|GO:0032094(response to food)"
Remark	"QUALIFY:PATO:0001997(decreased amount) NOT"
Remark	"Genotype \"XE1474(lin-15B(n744)X; eri-1(mg366)IV; rde-1(ne219)V; wpSi6[Pdat-1::rde-1:SL2:sid-1,Cbunc-119(+)]II)\""
Remark	"Published_as dop-3"
Remark	"RNAi against dop-3 blocked basal slowing in the control strain (susceptible to systemic RNAi) but did not affect basal slowing in the Pdat-1 strain (susceptibble to dopaminergic neuron-specific RNAi). Our results demonstrate that the dopamine receptor dop-3 does not function in the dopamine neurons."
Reference	"WBPaper00044483"


Anatomy_function : "WBbtf0671"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001221"
Gene	"WBGene00001612"
Not_involved	"WBbt:0006829"	Unnecessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0009612(response to mechanical stimulus)|WBbt:0008426(nose)|GO:0050975(sensory perception of touch)"
Remark	"QUALIFY:PATO:0001997(decreased amount) NOT"
Remark	"Genotype \"XE1474(lin-15B(n744)X; eri-1(mg366)IV; rde-1(ne219)V; wpSi11[Peat-4::rde-1:SL2:sid-1, Cbunc-119(+)]II)\""
Remark	"Published_as glr-1"
Remark	"We fed neuron-sensitized (lin15B; eri-1) animals dsRNA against glr-1. These animals were deficient in their ability to respond to nose touch when compared to controls. In contrast, RNAi against glr-1 did not affect the ability of the glutamate-specific (vis-a-vis RNAi susceptibility) strain to respond to nose touch.  Our results demonstrate that the glutamate receptor glr-1 does not function in the glutamate neurons."
Reference	"WBPaper00044483"


Anatomy_function : "WBbtf0672"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001182"	Nonautonomous
Gene	"WBGene00018008"
Not_involved	"WBbt:0006804"	Unnecessary
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|GO:0019915(lipid storage)"
Remark	"QUALIFY:PATO:000047(increased)"
Remark	"Expressing the vpr-1 genomic locus in vpr-1(tm1411) null worms rescued the fat metabolism defect in muscle, as well as the muscle mitochondrial defects, sterility, slow growth, and other phenotypes. Transgene array loss in the EMS lineage generates mosaic worms that have a subset of muscles lacking vpr-1 expression. These muscle cells exhibited low fat levels, identical to muscle cells that express vpr-1. Therefore, VPR-1 is not required in body wall muscle for fat accumulation."
Remark	"Genotype \"vpr-1(tm1411); Ex[vpr-1(+) sur-5::GFP]\""
Remark	"Published_as vpr-1"
Reference	"WBPaper00044483"


Anatomy_function : "WBbtf0673"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001182"
Gene	"WBGene00018008"
Not_involved	"WBbt:0005792"	Unnecessary
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|GO:0019915(lipid storage)"
Remark	"QUALIFY:PATO:000047(increased)"
Remark	"Expressing the vpr-1 genomic locus in vpr-1(tm1411) null worms rescued the fat metabolism defect in muscle, as well as the muscle mitochondrial defects, sterility, slow growth, and other phenotypes. Mosaic worms lacking vpr-1 in the E lineage, which generates the intestine, also did not exhibit elevated muscle fat droplets, indicating that vpr-1 is not required in the intestine."
Remark	"Genotype \"vpr-1(tm1411); Ex[vpr-1(+) sur-5::GFP]\""
Remark	"Published_as vpr-1"
Reference	"WBPaper00044483"


Anatomy_function : "WBbtf0674"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001182"	Nonautonomous
Gene	"WBGene00018008"
Involved	"WBbt:0003679"	Sufficient
Involved	"WBbt:0007846"	Sufficient
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|GO:0019915(lipid storage)"
Remark	"QUALIFY:PATO:000047(increased)"
Remark	"Expressing the vpr-1 genomic locus in vpr-1(tm1411) null worms rescued the fat metabolism defect in muscle, as well as the muscle mitochondrial defects, sterility, slow growth, and other phenotypes. In contrast to muscle and intestine loss, vpr-1 loss in the AB lineage, which generates the neurons, did cause increased fat droplets in muscles."
Remark	"Genotype \"vpr-1(tm1411); Ex[vpr-1(+) sur-5::GFP]\""
Remark	"Published_as vpr-1"
Reference	"WBPaper00044483"


Anatomy_function : "WBbtf0675"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001182"	Nonautonomous
Gene	"WBGene00018008"
Involved	"WBbt:0005784"	Sufficient
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|GO:0019915(lipid storage)"
Remark	"QUALIFY:PATO:000047(increased)"
Remark	"Expressing the vpr-1 genomic locus in vpr-1(tm1411) null worms rescued the fat metabolism defect in muscle, as well as the muscle mitochondrial defects, sterility, slow growth, and other phenotypes. Unexpectedly, we also found that vpr-1 loss in the germ cell lineage causes muscle fat accumulation."
Remark	"Genotype \"vpr-1(tm1411); Ex[vpr-1(+) sur-5::GFP]\""
Remark	"Published_as vpr-1"
Reference	"WBPaper00044483"


Anatomy_function : "WBbtf0676"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001182"	Nonautonomous
Gene	"WBGene00018008"
Not_involved	"WBbt:0007810"	Insufficient
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|GO:0019915(lipid storage)"
Remark	"QUALIFY:PATO:000047(increased)"
Remark	"Genotype \"vpr-1(tm1411); Ex[myo-3p::vpr-1\""
Remark	"Published_as vpr-1"
Remark	"To test whether VPR-1 expression is sufficient in neurons, we expressed VPR-1 under the control of tissue-specific promoters in vpr-1 null mutants. Consistent with genetic mosaic analysis, VPR-1 expression using the myo-3 muscle-specific promoter did not influence muscle fat levels."
Reference	"WBPaper00044483"


Anatomy_function : "WBbtf0677"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001182"	Nonautonomous
Gene	"WBGene00018008"
Not_involved	"WBbt:0005792"	Insufficient
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|GO:0019915(lipid storage)"
Remark	"QUALIFY:PATO:000047(increased)"
Remark	"Genotype \"vpr-1(tm1411); Ex[ges-1p::vpr-1\""
Remark	"Published_as vpr-1"
Remark	"To test whether VPR-1 expression is sufficient in neurons, we expressed VPR-1 under the control of tissue-specific promoters in vpr-1 null mutants. Consistent with genetic mosaic analysis, VPR-1 expression using the ges-1 intestine-specific promoter did not influence muscle fat levels."
Reference	"WBPaper00044483"


Anatomy_function : "WBbtf0678"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001182"	Nonautonomous
Gene	"WBGene00018008"
Involved	"WBbt:0003679"
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|GO:0019915(lipid storage)"
Remark	"QUALIFY:PATO:000047(increased) NOT"
Remark	"Genotype \"vpr-1(tm1411); Ex[unc-119p::vpr-1\""
Remark	"Published_as vpr-1"
Reference	"WBPaper00044483"


Anatomy_function : "WBbtf0679"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000391"
Gene	"WBGene00002189"
Involved	"WBbt:0005190"	Necessary
Remark	"ENTITY:WBbt:0008600(enteric muscle)|GO:0006936(muscle contraction)|GO:0030421(defecation)"
Remark	"QUALIFY:PATO:0002052(decreased occurrence)"
Remark	"Genotype \"vjIs76[ttx-3::RFP; Punc-47(FL):: kin-2a(G310D)]\""
Remark	"Published_as kin-1"
Remark	"To determine whether PKA functions in GABAergic neurons to control the Exp step, we generated worms expressing dominant negative PKA transgenes specifically in these neurons. We mutated the corresponding Gly residue to Asp (G310D) in the B site of the KIN-2a isoform (referred to as PKA[DN], and expressed this construct specifically in GABAergic motor neurons (using the full length unc-47 promoter). Two independently generated PKA[DN] transgenic lines displayed distended intestinal lumens, and dramatically reduced cycles in which Exp occurred."
Reference	"WBPaper00044263"


Anatomy_function : "WBbtf0680"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000625"
Gene	"WBGene00004047"
Not_involved	"WBbt:0005274"	Insufficient
Remark	"ENTITY:WBbt:0004858(DA8)|WBbt:0004857(DA9)|GO:0045202(synapse)|GO:0003002(regionalization)|GO:0048859(formation of anatomical boundary)|GO:0060386(synapse assembly involved in innervation)"
Remark	"QUALIFY:PATO:0001507(disrupted)"
Remark	"Genotype \"plx-1(nc36); Ex[Punc-129::plx-1]\""
Remark	"Published_as plx-1"
Remark	"We next asked in which cells plx-1 and semaphorins function by performing rescue experiments using several tissue-specific promoters. We used a truncated unc-129 promoter (Punc-129MN) expression in the DB class of dorsal motoneuron. Expression of PLX-1-encoding complementary DNA (cDNA) in DB class neurons or postsynaptic body wall muscles did not rescue the synaptic tiling phenotype in plx-1 mutants."
Reference	"WBPaper00042107"


Anatomy_function : "WBbtf0681"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000625"
Gene	"WBGene00004047"
Not_involved	"WBbt:0006804"	Insufficient
Remark	"ENTITY:WBbt:0004858(DA8)|WBbt:0004857(DA9)|GO:0045202(synapse)|GO:0003002(regionalization)|GO:0048859(formation of anatomical boundary)|GO:0060386(synapse assembly involved in innervation)"
Remark	"QUALIFY:PATO:0001507(disrupted)"
Remark	"Genotype \"plx-1(nc36); Ex[Phlh-1::plx-1]\""
Remark	"Published_as plx-1"
Remark	"We next asked in which cells plx-1 and semaphorins function by performing rescue experiments using several tissue-specific promoters. We used the hlh-1 promoter for expression in the body wall muscles. Expression of PLX-1-encoding complementary DNA (cDNA) in DB class neurons or postsynaptic body wall muscles did not rescue the synaptic tiling phenotype in plx-1 mutants."
Reference	"WBPaper00042107"


Anatomy_function : "WBbtf0682"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000625"
Gene	"WBGene00004047"
Involved	"WBbt:0005278"	Sufficient
Remark	"ENTITY:WBbt:0004858(DA8)|WBbt:0004857(DA9)|GO:0045202(synapse)|GO:0003002(regionalization)|GO:0048859(formation of anatomical boundary)|GO:0060386(synapse assembly involved in innervation)"
Remark	"QUALIFY:PATO:0001507(disrupted) NOT"
Remark	"Genotype \"plx-1(nc36); Ex[Punc-4c::plx-1]\""
Remark	"Published_as plx-1"
Remark	"We next asked in which cells plx-1 and semaphorins function by performing rescue experiments using several tissue-specific promoters. We used a truncated unc-4 promoter (unc-4c) for expression the plx-1 cDNA in the DA motor neurons including both DA8 and DA9. The synaptic tiling phenotype in plx-1 mutants was almost completely rescued."
Reference	"WBPaper00042107"


Anatomy_function : "WBbtf0683"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000625"
Gene	"WBGene00004047"
Involved	"WBbt:0004857"	Necessary
Remark	"ENTITY:WBbt:0004858(DA8)|WBbt:0004857(DA9)|GO:0045202(synapse)|GO:0003002(regionalization)|GO:0048859(formation of anatomical boundary)|GO:0060386(synapse assembly involved in innervation)"
Remark	"QUALIFY:PATO:0001507(disrupted)"
Remark	"Genotype \"plx-1(nc36); Ex[Punc-4c::plx-1]\""
Remark	"Published_as plx-1"
Remark	"We used a truncated unc-4 promoter (unc-4c) for expression the plx-1 cDNA in the DA motor neurons including both DA8 and DA9. The synaptic tiling phenotype in plx-1 mutants was almost completely rescued. Utilizing the mosaicism of the extrachromosomal array, we conducted genetic mosaic experiments with the Punc-4c::plx-1 transgene to clarify in which DA neurons PLX-1 functions. We found that mosaic animals that lost the rescuing array in DA9 did not rescue the plx-1 mutant phenotype, suggesting that PLX-1 is required in DA9."
Reference	"WBPaper00042107"


Anatomy_function : "WBbtf0684"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000625"
Gene	"WBGene00004047"
Involved	"WBbt:0004857"	Sufficient
Remark	"ENTITY:WBbt:0004858(DA8)|WBbt:0004857(DA9)|GO:0045202(synapse)|GO:0003002(regionalization)|GO:0048859(formation of anatomical boundary)|GO:0060386(synapse assembly involved in innervation)"
Remark	"QUALIFY:PATO:0001507(disrupted) NOT"
Remark	"Genotype \"plx-1(nc36); Ex[Pmig-13::plx-1]\""
Remark	"Published_as plx-1"
Remark	"We used a truncated unc-4 promoter (unc-4c) for expression the plx-1 cDNA in the DA motor neurons including both DA8 and DA9. The synaptic tiling phenotype in plx-1 mutants was almost completely rescued. Utilizing the mosaicism of the extrachromosomal array, we conducted genetic mosaic experiments with the Punc-4c::plx-1 transgene to clarify in which DA neurons PLX-1 functions. We found that mosaic animals that lost the rescuing array in DA9 did not rescue the plx-1 mutant phenotype, suggesting that PLX-1 is required in DA9. Consistent with these observations, PLX-1 expression in DA9, but not DA8 (Pmig-13), was also sufficient to rescue the plx-1 phenotype."
Reference	"WBPaper00042107"


Anatomy_function : "WBbtf0685"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000625"
Gene	"WBGene00004047"
Involved	"WBbt:0004857"	Sufficient
Remark	"ENTITY:WBbt:0004858(DA8)|WBbt:0004857(DA9)|GO:0045202(synapse)|GO:0003002(regionalization)|GO:0048859(formation of anatomical boundary)|GO:0060386(synapse assembly involved in innervation)"
Remark	"QUALIFY:PATO:0001507(disrupted) NOT"
Remark	"Genotype \"plx-1(nc36); Ex[Pitr-1::plx-1]\""
Remark	"Published_as plx-1"
Remark	"We also observed partial but significant rescue of synaptic tiling between DA8 and DA9 phenotype with another DA9 specific promoter (Pitr-1), which is active only in later larval stage (L3 to L4)."
Reference	"WBPaper00042107"


Anatomy_function : "WBbtf0686"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000625"
Gene	"WBGene00004889"
Not_involved	"WBbt:0005274"	Insufficient
Remark	"ENTITY:WBbt:0004858(DA8)|WBbt:0004857(DA9)|GO:0045202(synapse)|GO:0003002(regionalization)|GO:0048859(formation of anatomical boundary)|GO:0060386(synapse assembly involved in innervation)"
Remark	"QUALIFY:PATO:0001507(disrupted)"
Remark	"Genotype \"smp-1; smp-2; Ex[Punc-129::smp-1]\""
Remark	"Published_as smp-1"
Remark	"We next asked in which cells plx-1 and semaphorins function by performing rescue experiments using several tissue-specific promoters. We used a truncated unc-129 promoter (Punc-129MN) expression in the DB class of dorsal motoneuron. Expression of smp-1-encoding complementary DNA (cDNA) in DB class neurons or postsynaptic body wall muscles did not rescue the synaptic tiling phenotype in smp-1;smp-2 double mutants."
Reference	"WBPaper00042107"


Anatomy_function : "WBbtf0687"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000625"
Gene	"WBGene00004889"
Not_involved	"WBbt:0006804"	Insufficient
Remark	"ENTITY:WBbt:0004858(DA8)|WBbt:0004857(DA9)|GO:0045202(synapse)|GO:0003002(regionalization)|GO:0048859(formation of anatomical boundary)|GO:0060386(synapse assembly involved in innervation)"
Remark	"QUALIFY:PATO:0001507(disrupted)"
Remark	"Genotype \"smp-1; smp-2; Ex[Phlh-1::smp-1]\""
Remark	"Published_as smp-1"
Remark	"We next asked in which cells plx-1 and semaphorins function by performing rescue experiments using several tissue-specific promoters. We used the hlh-1 promoter for expression in the body wall muscles. Expression of SMP-1-encoding complementary DNA (cDNA) in DB class neurons or postsynaptic body wall muscles did not rescue the synaptic tiling phenotype in smp-1;smp-2 double mutants."
Reference	"WBPaper00042107"


Anatomy_function : "WBbtf0688"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000625"
Gene	"WBGene00004889"
Involved	"WBbt:0004857"	Necessary
Remark	"ENTITY:WBbt:0004858(DA8)|WBbt:0004857(DA9)|GO:0045202(synapse)|GO:0003002(regionalization)|GO:0048859(formation of anatomical boundary)|GO:0060386(synapse assembly involved in innervation)"
Remark	"QUALIFY:PATO:0001507(disrupted) NOT"
Remark	"Genotype \"smp-1; smp-2; Ex[Punc-4c::smp-1]\""
Remark	"Published_as smp-1"
Remark	"We used a truncated unc-4 promoter (unc-4c) for expression of the plx-1 cDNA in the DA motor neurons including both DA8 and DA9. The synaptic tiling phenotype in smp-1;smp-2 double mutants was almost completely rescued. Utilizing the mosaicism of the extrachromosomal array, we conducted genetic mosaic experiments with the Punc-4c::smp-1 transgene to clarify in which DA neurons SMP-1 functions. We found that mosaic animals that lost the rescuing array in DA9 did not rescue the smp-1 mutant phenotype, suggesting that SMP-1 is required in DA9."
Reference	"WBPaper00042107"


Anatomy_function : "WBbtf0689"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000625"
Gene	"WBGene00004889"
Involved	"WBbt:0005278"	Sufficient
Remark	"ENTITY:WBbt:0004858(DA8)|WBbt:0004857(DA9)|GO:0045202(synapse)|GO:0003002(regionalization)|GO:0048859(formation of anatomical boundary)|GO:0060386(synapse assembly involved in innervation)"
Remark	"QUALIFY:PATO:0001507(disrupted) NOT"
Remark	"Genotype \"smp-1; smp-2; Ex[Punc-4c::smp-1]\""
Remark	"Published_as smp-1"
Remark	"We next asked in which cells plx-1 and semaphorins function by performing rescue experiments using several tissue-specific promoters. We used a truncated unc-4 promoter (unc-4c) for expression the smp-1 cDNA in the DA motor neurons including both DA8 and DA9. The synaptic tiling phenotype in smp-1;smp-2 double mutants was almost completely rescued."
Reference	"WBPaper00042107"


Anatomy_function : "WBbtf0690"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000625"
Gene	"WBGene00004889"
Involved	"WBbt:0004857"	Sufficient
Remark	"ENTITY:WBbt:0004858(DA8)|WBbt:0004857(DA9)|GO:0045202(synapse)|GO:0003002(regionalization)|GO:0048859(formation of anatomical boundary)|GO:0060386(synapse assembly involved in innervation)"
Remark	"QUALIFY:PATO:0001507(disrupted) NOT"
Remark	"Genotype \"smp-1; smp-2; Ex[Pmig-13::smp-1]\""
Remark	"Published_as smp-1"
Remark	"We used a truncated unc-4 promoter (unc-4c) for expression the smp-1 cDNA in the DA motor neurons including both DA8 and DA9. The synaptic tiling phenotype in smp-1;smp-2 double mutants was almost completely rescued. Utilizing the mosaicism of the extrachromosomal array, we conducted genetic mosaic experiments with the Punc-4c::smp-1 transgene to clarify in which DA neurons SMP-1 functions. We found that mosaic animals that lost the rescuing array in DA9 did not rescue the mutant phenotype, suggesting that SMP-1 is required in DA9. Consistent with these observations, SMP-1 expression in DA9, but not DA8 (Pmig-13), was also sufficient to rescue the smp-1; smp-2 phenotype."
Reference	"WBPaper00042107"


Anatomy_function : "WBbtf0691"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000625"
Gene	"WBGene00004889"
Involved	"WBbt:0004857"	Sufficient
Remark	"ENTITY:WBbt:0004858(DA8)|WBbt:0004857(DA9)|GO:0045202(synapse)|GO:0003002(regionalization)|GO:0048859(formation of anatomical boundary)|GO:0060386(synapse assembly involved in innervation)"
Remark	"QUALIFY:PATO:0001507(disrupted) NOT"
Remark	"Genotype \"smp-1; smp-2; Ex[Pitr-1::smp-1]\""
Remark	"Published_as smp-1"
Remark	"We also observed partial but significant rescue of synaptic tiling between DA8 and DA9 phenotype with another DA9 specific promoter (Pitr-1), which is active only in later larval stage (L3 to L4)."
Reference	"WBPaper00042107"


Anatomy_function : "WBbtf0692"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000625"
Gene	"WBGene00002335"
Involved	"WBbt:0004857"	Necessary
Remark	"ENTITY:WBbt:0004858(DA8)|WBbt:0004857(DA9)|GO:0045202(synapse)|GO:0003002(regionalization)|GO:0048859(formation of anatomical boundary)|GO:0060386(synapse assembly involved in innervation)"
Remark	"QUALIFY:PATO:0001507(disrupted) NOT"
Remark	"Genotype \"let-60(n1046); Ex[mig-13::let-60(G10R)]\""
Remark	"Published_as let-60"
Remark	"We found that a gain-of-function mutant of Ras (let-60gf) showed a significant synaptic tiling defect. To test the cellular requirement of the Ras-induced synaptic tiling phenotype, we independently expressed two dominant-negative LET-60 Ras proteins (G10R and S89F) in DA9 using the mig-13 promoter. We found that DA9 expression of these two Ras constructs suppressed the let-60(gf) mutant phenotype, suggesting that Ras also function cell autonomously in DA9 to restrict its synaptic domain."
Reference	"WBPaper00042107"


Anatomy_function : "WBbtf0693"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000384"	Autonomous
Gene	"WBGene00017381"
Involved	"WBbt:0004078"	Necessary
Remark	"ENTITY:WBbt:0004078(PVPR)|GO:0030424(axon)|GO:0007411(axon guidance)|WBbt:0005829(ventral nerve cord)"
Remark	"QUALIFY:PATO:0001507(disrupted) NOT"
Remark	"Genotype \"ddr-1(ok874) ddr-2(ok574); hdIs29[odr-2::CFP, sra-6::DsRed2]; Ex[ddr-2(+) odr-2::GFP sra-6::GFP rol-6(su1006)]\""
Remark	"Published_as ddr-2"
Remark	"We performed a genetic mosaic analysis to test whether ddr-2 acts cell-autonomously in the PVPR neuron by correlating the presence or absence of a rescuing ddr-2 transgene in PVPR with the presence or absence of axonal defects. We found that loss of an extra-chromosomal array containing a functional ddr-2 gene in PVPR abolished the rescue of the pioneer navigation defects."
Reference	"WBPaper00041722"


Anatomy_function : "WBbtf0694"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000384"	Autonomous
Gene	"WBGene00017381"
Involved	"WBbt:0004082"	Necessary
Remark	"ENTITY:WBbt:0004082(PVPL)|GO:0030424(axon)|GO:0007411(axon guidance)|WBbt:0005829(ventral nerve cord)"
Remark	"QUALIFY:PATO:0001507(disrupted) NOT"
Remark	"Genotype \"ddr-1(ok874) ddr-2(ok574); hdIs29[odr-2::CFP, sra-6::DsRed2]; Ex[ddr-2(+) odr-2::GFP sra-6::GFP rol-6(su1006)]\""
Remark	"Published_as ddr-2"
Remark	"We performed a genetic mosaic analysis to test whether ddr-2 acts cell-autonomously in the PVPR neuron by correlating the presence or absence of a rescuing ddr-2 transgene in PVPR with the presence or absence of axonal defects. We found that loss of an extra-chromosomal array containing a functional ddr-2 gene in PVPR abolished the rescue of the pioneer navigation defects. Similarly loss of the transgene in PVPL abolished the rescue of PVPL defects."
Reference	"WBPaper00041722"


Anatomy_function : "WBbtf0695"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000384"
Gene	"WBGene00017381"
Involved	"WBbt:0004078"	Necessary
Remark	"ENTITY:WBbt:0004076(PVQL)|GO:0030424(axon)|GO:0007411(axon guidance)|WBbt:0005829(ventral nerve cord)"
Remark	"QUALIFY:PATO:0001507(disrupted)"
Remark	"Genotype \"ddr-1(ok874) ddr-2(ok574); hdIs29[odr-2::CFP, sra-6::DsRed2]; Ex[ddr-2(+) odr-2::GFP sra-6::GFP rol-6(su1006)]\""
Remark	"Published_as ddr-2"
Remark	"We performed a genetic mosaic analysis to test whether ddr-2 acts in the PVPR neuron by correlating the presence or absence of a rescuing ddr-2 transgene in PVPR with the presence or absence of axonal defects. Loss of the ddr-2 transgene in PVPR, but not in PVQL, lead to PVQL axon navigation defects comparable to those in ddr-1 ddr-2 double mutants."
Reference	"WBPaper00041722"


Anatomy_function : "WBbtf0696"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000384"	Nonautonomous
Gene	"WBGene00017381"
Not_involved	"WBbt:0004076"	Unnecessary
Remark	"ENTITY:WBbt:0004076(PVQL)|GO:0030424(axon)|GO:0007411(axon guidance)|WBbt:0005829(ventral nerve cord)"
Remark	"QUALIFY:PATO:0001507(disrupted) NOT"
Remark	"Genotype \"ddr-1(ok874) ddr-2(ok574); hdIs29[odr-2::CFP, sra-6::DsRed2]; Ex[ddr-2(+) odr-2::GFP sra-6::GFP rol-6(su1006)]\""
Remark	"Published_as ddr-2"
Remark	"We performed a genetic mosaic analysis to test whether ddr-2 acts in the PVPR neuron by correlating the presence or absence of a rescuing ddr-2 transgene in PVPR with the presence or absence of axonal defects. Loss of the ddr-2 transgene in PVPR, but not in PVQL, lead to PVQL axon navigation defects comparable to those in ddr-1 ddr-2 double mutants. Taken together these results indicate that ddr-2 functions cell-autonomously in the PVPR neuron to guide the pioneering axon and that the PVQL follower defects are a secondary consequence of pioneer defects."
Reference	"WBPaper00041722"


Anatomy_function : "WBbtf0697"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000550"
Gene	"WBGene00000912"
Involved	"WBbt:0005792"	Sufficient
Remark	"Aging C. elegans muscles resemble those of human sarcopenia patients, in which muscle filaments fragment and break. We found that expressing daf-16 exclusively in the intestine of daf-16(-); daf-2(-) mutants reduced this muscle deterioration and improved body movement."
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|PATO:0002037(degeneration)|GO:0007568(ageing)"
Remark	"QUALIFY:PATO:0000380(increased frequency) NOT"
Remark	"Published_as daf-16"
Reference	"WBPaper00041915"


Anatomy_function : "WBbtf0698"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000962"	Autonomous
Gene	"WBGene00000912"
Involved	"WBbt:0005792"	Sufficient
Remark	"ENTITY:WBbt:0005792(intestinal cell)|WBGene00004932(sod-3)|GO:0010467(gene expression)"
Remark	"QUALIFY:PATO:0001997(reduced) NOT"
Remark	"Published_as daf-16"
Remark	"We introduced transgenic reporters for these genes into daf-16(-); daf-2(-) mutants in which daf-16 was expressed in only one tissue: intestine. sod-3 was regulated in a strictly cell-autonomous fashion. The demonstration of cell autonomy was particularly striking in the intestine, because the ges-1 intestinal promoter we used did not fire evenly in all cells. We observed a close correlation between GFP::DAF-16 and reporter expression among individual intestinal cells."
Reference	"WBPaper00041915"


Anatomy_function : "WBbtf0699"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000962"	Autonomous
Gene	"WBGene00000912"
Involved	"WBbt:0005792"	Sufficient
Remark	"ENTITY:WBbt:0005792(intestinal cell)|WBGene00003096(lys-7)|GO:0010467(gene expression)"
Remark	"QUALIFY:PATO:0001997(reduced) NOT"
Remark	"Published_as daf-16"
Remark	"We introduced transgenic reporters for these genes into daf-16(-); daf-2(-) mutants in which daf-16 was expressed in only one tissue: intestine. lys-7 was regulated in a strictly cell-autonomous fashion. The demonstration of cell autonomy was particularly striking in the intestine, because the ges-1 intestinal promoter we used did not fire evenly in all cells. We observed a close correlation between GFP::DAF-16 and reporter expression among individual intestinal cells."
Reference	"WBPaper00041915"


Anatomy_function : "WBbtf0700"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000962"	Autonomous
Gene	"WBGene00000912"
Involved	"WBbt:0005792"	Sufficient
Remark	"ENTITY:WBbt:0005792(intestinal cell)|WBGene00003473(mtl-1)|GO:0010467(gene expression)"
Remark	"QUALIFY:PATO:0001997(reduced) NOT"
Remark	"Published_as daf-16"
Remark	"We introduced transgenic reporters for these genes into daf-16(-); daf-2(-) mutants in which daf-16 was expressed in only one tissue: intestine. mtl-1 was regulated in a strictly cell-autonomous fashion. The demonstration of cell autonomy was particularly striking in the intestine, because the ges-1 intestinal promoter we used did not fire evenly in all cells. We observed a close correlation between GFP::DAF-16 and reporter expression among individual intestinal cells."
Reference	"WBPaper00041915"


Anatomy_function : "WBbtf0701"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000962"	Autonomous
Gene	"WBGene00000912"
Involved	"WBbt:0005792"	Sufficient
Remark	"ENTITY:WBbt:0005792(intestinal cell)|WBGene00010745(dod-17)|GO:0010467(gene expression)"
Remark	"QUALIFY:PATO:0002051(increased occurence) NOT"
Remark	"Published_as daf-16"
Remark	"We introduced transgenic reporters for these genes into daf-16(-); daf-2(-) mutants in which daf-16 was expressed in only one tissue: intestine. dod-17 was regulated in a strictly cell-autonomous fashion. The demonstration of cell autonomy was particularly striking in the intestine, because the ges-1 intestinal promoter we used did not fire evenly in all cells. We observed a close correlation between GFP::DAF-16 and reporter expression among individual intestinal cells."
Reference	"WBPaper00041915"


Anatomy_function : "WBbtf0702"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000962"	Autonomous
Gene	"WBGene00000912"
Involved	"WBbt:0005792"	Sufficient
Remark	"ENTITY:WBbt:0005792(intestinal cell)|WBGene00001843(hgo-1)|GO:0010467(gene expression)"
Remark	"QUALIFY:PATO:0001997(reduced) NOT"
Remark	"Published_as daf-16"
Remark	"We introduced transgenic reporters for these genes into daf-16(-); daf-2(-) mutants in which daf-16 was expressed in only one tissue: intestine. hgo-1 was regulated in a strictly cell-autonomous fashion. The demonstration of cell autonomy was particularly striking in the intestine, because the ges-1 intestinal promoter we used did not fire evenly in all cells. We observed a close correlation between GFP::DAF-16 and reporter expression among individual intestinal cells."
Reference	"WBPaper00041915"


Anatomy_function : "WBbtf0703"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000962"	Autonomous
Gene	"WBGene00000912"
Involved	"WBbt:0005792"	Sufficient
Remark	"ENTITY:WBbt:0005792(intestinal cell)|WBGene00001684(gpd-2)|GO:0010467(gene expression)"
Remark	"QUALIFY:PATO:0001997(reduced) NOT"
Remark	"Published_as daf-16"
Remark	"We introduced transgenic reporters for these genes into daf-16(-); daf-2(-) mutants in which daf-16 was expressed in only one tissue: intestine. gpd-2 was regulated in a strictly cell-autonomous fashion. The demonstration of cell autonomy was particularly striking in the intestine, because the ges-1 intestinal promoter we used did not fire evenly in all cells. We observed a close correlation between GFP::DAF-16 and reporter expression among individual intestinal cells."
Reference	"WBPaper00041915"


Anatomy_function : "WBbtf0704"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000962"	Autonomous
Gene	"WBGene00000912"
Involved	"WBbt:0005792"	Sufficient
Remark	"ENTITY:WBbt:0005792(intestinal cell)|WBGene00001684(nnt-1)|GO:0010467(gene expression)"
Remark	"QUALIFY:PATO:0001997(reduced) NOT"
Remark	"Published_as daf-16"
Remark	"We introduced transgenic reporters for these genes into daf-16(-); daf-2(-) mutants in which daf-16 was expressed in only one tissue: intestine. nnt-1 was regulated in a strictly cell-autonomous fashion. The demonstration of cell autonomy was particularly striking in the intestine, because the ges-1 intestinal promoter we used did not fire evenly in all cells. We observed a close correlation between GFP::DAF-16 and reporter expression among individual intestinal cells."
Reference	"WBPaper00041915"


Anatomy_function : "WBbtf0705"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000962"	Autonomous
Gene	"WBGene00000912"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBbt:0003679(neuron)|WBGene00004932(sod-3)|GO:0010467(gene expression)"
Remark	"QUALIFY:PATO:0001997(reduced) NOT"
Remark	"Published_as daf-16"
Remark	"We introduced transgenic reporters for these genes into daf-16(-); daf-2(-) mutants in which daf-16 was expressed in only one tissue: neurons. sod-3 was regulated in a strictly cell-autonomous fashion."
Reference	"WBPaper00041915"


Anatomy_function : "WBbtf0706"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000962"	Autonomous
Gene	"WBGene00000912"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBbt:0003679(neuron)|WBGene00003096(lys-7)|GO:0010467(gene expression)"
Remark	"QUALIFY:PATO:0001997(reduced) NOT"
Remark	"Published_as daf-16"
Remark	"We introduced transgenic reporters for these genes into daf-16(-); daf-2(-) mutants in which daf-16 was expressed in only one tissue: neurons. lys-7 was regulated in a strictly cell-autonomous fashion."
Reference	"WBPaper00041915"


Anatomy_function : "WBbtf0707"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000962"	Autonomous
Gene	"WBGene00000912"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBbt:0003679(neuron)|WBGene00003473(mtl-1)|GO:0010467(gene expression)"
Remark	"QUALIFY:PATO:0001997(reduced) NOT"
Remark	"Published_as daf-16"
Remark	"We introduced transgenic reporters for these genes into daf-16(-); daf-2(-) mutants in which daf-16 was expressed in only one tissue: neurons. mtl-1 was regulated in a strictly cell-autonomous fashion."
Reference	"WBPaper00041915"


Anatomy_function : "WBbtf0708"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000962"	Autonomous
Gene	"WBGene00000912"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBbt:0003679(neuron)|WBGene00010745(dod-17)|GO:0010467(gene expression)"
Remark	"QUALIFY:PATO:0002051(increased occurence) NOT"
Remark	"Published_as daf-16"
Remark	"We introduced transgenic reporters for these genes into daf-16(-); daf-2(-) mutants in which daf-16 was expressed in only one tissue: neurons. dod-17 was regulated in a strictly cell-autonomous fashion."
Reference	"WBPaper00041915"


Anatomy_function : "WBbtf0709"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000962"	Autonomous
Gene	"WBGene00000912"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBbt:0003679(neuron)|WBGene00001843(hgo-1)|GO:0010467(gene expression)"
Remark	"QUALIFY:PATO:0001997(reduced) NOT"
Remark	"Published_as daf-16"
Remark	"We introduced transgenic reporters for these genes into daf-16(-); daf-2(-) mutants in which daf-16 was expressed in only one tissue: neurons. hgo-1 was regulated in a strictly cell-autonomous fashion."
Reference	"WBPaper00041915"


Anatomy_function : "WBbtf0710"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000962"	Autonomous
Gene	"WBGene00000912"
Involved	"WBbt:0005792"	Sufficient
Remark	"ENTITY:WBbt:0003679(neuron)|WBGene00001684(gpd-2)|GO:0010467(gene expression)"
Remark	"QUALIFY:PATO:0001997(reduced) NOT"
Remark	"Published_as daf-16"
Remark	"We introduced transgenic reporters for these genes into daf-16(-); daf-2(-) mutants in which daf-16 was expressed in only one tissue: neurons. gpd-2 was regulated in a strictly cell-autonomous fashion."
Reference	"WBPaper00041915"


Anatomy_function : "WBbtf0711"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000962"	Autonomous
Gene	"WBGene00000912"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBbt:0003679(neuron)|WBGene00001684(nnt-1)|GO:0010467(gene expression)"
Remark	"QUALIFY:PATO:0001997(reduced) NOT"
Remark	"Published_as daf-16"
Remark	"We introduced transgenic reporters for these genes into daf-16(-); daf-2(-) mutants in which daf-16 was expressed in only one tissue: neurons. nnt-1 was regulated in a strictly cell-autonomous fashion."
Reference	"WBPaper00041915"


Anatomy_function : "WBbtf0712"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000962"	Autonomous
Gene	"WBGene00000912"
Involved	"WBbt:0006804"	Sufficient
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|WBGene00004932(sod-3)|GO:0010467(gene expression)"
Remark	"QUALIFY:PATO:0001997(reduced) NOT"
Remark	"Published_as daf-16"
Remark	"We introduced transgenic reporters for these genes into daf-16(-); daf-2(-) mutants in which daf-16 was expressed in only one tissue: muscles. sod-3 was regulated in a strictly cell-autonomous fashion."
Reference	"WBPaper00041915"


Anatomy_function : "WBbtf0713"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000962"	Autonomous
Gene	"WBGene00000912"
Involved	"WBbt:0006804"	Sufficient
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|WBGene00003096(lys-7)|GO:0010467(gene expression)"
Remark	"QUALIFY:PATO:0001997(reduced) NOT"
Remark	"Published_as daf-16"
Remark	"We introduced transgenic reporters for these genes into daf-16(-); daf-2(-) mutants in which daf-16 was expressed in only one tissue: muscles. lys-7 was regulated in a strictly cell-autonomous fashion."
Reference	"WBPaper00041915"


Anatomy_function : "WBbtf0714"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000962"	Autonomous
Gene	"WBGene00000912"
Involved	"WBbt:0006804"	Sufficient
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|WBGene00003473(mtl-1)|GO:0010467(gene expression)"
Remark	"QUALIFY:PATO:0001997(reduced) NOT"
Remark	"Published_as daf-16"
Remark	"We introduced transgenic reporters for these genes into daf-16(-); daf-2(-) mutants in which daf-16 was expressed in only one tissue: muscles. mtl-1 was regulated in a strictly cell-autonomous fashion."
Reference	"WBPaper00041915"


Anatomy_function : "WBbtf0715"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000962"	Autonomous
Gene	"WBGene00000912"
Involved	"WBbt:0006804"	Sufficient
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|WBGene00001843(hgo-1)|GO:0010467(gene expression)"
Remark	"QUALIFY:PATO:0001997(reduced) NOT"
Remark	"Published_as daf-16"
Remark	"We introduced transgenic reporters for these genes into daf-16(-); daf-2(-) mutants in which daf-16 was expressed in only one tissue: muscles. hgo-1 was regulated in a strictly cell-autonomous fashion."
Reference	"WBPaper00041915"


Anatomy_function : "WBbtf0716"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000962"	Autonomous
Gene	"WBGene00000912"
Involved	"WBbt:0006804"	Sufficient
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|WBGene00001684(gpd-2)|GO:0010467(gene expression)"
Remark	"QUALIFY:PATO:0001997(reduced) NOT"
Remark	"Published_as daf-16"
Remark	"We introduced transgenic reporters for these genes into daf-16(-); daf-2(-) mutants in which daf-16 was expressed in only one tissue: muscles. gpd-2 was regulated in a strictly cell-autonomous fashion."
Reference	"WBPaper00041915"


Anatomy_function : "WBbtf0717"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000962"	Autonomous
Gene	"WBGene00000912"
Involved	"WBbt:0006804"	Sufficient
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|WBGene00001684(nnt-1)|GO:0010467(gene expression)"
Remark	"QUALIFY:PATO:0001997(reduced) NOT"
Remark	"Published_as daf-16"
Remark	"We introduced transgenic reporters for these genes into daf-16(-); daf-2(-) mutants in which daf-16 was expressed in only one tissue: muscles. nnt-1 was regulated in a strictly cell-autonomous fashion."
Reference	"WBPaper00041915"


Anatomy_function : "WBbtf0718"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000962"	Nonautonomous
Gene	"WBGene00000912"
Involved	"WBbt:0005792"	Sufficient
Remark	"ENTITY:WBbt:0005792(intestinal cell)|WBbt:0006804(body wall muscle cell)|WBbt:0007846(hypodermal cell)|WBGene00010790(dod-11)|GO:0010467(gene expression)"
Remark	"QUALIFY:PATO:0001997(reduced) NOT"
Remark	"In daf-2(-) mutants expressing daf-16(+) only in the intestine, expression of Pdod-11::rfp was induced in the hypodermis and muscles in multiple independent lines. Within the intestine itself, GFP::DAF-16-positive cells generally expressed Pdod-11::rfp, but we observed exceptions."
Remark	"Published_as daf-16"
Reference	"WBPaper00041915"


Anatomy_function : "WBbtf0719"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000962"	Nonautonomous
Gene	"WBGene00000912"
Involved	"WBbt:0006804"	Sufficient
Remark	"ENTITY:WBbt:0005792(intestinal cell)|WBbt:0006804(body wall muscle cell)|WBbt:0007846(hypodermal cell)|WBGene00010790(dod-11)|GO:0010467(gene expression)"
Remark	"QUALIFY:PATO:0001997(reduced) NOT"
Remark	"In daf-2(-) mutants expressing daf-16(+) only in muscles exhibited dod-11 induction in the muscles, intestine, and hypodermis."
Remark	"Published_as daf-16"
Reference	"WBPaper00041915"


Anatomy_function : "WBbtf0720"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000962"	Nonautonomous
Gene	"WBGene00000912"
Involved	"WBbt:0005792"	Sufficient
Remark	"ENTITY:WBbt:0005792(intestinal cell)|WBbt:0007846(hypodermal cell)|WBbt:0005792(hsp-12.6)|GO:0010467(gene expression)"
Remark	"QUALIFY:PATO:0001997(reduced) NOT"
Remark	"In daf-2(-) mutants intestine-expressed daf-16 induced hsp-12.6 expression in the intestine as well as in daf-16(-) tissues, such as the hypodermis."
Remark	"Published_as daf-16"
Reference	"WBPaper00041915"


Anatomy_function : "WBbtf0721"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000962"	Nonautonomous
Gene	"WBGene00000912"
Involved	"WBbt:0006804"	Sufficient
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|WBbt:0007846(hypodermal cell)|WBbt:0005792(hsp-12.6)|GO:0010467(gene expression)"
Remark	"QUALIFY:PATO:0001997(reduced) NOT"
Remark	"In daf-2(-) mutants muscle-expressed daf-16 was able to induce the hsp-12.6 reporter in both muscles and hypodermis."
Remark	"Published_as daf-16"
Reference	"WBPaper00041915"


Anatomy_function : "WBbtf0722"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000962"	Autonomous
Gene	"WBGene00000912"
Involved	"WBbt:0005792"	Sufficient
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|WBbt:0007846(hypodermal cell)|WBGene00007363(dod-8)|GO:0010467(gene expression)"
Remark	"QUALIFY:PATO:0002051(increased occurence) NOT"
Remark	"In two independent transgenic lines (daf-2 daf-16 mutant), intestinal DAF-16 activity strongly attenuated dod-8 reporter expression in the hypodermis and muscles."
Remark	"Published_as daf-16"
Reference	"WBPaper00041915"


Anatomy_function : "WBbtf0723"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000105"
Gene	"WBGene00002189"
Not_involved	"WBbt:0005784"	Unnecessary
Remark	"ENTITY:WBbt:0006797(oocyte)|GO:0001556(oocyte maturation)"
Remark	"QUALIFY:PATO:0002052(decreased occurance) NOT"
Remark	"Genotype \"kin-1(ok338); nEx109[kin-1(+) sur-5::gfp]\""
Remark	"Published_as kin-1"
Remark	"We conducted genetic mosaic analysis using the kin-1(ok338) deletion allele. Loss of kin-1(+) function in germ-line lineages (P3 and P4) did not affect viability or fertility. Thus, kin-1 is not required in the germ line for meiotic maturation."
Reference	"WBPaper00041364"


Anatomy_function : "WBbtf0724"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000106"
Gene	"WBGene00002189"
Not_involved	"WBbt:0005784"	Unnecessary
Remark	"ENTITY:WBbt:0006797(oocyte)|GO:0001556(oocyte maturation)|GO:1900194(negative regulation of oocyte maturation)"
Remark	"QUALIFY:PATO:0002052(decreased occurance) NOT"
Remark	"Genotype \"kin-1(ok338); nEx109[kin-1(+) sur-5::gfp]\""
Remark	"Published_as kin-1"
Remark	"To assess whether kin-1 might function in the germ line to inhibit meiotic maturation, we asked whether oocytes continue to undergo meiotic maturation and ovulation upon the depletion of sperm through self-fertilization in germline mosaics. We observed that kin-1 (ok338) germline mosaics produced a total of 10 +/- 14 unfertilized oocytes as compared to 14 +/- 21 unfertilized oocytes for nonmosaic siblings. Thus, kin-1(+) function is dispensable in the germ line both for meiotic maturation and also for its inhibition when sperm are absent or limiting."
Reference	"WBPaper00041364"


Anatomy_function : "WBbtf0725"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000105"
Gene	"WBGene00002189"
Involved	"WBbt:0005828"	Sufficient
Involved	"WBbt:0005828"	Necessary
Remark	"ENTITY:WBbt:0006797(oocyte)|GO:0001556(oocyte maturation)"
Remark	"QUALIFY:PATO:0002052(decreased occurance)"
Remark	"Genotype \"kin-1(ok338); nEx109[kin-1(+) sur-5::gfp]\""
Remark	"Published_as kin-1"
Remark	"We conducted genetic mosaic analysis using the kin-1(ok338) deletion allele. We sought array losses in the MS lineage, which gives rise to the somatic cells of the gonad. kin-1(+) somatic gonad-loss mosaics exhibit sterility because oocytes fail to undergo meiotic maturation, ovulation, and fertilization, Complex losses found within the sheath-spermathecal lineages suggest that kin-1 is needed in the gonadal sheath cells, not in the spermatheca, for meiotic maturation."
Reference	"WBPaper00041364"


Anatomy_function : "WBbtf0726"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000105"
Gene	"WBGene00019245"
Involved	"WBbt:0005784"	Necessary
Remark	"ENTITY:WBbt:0007849(hermaphrodite)|GO:0019953(sexual reproduction)"
Remark	"QUALIFY:PATO:0002052(decreased occurance) NOT"
Remark	"Genotype \"rrf-1(pk1417); acy-4(ok1806); tnEx37[acy-4(+) sur-5::gfp]\""
Remark	"Published_as sacy-1"
Remark	"To assess whether RNAi depletion of sacy-1 function in the germ line or somatic gonad mediates the suppression of acy-4 (lf) sterility, we conducted RNAi experiments in the somatic gonad RNAi-deficient rrf-1(pk1417) genetic background. sacy-1(RNAi) using rrf-1(pk1417); acy-4(ok1806); tnEx37 suppresses acy-4(lf) sterility in the F1 generation. Thus, reduction of sacy-1 function in the germ line suppresses acy-4(lf) sterility."
Reference	"WBPaper00041364"


Anatomy_function : "WBbtf0727"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000105"
Gene	"WBGene00006656"
Involved	"WBbt:0007815"	Necessary
Remark	"ENTITY:WBbt:0007849(hermaphrodite)|GO:0019953(sexual reproduction)"
Remark	"QUALIFY:PATO:0002052(decreased occurance) NOT"
Remark	"Genotype \"twk-1(tn1397); acy-4(ok1806); tnEx180[twk-1(+) sur-5::gfp]\""
Remark	"Published_as twk-1"
Remark	"To test more definitively whether acy-4(ok1806) sterility requires twk-1(+) function in the somatic gonad, we conducted genetic mosaic analysis of acy-4(lf) suppression. We sought fertile genetic mosaics among twk-1(tn1397); acy-4(ok1806); tnEx180[twk-1(+) sur-5::gfp] animals, produced by acy-4(ok1806)/+ heterozygous parents using nT1[qIs51] as a dominantly marked balancer chromosome for acy-4(ok1806). Two genetic mosaics with losses in the EMS founder cell, which is a precursor to the somatic gonad, were fertile in both gonad arms. These genetic mosaics produced GFP-containing progeny, indicating that their germ lines were twk-1(+). A third genetic mosaic animal resulted from complex losses within the Z1 lineage . This animal was fertile in the anterior gonad arm, but was sterile in the posterior gonad arm. All gonadal sheath cells in the anterior gonad arm of this mosaic were twk-1(tn1397) mutant, but the germline and several anterior spermathecal cells were twk-1(+). A fourth genetic mosaic, resulting from a loss in the Z4 somatic gonadal precursor cell (and some cells within the C lineage), was fertile in the posterior gonad arm, but not the anterior gonad arm. The germ line of this animal was also twk-1(+). We conclude that twk-1 functions downstream of acy-4 in the somatic gonad to regulate meiotic maturation."
Reference	"WBPaper00041364"


Anatomy_function : "WBbtf0728"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000415"
Gene	"WBGene00019245"
Involved	"WBbt:0005784"	Necessary
Remark	"ENTITY:WBbt:0006796(germ cell)|GO:0070265(necrotic cell death)"
Remark	"QUALIFY:PATO:0002052(decreased occurance) NOT"
Remark	"Genotype \"sacy-1(tm5503); unc-119(ed3); tnEx159[gfp::sacy-1 unc-119(+)]\""
Remark	"Published_as sacy-1"
Remark	"We sought genetic mosaics using the sacy-1(tm5503); unc-119(ed3); tnEx159[gfp::sacy-1 unc-119(+)] strain in which the rescuing GFP::SACY-1 fusion is expressed in most or all germline and somatic cells and serves as a cell-autonomous marker for mosaic analysis. The unc-119(ed3) genetic background was utilized as a marker for the AB lineage so as to identify rare non-Unc mosaics showing the sacy-1(tm5503) gamete degeneration phenotype. We found four genetic mosaics with P1 losses, a single mosaic with a P3 loss (this animal had an independent loss within the C lineage), and two mosaics with P4 losses. This result indicates that sacy-1(+) function is required in the germ line to prevent gamete degeneration."
Reference	"WBPaper00041364"


Anatomy_function : "WBbtf0729"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000029"
Gene	"WBGene00017445"
Involved	"WBbt:0005792"	Sufficient
Remark	"ENTITY: WBbt:0006804(body wall muscle cell)|GO:0016246(RNA interference)|GO:0009605(response to external stimulus)"
Remark	"QUALIFY:PATO:0002052(decreased occurrence) NOT"
Remark	"Genotype \"ccIs4251[myo-3p::GFP*] I; mIs11 [myo-2p::GFP] IV; sid-5(qt24)X; qtEx125[sid-2p::sid-5; sid-2p::DsRed]\""
Remark	"Intestinal SID-5 expression could restore silencing of transgenic (GFP) and endogenous (unc-22) bwm targets in response to environmental RNA."
Remark	"Published_as sid-5"
Reference	"WBPaper00041563"


Anatomy_function : "WBbtf0730"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000029"
Gene	"WBGene00017445"
Not_involved	"WBbt:0006804"	Insufficient
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|GO:0016246(RNA interference)|GO:0009605(response to external stimulus)"
Remark	"QUALIFY:PATO:0002052(decreased occurrence)"
Remark	"Genotype \"ccIs4251[myo-3::GFP*] I; mIs11[myo-2p::GFP] IV; sid-5(qt24) X;qtEx121[myo-3p::sid-5; pHC183 (myo-3p::DsRed)]\""
Remark	"In the case of sid-5 mutants, we found the opposite: intestinal SID-5 expression, but not bwm SID-5 expression, could restore silencing of both transgenic (GFP) and endogenous (unc-22) bwm targets in response to environmental RNAi."
Remark	"Published_as sid-5"
Reference	"WBPaper00041563"


Anatomy_function : "WBbtf0731"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000029"
Gene	"WBGene00004795"
Involved	"WBbt:0006804"	Sufficient
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|GO:0016246(RNA interference)|GO:0009605(response to external stimulus)"
Remark	"QUALIFY:PATO:0002052(decreased occurrence) NOT"
Remark	"Genotype \"ccIs4251[myo-3::GFP*] I; mIs11[myo-2p::GFP] IV; sid-1(qt9) X;qtEx[myo-3p::sid-1; pHC183 (myo-3p::DsRed)]\""
Remark	"Published_as sid-1"
Remark	"We tested myo-3::sid-1 extrachromosomal array for the ability to silence the bwm gene unc-22 in response to feeding RNAi. unc-22 silencing was observed when sid-1 was rescued in the bwm of the sid-1 mutant strain."
Reference	"WBPaper00041563"


Anatomy_function : "WBbtf0732"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000029"
Gene	"WBGene00017445"
Not_involved	"WBbt:0005792"	Insufficient
Remark	"ENTITY:WBbt:0006804(body wall muscle cell)|GO:0016246(RNA interference)|GO:0031668(cellular response to extracellular stimulus)"
Remark	"QUALIFY:PATO:0002052(decreased occurrence) NOT"
Remark	"Genotype \"ccIs4251[myo-3p::GFP*] I; qtIs3[myo-2::GFP-hpRNA] III; mIs11[myo-2p::GFP] IV; sid-5(qt24) X; qtEx127[sid-2p::sid-5; sid-2p::DsRed]\""
Remark	"It has recently been shown that some proteins required for RNAi, e.g., the RNA-binding protein RDE-4, can rescue the mutant phenotype when expressed in a third tissue, i.e., neither the sending or receiving cells. To test whether this could also be true for SID-5, we rescued SID-5 specifically in the intestine in sid-5 mutants expressing body wall muscle GFP and pharyngeal gfp-hpRNA. However, this did not restore silencing of bwm GFP after starvation."
Remark	"Published_as sid-5"
Reference	"WBPaper00041563"


Anatomy_function : "WBbtf0733"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000676"
Gene	"WBGene00006342"
Involved	"WBbt:0005208"	Necessary
Remark	"E(-) mosaics, those lacking the sup-37 (+) array in all cells of the intestine, were invariably slightly retarded in growth relative to non-mosaics on partially synchronous plates (L4s vs. adults)."
Remark	"ENTITY:WBbt:0007833(organism)|GO:0040007(growth)"
Remark	"QUALIFY:PATO:0000911(slow rate)"
Remark	"Genotype \"sup-37(tm356)V; fdEx174(sup-37+,sur-5::GFP)\""
Remark	"Published_as sup-37"
Reference	"WBPaper00041001"


Anatomy_function : "WBbtf0734"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000634"
Gene	"WBGene00006342"
Involved	"WBbt:0004458"	Necessary
Remark	"ENTITY:WBbt:0003681(pharynx)|GO:0007631(eating behavior)"
Remark	"QUALIFY:PATO:0000381(decreased frequency) NOT"
Remark	"Genotype \"sup-37(tm356)V; fdEx174(sup-37+,sur-5::GFP)\""
Remark	"Healthy genetic mosaics that segregated from WY733 were analyzed. Because these mosaics were healthy and had reached the L4 or young adult stage, it is reasonable to assume that wild-type sup-37 present on the fdEx174 array functioned in these mosaics in the proper part of the cell lineage required for normal pharyngeal pumping. The only early cells of the lineage that did not undergo losses of the array were P1; EMS, one of the daughters of P1; and MS, a granddaughter of P1, indicating that the focus of gene activity descends from MS."
Remark	"Published_as sup-37"
Reference	"WBPaper00041001"


Anatomy_function : "WBbtf0735"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000707"	Nonautonomous
Gene	"WBGene00002247"
Involved	"WBbt:0005792"	Sufficient
Remark	"Because several C. elegans tissues have been reported to express laminin, including the pharynx, intestine and BWMs, we investigated which cells must express lam-1 to properly orient PPC polarity. e constructed a homozygous lam-1(ok3139) strain that carried an extrachromosomal array (zuEx288) containing a wild-type lam-1(+) gene plus a cell-autonomous marker (SUR-5::GFP). We found that the pharynx had a single lumen in 6/8 animals with zuEx288 only in intestinal cells."
Remark	"ENTITY:WBbt:0003681(pharynx)|GO:0001738(morphogenesis of a polarized epithelium)"
Remark	"QUALIFY:PATO:0001507(disrupted) NOT"
Remark	"Genotype \"lam-1(ok3139); zuEx288[lam-1(+) SUR-5::GFP]\""
Remark	"Published_as lam-1"
Reference	"WBPaper00041027"


Anatomy_function : "WBbtf0736"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000707"	Nonautonomous
Gene	"WBGene00002247"
Involved	"WBbt:0006804"	Sufficient
Involved	"WBbt:0007846"	Sufficient
Remark	"Because several C. elegans tissues have been reported to express laminin, including the pharynx, intestine and BWMs, we investigated which cells must express lam-1 to properly orient PPC polarity. e constructed a homozygous lam-1(ok3139) strain that carried an extrachromosomal array (zuEx288) containing a wild-type lam-1(+) gene plus a cell-autonomous marker (SUR-5::GFP). We found that the pharynx had a single lumen in 14/17 animals with zuEx288 only in skin (hypodermal) cells and BWMs."
Remark	"ENTITY:WBbt:0003681(pharynx)|GO:0001738(morphogenesis of a polarized epithelium)"
Remark	"QUALIFY:PATO:0001507(disrupted) NOT"
Remark	"Genotype \"lam-1(ok3139); zuEx288[lam-1(+) SUR-5::GFP]\""
Remark	"Published_as lam-1"
Reference	"WBPaper00041027"


Anatomy_function : "WBbtf0737"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000828"	Nonautonomous
Gene	"WBGene00003029"
Not_involved	"WBbt:0008409"	Unnecessary
Remark	"ENTITY:WBbt:0008409(T cell)|GO:0007163(establishment or maintenance of cell polarity)|GO:0051301(cell division)"
Remark	"QUALIFY:PATO:0001507(disrupted)"
Remark	"Genotype \"lin-44; ncl-1(e1865) unc-36(e251); mnEx31[lin-44(+) ncl-1(+) unc-36(+)]\""
Remark	"Published_as lin-44"
Remark	"To generate lin-44 mosaics, we made lin-44; ncl-1 unc-36 animals transgenic for an extrachromosomal array of DNA, mnEx37, that contains wild-type copies of lin-44, ncl-1, and unc-36. Among the total of 15 animals in which both TL and TR were genotypically mutant, 12 showed normal polarity for both T cells. We conclude that lin-44 acts cell nonautonomously."
Reference	"WBPaper00002293"


Anatomy_function : "WBbtf0738"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000828"	Nonautonomous
Gene	"WBGene00003029"
Not_involved	"WBbt:0008409"	Unnecessary
Remark	"ENTITY:WBbt:0003825(B cell)|GO:0007163(establishment or maintenance of cell polarity)|GO:0051301(cell division)"
Remark	"QUALIFY:PATO:0001507(disrupted)"
Remark	"Genotype \"lin-44; ncl-1(e1865) unc-36(e251), him-5; mnEx31[lin-44(+) ncl-1(+) unc-36(+)]\""
Remark	"Published_as lin-44"
Remark	"To generate lin-44 mosaics, we made lin-44; ncl-1 unc-36 animals transgenic for an extrachromosomal array of DNA, mnEx31, that contains wild-type copies of lin-44, ncl-1, and unc-36. We also examined B cell polarity in mosaic males that had early losses in the AB.p lineage. We found five mosaic males of the desired type, three of which had lost the array at the division that generates AB, and all five males had normal B, TL, and TR cell polarities."
Reference	"WBPaper00002293"


Anatomy_function : "WBbtf0739"
Assay	"Blastomere_isolation"
Phenotype	"WBPhenotype:0000708"
Not_involved	"WBbt:0004015"	Unnecessary
Not_involved	"WBbt:0006873"	Unnecessary
Not_involved	"WBbt:0004458"	Unnecessary
Remark	"ENTITY:WBbt:0005792(intestinal cell)|GO:0009888(tissue development)"
Remark	"QUALIFY:PATO:0001507(disrupted) NOT"
Remark	"To determine if anterior endoderm requires contact with cells from other lineages, laser ablation was used to kill the non-gut progenitors of the first three cell divisions: AB at the 2-cell stage, P2 in the 4-cell stage (after the P2-EMS contact just mentioned), and MS at the 8-cell stage. In combination, these ablations eliminate all non-gut lineages. None of these ablations (including simultaneous ablation of AB, P2 and MS) prevent anterior gut marker expression, suggesting that gut patterning is lineage autonomous."
Reference	"WBPaper00003331"


Anatomy_function : "WBbtf0740"
Assay	"Blastomere_isolation"
Phenotype	"WBPhenotype:0000708"
Not_involved	"WBbt:0006612"	Unnecessary
Remark	"ENTITY:WBbt:0006733(Ea)|GO:0009888(tissue development)"
Remark	"QUALIFY:PATO:0001507(disrupted) NOT"
Remark	"Within the E lineage, ablation of Ep, the posterior daughter of the E cell, also does not prevent the formation of Ea-derived anterior gut."
Reference	"WBPaper00003331"


Anatomy_function : "WBbtf0741"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000111"
Involved	"WBbt:0004875"	Necessary
Involved	"WBbt:0004874"	Necessary
Remark	"ENTITY:WBbt:0007446(V5L.p)|WBbt:0007463(V5R.p)|GO:0010467(gene expression)|WBGene00003102(mab-5)"
Remark	"QUALITY:PATO:0000462(absent) NOT"
Remark	"We asked whether expression of a mab-5-GFP fusion could be switched on precociously in the V5 lineage following ablation of V6. We found that following ablation of V6, GFP expression was detected in V5.p and both seam cell daughters. We verified this finding using anti-MAB-5 antisera."
Reference	"WBPaper00003428"


Anatomy_function : "WBbtf0742"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000216"	Autonomous
Gene	"WBGene00003912"
Involved	"WBbt:0004875"	Necessary
Involved	"WBbt:0004874"	Necessary
Remark	"ENTITY: WBbt:0004874(V6R)|WBbt:0004875(V6L)|GO:0001708(cell fate specification)| WBbt:0006941(ray)|PATO:0002470(transformed to)|WBbt:0007832(alae)"
Remark	"QUALITY:PATO:0002470(absent)"
Remark	"Genotype \"pal-1(ct224) dpy-17(e164) ncl-1(e1865) unc-36(e251) III; him-8(e1489) IV; sDp3(III;f)\""
Remark	"Published_as pal-1"
Remark	"We isolated viable pal-1(ct224) genetic mosaics using the linked mutation ncl-1 as a genotypic marker. Among these mosaic animals were two males with Pal phenotypes; in both cases, the V6 cell was Ncl and therefore mutant for pal-1. This indicated that this V6 ray phenotype was indeed due to lack of pal-1 activity."
Reference	"WBPaper00003428"


Anatomy_function : "WBbtf0743"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000216"
Gene	"WBGene00003912"
Not_involved	"WBbt:0004890"	Unnecessary
Not_involved	"WBbt:0004876"	Unnecessary
Remark	"ENTITY: WBbt:0004874(V6R)|WBbt:0004875(V6L)|GO:0001708(cell fate specification)| WBbt:0006941(ray)|PATO:0002470(transformed to)|WBbt:0007832(alae)"
Remark	"QUALITY:PATO:0002470(absent) NOT"
Remark	"Genotype \"pal-1(ct224) dpy-17(e164) ncl-1(e1865) unc-36(e251) III; him-8(e1489) IV; sDp3(III;f)\""
Remark	"Published_as pal-1"
Remark	"We isolated viable pal-1(ct224) genetic mosaics using the linked mutation ncl-1 as a genotypic marker. We also identified several other Ncl-1 mosaic males in which other cells that require mab-5 activity were Ncl. Four of these animals were pal-1(&amp;#8722;) in ABp-derived cells and produced animals that appeared wild type. Since ABp gives rise to V5, this finding indicates that cells in the V5 lineage do not require pal-1 activity to develop normally."
Reference	"WBPaper00003428"


Anatomy_function : "WBbtf0744"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001585"	Autonomous
Gene	"WBGene00001194"
Involved	"WBbt:0008409"	Sufficient
Involved	"WBbt:0008409"	Necessary
Remark	"ENTITY:WBbt:0008409(T cell)|GO:0008356(asymmetric cell division)"
Remark	"QUALITY:PATO:0001511(defective)"
Remark	"Genotype \"unc-29(e1072); egl-27(mn553); mhEx7[unc-29(+) egl-27::gfp\""
Remark	"Published_as egl-27"
Remark	"To generate egl-27 mosaics, we made unc-29; egl-27 animals transgenic for an extrachromosomal array of DNA that contains the functional egl-27::gfp fusion and a wild-type copy of unc-29. We found 30 examples in which the polarity of the T cell was abnormal, and in 29 of these, the transgene was missing from the T cell descendants. By contrast, we found 242 examples of normal T cell polarity, and all 242 contained the transgene. We conclude that egl-27 is required cell autonomously within the T cells for normal polarity."
Reference	"WBPaper00003450"


Anatomy_function : "WBbtf0745"
Assay	"Blastomere_isolation"
Phenotype	"WBPhenotype:0001681"	Nonautonomous
Gene	"WBGene00003394"
Involved	"WBbt:0006873"	Sufficient
Involved	"WBbt:0006873"	Necessary
Remark	"ENTITY:WBbt:0006876(EMS)|GO:0000132(establishment of mitotic spindle orientation)"
Remark	"QUALITY:PATO:0001511(defective)"
Remark	"Published_as mom-1"
Remark	"We constructed genetic chimeras to determine if these and other genes are required in P2 to signal, or in EMS to respond to signaling. We isolated blastomeres from mutant and wild-type embryos, and in each experiment re-associated a mutant cell with a wild-type partner. When placed in contact with a wild-type EMS mom-1/porc mutant, P2 blastomeres failed to properly orient EMS mitotic spindles, whereas EMS cells from these mutant embryos were capable of responding to wild-type P2 cells."
Reference	"WBPaper00003645"


Anatomy_function : "WBbtf0746"
Assay	"Blastomere_isolation"
Phenotype	"WBPhenotype:0001681"	Nonautonomous
Gene	"WBGene00003395"
Involved	"WBbt:0006873"	Sufficient
Involved	"WBbt:0006873"	Necessary
Remark	"ENTITY:WBbt:0006876(EMS)|GO:0000132(establishment of mitotic spindle orientation)"
Remark	"QUALITY:PATO:0001511(defective)"
Remark	"Published_as mom-2"
Remark	"We constructed genetic chimeras to determine if these and other genes are required in P2 to signal, or in EMS to respond to signaling. We isolated blastomeres from mutant and wild-type embryos, and in each experiment re-associated a mutant cell with a wild-type partner. When placed in contact with a wild-type EMS, mom-2/wg mutant P2 blastomeres failed to properly orient EMS mitotic spindles, whereas EMS cells from these mutant embryos were capable of responding to wild-type P2 cells."
Reference	"WBPaper00003645"


Anatomy_function : "WBbtf0747"
Assay	"Blastomere_isolation"
Phenotype	"WBPhenotype:0001681"	Nonautonomous
Gene	"WBGene00003246"
Involved	"WBbt:0006873"	Sufficient
Involved	"WBbt:0006873"	Necessary
Remark	"ENTITY:WBbt:0006876(EMS)|GO:0000132(establishment of mitotic spindle orientation)"
Remark	"QUALITY:PATO:0001511(defective)"
Remark	"Published_as mom-3"
Remark	"We constructed genetic chimeras to determine if these and other genes are required in P2 to signal, or in EMS to respond to signaling. We isolated blastomeres from mutant and wild-type embryos, and in each experiment re-associated a mutant cell with a wild-type partner. When placed in contact with a wild-type EMS, mom-3 mutant P2 blastomeres failed to properly orient EMS mitotic spindles, whereas EMS cells from these mutant embryos were capable of responding to wild-type P2 cells."
Reference	"WBPaper00003645"


Anatomy_function : "WBbtf0748"
Assay	"Blastomere_isolation"
Phenotype	"WBPhenotype:0001681"	Autonomous
Gene	"WBGene00003397"
Involved	"WBbt:0006876"	Sufficient
Involved	"WBbt:0006876"	Necessary
Remark	"ENTITY:WBbt:0006876(EMS)|GO:0000132(establishment of mitotic spindle orientation)"
Remark	"QUALITY:PATO:0001511(defective)"
Remark	"Published_as mom-5"
Remark	"We constructed genetic chimeras to determine if these and other genes are required in P2 to signal, or in EMS to respond to signaling. We isolated blastomeres from mutant and wild-type embryos, and in each experiment re-associated a mutant cell with a wild-type partner.  EMS blastomeres from mom-5/fz mutants did not respond competently to wild-type P2 signaling, but mom-5/fz mutant P2 blastomeres properly oriented the spindle of wild-type EMS cells."
Reference	"WBPaper00003645"


Anatomy_function : "WBbtf0749"
Assay	"Blastomere_isolation"
Phenotype	"WBPhenotype:0001681"	Autonomous
Gene	"WBGene00001746"
Involved	"WBbt:0006876"	Sufficient
Involved	"WBbt:0006876"	Necessary
Remark	"ENTITY:WBbt:0006876(EMS)|GO:0000132(establishment of mitotic spindle orientation)"
Remark	"QUALITY:PATO:0001511(defective)"
Remark	"Published_as gsk-3"
Remark	"We constructed genetic chimeras to determine if these and other genes are required in P2 to signal, or in EMS to respond to signaling. We isolated blastomeres from mutant and wild-type embryos, and in each experiment re-associated a mutant cell with a wild-type partner.  EMS blastomeres from gsk-3 mutants did not respond competently to wild-type P2 signaling, but gsk-3 mutant P2 blastomeres properly oriented the spindle of wild-type EMS cells."
Reference	"WBPaper00003645"


Anatomy_function : "WBbtf0750"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001585"	Autonomous
Gene	"WBGene00004203"
Involved	"WBbt:0008409"	Necessary
Remark	"ENTITY:WBbt:0008409(T cell)|GO:0008356(asymmetric cell division)"
Remark	"QUALITY:PATO:0001511(defective)"
Remark	"Genotype \"unc-29(e1072); psa-1(os22); osEx77[psa-1::GFP unc-29(+)]\""
Remark	"Published_as psa-1"
Remark	"To analyze whether psa-1 is required in the T cell, we performed mosaic analyses. We constructed unc-29; psa-1 animals that were transgenic for an extrachromosomal array (osEx77) containing the wild-type unc-29 gene and functional psa-1 ::GFP. We found 10 examples in 115 non-Unc animals that showed the Psa phenotype. In all cases, the T cell descendants did not express GFP, indicating that the T cells did not have osEx77. Among them we found four examples in which we could not detect any GFP-negative cells except for the T cell descendants."
Reference	"WBPaper00004350"


Anatomy_function : "WBbtf0751"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000594"
Involved	"WBbt:0004578"	Necessary
Remark	"ENTITY:WBbt:0008606(P11/12L)|WBbt:0008607(P11/12R)|GO:0016477(cell migration)"
Remark	"QUALIFY:PATO:0000613(disoriented)"
Remark	"We ablated Y within 1 h after hatching. In the absence of Y, the bias in P(11/12)L/R migration is lost, as in lin-12(lf) mutants. Thus, the Y cell is required for the bias in P(11/12)L/R migration."
Reference	"WBPaper00004662"


Anatomy_function : "WBbtf0752"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000216"
Not_involved	"WBbt:0004250"	Unnecessary
Remark	"ENTITY:WBbt:0007446(V5L.p)|GO:0001708(cell fate specification)"
Remark	"QUALIFY:PATO:0000461(normal)"
Remark	"Using a laser microbeam, we ablated one of the V5 daughters shortly after the V5 cell division and then examined the fate adopted by the remaining daughter. Following V5.a ablation in wild-type animals, V5.p always adopted the expected seam fate."
Reference	"WBPaper00004436"


Anatomy_function : "WBbtf0753"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000216"
Not_involved	"WBbt:0007446"	Unnecessary
Remark	"ENTITY:WBbt:0004250(V5L.a)|GO:0001708(cell fate specification)"
Remark	"QUALIFY:PATO:0000461(normal)"
Remark	"Using a laser microbeam, we ablated one of the V5 daughters shortly after the V5 cell division and then examined the fate adopted by the remaining daughter. When V5.p was ablated, V5.a always adopted the syncytial fat."
Reference	"WBPaper00004436"


Anatomy_function : "WBbtf0754"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000216"
Not_involved	"WBbt:0007463"	Unnecessary
Remark	"ENTITY:WBbt:0004246(V5R.a)|GO:0001708(cell fate specification)"
Remark	"QUALIFY:PATO:0000461(normal)"
Remark	"Using a laser microbeam, we ablated one of the V5 daughters shortly after the V5 cell division and then examined the fate adopted by the remaining daughter. When V5.p was ablated, V5.a always adopted the syncytial fat."
Reference	"WBPaper00004436"


Anatomy_function : "WBbtf0755"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000216"
Not_involved	"WBbt:0004220"	Unnecessary
Remark	"ENTITY:WBbt:0007463(V5R.p)|GO:0001708(cell fate specification)"
Remark	"QUALIFY:PATO:0000461(normal)"
Remark	"Using a laser microbeam, we ablated one of the V5 daughters shortly after the V5 cell division and then examined the fate adopted by the remaining daughter. Following V5.a ablation in wild-type animals, V5.p always adopted the expected seam fate."
Reference	"WBPaper00004436"


Anatomy_function : "WBbtf0756"
Assay	"Blastomere_isolation"
Phenotype	"WBPhenotype:0000216"
Involved	"WBbt:0003810"	Sufficient
Remark	"ENTITY:WBbt:0007846(hypodermal cell)|GO:0001708(cell fate specification)"
Remark	"QUALIFY:PATO:0000057(occurence)"
Remark	"We analyzed the differentiated cell types produced. An isolated wild-type C blastomere always produced epidermis."
Reference	"WBPaper00004636"


Anatomy_function : "WBbtf0757"
Assay	"Blastomere_isolation"
Phenotype	"WBPhenotype:0000216"
Not_involved	"WBbt:0004458"	Insufficient
Remark	"ENTITY:WBbt:0007846(hypodermal cell)|GO:0001708(cell fate specification)"
Remark	"QUALIFY:PATO:0001507(disrupted)"
Remark	"We analyzed the differentiated cell types produced. An isolated wild-type C blastomere always produced epidermis; an isolated MS cell never did."
Reference	"WBPaper00004636"


Anatomy_function : "WBbtf0758"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000216"
Involved	"WBbt:0006876"	Necessary
Remark	"EMS-ablated wild-type embryos always lack gut and pharynx (Pharynx cells were scored by expression of ceh-22 ::GFP)."
Remark	"ENTITY:WBbt:0005451(pharyngeal muscle cell)|GO:0001708(cell fate specification)"
Remark	"QUALIFY:PATO:0000057(occurence) NOT"
Reference	"WBPaper00004636"


Anatomy_function : "WBbtf0759"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000216"
Involved	"WBbt:0006876"	Necessary
Remark	"EMS-ablated wild-type embryos always lack gut (Intestinal cells were scored by polarized light birefringence or expression of elt-2::GFP) and pharynx."
Remark	"ENTITY:WBbt:0005792(intestinal cell)|GO:0001708(cell fate specification)"
Remark	"QUALIFY:PATO:0000057(occurence) NOT"
Reference	"WBPaper00004636"


Anatomy_function : "WBbtf0760"
Assay	"Blastomere_isolation"
Phenotype	"WBPhenotype:0001681"
Gene	"WBGene00005077"
Not_involved	"WBbt:0006873"	Unnecessary
Remark	"ENTITY:WBbt:0006876(EMS)|GO:0000132(establishment of mitotic spindle orientation)"
Remark	"QUALITY:PATO:0001511(defective) NOT"
Remark	"Isolated wild-type EMS cells placed back in contact with P2 (but not two EMS cells placed together), correctly orient their mitotic spindles in accordance with the P2 contact site. We next examined chimeric embryos assembled using a combination of wild-type and src-1 mutant blastomeres. We found that chimeric embryos lacking src-1 function in P2 exhibited a wild-type orientation of the EMS division axis."
Remark	"Published_as src-1"
Reference	"WBPaper00005375"


Anatomy_function : "WBbtf0761"
Assay	"Blastomere_isolation"
Phenotype	"WBPhenotype:0001681"	Autonomous
Gene	"WBGene00005077"
Involved	"WBbt:0006876"	Necessary
Remark	"ENTITY:WBbt:0006876(EMS)|GO:0000132(establishment of mitotic spindle orientation)"
Remark	"QUALITY:PATO:0001511(defective)"
Remark	"Isolated wild-type EMS cells placed back in contact with P2 (but not two EMS cells placed together), correctly orient their mitotic spindles in accordance with the P2 contact site. We next examined chimeric embryos assembled using a combination of wild-type and src-1 mutant blastomeres. We found that chimeric embryos lacking src-1 function in P2 exhibited a wild-type orientation of the EMS division axis, while embryos lacking src-1 function in EMS always failed to do so."
Remark	"Published_as src-1"
Reference	"WBPaper00005375"


Anatomy_function : "WBbtf0762"
Assay	"Blastomere_isolation"
Phenotype	"WBPhenotype:0001681"
Gene	"WBGene00003219"
Involved	"WBbt:0006876"	Necessary
Remark	"ENTITY:WBbt:0006876(EMS)|GO:0000132(establishment of mitotic spindle orientation)"
Remark	"QUALITY:PATO:0001511(defective)"
Remark	"Isolated wild-type EMS cells placed back in contact with P2 (but not two EMS cells placed together), correctly orient their mitotic spindles in accordance with the P2 contact site. We found that mes-1(+) activity was required in both EMS and P2 to orient the mitotic spindle of EMS."
Remark	"Published_as mes-1"
Reference	"WBPaper00005375"


Anatomy_function : "WBbtf0763"
Assay	"Blastomere_isolation"
Phenotype	"WBPhenotype:0001681"
Gene	"WBGene00003219"
Involved	"WBbt:0006873"	Necessary
Remark	"ENTITY:WBbt:0006876(EMS)|GO:0000132(establishment of mitotic spindle orientation)"
Remark	"QUALITY:PATO:0001511(defective)"
Remark	"Isolated wild-type EMS cells placed back in contact with P2 (but not two EMS cells placed together), correctly orient their mitotic spindles in accordance with the P2 contact site. We found that mes-1(+) activity was required in both EMS and P2 to orient the mitotic spindle of EMS."
Remark	"Published_as mes-1"
Reference	"WBPaper00005375"


Anatomy_function : "WBbtf0764"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000220"
Involved	"WBbt:0005175"	Necessary
Remark	"ENTITY:WBbt:000689(P5.p)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0001507(disrupted)"
Remark	"P5.p VPC failed to adopt the vulval cell fate as the gonadal primoridum was removed by laser ablation during the L1 larval stage."
Reference	"WBPaper00005632"


Anatomy_function : "WBbtf0765"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000220"
Involved	"WBbt:0005175"	Necessary
Remark	"ENTITY:WBbt:0006894(P6.p)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0001507(disrupted)"
Remark	"P6.p VPC failed to adopt the vulval cell fate as the gonadal primoridum was removed by laser ablation during the L1 larval stage."
Reference	"WBPaper00005632"


Anatomy_function : "WBbtf0766"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000220"
Involved	"WBbt:0005175"	Necessary
Remark	"ENTITY:WBbt:0006895(P7.p)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0001507(disrupted)"
Remark	"P7.p VPC failed to adopt the vulval cell fate as the gonadal primoridum was removed by laser ablation during the L1 larval stage."
Reference	"WBPaper00005632"


Anatomy_function : "WBbtf0767"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000470"	Autonomous
Gene	"WBGene00003238"
Involved	"WBbt:0006830"	Sufficient
Remark	"ENTITY:WBbt:0006830(HSN)|GO:0016477(cell migration)"
Remark	"QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"mig-1(e1787); gmEx384(Punc-86::mig-1::gfp)\""
Remark	"Published_as mig-1"
Remark	"We generated transgenic animals that used unc-86 sequences to drive expression of a mig-1 cDNA fused to GFP (gmEx384). In the posterior of the transgenic embryos, only the HSNs and PLM neurons expressed GFP. Expression of MIG-1::GFP in the HSNs rescued the HSN migration defects of mig-1 mutants, suggesting that MIG-1 functions in the HSNs to promote their migration."
Reference	"WBPaper00027140"


Anatomy_function : "WBbtf0768"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000384"	Autonomous
Gene	"WBGene00003238"
Involved	"WBbt:0003832"	Sufficient
Remark	"ENTITY:WBbt:0003832(AVM)|GO:0007411(axon guidance)"
Remark	"QUALITY:PATO:0000460(defective) NOT"
Remark	"Genotype \"mig-1(e1787) mom-5(ne12); gmEx414[mec-7::MIG-1::GFP])\""
Remark	"Published_as mig-1"
Remark	"To test whether Wnts act directly on the AVM/PVM neurons, we asked whether expression of MIG-1 in these cells could rescue their A/P guidance defects in mig-1 mom-5 mutants. We generated transgenic animals that expressed a mig-1 cDNA fused to GFP from the mec-7 promoter (gmEx414). Expression of MIG-1::GFP in the AVM/PVM rescues the migration defects of their growth cones in the mig-1(e1787) mom-5(ne12) mutants."
Reference	"WBPaper00027140"


Anatomy_function : "WBbtf0769"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000384"	Autonomous
Gene	"WBGene00003238"
Involved	"WBbt:0004086"	Sufficient
Remark	"ENTITY:WBbt:0004086(PVM)|GO:0007411(axon guidance)"
Remark	"QUALITY:PATO:0000460(defective) NOT"
Remark	"Genotype \"mig-1(e1787) mom-5(ne12); gmEx414[mec-7::MIG-1::GFP])\""
Remark	"Published_as mig-1"
Remark	"To test whether Wnts act directly on the AVM/PVM neurons, we asked whether expression of MIG-1 in these cells could rescue their A/P guidance defects in mig-1 mom-5 mutants. We generated transgenic animals that expressed a mig-1 cDNA fused to GFP from the mec-7 promoter (gmEx414). Expression of MIG-1::GFP in the AVM/PVM rescues the migration defects of their growth cones in the mig-1(e1787) mom-5(ne12) mutants."
Reference	"WBPaper00027140"


Anatomy_function : "WBbtf0770"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000470"	Autonomous
Gene	"WBGene00003238"
Involved	"WBbt:0006830"	Sufficient
Remark	"Entity: WBbt:0006830(HSN)|GO:0016477(cell migration)"
Remark	"Quality:PATO:0000375(decreased distance) NOT"
Remark	"Genotype \"mig-1(e1787); Ex[Punc-86::mig-1::gfp]\""
Remark	"Published_as mig-1"
Remark	"We generated transgenic animals that used unc-86 sequences to drive expression of a mig-1 cDNA fused to GFP (gmEx384). In the posterior of the transgenic embryos, only the HSNs and PLM neurons expressed GFP. Expression of MIG-1::GFP in the HSNs rescued the HSN migration defects of mig-1 mutants, suggesting that MIG-1 functions in the HSNs to promote their migration."
Reference	"WBPaper00027140"


Anatomy_function : "WBbtf0771"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000470"	Autonomous
Gene	"WBGene00003238"
Involved	"WBbt:0005237"	Sufficient
Remark	"Entity:WBbt:0003832(AVM)|WBbt:0004086(PVM)|GO:1990138(neuron projection extension)"
Remark	"Quality:PATO:0000574(decreased length) NOT"
Remark	"Genotype \"mig-1(e1787); mom-5(ne12); Ex[Pmec-7::mig-1::gfp]\""
Remark	"Published_as mig-1"
Remark	"We generated transgenic animals that expressed a mig-1 cDNA fused to GFP from the mec-7 promoter (gmEx414). Expression of MIG-1::GFP in the AVM and PVM of mig-1 mom-5 mutants significantly rescued their A/P guidance defects, suggesting that MIG-1 functions in the AVM and PVM to promote the anterior growth of their processes."
Reference	"WBPaper00027140"


Anatomy_function : "WBbtf0772"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000155"	Autonomous
Gene	"WBGene00003006"
Involved	"WBbt:0005237"	Sufficient
Remark	"Entity:WBbt:0005490(PLM)|GO:0048812(neuron projection morphogenesis)|GO:0009948(anterior/posterior axis specification)"
Remark	"Quality:PATO:0000625(reversed) NOT"
Remark	"Genotype \"lin-17(n677); kyEx738(mec-7::lin-17)\""
Remark	"Published_as lin-17"
Remark	"To determine whether lin-17 functions cell autonomously in PLM, we expressed a wild-type lin-17 cDNA selectively in mechanosensory neurons of lin-17 mutants by using mec-4 or mec-7 promoters, which direct expression in PLM, ALM, AVM, and PVM mechanosensory neurons. mec-4::lin-17 and mec-7::lin-17 transgenes were both able to rescue the PLM defects of lin-17 mutants with high efficiency."
Reference	"WBPaper00027140"


Anatomy_function : "WBbtf0773"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000155"	Autonomous
Gene	"WBGene00003006"
Involved	"WBbt:0005237"	Sufficient
Remark	"Entity:WBbt:0005490(PLM)|GO:0048812(neuron projection morphogenesis)|GO:0009948(anterior/posterior axis specification)"
Remark	"Quality:PATO:0000625(reversed) NOT"
Remark	"Genotype \"lin-17(n677); kyEx739(mec-4::lin-17)\""
Remark	"Published_as lin-17"
Remark	"To determine whether lin-17 functions cell autonomously in PLM, we expressed a wild-type lin-17 cDNA selectively in mechanosensory neurons of lin-17 mutants by using mec-4 or mec-7 promoters, which direct expression in PLM, ALM, AVM, and PVM mechanosensory neurons. mec-4::lin-17 and mec-7::lin-17 transgenes were both able to rescue the PLM defects of lin-17 mutants with high efficiency."
Reference	"WBPaper00027140"


Anatomy_function : "WBbtf0774"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000529"
Involved	"WBbt:0007026"	Necessary
Involved	"WBbt:0004506"	Necessary
Remark	"ENTITY:WBbt:0006865(DTC)|GO:0030154(cell differentiation)"
Remark	"QUALITY:PATO:0000462(absent)"
Remark	"Wild-type animals with laser-ablated Z1.aa and Z4.pp failed to produce DTC (lag-2::GFP expressing cell)."
Reference	"WBPaper00029347"


Anatomy_function : "WBbtf0775"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000704"	Autonomous
Gene	"WBGene00010497"
Involved	"WBbt:0005812"	Sufficient
Remark	"ENTITY:WBbt:0005812(excretory cell)|WBbt:0005775(excretory canal)|GO:0044463(cell projection part)|GO:0048858(cell projection morphogenesis)"
Remark	"QUALITY:PATO:0000628(ectopic) NOT"
Remark	"Genotype \"axl-1(tm1095);huEx102[vha-1&amp;#8759;axl-1;myo-2&amp;#8759;gfp]\""
Remark	"Published_as axl-1"
Remark	"The formation of excretory canal ectopic branch phenotype was rescued by excretory cell-specific expression of axl-1 (using the promoter of the vha-1 gene), demonstrating that AXL-1 functions cell autonomously in excretory cell development."
Reference	"WBPaper00030820"


Anatomy_function : "WBbtf0776"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001798"
Gene	"WBGene00003006"
Involved	"WBbt:0004857"	Sufficient
Remark	"ENTITY:WBbt:0004857(DA9)|GO:0030425(dendrite)|GO:0007416(synapse assembly)"
Remark	"QUALITY:PATO:0000628(ectopic) NOT"
Remark	"Genotype \"lin-17(n671);wyEx656[Pmig-13::lin-17]\""
Remark	"Published_as lin-17"
Remark	"We first determined in which cell(s) lin-17 cDNA expression is sufficient to rescue the DA9 presynaptic phenotype using a variety of cell-specific promoters. Expression in muscle and the majority of DA/DB neurons (excepting DA8/9) using the unc-129 promoter was not sufficient to rescue the lin-17 null phenotype. The mig-13 promoter, which we use to label DA9, rescued the positioning of DA9 presynapses."
Reference	"WBPaper00030926"


Anatomy_function : "WBbtf0777"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001272"
Gene	"WBGene00000289"
Not_involved	"WBbt:0007809"	Insufficient
Remark	"ENTITY:WBbt:0007809(VPC)|GO:0045165(cell fate commitment)"
Remark	"QUALITY:PATO:0002051(increased occurrence)"
Remark	"Genotype \"lin-17(n671);cam-1(gm122);syIs198[Plst-1::CAM-1::GFP]\""
Remark	"Published_as cam-1"
Remark	"To test whether cam-1 acts in the VPCs, we tried to rescue the lin-17(lf); cam-1(lf) OI phenotype with an integrated VPC-specific CAM-1::GFP transgene driven by the lst-1 promoter. Although Plst-1::CAM-1::GFP was expressed in the relevant VPCs, it failed to rescue the OI phenotype suggesting that CAM-1 is required in other tissues to negatively regulate vulval induction."
Reference	"WBPaper00031110"


Anatomy_function : "WBbtf0778"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000239"
Gene	"WBGene00003246"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBbt:0008117(P4.p hermaphrodite)|GO:0045165(cell fate commitment)"
Remark	"QUALITY:PATO:0000460(abnormal) NOT"
Remark	"Genotype \"mig-14(ga62);arIs99[dpy-7::2Xnls::yfp]; Ex[PF25B3.3::mig-14; myo-3::mCherry\""
Remark	"Published_as mig-14"
Remark	"We analyzed transgenes expressing MIG-14(+) in specific tissues for their ability to rescue the inappropriate fusion of P4.p to hyp7 in a mig-14(ga62);arIs99 background. We used well characterized tissue-specific promoters that are expressed continuously in muscles, neurons, hypodermis, or intestine from the L1 stage through the time of vulval induction to drive MIG-14() expression. At least one wnt is expressed in each of these tissues. Our results demonstrate that expression of MIG-14 in muscles, neurons, or hypodermis can partially rescue the P4.p defect, suggesting that Wnt signaling from all of these sources contributes to VPC competence."
Reference	"WBPaper00031325"


Anatomy_function : "WBbtf0779"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000239"
Gene	"WBGene00003246"
Involved	"WBbt:0003675"	Sufficient
Remark	"ENTITY:WBbt:0008117(P4.p hermaphrodite)|GO:0045165(cell fate commitment)"
Remark	"QUALITY:PATO:0000460(abnormal) NOT"
Remark	"Genotype \"mig-14(ga62);arIs99[dpy-7::2Xnls::yfp]; Ex[Pmyo-3::mig-14; myo-3::mCherry\""
Remark	"Published_as mig-14"
Remark	"We analyzed transgenes expressing MIG-14(+) in specific tissues for their ability to rescue the inappropriate fusion of P4.p to hyp7 in a mig-14(ga62);arIs99 background. We used well characterized tissue-specific promoters that are expressed continuously in muscles, neurons, hypodermis, or intestine from the L1 stage through the time of vulval induction to drive MIG-14() expression. At least one wnt is expressed in each of these tissues. Our results demonstrate that expression of MIG-14 in muscles, neurons, or hypodermis can partially rescue the P4.p defect, suggesting that Wnt signaling from all of these sources contributes to VPC competence."
Reference	"WBPaper00031325"


Anatomy_function : "WBbtf0780"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000239"
Gene	"WBGene00003246"
Involved	"WBbt:0007846"	Sufficient
Remark	"ENTITY:WBbt:0008117(P4.p hermaphrodite)|GO:0045165(cell fate commitment)"
Remark	"QUALITY:PATO:0000460(abnormal) NOT"
Remark	"Genotype \"mig-14(ga62);arIs99[dpy-7::2Xnls::yfp]; Ex[Pdpy-7::mig-14; myo-3::mCherry\""
Remark	"Published_as mig-14"
Remark	"We analyzed transgenes expressing MIG-14(+) in specific tissues for their ability to rescue the inappropriate fusion of P4.p to hyp7 in a mig-14(ga62);arIs99 background. We used well characterized tissue-specific promoters that are expressed continuously in muscles, neurons, hypodermis, or intestine from the L1 stage through the time of vulval induction to drive MIG-14() expression. At least one wnt is expressed in each of these tissues. Our results demonstrate that expression of MIG-14 in muscles, neurons, or hypodermis can partially rescue the P4.p defect, suggesting that Wnt signaling from all of these sources contributes to VPC competence."
Reference	"WBPaper00031325"


Anatomy_function : "WBbtf0781"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000239"
Gene	"WBGene00003246"
Not_involved	"WBbt:0005792"	Insufficient
Remark	"ENTITY:WBbt:0008117(P4.p hermaphrodite)|GO:0045165(cell fate commitment)"
Remark	"QUALITY:PATO:0000460(abnormal)"
Remark	"Genotype \"mig-14(ga62);arIs99[dpy-7::2Xnls::yfp]; Ex[Pvha-6::mig-14; myo-3::mCherry\""
Remark	"Published_as mig-14"
Remark	"We analyzed transgenes expressing MIG-14(+) in specific tissues for their ability to rescue the inappropriate fusion of P4.p to hyp7 in a mig-14(ga62);arIs99 background. We used well characterized tissue-specific promoters that are expressed continuously in muscles, neurons, hypodermis, or intestine from the L1 stage through the time of vulval induction to drive MIG-14() expression. At least one wnt is expressed in each of these tissues. Our results demonstrate that expression of MIG-14 in muscles, neurons, or hypodermis can partially rescue the P4.p defect, suggesting that Wnt signaling from all of these sources contributes to VPC competence."
Reference	"WBPaper00031325"


Anatomy_function : "WBbtf0782"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000239"
Involved	"WBbt:0007815"	Necessary
Remark	"ENTITY:WBbt:0008117(P4.p hermaphrodite)|WBbt:0008121(P5.p hermaphrodite)|WBbt:0008125(P6.p hermaphrodite)|GO:0045165(cell fate commitment)"
Remark	"QUALITY:PATO:0000460(abnormal)"
Remark	"Genotype \"cwn-1(ok546); egl-20(n585);arIs99[dpy-7::2Xnls::yfp]\""
Remark	"We ablated the gonad in L1 cwn-1; egl-20; arIs99 hermaphrodites and found that P5.p, P6.p, and P7.p adopted the F (fused with hyp7) fate more frequently."
Reference	"WBPaper00031325"


Anatomy_function : "WBbtf0783"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001140"	Autonomous
Gene	"WBGene00003247"
Involved	"WBbt:0004096"	Sufficient
Involved	"WBbt:0004096"	Necessary
Remark	"ENTITY:WBbt:0004096(PQR)|GO:0001764(neuron migration)"
Remark	"QUALITY:PATO:0001511(defective)"
Remark	"Genotype \"mig-15(rh80);Ex[mig-15(+)\""
Remark	"Mosaic analysis was used to determine if mig-15 acts cell-autonomously. Forty seven mosaics had losses in the PQR lineage and displayed PQR direction and migration defects similar to mig-15(rh80) alone. Twenty-&amp;#64257;ve PQR(&amp;#8722;) mosaics had detectable losses only in PQR displayed PQR migration defects."
Remark	"Mosaic analysis was used to determine if mig-15 acts cell-autonomously. Of 64 mosaics that retained mig-15(+) in PQR, 62 displayed normal PQR migration."
Remark	"Published_as mig-15"
Reference	"WBPaper00032247"


Anatomy_function : "WBbtf0784"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001140"	Autonomous
Gene	"WBGene00003247"
Involved	"WBbt:0003927"	Sufficient
Involved	"WBbt:0003927"	Necessary
Remark	"ENTITY:WBbt:0003927(AQR)|GO:0001764(neuron migration)"
Remark	"QUALITY:PATO:0001511(defective)"
Remark	"Genotype \"mig-15(rh80);Ex[mig-15(+)\""
Remark	"Mosaic analysis was used to determine if mig-15 acts cell-autonomously. Of 61 mosaics that retained mig-15(+) in AQR, 60 showed normal AQR migration. 12 mosaics with losses in URXR, an AB.a derivative, but not AQR had normal AQR migration."
Remark	"Mosaic analysis was used to determine if mig-15 acts cell-autonomously. Thirty three mosaics were identi&amp;#64257;ed that had lost mig-15(+) in AQR and displayed AQR migration defects similar to mig-15(rh80) alone. 22 mosaics with losses in AQR but not in URXR had defective migration of the Q cell descendant neurons."
Remark	"Published_as mig-15"
Reference	"WBPaper00032247"


Anatomy_function : "WBbtf0785"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000239"
Involved	"WBbt:0004522"	Necessary
Remark	"ENTITY:WBbt:0007809(VPC)|GO:0001709(cell fate determination)"
Remark	"QUALITY:PATO:0001511(defective)"
Remark	"Strain name N2"
Remark	"We ablated the anchor cell (the EGF-sending cell) at successive time points during vulval induction. In all three isolates (N2, CB4856, and AB1), the number of induced cells was very low for early ablations (lethargic L2 stage), increased for intermediate time-point ablations and reached full induction level for late ablations (when the tertiary cells have divided)."
Reference	"WBPaper00032332"


Anatomy_function : "WBbtf0786"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000239"
Involved	"WBbt:0004522"	Necessary
Remark	"ENTITY:WBbt:0007809(VPC)|GO:0001709(cell fate determination)"
Remark	"QUALITY:PATO:0001511(defective)"
Remark	"Strain name CB4856"
Remark	"We ablated the anchor cell (the EGF-sending cell) at successive time points during vulval induction. In all three isolates (N2, CB4856, and AB1), the number of induced cells was very low for early ablations (lethargic L2 stage), increased for intermediate time-point ablations and reached full induction level for late ablations (when the tertiary cells have divided)."
Reference	"WBPaper00032332"


Anatomy_function : "WBbtf0787"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000239"
Involved	"WBbt:0004522"	Necessary
Remark	"ENTITY:WBbt:0007809(VPC)|GO:0001709(cell fate determination)"
Remark	"QUALITY:PATO:0001511(defective)"
Remark	"Strain name AB1"
Remark	"We ablated the anchor cell (the EGF-sending cell) at successive time points during vulval induction. In all three isolates (N2, CB4856, and AB1), the number of induced cells was very low for early ablations (lethargic L2 stage), increased for intermediate time-point ablations and reached full induction level for late ablations (when the tertiary cells have divided)."
Reference	"WBPaper00032332"


Anatomy_function : "WBbtf0788"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000384"	Autonomous
Gene	"WBGene00003006"
Involved	"WBbt:0005270"	Sufficient
Involved	"WBbt:0005303"
Remark	"Because Wnt signaling is known to affect a variety of cells in the C. elegans tail,"
Remark	"ENTITY:WBbt:0005270(DD neuron)|WBbt:0005303(VD neuron)|GO:0007411(axon guidance)"
Remark	"QUALITY:PATO:0001511(defective) NOT"
Remark	"Genotype \"lin-17(n671); Ex[Punc-47::lin-17]\""
Remark	"Published_as lin-17"
Reference	"WBPaper00032955"


Anatomy_function : "WBbtf0789"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000384"	Autonomous
Gene	"WBGene00000238"
Involved	"WBbt:0005270"	Sufficient
Involved	"WBbt:0005303"	Sufficient
Remark	"ENTITY:WBbt:0005270(DD neuron)|WBbt:0005303(VD neuron)|GO:0007411(axon guidance)"
Remark	"QUALITY:PATO:0001511(defective) NOT"
Remark	"Genotype \"bar-1(ga80); Ex[Punc-47::bar-1::GFP]\""
Remark	"Published_as bar-1"
Remark	"We first examined if bar-1 function was required cell-autonomously for D-type axon guidance. A functional BAR-1::GFP fusion protein was expressed specifically in all GABAergic neurons, including the D-type motor neurons, using the unc-47 promoter. This construct significantly rescued the D-type axon guidance defect."
Reference	"WBPaper00032955"


Anatomy_function : "WBbtf0790"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000195"	Nonautonomous
Gene	"WBGene00004749"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBbt:0006863(hermaphrodite distal tip cell)|GO:0016477(cell migration)"
Remark	"QUALITY:PATO:0001511(defective) NOT"
Remark	"Genotype \"unc-5(e152); sdn-1(zh20); Ex[Punc-119::sdn-1]\""
Remark	"Published_as sdn-1"
Remark	"We tested both unc-119::sdn-1 and dpy-7::sdn-1, as well as sdn1::sdn-1 for their ability to rescue the enhancement of unc-5 DTC defects by sdn-1(zh20). As expected, sdn-1::sdn-1 rescued the enhancement of unc-5(e152) DTC migration defects in an sdn-1 (zh20) background (Table 2). unc-119::sdn-1 and dpy-7::sdn-1 each partially reduced the frequency of migration defects. As an additional control, we constructed a lag-2::sdn-1 transgene (pMS1) to drive expression of an sdn-1 cDNA in the DTCs and test for rescue of the enhancement. No rescue was observed when this construct was crossed into the unc-5(e152); sdn-1(zh20) background."
Reference	"WBPaper00034762"


Anatomy_function : "WBbtf0791"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000195"	Nonautonomous
Gene	"WBGene00004749"
Involved	"WBbt:0007846"	Sufficient
Remark	"ENTITY:WBbt:0006863(hermaphrodite distal tip cell)|GO:0016477(cell migration)"
Remark	"QUALITY:PATO:0001511(defective) NOT"
Remark	"Genotype \"unc-5(e152); sdn-1(zh20); Ex[Pdpy-7::sdn-1]\""
Remark	"Published_as sdn-1"
Remark	"We tested both unc-119::sdn-1 and dpy-7::sdn-1, as well as sdn1::sdn-1 for their ability to rescue the enhancement of unc-5 DTC defects by sdn-1(zh20). As expected, sdn-1::sdn-1 rescued the enhancement of unc-5(e152) DTC migration defects in an sdn-1 (zh20) background (Table 2). unc-119::sdn-1 and dpy-7::sdn-1 each partially reduced the frequency of migration defects. As an additional control, we constructed a lag-2::sdn-1 transgene (pMS1) to drive expression of an sdn-1 cDNA in the DTCs and test for rescue of the enhancement. No rescue was observed when this construct was crossed into the unc-5(e152); sdn-1(zh20) background."
Reference	"WBPaper00034762"


Anatomy_function : "WBbtf0792"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000195"	Nonautonomous
Gene	"WBGene00004749"
Not_involved	"WBbt:0006863"	Insufficient
Remark	"ENTITY:WBbt:0006863(hermaphrodite distal tip cell)|GO:0016477(cell migration)"
Remark	"QUALITY:PATO:0001511(defective)"
Remark	"Genotype \"unc-5(e152); sdn-1(zh20); Ex[Plag-2::sdn-1]\""
Remark	"Published_as sdn-1"
Remark	"We tested both unc-119::sdn-1 and dpy-7::sdn-1, as well as sdn1::sdn-1 for their ability to rescue the enhancement of unc-5 DTC defects by sdn-1(zh20). As expected, sdn-1::sdn-1 rescued the enhancement of unc-5(e152) DTC migration defects in an sdn-1 (zh20) background (Table 2). unc-119::sdn-1 and dpy-7::sdn-1 each partially reduced the frequency of migration defects. As an additional control, we constructed a lag-2::sdn-1 transgene (pMS1) to drive expression of an sdn-1 cDNA in the DTCs and test for rescue of the enhancement. No rescue was observed when this construct was crossed into the unc-5(e152); sdn-1(zh20) background."
Reference	"WBPaper00034762"


Anatomy_function : "WBbtf0793"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000852"
Involved	"WBbt:0004458"	Necessary
Remark	"ENTITY:WBbt:0005751(coelomocyte)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0000462(absent)"
Remark	"Table 3 shows that in wild-type, laser ablating MS removes coelomocytes (cup-4::GFP positive cells) from partially-developed embryos."
Reference	"WBPaper00035290"


Anatomy_function : "WBbtf0794"
Assay	"Blastomere_isolation"
Phenotype	"WBPhenotype:0000852"
Involved	"WBbt:0004458"	Sufficient
Remark	"ENTITY:WBbt:0005751(coelomocyte)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0000462(absent) NOT"
Remark	"Table 3 shows that wild-type embryos with isolated E blastomere are able to produce coelomocytes (cup-4::GFP positive cells)."
Reference	"WBPaper00035290"


Anatomy_function : "WBbtf0795"
Assay	"Blastomere_isolation"
Phenotype	"WBPhenotype:0000852"
Not_involved	"WBbt:0004804"	Insufficient
Remark	"ENTITY:WBbt:0005751(coelomocyte)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0000462(absent)"
Remark	"Table 3 shows that wild-type embryos with isolated E blastomere are not able to produce coelomocytes (cup-4::GFP positive cells)."
Reference	"WBPaper00035290"


Anatomy_function : "WBbtf0796"
Assay	"Blastomere_isolation"
Phenotype	"WBPhenotype:0000815"
Not_involved	"WBbt:0004804"	Insufficient
Remark	"ENTITY:WBbt:0007810(body muscle cell)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0000462(absent)"
Remark	"Table 3 shows that wild-type embryos with isolated E blastomere are not able to produce body muscle cells (unc-120::GFP positive cells)."
Reference	"WBPaper00035290"


Anatomy_function : "WBbtf0797"
Assay	"Blastomere_isolation"
Phenotype	"WBPhenotype:0000701"
Not_involved	"WBbt:0004804"	Insufficient
Remark	"ENTITY:WBbt:0007846(hypodermal cell)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0000462(absent)"
Remark	"Table 3 shows that wild-type embryos with isolated E blastomere are not able to produce epidermis (nhr-25::YFP positive cells)."
Reference	"WBPaper00035290"


Anatomy_function : "WBbtf0798"
Assay	"Blastomere_isolation"
Phenotype	"WBPhenotype:0000701"
Involved	"WBbt:0003810"	Sufficient
Remark	"ENTITY:WBbt:0007846(hypodermal cell)|GO:0001708(cell fate specification)"
Remark	"QUALITY:PATO:0000462(absent) NOT"
Remark	"Table 3 shows that wild-type embryos with isolated C blastomere are able to produce epidermis (nhr-25::YFP positive cells)."
Reference	"WBPaper00035290"


Anatomy_function : "WBbtf0799"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000883"
Gene	"WBGene00000858"
Involved	"WBbt:0006804"	Sufficient
Remark	"ENTITY:WBbt:0006749(nerve ring)|GO:0010159(specification of organ position)"
Remark	"QUALITY:PATO:0001921(mislocalised anteriorly) NOT"
Remark	"Genotype \"cwn-2(ky756); Ex[myo-3::cwn-2]\""
Remark	"Published_as cwn-2"
Remark	"To determine which tissues could provide cwn-2 function for nerve ring development, a cwn-2 cDNA was expressed in cwn-2 mutants under the control of well-characterized promoters covering parts of its normal expression pattern. cwn-2 expression in body wall muscles (myo-3 promoter), pharynx (myo-2 promoter) or intestine (elt-2 promoter) rescued the nerve ring defects of cwn-2 mutants, suggesting that the complete cwn-2 expression pattern is not essential for nerve ring development."
Reference	"WBPaper00035405"


Anatomy_function : "WBbtf0800"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000883"
Gene	"WBGene00000858"
Involved	"WBbt:0005451"	Sufficient
Remark	"ENTITY:WBbt:0006749(nerve ring)|GO:0010159(specification of organ position)"
Remark	"QUALITY:PATO:0001921(mislocalised anteriorly) NOT"
Remark	"Genotype \"cwn-2(ky756); Ex[myo-2::cwn-2]\""
Remark	"Published_as cwn-2"
Remark	"To determine which tissues could provide cwn-2 function for nerve ring development, a cwn-2 cDNA was expressed in cwn-2 mutants under the control of well-characterized promoters covering parts of its normal expression pattern. cwn-2 expression in body wall muscles (myo-3 promoter), pharynx (myo-2 promoter) or intestine (elt-2 promoter) rescued the nerve ring defects of cwn-2 mutants, suggesting that the complete cwn-2 expression pattern is not essential for nerve ring development."
Reference	"WBPaper00035405"


Anatomy_function : "WBbtf0801"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000883"
Gene	"WBGene00000858"
Involved	"WBbt:0005792"	Sufficient
Remark	"ENTITY:WBbt:0006749(nerve ring)|GO:0010159(specification of organ position)"
Remark	"QUALITY:PATO:0001921(mislocalised anteriorly) NOT"
Remark	"Genotype \"cwn-2(ky756); Ex[elt-2::cwn-2]\""
Remark	"Published_as cwn-2"
Remark	"To determine which tissues could provide cwn-2 function for nerve ring development, a cwn-2 cDNA was expressed in cwn-2 mutants under the control of well-characterized promoters covering parts of its normal expression pattern. cwn-2 expression in body wall muscles (myo-3 promoter), pharynx (myo-2 promoter) or intestine (elt-2 promoter) rescued the nerve ring defects of cwn-2 mutants, suggesting that the complete cwn-2 expression pattern is not essential for nerve ring development."
Reference	"WBPaper00035405"


Anatomy_function : "WBbtf0802"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000883"
Gene	"WBGene00000289"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBbt:0006749(nerve ring)|GO:0010159(specification of organ position)"
Remark	"QUALITY:PATO:0001921(mislocalised anteriorly) NOT"
Remark	"Genotype \"cam-1(gm122); Ex[unc-119::cam-1A]\""
Remark	"Published_as cam-1"
Remark	"cam-1A and cam-1B upstream regions drive overlapping expression in neurons and head muscles, and pan-neuronal expression of cam-1A from the unc-119 promoter rescued nerve ring placement, suggesting a neuronal site of action."
Reference	"WBPaper00035405"


Anatomy_function : "WBbtf0803"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000883"
Gene	"WBGene00000289"
Not_involved	"WBbt:0006825"	Insufficient
Not_involved	"WBbt:0005672"	Insufficient
Not_involved	"WBbt:0005671"	Insufficient
Not_involved	"WBbt:0005668"	Insufficient
Not_involved	"WBbt:0005666"	Insufficient
Not_involved	"WBbt:0005665"	Insufficient
Not_involved	"WBbt:0006834"	Insufficient
Not_involved	"WBbt:0005836"	Insufficient
Not_involved	"WBbt:0005413"	Insufficient
Not_involved	"WBbt:0006814"	Insufficient
Not_involved	"WBbt:0005662"	Insufficient
Not_involved	"WBbt:0005661"	Insufficient
Not_involved	"WBbt:0005660"	Insufficient
Not_involved	"WBbt:0006811"	Insufficient
Not_involved	"WBbt:0006976"	Insufficient
Not_involved	"WBbt:0005840"	Insufficient
Remark	"ENTITY:WBbt:0006749(nerve ring)|GO:0010159(specification of organ position)"
Remark	"QUALITY:PATO:0001921(mislocalised anteriorly)"
Remark	"Genotype \"cam-1(gm122); Ex[nsy-5::cam-1A]\""
Remark	"Published_as cam-1"
Remark	"cam-1A and cam-1B upstream regions drive overlapping expression in neurons and head muscles, and pan-neuronal expression of cam-1A from the unc-119 promoter rescued nerve ring placement, suggesting a neuronal site of action. Subsets of head neurons were tested using promoter fragments expressed around the comma stage of embryogenesis. Transgenes that were expressed in multiple sensory neurons and interneurons failed to rescue cam-1 efficiently (nsy-5::cam-1A, ncs-1::cam-1A, opt-3::cam-1A), although these cells overlap with those that normally express cam-1."
Reference	"WBPaper00035405"


Anatomy_function : "WBbtf0804"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000883"
Gene	"WBGene00000289"
Not_involved	"WBbt:0006825"	Insufficient
Not_involved	"WBbt:0005672"	Insufficient
Not_involved	"WBbt:0005671"	Insufficient
Not_involved	"WBbt:0003744"	Insufficient
Not_involved	"WBbt:0005670"	Insufficient
Not_involved	"WBbt:0006823"	Insufficient
Not_involved	"WBbt:0005664"	Insufficient
Not_involved	"WBbt:0005663"	Insufficient
Not_involved	"WBbt:0005413"	Insufficient
Not_involved	"WBbt:0007808"	Insufficient
Not_involved	"WBbt:0005662"	Insufficient
Not_involved	"WBbt:0007807"	Insufficient
Not_involved	"WBbt:0005660"	Insufficient
Not_involved	"WBbt:0006842"	Insufficient
Remark	"ENTITY:WBbt:0006749(nerve ring)|GO:0010159(specification of organ position)"
Remark	"QUALITY:PATO:0001921(mislocalised anteriorly)"
Remark	"Genotype \"cam-1(gm122); Ex[ncs-1::cam-1A]\""
Remark	"Published_as cam-1"
Remark	"cam-1A and cam-1B upstream regions drive overlapping expression in neurons and head muscles, and pan-neuronal expression of cam-1A from the unc-119 promoter rescued nerve ring placement, suggesting a neuronal site of action. Subsets of head neurons were tested using promoter fragments expressed around the comma stage of embryogenesis. Transgenes that were expressed in multiple sensory neurons and interneurons failed to rescue cam-1 efficiently (nsy-5::cam-1A, ncs-1::cam-1A, opt-3::cam-1A), although these cells overlap with those that normally express cam-1."
Reference	"WBPaper00035405"


Anatomy_function : "WBbtf0805"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000883"
Gene	"WBGene00000289"
Not_involved	"WBbt:0003681"	Insufficient
Not_involved	"WBbt:0005842"	Insufficient
Not_involved	"WBbt:0005237"	Insufficient
Remark	"ENTITY:WBbt:0006749(nerve ring)|GO:0010159(specification of organ position)"
Remark	"QUALITY:PATO:0001921(mislocalised anteriorly)"
Remark	"Genotype \"cam-1(gm122); Ex[opt-3::cam-1A]\""
Remark	"Published_as cam-1"
Remark	"cam-1A and cam-1B upstream regions drive overlapping expression in neurons and head muscles, and pan-neuronal expression of cam-1A from the unc-119 promoter rescued nerve ring placement, suggesting a neuronal site of action. Subsets of head neurons were tested using promoter fragments expressed around the comma stage of embryogenesis. Transgenes that were expressed in multiple sensory neurons and interneurons failed to rescue cam-1 efficiently (nsy-5::cam-1A, ncs-1::cam-1A, opt-3::cam-1A), although these cells overlap with those that normally express cam-1."
Reference	"WBPaper00035405"


Anatomy_function : "WBbtf0806"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000883"
Gene	"WBGene00000289"
Involved	"WBbt:0005361"	Sufficient
Involved	"WBbt:0005359"	Sufficient
Involved	"WBbt:0005353"	Sufficient
Remark	"ENTITY:WBbt:0006749(nerve ring)|GO:0010159(specification of organ position)"
Remark	"QUALITY:PATO:0001921(mislocalised anteriorly) NOT"
Remark	"Genotype \"cam-1(gm122); Ex[ceh-24::cam-1A]\""
Remark	"However, cam-1A expression in SIA, SIB and SMD motoneurons from the ceh-24 promoter resulted in near-complete rescue of the cam-1 nerve ring defect. A mig-1::cam-1A transgene also rescued cam-1 mutants; this transgene overlaps with ceh-24 in SIA and SIB, but not SMD, neurons. A cwn-2::cam-1A transgene failed to rescue cam-1 mutants; this transgene overlaps with ceh-24 in SMD neurons and is also expressed in muscles. These experiments suggest that a specific spatial expression pattern that includes SIA and SIB neurons is required for cam-1 rescue."
Remark	"Published_as cam-1"
Reference	"WBPaper00035405"


Anatomy_function : "WBbtf0807"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000883"
Gene	"WBGene00000289"
Involved	"WBbt:0005361"	Sufficient
Involved	"WBbt:0005359"	Sufficient
Remark	"ENTITY:WBbt:0006749(nerve ring)|GO:0010159(specification of organ position)"
Remark	"QUALITY:PATO:0001921(mislocalised anteriorly) NOT"
Remark	"Genotype \"cam-1(gm122); Ex[mig-1::cam-1A]\""
Remark	"However, cam-1A expression in SIA, SIB and SMD motoneurons from the ceh-24 promoter resulted in near-complete rescue of the cam-1 nerve ring defect. A mig-1::cam-1A transgene also rescued cam-1 mutants; this transgene overlaps with ceh-24 in SIA and SIB, but not SMD, neurons (S. Clark and C.I.B., unpublished observations). A cwn-2::cam-1A transgene failed to rescue cam-1 mutants; this transgene overlaps with ceh-24 in SMD neurons and is also expressed in muscles. These experiments suggest that a specific spatial expression pattern that includes SIA and SIB neurons is required for cam-1 rescue."
Remark	"However, cam-1A expression in SIA, SIB and SMD motoneurons from the ceh-24 promoter resulted in near-complete rescue of the cam-1 nerve ring defect. A mig-1::cam-1A transgene also rescued cam-1 mutants; this transgene overlaps with ceh-24 in SIA and SIB, but not SMD, neurons. A cwn-2::cam-1A transgene failed to rescue cam-1 mutants; this transgene overlaps with ceh-24 in SMD neurons and is also expressed in muscles. These experiments suggest that a specific spatial expression pattern that includes SIA and SIB neurons is required for cam-1 rescue."
Remark	"Published_as cam-1"
Reference	"WBPaper00035405"


Anatomy_function : "WBbtf0808"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000883"
Gene	"WBGene00000289"
Not_involved	"WBbt:0005353"	Insufficient
Remark	"ENTITY:WBbt:0006749(nerve ring)|GO:0010159(specification of organ position)"
Remark	"QUALITY:PATO:0001921(mislocalised anteriorly)"
Remark	"Genotype \"cam-1(gm122); Ex[cwn-2::cam-1A]\""
Remark	"However, cam-1A expression in SIA, SIB and SMD motoneurons from the ceh-24 promoter resulted in near-complete rescue of the cam-1 nerve ring defect. A mig-1::cam-1A transgene also rescued cam-1 mutants; this transgene overlaps with ceh-24 in SIA and SIB, but not SMD, neurons. A cwn-2::cam-1A transgene failed to rescue cam-1 mutants; this transgene overlaps with ceh-24 in SMD neurons and is also expressed in muscles. These experiments suggest that a specific spatial expression pattern that includes SIA and SIB neurons is required for cam-1 rescue."
Remark	"Published_as cam-1"
Reference	"WBPaper00035405"


Anatomy_function : "WBbtf0809"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000883"
Gene	"WBGene00003238"
Involved	"WBbt:0005353"	Sufficient
Involved	"WBbt:0005361"	Sufficient
Involved	"WBbt:0005359"	Sufficient
Remark	"ENTITY:WBbt:0006749(nerve ring)|GO:0010159(specification of organ position)"
Remark	"QUALITY:PATO:0001921(mislocalised anteriorly) NOT"
Remark	"Expression of mig-1 cDNA under the ceh-24 promoter partially rescued the nerve ring defect in mig-1 cam-1(ks52) animals, and, similarly, a ceh-24::sax-3 transgene partially rescued the sax-3 nerve ring defect. These results suggest that mig-1 (Frizzled) and sax-3 (Robo) can act in the SIA, SIB or SMD neurons."
Remark	"Genotype \"mig-1(e1787) cam-1(ks52); Ex[ceh-24::mig-1]\""
Remark	"Published_as mig-1"
Reference	"WBPaper00035405"


Anatomy_function : "WBbtf0810"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000883"
Gene	"WBGene00003238"
Involved	"WBbt:0005353"	Sufficient
Involved	"WBbt:0005361"	Sufficient
Involved	"WBbt:0005359"	Sufficient
Remark	"ENTITY:WBbt:0006749(nerve ring)|GO:0010159(specification of organ position)"
Remark	"QUALITY:PATO:0001921(mislocalised anteriorly) NOT"
Remark	"Expression of mig-1 cDNA under the ceh-24 promoter partially rescued the nerve ring defect in mig-1 cam-1(ks52) animals, and, similarly, a ceh-24::sax-3 transgene partially rescued the sax-3 nerve ring defect. These results suggest that mig-1 (Frizzled) and sax-3 (Robo) can act in the SIA, SIB or SMD neurons."
Remark	"Genotype \"sax-3(ky123); Ex[ceh-24::sax-3]\""
Remark	"Published_as mig-1"
Reference	"WBPaper00035405"


Anatomy_function : "WBbtf0811"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000883"
Gene	"WBGene00000478"
Not_involved	"WBbt:0005353"	Insufficient
Not_involved	"WBbt:0005361"	Insufficient
Not_involved	"WBbt:0005359"	Insufficient
Remark	"A ceh-24::cfz-2 transgene did not rescue a cfz-2 mutant nerve ring anterior displacement phenotype."
Remark	"ENTITY:WBbt:0006749(nerve ring)|GO:0010159(specification of organ position)"
Remark	"QUALITY:PATO:0001921(mislocalised anteriorly)"
Remark	"Genotype \"cfz-2(ok1201); Ex[ceh-24::cfz-2]\""
Remark	"Published_as cfz-2"
Reference	"WBPaper00035405"


Anatomy_function : "WBbtf0812"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000883"
Involved	"WBbt:0005353"	Sufficient
Involved	"WBbt:0005361"	Sufficient
Involved	"WBbt:0005359"	Sufficient
Remark	"ENTITY:WBbt:0006749(nerve ring)|GO:0010159(specification of organ position)"
Remark	"QUALITY:PATO:0001921(mislocalised anteriorly)"
Remark	"Genotype \"Ex[ceh-24::egl-1]\""
Remark	"To further characterize the role of the SIA and SIB neurons in nerve ring development, we killed them by expressing the egl-1 BH3 cell death gene in SIA, SIB and SMD neurons under the ceh-24 promoter. The resulting transgene killed SIA, SIB and SMD neurons inefficiently, sparing a subset of neurons in most animals. Despite this inefficiency, 20% of animals with the transgene had a nerve ring placement defect resembling that of cwn-2 mutants. These results demonstrate that ceh-24-expressing neurons affect placement of the developing nerve ring."
Reference	"WBPaper00035405"


Anatomy_function : "WBbtf0813"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000232"	Autonomous
Gene	"WBGene00006770"
Involved	"WBbt:0006827"	Sufficient
Remark	"ENTITY:WBbt:0006827(CAN)|GO:0001764(neuron migration)"
Remark	"QUALITY:PATO:0001507(disrupted)"
Remark	"Genotype \"unc-34(e951); gmEx249[Pceh-23::unc-34::gfp rol-6(su1006)]\""
Remark	"Published_as unc-34"
Remark	"To test for a cell autonomous role of UNC-34 in CAN cell migration, we expressed an unc-34 cDNA tagged with GFP from a ceh-23 promoter, which drove expression in the CAN and in a small subset of sensory neurons. In the null mutant unc-34(e951), only 24% of the CAN cells migrate to the wild-type location. Expression of UNC-34::GFP within the CAN increases the number of cells that reach the wild-type location to 75%. Thus, UNC-34 expression within the CAN is capable of rescuing a significant portion of the unc-34(e951) CAN cell migration defects. These results indicate that UNC-34 acts in the CAN cell to promote its migration."
Reference	"WBPaper00036239"


Anatomy_function : "WBbtf0814"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001801"	Autonomous
Gene	"WBGene00006770"
Involved	"WBbt:0005406"	Sufficient
Remark	"ENTITY:WBbt:0005406(ALM)|GO:0033564(anterior/posterior axon guidance)"
Remark	"QUALITY:PATO:0001507(disrupted)"
Remark	"Genotype \"cwn-1(ok546); unc-34(gm104); kyEx710[Punc-86::GFP::unc-34 Podr-1::dsRed]\""
Remark	"Published_as unc-34"
Remark	"We were also able to rescue partially the synthetic ALM defect of cwn-1; unc-34(gm104) mutants by expressing unc-34 in the ALM from the unc-86 promoter, which is expressed in many neurons including the ALM, but not in non-neuronal cells. This finding suggests that UNC-34 functions in the ALM to establish its polarity."
Reference	"WBPaper00036239"


Anatomy_function : "WBbtf0815"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001801"	Autonomous
Gene	"WBGene00003243"
Involved	"WBbt:0005406"	Sufficient
Remark	"ENTITY:WBbt:0005406(ALM)|GO:0033564(anterior/posterior axon guidance)"
Remark	"QUALITY:PATO:0001507(disrupted)"
Remark	"Genotype \"cwn-1(ok546); mig-10(ct41); kyEx926[Punc-86::mig-10::YFP Podr-1::dsRed]\""
Remark	"Published_as mig-10"
Remark	"We found that like mutations in unc-34 and ced-10, a mig-10 mutation did not cause an ALM polarity defect but did generate a synthetic phenotype with cwn-1. The ability of a Punc-86::mig-10::gfp transgene to partially rescue the synthetic phenotype suggests that mig-10 also acts in the ALM to regulate its polarity."
Reference	"WBPaper00036239"


Anatomy_function : "WBbtf0816"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001637"
Involved	"WBbt:0004804"	Sufficient
Remark	"ENTITY:WBbt:0005792(intestinal cell)|GO:0030154(cell differentiation)"
Remark	"QUALITY:PATO:0000462(absent)"
Remark	"Genotype \"Is[elt-2::GFP]\""
Remark	"We found that laser ablation of the E cell in early (six- to seven-cell stage) embryos eliminated all differentiated gut nuclei in wild-type embryos."
Reference	"WBPaper00037107"


Anatomy_function : "WBbtf0817"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000111"
Not_involved	"WBbt:0005178"	Unnecessary
Remark	"ENTITY:WBbt:0007809(VPC)|WBGene00003024(lin-39)|GO:0006351(transcription, DNA-templated)"
Remark	"QUALITY:PATO:0002175(deviation) NOT"
Remark	"Genotype \"ehn-3(q689); hnd-1(q740)\""
Remark	"In order to determine whether the gonad in&amp;#64258;uenced the LIN-39 pro&amp;#64257;le in vulval precursor cells, we quanti&amp;#64257;ed LIN-39 level by immunostaining in an ehn-3(q689); hnd-1(q740) double mutant, where the gonadal progenitor cells Z1 and Z4 die at early stages. The LIN-39 pro&amp;#64257;le was not affected in ehn-3(q689); hnd-1(q740) double mutants compared to N2, which excluded the gonad as a source of asymmetry for the early L2 stage LIN-39 pro&amp;#64257;le."
Reference	"WBPaper00039829"


Anatomy_function : "WBbtf0818"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000882"	Autonomous
Gene	"WBGene00003006"
Involved	"WBbt:0004096"	Sufficient
Remark	"ENTITY:WBbt:0004096(PQR)|GO:0030425(dendrite)|GO:0048813(dendrite morphogenesis)"
Remark	"QUALITY:PATO:0000460(abnormal) NOT"
Remark	"Genotype \"lin-17(n677);Ex[Pegl-17::LIN-17::YFP]\""
Remark	"LIN-17 is expressed extensively and dynamically in several cells of the tail region including PQR. To test this possibility we used the egl-17 promoter that is highly and selectively expressed in the precursors of PQR during the L1 stage to drive LIN-17 expression from the time PQR was born. Wild-type LIN-17 cDNA expressed by the egl-17 promoter (Pegl-17::LIN-17::YFP) strongly rescued the PQR dendrite defects of lin-17 mutants, to levels similar to that of the endogenous promoter (Plin-17::LIN-17::YFP)."
Remark	"Published_as lin-17"
Reference	"WBPaper00040245"


Anatomy_function : "WBbtf0819"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000882"
Not_involved	"WBbt:0008410"	Unnecessary
Remark	"ENTITY:WBbt:0004096(PQR)|GO:0030425(dendrite)|GO:0048813(dendrite morphogenesis)"
Remark	"QUALITY:PATO:0000460(abnormal) NOT"
Remark	"Recent results in different systems have demonstrated a role of the support cells in regulating dendrite development. To determine if similar mechanisms were in place for PQR development, we next performed cell-ablation experiments whereby we selectively eliminated the socket cells or the socket cells together with the sheath cells. PQR morphology in ablated animals was largely normal, with only a small number of animals presenting short dendrites when left and right phasmid socket cells were ablated (3/15) or when left phasmid socket and left sheath cells were ablated (2/19)."
Reference	"WBPaper00040245"


Anatomy_function : "WBbtf0820"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000882"
Not_involved	"WBbt:0004116"	Unnecessary
Remark	"ENTITY:WBbt:0004096(PQR)|GO:0030425(dendrite)|GO:0048813(dendrite morphogenesis)"
Remark	"QUALITY:PATO:0000460(abnormal) NOT"
Remark	"Recent results in different systems have demonstrated a role of the support cells in regulating dendrite development. To determine if similar mechanisms were in place for PQR development, we next performed cell-ablation experiments whereby we selectively eliminated the socket cells or the socket cells together with the sheath cells. PQR morphology in ablated animals was largely normal, with only a small number of animals presenting short dendrites when left and right phasmid socket cells were ablated (3/15) or when left phasmid socket and left sheath cells were ablated (2/19)."
Reference	"WBPaper00040245"


Anatomy_function : "WBbtf0821"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000882"
Not_involved	"WBbt:0004366"	Unnecessary
Not_involved	"WBbt:0004364"	Unnecessary
Remark	"ENTITY:WBbt:0004096(PQR)|GO:0030425(dendrite)|GO:0048813(dendrite morphogenesis)"
Remark	"QUALITY:PATO:0000460(abnormal) NOT"
Remark	"Recent results in different systems have demonstrated a role of the support cells in regulating dendrite development. To determine if similar mechanisms were in place for PQR development, we next performed cell-ablation experiments whereby we selectively eliminated the socket cells or the socket cells together with the sheath cells. PQR morphology in ablated animals was largely normal, with only a small number of animals presenting short dendrites when left and right phasmid socket cells were ablated (3/15) or when left phasmid socket and left sheath cells were ablated (2/19). In addition, ablations of the phasmid neurons PHA and PHB also had no effect on PQR dendrite development."
Reference	"WBPaper00040245"


Anatomy_function : "WBbtf0822"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000469"	Autonomous
Gene	"WBGene00003252"
Involved	"WBbt:0008598"	Sufficient
Remark	"ENTITY:WBbt:0008598(Q cell)|GO:0016477(cell migration)"
Remark	"QUALITY:PATO:0000460(abnormal) NOT"
Remark	"Genotype \"mig-21(u787); Ex[Pegl-17::mig-21]\""
Remark	"Published_as mig-21"
Remark	"To investigate whether expression of mig-21 in the Q neuroblasts is suf&amp;#64257;cient for the function of mig-21 in Q cell polarization and migration, we expressed wild type mig-21 using the egl-17 promoter in mig-21 mutants. At the L1 stage of larval development, the egl-17 promoter is expressed in the Q neuroblasts and in a subset of cells in the head. Importantly, the egl-17 promoter is not expressed in body wall muscle cells, as con&amp;#64257;rmed by smFISH analysis of mig-21(u787); Pegl-17::mig-21 animals, which showed clear overexpression of mig-21 in the Q neuroblasts but not in body wall muscle cells. We found that Q neuroblast speci&amp;#64257;c expression of mig-21 almost fully rescued the mig-21 mutant phenotype, consistent with a cell autonomous function of mig-21 in the Q neuroblasts."
Reference	"WBPaper00040419"


Anatomy_function : "WBbtf0823"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000345"	Autonomous
Gene	"WBGene00000913"
Involved	"WBbt:0007809"
Remark	"ENTITY:WBbt:0007809(vulval precursor cell)|GO:0051301(cell division)"
Remark	"QUALITY:PATO:0000470(increased) NOT"
Remark	"Genotype \"let-23(sy1); daf-18(ok480); zhEx358[Plin-31::daf-18::gfp]\""
Remark	"Published_as daf-18"
Reference	"WBPaper00041458"


Anatomy_function : "WBbtf0824"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000345"
Gene	"WBGene00000913"
Not_involved	"WBbt:0005178"	Unnecessary
Remark	"Besides the vulval cells, the DAF-18::GFP reporter was also expressed at the L3 to L4 larval stages in several cells of the uterus, which is part of the somatic gonad. We thus tested if the daf-18-mediated repression of vulval induction requires the gonad by ablating the Z1 to Z4 somatic gonad and germline precursor cells at the L1 stage. In gonad-ablated daf-18(lf) let-60(gf) double mutants, vulval induction was higher than in gonad-ablated let-60(gf) single mutants, indicating that DAF-18 represses vulval induction independently of a signal from the gonad. Thus, DAF-18 probably acts predominantly in the VPCs to inhibit MAPK signaling during vulval induction."
Remark	"ENTITY:WBbt:0007809(vulval precursor cell)|GO:0051301(cell division)"
Remark	"QUALITY:PATO:0000470(increased)"
Remark	"Published_as daf-18"
Reference	"WBPaper00041458"


Anatomy_function : "WBbtf0825"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000469"
Gene	"WBGene00006776"
Involved	"WBbt:0005753"	Sufficient
Involved	"WBbt:0008598"	Sufficient
Remark	"ENTITY:WBbt:0003927(AQR)|WBbt:0004096(PQR)|GO:0016477(cell migration)"
Remark	"QUALITY:PATO:0000460(defective) NOT"
Remark	"Genotype \"unc-40(n324); lqIs151[Pscm::unc-40::gfp]\""
Remark	"Published_as unc-40"
Remark	"We drove the expression of the unc-40 coding region fused to green &amp;#64258;uorescent protein (gfp) in the seam cells and Q cells using the scm promoter. This construct was expressed in these cells, and UNC-40::GFP accumulated at the cell margins of the seam cells and Q cells. Furthermore, Pscm::unc-40::gfp rescued the AQR and PQR migration defects of unc-40(n324), suggesting that UNC-40 activity in the seam cells and/or Q cells is suf&amp;#64257;cient for AQR and PQR migration."
Reference	"WBPaper00041597"


Anatomy_function : "WBbtf0826"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000469"
Gene	"WBGene00006776"
Involved	"WBbt:0008598"
Remark	"ENTITY:WBbt:0003927(AQR)|WBbt:0004096(PQR)|GO:0016477(cell migration)"
Remark	"QUALITY:PATO:0000460(defective) NOT"
Remark	"Genotype \"unc-40(n324); Ex[Pegl-17::unc-40]\""
Remark	"Published_as unc-40"
Reference	"WBPaper00041597"


Anatomy_function : "WBbtf0827"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000469"
Gene	"WBGene00006776"
Involved	"WBbt:0008598"	Necessary
Involved	"WBbt:0005753"	Necessary
Remark	"ENTITY:WBbt:0003927(AQR)|WBbt:0004096(PQR)|GO:0016477(cell migration)"
Remark	"QUALITY:PATO:0000460(defective)"
Remark	"Genotype \"ptp-3(mu256); mig-21(u787); Ex[Pscm::unc-40(RNAi)]\""
Remark	"Published_as unc-40"
Remark	"We used a cell-specific transgenic RNAi approach. Transgenic animals were predicted to express both sense and antisense RNAs driven by the scm promoter in the seam cells and Q cell. unc-40 RNAi driven by the scm promoter enhanced QL/QR and AQR/PQR migration defects of ptp-3 and mig-21, suggesting that UNC-40 acts in the seam cells and/or Q cells."
Reference	"WBPaper00041597"


Anatomy_function : "WBbtf0828"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000469"
Gene	"WBGene00003252"
Involved	"WBbt:0008598"	Necessary
Involved	"WBbt:0005753"	Necessary
Remark	"ENTITY:WBbt:0003927(AQR)|WBbt:0004096(PQR)|GO:0016477(cell migration)"
Remark	"QUALITY:PATO:0000460(defective)"
Remark	"Genotype \"Ex[Pscm::mig-21(RNAi)]\""
Remark	"Published_as mig-21"
Remark	"We found that mig-21 RNAi expressed from the scm promoter caused AQR and PQR migration defects."
Reference	"WBPaper00041597"


Anatomy_function : "WBbtf0829"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000469"
Gene	"WBGene00004215"
Involved	"WBbt:0007846"	Sufficient
Remark	"A transgene containing the endogenous ptp-3B gene under its own promoter fused to gfp rescued AQR and PQR migration defects of ptp-3(mu256), as did expression from the dpy-7 promoter active in all hypodermis including the seam cells and the early Q cells."
Remark	"ENTITY:WBbt:0003927(AQR)|WBbt:0004096(PQR)|GO:0016477(cell migration)"
Remark	"QUALITY:PATO:0000460(defective) NOT"
Remark	"Genotype \"ptp-3(mu256); Ex[Pdpy-7::ptp-3B::gfp]\""
Remark	"Published_as ptp-3"
Reference	"WBPaper00041597"


Anatomy_function : "WBbtf0830"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000469"	Autonomous
Gene	"WBGene00004215"
Involved	"WBbt:0008598"	Sufficient
Remark	"ENTITY:WBbt:0003927(AQR)|WBbt:0004096(PQR)|GO:0016477(cell migration)"
Remark	"QUALITY:PATO:0000460(defective) NOT"
Remark	"Genotype \"ptp-3(mu256); Ex[Pegl-17::ptp-3B]\""
Remark	"Published_as ptp-3"
Remark	"Q-cell-specific Pegl-17::ptp-3B expression also rescued ptp-3(mu256) and ptp-3(mu245) AQR and PQR migration defects, suggesting autonomy of ptp-3 function in the Q cells."
Reference	"WBPaper00041597"


Anatomy_function : "WBbtf0831"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000944"
Gene	"WBGene00001475"
Not_involved	"WBbt:0006832"	Insufficient
Not_involved	"WBbt:0006976"	Insufficient
Not_involved	"WBbt:0005278"	Insufficient
Not_involved	"WBbt:0005274"	Insufficient
Not_involved	"WBbt:0005339"	Insufficient
Not_involved	"WBbt:0005336"	Insufficient
Remark	"ENTITY:WBbt:0005303(VD neuron)|GO:0043005(neuron projection)|GO:0097485(neuron projection guidance)|GO:0009949(polarity specification of anterior/posterior axis)"
Remark	"QUALITY:PATO:0000460(defective)"
Remark	"Expression of FMI-1 in a subset of neurons in VNC is not sufficient to rescue the PN (posterior neurite) defects. A combination of cell specific promoters (Podr-2, Psra-6, Pacr-2) was used to drive FMI-1 in cells whose axons contribute to the VNC."
Remark	"Genotype \"fmi-1(tm306);juIs76[Punc-25::gfp];Ex[(Podr-2,Psra-6,Pacr-2)::fmi-1]\""
Remark	"Published_as fmi-1"
Reference	"WBPaper00041941"


Anatomy_function : "WBbtf0832"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000944"
Gene	"WBGene00001475"
Not_involved	"WBbt:0004585"	Insufficient
Not_involved	"WBbt:0005270"	Insufficient
Remark	"ENTITY:WBbt:0005303(VD neuron)|GO:0043005(neuron projection)|GO:0097485(neuron projection guidance)|GO:0009949(polarity specification of anterior/posterior axis)"
Remark	"QUALITY:PATO:0000460(defective)"
Remark	"In addition, we were unable to rescue the PN (posterior neurite) phenotype by expression of FMI-1 specifically in the DD and VD neurons (6 lines)."
Remark	"Published_as fmi-1"
Reference	"WBPaper00041941"


Anatomy_function : "WBbtf0833"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000220"	Nonautonomous
Gene	"WBGene00006874"
Involved	"WBbt:0006827"	Sufficient
Remark	"ENTITY:WBbt:0007809(VPC)|GO:0001709(cell fate determination)"
Remark	"QUALITY:PATO:0000460(defective) NOT"
Remark	"Genotype \"let-23(sy1); vab-8(gm138); dyEx20[PCAN(ceh-23/pes-10)::vab-8s]\""
Remark	"Published_as vab-8"
Remark	"We used a previously described CAN-specific enhancer to create an expression vector to specifically restore VAB-8S and proper positioning only to the CANs. When expressed from the CAN-specific promoter (PCAN::vab-8s), but not the control minimal pes-10 promoter, VAB-8S also restored full inhibition to vulval fate signaling in P6.p in egfr/let-23(lf); vab-8(gm138) double mutant.vulval fate signaling in P6.p in egfr/let-23(lf); vab-8(gm138) double mutants. This transgene also fully suppressed the other vab-8(gm138) epidermal phenotypes, including the ectopic vulval fates at P8.p, the increased frequency of P3.p becoming a vulval progenitor, and the P-Rvl phenotype (0%, n=64). Thus, VAB-8 acts in the CANs to regulate epidermal development."
Reference	"WBPaper00041988"


Anatomy_function : "WBbtf0834"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000220"	Nonautonomous
Gene	"WBGene00000289"
Involved	"WBbt:0006827"	Sufficient
Remark	"ENTITY:WBbt:0007809(VPC)|GO:0001709(cell fate determination)"
Remark	"QUALITY:PATO:0000644(hyperplastic) NOT"
Remark	"Genotype \"cam-1(gm122); lin-3(n378); PCAN(ceh-23)::cam-1::gfp\""
Remark	"Published_as cam-1"
Remark	"To test whether Ror/CAM-1 expression in the CANs is sufficient to restore some aspect of normal inhibition of Wnt activity in epidermal progenitors, we transgenically expressed CAM-1 only in the CANs of cam-1(null); egf/lin-3(lf) double mutants, which have elevated Wnt signaling in the epidermal progenitors. However, of those animals displaying normal migration of at least one of the two CAN cell bodies, CAN-expressed Ror/CAM-1 completely restored the parental egf/lin-3(lf) underinduced phenotype. This result indicates that epidermal progenitors such as P6.p no longer receive abnormally high Wnt signaling when Ror/CAM-1 is expressed only in the CANs of cam-1(null) mutants."
Reference	"WBPaper00041988"


Anatomy_function : "WBbtf0835"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000469"	Autonomous
Gene	"WBGene00003245"
Involved	"WBbt:0007274"	Sufficient
Involved	"WBbt:0007279"	Sufficient
Involved	"WBbt:0003927"	Sufficient
Involved	"WBbt:0004096"	Sufficient
Remark	"ENTITY:WBbt:0003927(AQR)|GO:0016477(cell migration)"
Remark	"QUALITY:PATO:0000574(decreased length) NOT"
Remark	"Genotype \"casEx779[Pegl-13::mig-13];mig-13(cas15);zdIs5[Pmec-4::GFP]; casIs35[Pgcy-32::mCherry]\""
Remark	"Published_as mig-13"
Remark	"We next performed cell type-specific rescue experiments to examine the cell-autonomous function of mig-13 in cell migration. We used four distinct promoters to express the mig-13a isoform, the longest isoform of mig-13, in different Q-cell progenies: the egl-13 promoter (Pegl-13) specifically expresses in the Q.a lineage, Pgcy-32 expresses in Q.ap, Pegl-46 expresses in Q.a/Q.ap and Q.pa/Q.paa, and Pmec-7 expresses in Q.paa. By quantifying the final positions of Q-cell progenies, we showed that AQR migration defects in mig-13 mutants can be completely or partially rescued by the expression of mig-13 under the control of QR.a/ap-specific promoters, but not QR.p/paa promoter."
Reference	"WBPaper00042520"


Anatomy_function : "WBbtf0836"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000469"	Autonomous
Gene	"WBGene00003245"
Involved	"WBbt:0003927"	Sufficient
Involved	"WBbt:0004096"	Sufficient
Remark	"ENTITY:WBbt:0003927(AQR)|GO:0016477(cell migration)"
Remark	"QUALITY:PATO:0000574(decreased length) NOT"
Remark	"Genotype \"casEx596[Pgcy-32::mig-13]; mig-13(cas15); zdIs5[Pmec-4::GFP]; casIs35[Pgcy-32::mCherry]\""
Remark	"Published_as mig-13"
Remark	"We next performed cell type-specific rescue experiments to examine the cell-autonomous function of mig-13 in cell migration. We used four distinct promoters to express the mig-13a isoform, the longest isoform of mig-13, in different Q-cell progenies: the egl-13 promoter (Pegl-13) specifically expresses in the Q.a lineage, Pgcy-32 expresses in Q.ap, Pegl-46 expresses in Q.a/Q.ap and Q.pa/Q.paa, and Pmec-7 expresses in Q.paa. By quantifying the final positions of Q-cell progenies, we showed that AQR migration defects in mig-13 mutants can be completely or partially rescued by the expression of mig-13 under the control of QR.a/ap-specific promoters, but not QR.p/paa promoter."
Reference	"WBPaper00042520"


Anatomy_function : "WBbtf0837"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000469"	Autonomous
Gene	"WBGene00003245"
Involved	"WBbt:0007279"	Sufficient
Involved	"WBbt:0007274"	Sufficient
Involved	"WBbt:0003927"	Sufficient
Involved	"WBbt:0004096"	Sufficient
Involved	"WBbt:0007277"	Sufficient
Involved	"WBbt:0007282"	Sufficient
Involved	"WBbt:0004086"	Sufficient
Involved	"WBbt:0003832"	Sufficient
Remark	"ENTITY:WBbt:0003927(AQR)|GO:0016477(cell migration)"
Remark	"QUALITY:PATO:0000574(decreased length) NOT"
Remark	"Genotype \"casEx600[Pegl-46::mig-13]; mig-13(cas15); zdIs5[Pmec-4::GFP]; casIs35[Pgcy-32::mCherry]\""
Remark	"Published_as mig-13"
Remark	"We next performed cell type-specific rescue experiments to examine the cell-autonomous function of mig-13 in cell migration. We used four distinct promoters to express the mig-13a isoform, the longest isoform of mig-13, in different Q-cell progenies: the egl-13 promoter (Pegl-13) specifically expresses in the Q.a lineage, Pgcy-32 expresses in Q.ap, Pegl-46 expresses in Q.a/Q.ap and Q.pa/Q.paa, and Pmec-7 expresses in Q.paa. By quantifying the final positions of Q-cell progenies, we showed that AQR migration defects in mig-13 mutants can be completely or partially rescued by the expression of mig-13 under the control of QR.a/ap-specific promoters, but not QR.p/paa promoter."
Reference	"WBPaper00042520"


Anatomy_function : "WBbtf0838"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000469"
Gene	"WBGene00003245"
Not_involved	"WBbt:0004086"	Insufficient
Not_involved	"WBbt:0003832"	Insufficient
Remark	"ENTITY:WBbt:0003927(AQR)|GO:0016477(cell migration)"
Remark	"QUALITY:PATO:0000574(decreased length)"
Remark	"Genotype \"casEx1129[Pmec-7::MIG-13::GFP]; mig-13(cas15); zdIs5[Pmec-4::GFP]; casIs35[Pgcy-32::mCherry]\""
Remark	"Published_as mig-13"
Remark	"We next performed cell type-specific rescue experiments to examine the cell-autonomous function of mig-13 in cell migration. We used four distinct promoters to express the mig-13a isoform, the longest isoform of mig-13, in different Q-cell progenies: the egl-13 promoter (Pegl-13) specifically expresses in the Q.a lineage, Pgcy-32 expresses in Q.ap, Pegl-46 expresses in Q.a/Q.ap and Q.pa/Q.paa, and Pmec-7 expresses in Q.paa. By quantifying the final positions of Q-cell progenies, we showed that AQR migration defects in mig-13 mutants can be completely or partially rescued by the expression of mig-13 under the control of QR.a/ap-specific promoters, but not QR.p/paa promoter."
Reference	"WBPaper00042520"


Anatomy_function : "WBbtf0839"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000469"
Gene	"WBGene00003245"
Not_involved	"WBbt:0005190"	Insufficient
Remark	"ENTITY:WBbt:0003927(AQR)|GO:0016477(cell migration)"
Remark	"QUALITY:PATO:0000574(decreased length)"
Remark	"Genotype \"casEx5002[Punc-47::MIG-13::GFP]; zdIs5[Pmec-4::GFP]; mig-13(mu225) casIs35[Pgcy-32::mCherry]\""
Remark	"Published_as mig-13"
Remark	"The previous study suggested that mig-13 acted in the motor neurons to promote QR.x migration. To examine this possibility, we expressed mig-13a using a motor neuron-specific promoter, Punc-47, in mig-13 mutants, and we found that Punc-47::mig-13 transgene failed to rescue the migration defects of AQR and AVM."
Reference	"WBPaper00042520"


Anatomy_function : "WBbtf0840"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000469"
Gene	"WBGene00003245"
Not_involved	"WBbt:0007274"	Insufficient
Not_involved	"WBbt:0007279"	Insufficient
Not_involved	"WBbt:0003927"	Insufficient
Not_involved	"WBbt:0004096"	Insufficient
Remark	"ENTITY:WBbt:0003832(AVM)|GO:0016477(cell migration)"
Remark	"QUALITY:PATO:0000574(decreased length)"
Remark	"Genotype \"casEx779[Pegl-13::mig-13];mig-13(cas15);zdIs5[Pmec-4::GFP]; casIs35[Pgcy-32::mCherry]\""
Remark	"Published_as mig-13"
Remark	"We next performed cell type-specific rescue experiments to examine the cell-autonomous function of mig-13 in cell migration. We used four distinct promoters to express the mig-13a isoform, the longest isoform of mig-13, in different Q-cell progenies: the egl-13 promoter (Pegl-13) specifically expresses in the Q.a lineage, Pgcy-32 expresses in Q.ap, Pegl-46 expresses in Q.a/Q.ap and Q.pa/Q.paa, and Pmec-7 expresses in Q.paa. The final positions of AVM in mig-13 mutants were consistently restored if mig-13 was expressed in AVM but not in AQR."
Reference	"WBPaper00042520"


Anatomy_function : "WBbtf0841"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000469"
Gene	"WBGene00003245"
Not_involved	"WBbt:0003927"	Insufficient
Not_involved	"WBbt:0004096"	Insufficient
Remark	"ENTITY:WBbt:0003832(AVM)|GO:0016477(cell migration)"
Remark	"QUALITY:PATO:0000574(decreased length)"
Remark	"Genotype \"casEx596[Pgcy-32::mig-13]; mig-13(cas15); zdIs5[Pmec-4::GFP]; casIs35[Pgcy-32::mCherry]\""
Remark	"Published_as mig-13"
Remark	"We next performed cell type-specific rescue experiments to examine the cell-autonomous function of mig-13 in cell migration. We used four distinct promoters to express the mig-13a isoform, the longest isoform of mig-13, in different Q-cell progenies: the egl-13 promoter (Pegl-13) specifically expresses in the Q.a lineage, Pgcy-32 expresses in Q.ap, Pegl-46 expresses in Q.a/Q.ap and Q.pa/Q.paa, and Pmec-7 expresses in Q.paa. The final positions of AVM in mig-13 mutants were consistently restored if mig-13 was expressed in AVM but not in AQR."
Reference	"WBPaper00042520"


Anatomy_function : "WBbtf0842"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000469"	Autonomous
Gene	"WBGene00003245"
Involved	"WBbt:0007279"	Sufficient
Involved	"WBbt:0007274"	Sufficient
Involved	"WBbt:0003927"	Sufficient
Involved	"WBbt:0004096"	Sufficient
Involved	"WBbt:0007277"	Sufficient
Involved	"WBbt:0007282"	Sufficient
Involved	"WBbt:0004086"	Sufficient
Involved	"WBbt:0003832"	Sufficient
Remark	"ENTITY:WBbt:0003832(AVM)|GO:0016477(cell migration)"
Remark	"QUALITY:PATO:0000574(decreased length) NOT"
Remark	"Genotype \"casEx600[Pegl-46::mig-13]; mig-13(cas15); zdIs5[Pmec-4::GFP]; casIs35[Pgcy-32::mCherry]\""
Remark	"Published_as mig-13"
Remark	"We next performed cell type-specific rescue experiments to examine the cell-autonomous function of mig-13 in cell migration. We used four distinct promoters to express the mig-13a isoform, the longest isoform of mig-13, in different Q-cell progenies: the egl-13 promoter (Pegl-13) specifically expresses in the Q.a lineage, Pgcy-32 expresses in Q.ap, Pegl-46 expresses in Q.a/Q.ap and Q.pa/Q.paa, and Pmec-7 expresses in Q.paa. The final positions of AVM in mig-13 mutants were consistently restored if mig-13 was expressed in AVM but not in AQR."
Reference	"WBPaper00042520"


Anatomy_function : "WBbtf0843"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000469"	Autonomous
Gene	"WBGene00003245"
Involved	"WBbt:0004086"	Sufficient
Involved	"WBbt:0003832"	Sufficient
Remark	"ENTITY:WBbt:0003832(AVM)|GO:0016477(cell migration)"
Remark	"QUALITY:PATO:0000574(decreased length) NOT"
Remark	"Genotype \"casEx1129[Pmec-7::MIG-13::GFP]; mig-13(cas15); zdIs5[Pmec-4::GFP]; casIs35[Pgcy-32::mCherry]\""
Remark	"Published_as mig-13"
Remark	"We next performed cell type-specific rescue experiments to examine the cell-autonomous function of mig-13 in cell migration. We used four distinct promoters to express the mig-13a isoform, the longest isoform of mig-13, in different Q-cell progenies: the egl-13 promoter (Pegl-13) specifically expresses in the Q.a lineage, Pgcy-32 expresses in Q.ap, Pegl-46 expresses in Q.a/Q.ap and Q.pa/Q.paa, and Pmec-7 expresses in Q.paa. The final positions of AVM in mig-13 mutants were consistently restored if mig-13 was expressed in AVM but not in AQR."
Reference	"WBPaper00042520"


Anatomy_function : "WBbtf0844"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000469"
Gene	"WBGene00003245"
Not_involved	"WBbt:0005190"	Insufficient
Remark	"ENTITY:WBbt:0003832(AVM)|GO:0016477(cell migration)"
Remark	"QUALITY:PATO:0000574(decreased length)"
Remark	"Genotype \"casEx5002[Punc-47::MIG-13::GFP]; zdIs5[Pmec-4::GFP]; mig-13(mu225) casIs35[Pgcy-32::mCherry]\""
Remark	"Published_as mig-13"
Remark	"The previous study suggested that mig-13 acted in the motor neurons to promote QR.x migration. To examine this possibility, we expressed mig-13a using a motor neuron-specific promoter, Punc-47, in mig-13 mutants, and we found that Punc-47::mig-13 transgene failed to rescue the migration defects of AQR and AVM."
Reference	"WBPaper00042520"


Anatomy_function : "WBbtf0845"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000239"
Involved	"WBbt:0008125"	Necessary
Remark	"ENTITY:WBbt:0008129(P7.p)|GO:0048468(cell development)|GO:0009949(polarity specification of anterior/posterior axis)"
Remark	"QUALITY:PATO:0000625(inverted)"
Remark	"Genotype \"lin-18(e620)\""
Remark	"We ablated P6.p after it received its induction cue, but prior to any polarity choice of P7.p. We used a Pegl-17::gfp construct to time induction, and ablated the primary cell in both a wild-type background as well as a lin-18(e620) background to sensitize the animals to defects in FGF signaling.  Similarly to the single mutants of the FGF pathway, ablating P6.p in a wild-type background does not lead to any instances of the P-Rvl phenotype. However, the ablation of P6.p in a lin-18(e620) background showed a strong enhancement of the lin-18(e620) P-Rvl phenotype."
Reference	"WBPaper00044058"


Anatomy_function : "WBbtf0846"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000239"
Involved	"WBbt:0004489"	Necessary
Remark	"ENTITY:WBbt:0008129(P7.p)|GO:0048468(cell development)|GO:0009949(polarity specification of anterior/posterior axis)"
Remark	"QUALITY:PATO:0000625(inverted)"
Remark	"Genotype \"lin-18(e620)\""
Remark	"We ablated the M cell, the precursor to both the left and right SMs, in 29 worms, ~10 hours post-hatching, in a lin-18(e620) background.  Ablation of the M cell resulted in a strong enhancement of the lin-18(e620) phenotype in the same manner as all FGF mutants as well as in the ablation of P6.p."
Reference	"WBPaper00044058"


Anatomy_function : "WBbtf0847"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000239"
Involved	"WBbt:0008605"	Necessary
Remark	"Because the M cell descendants also contribute to the posterior body wall muscle and coelomocytes, we sought a cleaner way to eliminate the SMs before the polarity cue. The SoxC ortholog sem-2(n1343) alters the M cell lineage and prevents the formation of the SMs by driving the cells initially destined to become SMs to become posterior body wall muscle. Constructing sem-2(n1343); lin-18(e620) double mutants results in a 68% P-Rvl phenotype, confirming that the SMs influence the polarity choice of P7.p."
Remark	"ENTITY:WBbt:0008129(P7.p)|GO:0048468(cell development)|GO:0009949(polarity specification of anterior/posterior axis)"
Remark	"QUALITY:PATO:0000625(inverted)"
Remark	"Genotype \"sem-2(n1343); lin-18(e620\""
Reference	"WBPaper00044058"


Anatomy_function : "WBbtf0848"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000572"	Autonomous
Gene	"WBGene00023404"
Involved	"WBbt:0003850"	Sufficient
Remark	"ENTITY:WBbt:0003850(AVG)|GO:1990138(neuron projection extension)|GO:0009949(polarity specification of anterior/posterior axis)"
Remark	"QUALITY:PATO:0001511(defective)"
Remark	"Genotype \"plr-1(zd165); Ex[lin-11::SL2::plr-1-gfp]\""
Remark	"Published_as plr-1"
Remark	"To address whether PLR-1 acts in AVG, we expressed PLR-1-GFP in AVG and several other head neurons during early differentiation using lin-11 regulatory sequences. We found that lin-11::SL2::plr-1-gfp rescues the plr-1 AVG polarity defect. Because other lin-11-expressing neurons are not close to or in contact with AVG, we conclude that PLR-1 acts autonomously to control AVG anteroposterior polarity."
Reference	"WBPaper00044679"


Anatomy_function : "WBbtf0849"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001273"
Gene	"WBGene00000553"
Not_involved	"WBbt:0005662"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0009408(response to heat)"
Remark	"QUALITY:PATO:0001997(reduced)"
Remark	"Genotype \"cmk-1(pg58);Ex[gcy-8p::cmk-1]\""
Remark	"Published_as cmk-1"
Remark	"cmk-1(pg58) homozygous animals carrying AFD-specific gcy-8 promoter showed no rescue of noxious heat avoidance in three independent lines."
Reference	"WBPaper00046106"


Anatomy_function : "WBbtf0850"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0001273"
Not_involved	"WBbt:0005662"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0009408(response to heat)"
Remark	"QUALITY:PATO:0001997(reduced) NOT"
Remark	"We genetically ablated AFD in wild-type and the cmk-1(pg58) background. AFD ablation was achieved genetically in animals expressing a reconstituted caspase in AFD. Animals without AFD avoided heat similarly as those with intact AFD neurons."
Reference	"WBPaper00046106"


Anatomy_function : "WBbtf0851"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001273"
Gene	"WBGene00000553"
Not_involved	"WBbt:0005662"	Insufficient
Not_involved	"WBbt:0005672"	Insufficient
Not_involved	"WBbt:0005666"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0009408(response to heat)"
Remark	"QUALITY:PATO:0001997(reduced)"
Remark	"Genotype \"cmk-1(pg58); Ex[tax-4p::cmk-1]\""
Remark	"Published_as cmk-1"
Remark	"We extended cell-specific rescue experiments to other neurons, focusing on those previously shown to be thermosensitive: AWC, ASI, PVD, and FLP. We observed no rescue effect with the tax-4 promoter, which drives expression in AWC, ASI, AFD, and several other classes of sensory neurons."
Reference	"WBPaper00046106"


Anatomy_function : "WBbtf0852"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001273"
Gene	"WBGene00000553"
Involved	"WBbt:0006828"	Sufficient
Involved	"WBbt:0006831"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0009408(response to heat)"
Remark	"QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"cmk-1(pg58); Ex[egl-46::cmk-1]\""
Remark	"Published_as cmk-1"
Remark	"We extended cell-specific rescue experiments to other neurons, focusing on those previously shown to be thermosensitive: AWC, ASI, PVD, and FLP. We observed a significant rescue effect with the egl-46 promoter, exclusively driving expression in the FLP and PVD neurons in adults."
Reference	"WBPaper00046106"


Anatomy_function : "WBbtf0853"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001273"
Gene	"WBGene00000553"
Involved	"WBbt:0006828"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0009408(response to heat)"
Remark	"QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"cmk-1(pg58); Ex[mec-3p::cmk-1]\""
Remark	"Published_as cmk-1"
Remark	"We extended cell-specific rescue experiments to other neurons, focusing on those previously shown to be thermosensitive: AWC, ASI, PVD, and FLP. We observed a significant rescue effect with the mec-3 promoter, driving expression into the touch receptor neurons (TRNs), PVD and FLP. We further analyzed transgenic animals from one mec-3p::cmk-1 rescue line by separately scoring individuals that were expressing GFP in FLP and individuals that were not. Strikingly, rescue was detected only in animals expressing the transgene in FLP. These data imply that expression of wild-type cmk-1 in FLP is sufficient to restore noxious heat avoidance."
Reference	"WBPaper00046106"


Anatomy_function : "WBbtf0854"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0001273"
Involved	"WBbt:0006828"	Necessary
Involved	"WBbt:0005490"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0009408(response to heat)"
Remark	"QUALITY:PATO:0001997(reduced)"
Remark	"Genotype \"domEx303[mec-3p::CZcasp3, flp-4p::QF, QUAS::casp3NZ::SL2mCherry, unc-122p::RFP]\""
Remark	"To determine if FLP neurons were necessary for noxious heat avoidance, we evaluated the effect of ablating FLP neurons on noxious heat avoidance. We generated a line expressing a caspase suicide transgene to ablate FLP neurons. This line also ablated PLM. In a wild-type cmk-1 background, ablating FLP (and PLM) produced a partial defect in heat avoidance."
Reference	"WBPaper00046106"


Anatomy_function : "WBbtf0855"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001012"
Gene	"WBGene00000903"
Involved	"WBbt:0005667"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0002209(behavioral defense response)|GO:0042742(defense response to bacterium)|NCBITaxon:287(Pseudomonas aeruginosa)"
Remark	"QUALITY: PATO:0002052(decreased occurrence) NOT"
Remark	"Genotype \"daf-7(ok3125);Ex[Ptrx-1::daf-7]\""
Remark	"Published_as daf-7"
Remark	"We determined that transgenic overexpression of daf-7 under the native daf-7 promoter or the ASJ-speci&amp;#64257;c trx-1 promoter, as well as under the ASI-speci&amp;#64257;c str-3 promoter, were each suf&amp;#64257;cient to restore wild-type pathogen avoidance and susceptibility in the daf-7(ok3125) mutant background, consistent with the activity of DAF-7 as a secreted ligand."
Reference	"WBPaper00045859"


Anatomy_function : "WBbtf0856"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001012"
Gene	"WBGene00000903"
Involved	"WBbt:0005666"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0002209(behavioral defense response)|GO:0042742(defense response to bacterium)|NCBITaxon:287(Pseudomonas aeruginosa)"
Remark	"QUALITY: PATO:0002052(decreased occurrence) NOT"
Remark	"Genotype \"daf-7(ok3125);Ex[Pstr-3::daf-7]\""
Remark	"Published_as daf-7"
Remark	"We determined that transgenic overexpression of daf-7 under the native daf-7 promoter or the ASJ-speci&amp;#64257;c trx-1 promoter, as well as under the ASI-speci&amp;#64257;c str-3 promoter, were each suf&amp;#64257;cient to restore wild-type pathogen avoidance and susceptibility in the daf-7(ok3125) mutant background, consistent with the activity of DAF-7 as a secreted ligand."
Reference	"WBPaper00045859"


Anatomy_function : "WBbtf0857"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000062"
Gene	"WBGene00000903"
Involved	"WBbt:0005667"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0016265(death)|NCBITaxon:287(Pseudomonas aeruginosa)"
Remark	"QUALITY: PATO:0002052(decreased occurrence) NOT"
Remark	"Genotype \"daf-7(ok3125);Ex[Ptrx-1::daf-7]\""
Remark	"Published_as daf-7"
Remark	"We determined that transgenic overexpression of daf-7 under the native daf-7 promoter or the ASJ-speci&amp;#64257;c trx-1 promoter, as well as under the ASI-speci&amp;#64257;c str-3 promoter, were each suf&amp;#64257;cient to restore wild-type pathogen avoidance and susceptibility in the daf-7(ok3125) mutant background, consistent with the activity of DAF-7 as a secreted ligand."
Reference	"WBPaper00045859"


Anatomy_function : "WBbtf0858"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000062"
Gene	"WBGene00000903"
Involved	"WBbt:0005666"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0016265(death)|NCBITaxon:287(Pseudomonas aeruginosa)"
Remark	"QUALITY: PATO:0002052(decreased occurrence) NOT"
Remark	"Genotype \"daf-7(ok3125);Ex[Pstr-3::daf-7]\""
Remark	"Published_as daf-7"
Remark	"We determined that transgenic overexpression of daf-7 under the native daf-7 promoter or the ASJ-speci&amp;#64257;c trx-1 promoter, as well as under the ASI-speci&amp;#64257;c str-3 promoter, were each suf&amp;#64257;cient to restore wild-type pathogen avoidance and susceptibility in the daf-7(ok3125) mutant background, consistent with the activity of DAF-7 as a secreted ligand."
Reference	"WBPaper00045859"


Anatomy_function : "WBbtf0859"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0001012"
Involved	"WBbt:0005667"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0002209(behavioral defense response)|GO:0042742(defense response to bacterium)|NCBITaxon:287(Pseudomonas aeruginosa)"
Remark	"QUALITY: PATO:0002052(decreased occurrence) NOT"
Remark	"Genotype \"jxEx[trx-1::ICE+ofm-1::gfp]\""
Remark	"We also observed that the genetic ablation of the ASJ neuron pair conferred a partial deficit in P. aeruginosa avoidance and susceptibility, demonstrating that the ASJ neurons are necessary for the complete protective response to P. aeruginosa."
Reference	"WBPaper00045859"


Anatomy_function : "WBbtf0860"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000062"
Involved	"WBbt:0005667"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0016265(death)|NCBITaxon:287(Pseudomonas aeruginosa)"
Remark	"QUALITY: PATO:0002052(decreased occurrence) NOT"
Remark	"Genotype \"jxEx[trx-1::ICE+ofm-1::gfp]\""
Remark	"We also observed that the genetic ablation of the ASJ neuron pair conferred a partial deficit in P. aeruginosa avoidance and susceptibility, demonstrating that the ASJ neurons are necessary for the complete protective response to P. aeruginosa."
Reference	"WBPaper00045859"


Anatomy_function : "WBbtf0861"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001012"
Gene	"WBGene00000897"
Involved	"WBbt:0006834"	Sufficient
Involved	"WBbt:0005835"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0002209(behavioral defense response)|GO:0042742(defense response to bacterium)|NCBITaxon:287(Pseudomonas aeruginosa)"
Remark	"QUALITY:PATO:0002052(decreased occurrence) NOT"
Remark	"Expression of daf-1 in only the RIM/RIC interneurons under the tdc-1 promoter was sufficient to restore pathogen avoidance behavior in the daf-1 mutant to wild-type levels."
Remark	"Genotype \"daf-1(m40); ftEX205[ptdc-1::daf-1-gfp; odr-1::dsRED]\""
Remark	"Published_as daf-1"
Reference	"WBPaper00045859"


Anatomy_function : "WBbtf0862"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001012"
Gene	"WBGene00000897"
Not_involved	"WBbt:0006816"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0002209(behavioral defense response)|GO:0042742(defense response to bacterium)|NCBITaxon:287(Pseudomonas aeruginosa)"
Remark	"QUALITY:PATO:0002052(decreased occurrence)"
Remark	"Genotype \"daf-1(m40); ftEX83[posm-6::daf-1::GFP; odr-1::dsRED]\""
Remark	"Published_as daf-1"
Remark	"Using daf-1 mutant strains in which transgenic expression of daf-1 is directed in subsets of neurons, we observed that daf-1 expression under its native promoter or the panneuronal egl-3 promoter rescued P. aeruginosa avoidance to wild-type levels, but no rescue was observed when daf-1 was expressed in ~60 ciliated sensory neurons (including ASI and ASJ), using either the osm-6 or bbs-1 promoters."
Reference	"WBPaper00045859"


Anatomy_function : "WBbtf0863"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001012"
Gene	"WBGene00000897"
Not_involved	"WBbt:0006816"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0002209(behavioral defense response)|GO:0042742(defense response to bacterium)|NCBITaxon:287(Pseudomonas aeruginosa)"
Remark	"QUALITY:PATO:0002052(decreased occurrence)"
Remark	"Genotype \"daf-1(m40); ftEX70[pbbs-1::daf-1::GFP; odr-1::dsRED]\""
Remark	"Published_as daf-1"
Remark	"Using daf-1 mutant strains in which transgenic expression of daf-1 is directed in subsets of neurons, we observed that daf-1 expression under its native promoter or the panneuronal egl-3 promoter rescued P. aeruginosa avoidance to wild-type levels, but no rescue was observed when daf-1 was expressed in ~60 ciliated sensory neurons (including ASI and ASJ), using either the osm-6 or bbs-1 promoters."
Reference	"WBPaper00045859"


Anatomy_function : "WBbtf0864"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001012"	Autonomous
Gene	"WBGene00001665"
Involved	"WBbt:0005667"	Sufficient
Remark	"ENTITY:WBbt:0005667(ASJ)|WBGene00000903(daf-7)|GO:0010467(gene expression)|GO:0042742(defense response to bacterium)|NCBITaxon:287(Pseudomonas aeruginosa)"
Remark	"QUALITY:PATO:0002052(decreased occurrence) NOT"
Remark	"Genotype \"ksIs2; gpa-2(pk16) gpa-3(pk35); qdEx67[trx-1p::gpa-3 + ofm-1::gfp]\""
Remark	"Published_as gpa-3"
Remark	"To determine if GPA-3 acts cell autonomously in the ASJ neurons to mediate the response to P. aeruginosa , we expressed wild-type copies of gpa-3 cDNA under heterologous promoters in the gpa-2(pk16) gpa-3(pk35) background. Under control of either the panciliated neuronal promoter bbs-1 or the ASJ-specific promoter trx-1, gpa-3 cDNA was able to rescue the daf-7 ASJ expression defect, indicating that GPA-3 acts cell autonomously in ASJ to mediate the response to P. aeruginosa."
Reference	"WBPaper00045859"


Anatomy_function : "WBbtf0865"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001012"	Autonomous
Gene	"WBGene00001664"
Involved	"WBbt:0005667"	Sufficient
Remark	"ENTITY:WBbt:0005667(ASJ)|WBGene00000903(daf-7)|GO:0010467(gene expression)|GO:0042742(defense response to bacterium)|NCBITaxon:287(Pseudomonas aeruginosa)"
Remark	"QUALITY:PATO:0002052(decreased occurrence) NOT"
Remark	"Genotype \"ksIs2; gpa-2(pk16) gpa-3(pk35); qdEx95[trx-1p::gpa-2 + ofm-1::gfp]\""
Remark	"Published_as gpa-2"
Remark	"To determine the site of action for gpa-2 in the response to P.aeruginosa, we expressed wild-type copies of gpa-2 cDNA under heterologous promoters in the gpa-2(pk16) gpa-3(pk35) background. To our surprise, expression of gpa-2 driven by either the panciliated neuronal promoter bbs-1 or the ASJ-specific promoter trx-1 was able to rescue the daf-7p::gfp phenotype, but expression of gpa-2 in the AWC neurons under the ceh-36 promoter was not able to rescue the gpa-2 gpa-3 mutant phenotype. This indicates that GPA-2, like GPA-3, also acts cell autonomously in ASJ to induce daf-7 expression in response to P. aeruginosa."
Reference	"WBPaper00045859"


Anatomy_function : "WBbtf0866"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001012"
Gene	"WBGene00001664"
Not_involved	"WBbt:0005672"	Insufficient
Remark	"ENTITY:WBbt:0005667(ASJ)|WBGene00000903(daf-7)|GO:0010467(gene expression)|GO:0042742(defense response to bacterium)|NCBITaxon:287(Pseudomonas aeruginosa)"
Remark	"QUALITY:PATO:0002052(decreased occurrence)"
Remark	"Genotype \"ksIs2; gpa-2(pk16) gpa-3(pk35); qdEx96[ceh-36p::gpa-2 + ofm-1::gfp]\""
Remark	"Published_as gpa-2"
Remark	"To determine the site of action for gpa-2 in the response to P.aeruginosa, we expressed wild-type copies of gpa-2 cDNA under heterologous promoters in the gpa-2(pk16) gpa-3(pk35) background. To our surprise, expression of gpa-2 driven by either the panciliated neuronal promoter bbs-1 or the ASJ-specific promoter trx-1 was able to rescue the daf-7p::gfp phenotype, but expression of gpa-2 in the AWC neurons under the ceh-36 promoter was not able to rescue the gpa-2 gpa-3 mutant phenotype. This indicates that GPA-2, like GPA-3, also acts cell autonomously in ASJ to induce daf-7 expression in response to P. aeruginosa."
Reference	"WBPaper00045859"


Anatomy_function : "WBbtf0867"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000399"
Not_involved	"WBbt:0006782"	Unnecessary
Remark	"ENTITY:WBbt:0006789(uterine seam cell)|GO:0035847(uterine epithelium development)|GO:0003382(epithelial cell morphogenesis)"
Remark	"QUALITY:PATO:0000460(abnormal) NOT"
Remark	"We hypothesized that the du cell could potentially be pushing downward on the utse, causing it to stretch outward. However, du ablation had no effect on utse cell behavior."
Reference	"WBPaper00045833"


Anatomy_function : "WBbtf0868"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000399"
Involved	"WBbt:0006785"	Necessary
Remark	"Ablations of uterine toroid 1 (ut1) or uterine toroid 2 (ut2) caused defects in utse development. 88% of ut1-ablated worms showed defects in nuclear migration and had utse cell bodies that were both shorter than wild type and missing portions."
Remark	"ENTITY:WBbt:0006789(uterine seam cell)|GO:0035847(uterine epithelium development)|GO:0003382(epithelial cell morphogenesis)"
Remark	"QUALITY:PATO:0000460(abnormal)"
Reference	"WBPaper00045833"


Anatomy_function : "WBbtf0869"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000399"
Involved	"WBbt:0006786"	Necessary
Remark	"Ablations of uterine toroid 1 (ut1) or uterine toroid 2 (ut2) caused defects in utse development. 91% of ut2 ablated worms showed defects including reduced distance between utse nuclei in ut2 ablated worms and a shorter cell bodies containing missing portions and vacuoles."
Remark	"ENTITY:WBbt:0006789(uterine seam cell)|GO:0035847(uterine epithelium development)|GO:0003382(epithelial cell morphogenesis)"
Remark	"QUALITY:PATO:0000460(abnormal)"
Reference	"WBPaper00045833"


Anatomy_function : "WBbtf0870"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000399"
Not_involved	"WBbt:0006787"	Unnecessary
Remark	"Ablation of the next most distal ut cell, ut3 which has no direct contact with the utse, caused no defects in nuclear migration or cell outgrowth."
Remark	"ENTITY:WBbt:0006789(uterine seam cell)|GO:0035847(uterine epithelium development)|GO:0003382(epithelial cell morphogenesis)"
Remark	"QUALITY:PATO:0000460(abnormal) NOT"
Reference	"WBPaper00045833"


Anatomy_function : "WBbtf0871"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000399"
Involved	"WBbt:0005728"	Necessary
Remark	"ENTITY:WBbt:0006789(uterine seam cell)|GO:0035847(uterine epithelium development)|GO:0003382(epithelial cell morphogenesis)"
Remark	"QUALITY:PATO:0000460(abnormal)"
Remark	"We performed the anchor cell ablations after mid L4, the stage at which the AC had already induced pi cells, fused with the upsilon cell nuclei, and its nucleus could be easily identifies due to its position in a unique plane of focus relative to other nuclei in the worm. C nuclear ablation caused defects in utse development. utse nuclei were clustered together in AC nuclear ablated worms and utse cell bodies were short and deformed."
Reference	"WBPaper00045833"


Anatomy_function : "WBbtf0872"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000399"
Involved	"WBbt:0008605"	Necessary
Remark	"ENTITY:WBbt:0006789(uterine seam cell)|GO:0035847(uterine epithelium development)|GO:0003382(epithelial cell morphogenesis)"
Remark	"QUALITY:PATO:0000460(abnormal)"
Remark	"We ablated the M cell in the L1 larval stage, and then observed the utse at L4. In the absence of the SMs, the utse cell body exhibits abnormal morphology and expands beyond its normal position."
Reference	"WBPaper00045833"


Anatomy_function : "WBbtf0873"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001764"
Gene	"WBGene00001844"
Involved	"WBbt:0003679"	Sufficient
Remark	"ENTITY:WBbt:0003681(pharynx)|GO:0043050(pharyngeal pumping)|PATO:0000161(rate)|GO:0010035(response to inorganic substance)|CHEBI:16526(carbon dioxide)"
Remark	"QUALITY:PATO:0002302(decreased process quality) NOT"
Remark	"Genotype \"hid-1(sa722); lin-15(n765); jsEx897[rab-3p::HID-1::GFP\""
Remark	"Published_as hid-1"
Remark	"To test whether inhibition of pharynx pumping in response to 10% CO2 requires expression of hid-1 in the gut, neurons, or both, we used transgenic lines that express HID-1 fused to GFP driven by either the pan-neuronal promoter rab-3 or the gut-specific promoter ges-1. Expression of HID-1 under the rab-3 promoter in neurons of hid-1(sa722) background was sufficient to restore inhibition of the pharynx pumping almost to the levels shown by wild-type animals."
Reference	"WBPaper00045598"


Anatomy_function : "WBbtf0874"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001764"
Gene	"WBGene00001844"
Not_involved	"WBbt:0005792"	Insufficient
Remark	"ENTITY:WBbt:0003681(pharynx)|GO:0043050(pharyngeal pumping)|PATO:0000161(rate)|GO:0010035(response to inorganic substance)|CHEBI:16526(carbon dioxide)"
Remark	"QUALITY:PATO:0002302(decreased process quality)"
Remark	"Genotype \"hid-1(sa722); lin-15(n765); jsEx909[ges-1p::HID-1::GFP\""
Remark	"Published_as hid-1"
Remark	"To test whether inhibition of pharynx pumping in response to 10% CO2 requires expression of hid-1 in the gut, neurons, or both, we used transgenic lines that express HID-1 fused to GFP driven by either the pan-neuronal promoter rab-3 or the gut-specific promoter ges-1. Expression of HID-1 under the rab-3 promoter in neurons of hid-1(sa722) background was sufficient to restore inhibition of the pharynx pumping almost to the levels shown by wild-type animals. In contrast, expression of HID-1 under the ges-1 promoter in the gut of hid-1(sa722) had no significant effect on the response of the pharynx to 10% CO2."
Reference	"WBPaper00045598"


Anatomy_function : "WBbtf0875"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001764"
Gene	"WBGene00001844"
Not_involved	"WBbt:0005662"	Insufficient
Remark	"ENTITY:WBbt:0003681(pharynx)|GO:0043050(pharyngeal pumping)|PATO:0000161(rate)|GO:0010035(response to inorganic substance)|CHEBI:16526(carbon dioxide)"
Remark	"QUALITY:PATO:0002302(decreased process quality)"
Remark	"Genotype \"hid-1(sa722); ygEx317[gcy-8p::HID-1::GFP]\""
Remark	"Published_as hid-1"
Remark	"Transgenic expression of HID-1::GFP driven by a gcy-8 promoter in the thermosensory AFD of hid-1(sa722) background did not restore the CO2-mediated pumping inhibition."
Reference	"WBPaper00045598"


Anatomy_function : "WBbtf0876"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001764"
Gene	"WBGene00001844"
Not_involved	"WBbt:0005663"	Insufficient
Remark	"ENTITY:WBbt:0003681(pharynx)|GO:0043050(pharyngeal pumping)|PATO:0000161(rate)|GO:0010035(response to inorganic substance)|CHEBI:16526(carbon dioxide)"
Remark	"QUALITY:PATO:0002302(decreased process quality)"
Remark	"Genotype \"hid-1(sa722); Ex[osm-6p::HID-1::GFP]\""
Remark	"Published_as hid-1"
Remark	"Transgenic expression of HID-1::GFP driven by the osm-6 promoter, which was expressed in ASE neurons (undetected in BAG neurons), did not restore the CO2-mediated pumping inhibition."
Reference	"WBPaper00045598"


Anatomy_function : "WBbtf0877"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001764"
Gene	"WBGene00001844"
Involved	"WBbt:0006825"	Sufficient
Remark	"ENTITY:WBbt:0003681(pharynx)|GO:0043050(pharyngeal pumping)|PATO:0000161(rate)|GO:0010035(response to inorganic substance)|CHEBI:16526(carbon dioxide)"
Remark	"QUALITY:PATO:0002302(decreased process quality) NOT"
Remark	"Genotype \"hid-1(sa722); ygEx319 [flp-17-p::HID-1::GFP\""
Remark	"Published_as hid-1"
Remark	"Transgenic lines expressing HID-1::GFP under the promoter of flp-17 showed expression in the BAG neurons. This expression was sufficient to fully restore the CO2-dependent pumping inhibition."
Reference	"WBPaper00045598"


Anatomy_function : "WBbtf0878"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001764"
Gene	"WBGene00001844"
Involved	"WBbt:0006825"	Sufficient
Remark	"ENTITY:WBbt:0003681(pharynx)|GO:0043050(pharyngeal pumping)|PATO:0000161(rate)|GO:0010035(response to inorganic substance)|CHEBI:16526(carbon dioxide)"
Remark	"QUALITY:PATO:0002302(decreased process quality) NOT"
Remark	"Genotype \"hid-1(sa722); ygEx320 [gcy-33-p::HID-1::GFP\""
Remark	"Published_as hid-1"
Remark	"The expression of HID-1::GFP under the gcy-33 promoter in hid-1(sa722)background was specific to the BAG neurons. This expression was sufficient to fully restore the CO2-dependent pumping inhibition."
Reference	"WBPaper00045598"


Anatomy_function : "WBbtf0879"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001764"
Involved	"WBbt:0006825"	Necessary
Remark	"ENTITY:WBbt:0003681(pharynx)|GO:0043050(pharyngeal pumping)|PATO:0000161(rate)|GO:0010035(response to inorganic substance)|CHEBI:16526(carbon dioxide)"
Remark	"QUALITY:PATO:0002302(decreased process quality)"
Remark	"We also ablated the BAG neurons in wild-type background using GFP driven by gcy-33 promoter as a marker. We found that following ablation of the BAG neurons, the pumping in response to 10% CO2 was similar to that in HID-1-null animals (Figure 4C). These results suggest that the BAG neurons are required for the pumping inhibition."
Reference	"WBPaper00045598"


Anatomy_function : "WBbtf0880"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000738"
Involved	"WBbt:0006828"	Necessary
Involved	"WBbt:0005237"	Necessary
Involved	"WBbt:0006831"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0009270(response to humidity)"
Remark	"QUALITY:PATO:0000460(defective)"
Remark	"Genotype \"vxEx284[Pmec-10::ICE+Pmyo-2::mCherry]\""
Remark	"To test the requirement of these different sensory neurons in hygrotaxis, we used strains with different subsets of neurons that had been destroyed via expression of a human cell death caspase (ICE) or via a gain-of-function mutation in mec-4. We found that ablation of the touch and multidendritic neurons (via Pmec-10::ICE or Pmec-3::ICE) abolished hygrotaxis."
Reference	"WBPaper00045291"


Anatomy_function : "WBbtf0881"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000738"
Involved	"WBbt:0006828"	Necessary
Involved	"WBbt:0005237"	Necessary
Involved	"WBbt:0006831"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0009270(response to humidity)"
Remark	"QUALITY:PATO:0000460(defective)"
Remark	"Genotype \"vxEx277[Pmec-3::ICE+Pmyo-2::mCherry]\""
Remark	"To test the requirement of these different sensory neurons in hygrotaxis, we used strains with different subsets of neurons that had been destroyed via expression of a human cell death caspase (ICE) or via a gain-of-function mutation in mec-4. We found that ablation of the touch and multidendritic neurons (via Pmec-10::ICE or Pmec-3::ICE) abolished hygrotaxis."
Reference	"WBPaper00045291"


Anatomy_function : "WBbtf0882"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000738"
Not_involved	"WBbt:0005237"	Unnecessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0009270(response to humidity)"
Remark	"QUALITY:PATO:0000460(defective) NOT"
Remark	"Genotype \"mec-4(e1611) X\""
Remark	"To test the requirement of these different sensory neurons in hygrotaxis, we used strains with different subsets of neurons that had been destroyed via expression of a human cell death caspase (ICE) or via a gain-of-function mutation in mec-4. We found that ablation of the touch neurons [via mec-4(d)] had no effect on hygrotaxis."
Reference	"WBPaper00045291"


Anatomy_function : "WBbtf0883"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000738"
Not_involved	"WBbt:0005244"	Unnecessary
Not_involved	"WBbt:0005415"	Unnecessary
Not_involved	"WBbt:0006747"	Unnecessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0009270(response to humidity)"
Remark	"QUALITY:PATO:0000460(defective) NOT"
Remark	"Genotype \"Ex[Pdat-1::ICE]\""
Remark	"To test the requirement of these different sensory neurons in hygrotaxis, we used strains with different subsets of neurons that had been destroyed via expression of a human cell death caspase (ICE) or via a gain-of-function mutation in mec-4. We found that ablation of the mechanosensitive dopamine neurons (CEP, ADE, and PED via Pdat-1::ICE) had no effect on hygrotaxis."
Reference	"WBPaper00045291"


Anatomy_function : "WBbtf0884"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000738"
Involved	"WBbt:0006828"	Necessary
Involved	"WBbt:0006826"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0009270(response to humidity)"
Remark	"QUALITY:PATO:0000460(defective)"
Remark	"Genotype \"vxEx279[Psto-5::ICE+Pmyo-2::mCherry]\""
Remark	"To test the requirement of these different sensory neurons in hygrotaxis, we used strains with different subsets of neurons that had been destroyed via expression of a human cell death caspase (ICE) or via a gain-of-function mutation in mec-4. To test the FLP neurons, we ablated them via expression of Psto-5::ICE and found that this strain failed to perform hygrotaxis."
Reference	"WBPaper00045291"


Anatomy_function : "WBbtf0885"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000738"
Gene	"WBGene00022815"
Involved	"WBbt:0006828"	Sufficient
Involved	"WBbt:0006826"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0009270(response to humidity)"
Remark	"QUALITY:PATO:0000460(defective) NOT"
Remark	"Genotype \"asic-1(ok415) I; vxEx284[Psto-5::ASIC-1+Pcoel::GFP]\""
Remark	"Published_as asic-1"
Remark	"We then assessed whether asic-1(null) mutant worms with asic-1 rescued in FLP using the Psto-5 promoter could perform hygrotaxis. These asic-1 (FLP+) transgenic worms displayed significant improvement in hygrotaxis performance while their untransformed sisters performed similarly to the asic-1(null) mutant."
Reference	"WBPaper00045291"


Anatomy_function : "WBbtf0886"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000738"
Involved	"WBbt:0005662"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0009270(response to humidity)"
Remark	"QUALITY:PATO:0000460(defective)"
Remark	"Genotype \"vxEx289[Pgcy-8::ICE+Pmyo-2::mCherry]\""
Remark	"To independently test the role of AFD neurons in hygrosensation, we genetically ablated them by expressing ICE with the AFD-specific promoter Pgcy-8. This AFD-ablated strain failed to perform hygrotaxis."
Reference	"WBPaper00045291"


Anatomy_function : "WBbtf0887"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000738"
Gene	"WBGene00006526"
Involved	"WBbt:0005662"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0009270(response to humidity)"
Remark	"QUALITY:PATO:0000460(defective) NOT"
Remark	"Genotype \"tax-4(p678) III. VxEx291[Pgcy-8::tax-4+Pmyo-2::mCherry]\""
Remark	"Published_as tax-4"
Remark	"The tax-4 gene is widely expressed in various sensory neurons. To determine whether tax-4 is required in AFD neurons for hygrotaxis, we expressed it in a tax-4 mutant background in AFD, which partially rescued hygrotaxis."
Reference	"WBPaper00045291"


Anatomy_function : "WBbtf0888"
Assay	"Optogenetic"
Phenotype	"WBPhenotype:0001006"
Involved	"WBbt:0003638"	Sufficient
Remark	"ENTITY:WBbt:0003681(pharynx)|GO:0006936(muscle contraction)|GO:0043050(pharyngeal pumping)"
Remark	"QUALITY:PATO:0000912(increased rate)"
Remark	"Genotype \"lin-15(n765ts) vsIs48[unc-17::GFP] X; zxIs6[Punc-17::ChR2(H134R)::YFP; lin-15(+)] V\""
Remark	"We found that optogenetic excitation of the MC neurons stimulated pumping. Stimulation of the MCs still excited pumping after the ablation of the M2 neurons, demonstrating that the MCs can directly stimulate pumping."
Reference	"WBPaper00045312"


Anatomy_function : "WBbtf0889"
Assay	"Optogenetic"
Phenotype	"WBPhenotype:0001006"
Involved	"WBbt:0003634"	Sufficient
Remark	"ENTITY:WBbt:0003681(pharynx)|GO:0006936(muscle contraction)|GO:0043050(pharyngeal pumping)"
Remark	"QUALITY:PATO:0000912(increased rate)"
Remark	"Genotype \"lin-15(n765ts) vsIs48[unc-17::GFP] X; zxIs6[Punc-17::ChR2(H134R)::YFP; lin-15(+)] V\""
Remark	"We found that optogenetic stimulation of the M2s increased pump rate to a similar level as that observed during MC stimulation. Furthermore, M2 excitation stimulated pumping in the absence of the MC neurons, demonstrating that the M2s, like the MCs, can stimulate pumping directly."
Reference	"WBPaper00045312"


Anatomy_function : "WBbtf0890"
Assay	"Optogenetic"
Phenotype	"WBPhenotype:0001006"
Involved	"WBbt:0004467"	Sufficient
Remark	"ENTITY:WBbt:0003681(pharynx)|GO:0006936(muscle contraction)|GO:0043050(pharyngeal pumping)"
Remark	"QUALITY:PATO:0000912(increased rate)"
Remark	"Genotype \"lin-15(n765ts) vsIs48[unc-17::GFP] X; zxIs6[Punc-17::ChR2(H134R)::YFP; lin-15(+)] V\""
Remark	"We found that optogenetic excitation of the M4 neuron caused an increase in pumping to a similar level as that observed during MC or M2 stimulation."
Reference	"WBPaper00045312"


Anatomy_function : "WBbtf0891"
Assay	"Optogenetic"
Phenotype	"WBPhenotype:0002056"
Involved	"WBbt:0004467"	Sufficient
Remark	"ENTITY:WBbt:0003734(isthmus)|GO:0030432(peristalsis)"
Remark	"QUALITY:PATO:0000912(increased rate)"
Remark	"Genotype \"lin-15(n765ts) vsIs48[unc-17::GFP] X; zxIs6[Punc-17::ChR2(H134R)::YFP; lin-15(+)] V\""
Remark	"Optogenetic excitation of M4 caused a greater proportion of pumps to be followed by peristalsis than during MC stimulation."
Reference	"WBPaper00045312"


Anatomy_function : "WBbtf0892"
Assay	"Optogenetic"
Phenotype	"WBPhenotype:0001006"
Not_involved	"WBbt:0004488"	Insufficient
Remark	"ENTITY:WBbt:0003681(pharynx)|GO:0006936(muscle contraction)|GO:0043050(pharyngeal pumping)"
Remark	"QUALITY:PATO:0000912(increased rate)"
Remark	"Genotype \"lin-15(n765ts) vsIs48[unc-17::GFP] X; zxIs6[Punc-17::ChR2(H134R)::YFP; lin-15(+)] V\""
Remark	"In contrast to the other cholinergic pharyngeal neurons, we did not find M1 optogenetic stimulation to affect pump rate."
Reference	"WBPaper00045312"


Anatomy_function : "WBbtf0893"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001006"
Involved	"WBbt:0003649"	Necessary
Remark	"Ablation of the I1 neurons has no effect on the pump rate in the presence of food. However, we found that the I1s are required for pumping in the absence of food."
Remark	"ENTITY:WBbt:0003681(pharynx)|GO:0006936(muscle contraction)|GO:0043050(pharyngeal pumping)"
Remark	"QUALITY:PATO:0000912(increased rate) NOT"
Reference	"WBPaper00045312"


Anatomy_function : "WBbtf0894"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001006"
Involved	"WBbt:0003638"	Necessary
Involved	"WBbt:0003634"	Necessary
Remark	"ENTITY:WBbt:0003681(pharynx)|GO:0006936(muscle contraction)|GO:0043050(pharyngeal pumping)"
Remark	"QUALITY:PATO:0000912(increased rate) NOT"
Remark	"I1 stimulation excited pumping following the ablation of either the MCs or the M2s, but not following ablation of both neuron types, demonstrating that the I1s can stimulate pumping through the MCs, through the M2s, or through both the MCs and the M2s."
Reference	"WBPaper00045312"


Anatomy_function : "WBbtf0895"
Assay	"Optogenetic"
Phenotype	"WBPhenotype:0001006"
Involved	"WBbt:0003649"	Sufficient
Remark	"ENTITY:WBbt:0003681(pharynx)|GO:0006936(muscle contraction)|GO:0043050(pharyngeal pumping)"
Remark	"QUALITY:PATO:0000912(increased rate)"
Remark	"Genotype \"lin-15(n765ts) vsIs48[unc-17::GFP] X; zxIs6[Punc-17::ChR2(H134R)::YFP; lin-15(+)] V\""
Remark	"Optogenetic stimulation of the I1 neurons increases pumping rate in an ATR-dependent manner to a level similar to that seen with MC or M2 stimulation."
Reference	"WBPaper00045312"


Anatomy_function : "WBbtf0896"
Assay	"Optogenetic"
Phenotype	"WBPhenotype:0001006"
Not_involved	"WBbt:0004488"	Unnecessary
Remark	"ENTITY:WBbt:0003681(pharynx)|GO:0006936(muscle contraction)|GO:0043050(pharyngeal pumping)"
Remark	"QUALITY:PATO:0000912(increased rate)"
Remark	"Genotype \"lite-1(ce314) X; zxEx620[Punc-17::Mac::YFP; Pelt-2::mCherry]\""
Remark	"Optogenetic inhibition of M1 had no effect on pump rate, suggesting that M1 is not required for pump rate regulation."
Reference	"WBPaper00045312"


Anatomy_function : "WBbtf0897"
Assay	"Optogenetic"
Phenotype	"WBPhenotype:0001006"
Involved	"WBbt:0003638"	Necessary
Remark	"ENTITY:WBbt:0003681(pharynx)|GO:0006936(muscle contraction)|GO:0043050(pharyngeal pumping)"
Remark	"QUALITY:PATO:0000912(increased rate) NOT"
Remark	"Genotype \"lite-1(ce314) X; zxEx620[Punc-17::Mac::YFP; Pelt-2::mCherry]\""
Remark	"We found that optogenetic inhibition of the MCs, the M2s, or M4 reduced pump rate, indicating that an endogenous function of these neurons is to stimulate pumping."
Reference	"WBPaper00045312"


Anatomy_function : "WBbtf0898"
Assay	"Optogenetic"
Phenotype	"WBPhenotype:0001006"
Involved	"WBbt:0003634"	Necessary
Remark	"ENTITY:WBbt:0003681(pharynx)|GO:0006936(muscle contraction)|GO:0043050(pharyngeal pumping)"
Remark	"QUALITY:PATO:0000912(increased rate) NOT"
Remark	"Genotype \"lite-1(ce314) X; zxEx620[Punc-17::Mac::YFP; Pelt-2::mCherry]\""
Remark	"We found that optogenetic inhibition of the MCs, the M2s, or M4 reduced pump rate, indicating that an endogenous function of these neurons is to stimulate pumping."
Reference	"WBPaper00045312"


Anatomy_function : "WBbtf0899"
Assay	"Optogenetic"
Phenotype	"WBPhenotype:0001006"
Involved	"WBbt:0003677"	Necessary
Remark	"ENTITY:WBbt:0003681(pharynx)|GO:0006936(muscle contraction)|GO:0043050(pharyngeal pumping)"
Remark	"QUALITY:PATO:0000912(increased rate) NOT"
Remark	"Genotype \"lite-1(ce314) X; zxEx620[Punc-17::Mac::YFP; Pelt-2::mCherry]\""
Remark	"We found that optogenetic inhibition of the MCs, the M2s, or M4 reduced pump rate, indicating that an endogenous function of these neurons is to stimulate pumping."
Reference	"WBPaper00045312"


Anatomy_function : "WBbtf0900"
Assay	"Optogenetic"
Phenotype	"WBPhenotype:0001006"
Involved	"WBbt:0003649"	Necessary
Remark	"ENTITY:WBbt:0003681(pharynx)|GO:0006936(muscle contraction)|GO:0043050(pharyngeal pumping)"
Remark	"QUALITY:PATO:0000912(increased rate) NOT"
Remark	"Genotype \"lite-1(ce314) X; zxEx620[Punc-17::Mac::YFP; Pelt-2::mCherry]\""
Remark	"The I1 interneurons regulate pumping endogenously via the MCs and the M2s. As with MC, M2, and M4, we found that I1 inhibition caused a decrease in pumping."
Reference	"WBPaper00045312"


Anatomy_function : "WBbtf0901"
Assay	"Optogenetic"
Phenotype	"WBPhenotype:0001006"
Involved	"WBbt:0003638"	Necessary
Involved	"WBbt:0003634"	Necessary
Remark	"ENTITY:WBbt:0003681(pharynx)|GO:0006936(muscle contraction)|GO:0043050(pharyngeal pumping)|GO:0043051(regulation of pharyngeal pumping)|WBbt:0003649(I1 neuron)"
Remark	"QUALITY:PATO:0000912(increased rate) NOT"
Remark	"Genotype \"lite-1(ce314) X; zxEx620[Punc-17::Mac::YFP; Pelt-2::mCherry]\""
Remark	"However, inhibition of the I1s simultaneously with inhibition of both the MCs and the M2s did not cause slower pumping than that seen with inhibition of the MCs and the M2s alone, indicating that effect of I1 inhibition on pumping rate requires the MCs and the M2s."
Reference	"WBPaper00045312"


Anatomy_function : "WBbtf0902"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0001455"
Not_involved	"WBbt:0005671"	Unnecessary
Remark	"Animals in which AWB or AWC were genetically ablated showed no defects in chemotaxis in response to high diacetyl concentrations."
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050919(negative chemotaxis)|PATO:0001159(concentrated)|MI:0351(pure)|CHEBI:16583(diacetyl)"
Remark	"QUALITY: PATO:0002052(decreased occurrence) NOT"
Remark	"Genotype \"Ex[Pstr-1::mCasp1]\""
Reference	"WBPaper00045214"


Anatomy_function : "WBbtf0903"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0001455"
Not_involved	"WBbt:0005672"	Unnecessary
Remark	"Animals in which AWB or AWC were genetically ablated showed no defects in chemotaxis in response to high diacetyl concentrations."
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050919(negative chemotaxis)|PATO:0001159(concentrated)|MI:0351(pure)|CHEBI:16583(diacetyl)"
Remark	"QUALITY: PATO:0002052(decreased occurrence) NOT"
Remark	"Genotype \"Ex[Pceh-36::mCasp1]\""
Reference	"WBPaper00045214"


Anatomy_function : "WBbtf0904"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0001455"
Involved	"WBbt:0005665"	Necessary
Remark	"Animals in which AWB or AWC were genetically ablated showed no defects in chemotaxis in response to high diacetyl concentrations. However, ablation of ASH neurons inhibited this avoidance behavior."
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050919(negative chemotaxis)|PATO:0001159(concentrated)|MI:0351(pure)|CHEBI:16583(diacetyl)"
Remark	"QUALITY: PATO:0002052(decreased occurrence)"
Remark	"Genotype \"Ex[Psra-6::mCasp1]\""
Reference	"WBPaper00045214"


Anatomy_function : "WBbtf0905"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001455"
Gene	"WBGene00005526"
Involved	"WBbt:0005665"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050919(negative chemotaxis)|PATO:0001159(concentrated)|MI:0351(pure)|CHEBI:16583(diacetyl)"
Remark	"QUALITY: PATO:0002052(decreased occurrence)"
Remark	"Genotype \"Ex[Psra-6::sri-14RNAi]\""
Remark	"Published_as sri-14"
Remark	"To determine whether SRI-14 functions in AWC or ASH neurons in the response to high concentrations of diacetyl, we performed neuron-specific knockdown of sri-14 in AWC and ASH neurons. ASH-specific knockdown of sri-14 caused a defect in diacetyl avoidance, but AWC-specific knockdown did not."
Reference	"WBPaper00045214"


Anatomy_function : "WBbtf0906"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001455"
Gene	"WBGene00005526"
Not_involved	"WBbt:0005672"	Unnecessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050919(negative chemotaxis)|PATO:0001159(concentrated)|MI:0351(pure)|CHEBI:16583(diacetyl)"
Remark	"QUALITY: PATO:0002052(decreased occurrence) NOT"
Remark	"Genotype \"Ex[Pceh-36::sri-14RNAi]\""
Remark	"Published_as sri-14"
Remark	"To determine whether SRI-14 functions in AWC or ASH neurons in the response to high concentrations of diacetyl, we performed neuron-specific knockdown of sri-14 in AWC and ASH neurons. ASH-specific knockdown of sri-14 caused a defect in diacetyl avoidance, but AWC-specific knockdown did not."
Reference	"WBPaper00045214"


Anatomy_function : "WBbtf0907"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001455"
Gene	"WBGene00005526"
Not_involved	"WBbt:0005672"	Unnecessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050919(negative chemotaxis)|PATO:0001159(concentrated)|MI:0351(pure)|CHEBI:16583(diacetyl)"
Remark	"QUALITY: PATO:0002052(decreased occurrence) NOT"
Remark	"Genotype \"Ex[Pceh-36::sri-14RNAi]\""
Remark	"Published_as sri-14"
Remark	"To determine whether SRI-14 functions in AWC or ASH neurons in the response to high concentrations of diacetyl, we performed neuron-specific knockdown of sri-14 in AWC and ASH neurons. ASH-specific knockdown of sri-14 caused a defect in diacetyl avoidance, but AWC-specific knockdown did not."
Reference	"WBPaper00045214"


Anatomy_function : "WBbtf0908"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001455"
Gene	"WBGene00005526"
Involved	"WBbt:0005665"	Sufficient
Remark	"Defects of the sri-14 mutants in the avoidance of high diacetyl concentrations were rescued by the ASH-specific expression of sri-14 complementary DNA."
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050919(negative chemotaxis)|PATO:0001159(concentrated)|MI:0351(pure)|CHEBI:16583(diacetyl)"
Remark	"QUALITY: PATO:0002052(decreased occurrence) NOT"
Remark	"Genotype \"sri-14(ok2865); Ex[Psra-6::sri-14]\""
Remark	"Published_as sri-14"
Reference	"WBPaper00045214"


Anatomy_function : "WBbtf0909"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001455"
Gene	"WBGene00005526"
Not_involved	"WBbt:0005670"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050919(negative chemotaxis)|PATO:0001159(concentrated)|MI:0351(pure)|CHEBI:16583(diacetyl)"
Remark	"QUALITY: PATO:0002052(decreased occurrence)"
Remark	"Genotype \"sri-14(ok2865); Ex[Podr-10::sri-14]\""
Remark	"Moreover, defects of the sri-14 mutants in the avoidance of high diacetyl concentrations were rescued by the ASH-specific expression of sri-14 complementary DNA (cDNA), but were only partially rescued or not rescued by specific expression in AWA, AWB, or AWC olfactory neurons."
Remark	"Published_as sri-14"
Reference	"WBPaper00045214"


Anatomy_function : "WBbtf0910"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001455"
Gene	"WBGene00005526"
Not_involved	"WBbt:0005671"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050919(negative chemotaxis)|PATO:0001159(concentrated)|MI:0351(pure)|CHEBI:16583(diacetyl)"
Remark	"QUALITY: PATO:0002052(decreased occurrence)"
Remark	"Genotype \"sri-14(ok2865); Ex[Pstr-1::sri-14]\""
Remark	"Moreover, defects of the sri-14 mutants in the avoidance of high diacetyl concentrations were rescued by the ASH-specific expression of sri-14 complementary DNA (cDNA), but were only partially rescued or not rescued by specific expression in AWA, AWB, or AWC olfactory neurons."
Remark	"Published_as sri-14"
Reference	"WBPaper00045214"


Anatomy_function : "WBbtf0911"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001455"
Gene	"WBGene00005526"
Not_involved	"WBbt:0005672"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050919(negative chemotaxis)|PATO:0001159(concentrated)|MI:0351(pure)|CHEBI:16583(diacetyl)"
Remark	"QUALITY: PATO:0002052(decreased occurrence)"
Remark	"Genotype \"sri-14(ok2865); Ex[Pceh-36::sri-14]\""
Remark	"Moreover, defects of the sri-14 mutants in the avoidance of high diacetyl concentrations were rescued by the ASH-specific expression of sri-14 complementary DNA (cDNA), but were only partially rescued or not rescued by specific expression in AWA, AWB, or AWC olfactory neurons."
Remark	"Published_as sri-14"
Reference	"WBPaper00045214"


Anatomy_function : "WBbtf0912"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0001455"
Involved	"WBbt:0005670"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050919(negative chemotaxis)|PATO:0001159(concentrated)|MI:0351(pure)|CHEBI:16583(diacetyl)"
Remark	"QUALITY: PATO:0002052(decreased occurrence)"
Remark	"Genotype \"Ex[Podr-10::mCap1]\""
Remark	"We analyzed behavioral responses of animals in which the AWA neurons were specifically ablated. AWA-ablated animals exhibited decreased avoidance of high diacetyl concentrations."
Reference	"WBPaper00045214"


Anatomy_function : "WBbtf0913"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000265"
Involved	"WBbt:0005670"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050918(positive chemotaxis)|CHEBI:16583(diacetyl)"
Remark	"QUALITY: PATO:0002052(decreased occurrence)"
Remark	"Genotype \"Ex[Podr-10::mCap1]\""
Remark	"We analyzed behavioral responses of animals in which the AWA neurons were specifically ablated. AWA-ablated animals exhibited decreased avoidance of high diacetyl concentrations, as well as reduced attraction to low concentration."
Reference	"WBPaper00045214"


Anatomy_function : "WBbtf0914"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0001455"
Involved	"WBbt:0005670"	Necessary
Involved	"WBbt:0005665"	Necessary
Remark	"Double ablation of both AWA and ASH caused a more severe defect than did single ablation, indicating that AWA and ASH act in parallel in the response to high diacetyl concentrations."
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050919(negative chemotaxis)|PATO:0001159(concentrated)|MI:0351(pure)|CHEBI:16583(diacetyl)"
Remark	"QUALITY: PATO:0002052(decreased occurrence)"
Remark	"Genotype \"Ex[Podr-10::mCap1+Psra-6::mCap1]\""
Reference	"WBPaper00045214"


Anatomy_function : "WBbtf0915"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0001455"
Involved	"WBbt:0006812"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050919(negative chemotaxis)|PATO:0001159(concentrated)|MI:0351(pure)|CHEBI:16583(diacetyl)"
Remark	"QUALITY:PATO:0000625(reversed)"
Remark	"Functional inhibition of AIA, AIY, or AIZ interneurons changed the response from avoidance to attraction in worms exposed to high diacetyl concentrations, and inhibition of AIB impaired the avoidance response."
Remark	"Genotype \"Ex[Pgcy-28.d::unc-103(gf)]\""
Reference	"WBPaper00045214"


Anatomy_function : "WBbtf0916"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0001455"
Involved	"WBbt:0005413"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050919(negative chemotaxis)|PATO:0001159(concentrated)|MI:0351(pure)|CHEBI:16583(diacetyl)"
Remark	"QUALITY:PATO:0000625(reversed)"
Remark	"Functional inhibition of AIA, AIY, or AIZ interneurons changed the response from avoidance to attraction in worms exposed to high diacetyl concentrations, and inhibition of AIB impaired the avoidance response."
Remark	"Genotype \"Ex[Pttx-3::unc-103(gf)]\""
Reference	"WBPaper00045214"


Anatomy_function : "WBbtf0917"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0001455"
Involved	"WBbt:0005836"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050919(negative chemotaxis)|PATO:0001159(concentrated)|MI:0351(pure)|CHEBI:16583(diacetyl)"
Remark	"QUALITY:PATO:0000625(reversed)"
Remark	"Functional inhibition of AIA, AIY, or AIZ interneurons changed the response from avoidance to attraction in worms exposed to high diacetyl concentrations, and inhibition of AIB impaired the avoidance response."
Remark	"Genotype \"Ex[Plin-11::unc-103(gf)]\""
Reference	"WBPaper00045214"


Anatomy_function : "WBbtf0918"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0001455"
Involved	"WBbt:0006813"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050919(negative chemotaxis)|PATO:0001159(concentrated)|MI:0351(pure)|CHEBI:16583(diacetyl)"
Remark	"QUALITY:PATO:0002052(decreased occurrence)"
Remark	"Functional inhibition of AIA, AIY, or AIZ interneurons changed the response from avoidance to attraction in worms exposed to high diacetyl concentrations, and inhibition of AIB impaired the avoidance response."
Remark	"Genotype \"Ex[Pnpr-9::unc-103(gf)]\""
Reference	"WBPaper00045214"


Anatomy_function : "WBbtf0919"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000265"
Not_involved	"WBbt:0006812"	Unnecessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050918(positive chemotaxis)|CHEBI:16583(diacetyl)"
Remark	"QUALITY:PATO:0002052(decreased occurrence) NOT"
Remark	"Genotype \"Ex[Pgcy-28.d::unc-103(gf)]\""
Remark	"In contrast, with the exception of AIY, attraction to low concentrations (1,000X dilution) of diacetyl was unaffected by inhibition of these interneurons (AIA, AIB, AIY or AIZ)."
Reference	"WBPaper00045214"


Anatomy_function : "WBbtf0920"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000265"
Not_involved	"WBbt:0006813"	Unnecessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050918(positive chemotaxis)|CHEBI:16583(diacetyl)"
Remark	"QUALITY:PATO:0002052(decreased occurrence) NOT"
Remark	"Genotype \"Ex[Pnpr-9::unc-103(gf)]\""
Remark	"In contrast, with the exception of AIY, attraction to low concentrations (1,000X dilution) of diacetyl was unaffected by inhibition of these interneurons (AIA, AIB, AIY or AIZ)."
Reference	"WBPaper00045214"


Anatomy_function : "WBbtf0921"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000265"
Not_involved	"WBbt:0005836"	Unnecessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050918(positive chemotaxis)|CHEBI:16583(diacetyl)"
Remark	"QUALITY:PATO:0002052(decreased occurrence) NOT"
Remark	"Genotype \"Ex[Plin-11::unc-103(gf)]\""
Remark	"In contrast, with the exception of AIY, attraction to low concentrations (1,000X dilution) of diacetyl was unaffected by inhibition of these interneurons (AIA, AIB, AIY or AIZ)."
Reference	"WBPaper00045214"


Anatomy_function : "WBbtf0922"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0001048"
Involved	"WBbt:0005670"	Necessary
Remark	"Because we observed that ablation of AWA altered the response to diacetyl, we also tested the effect of AWA ablation on the calcium responses induced by a high concentration (10**(-3) of diacetyl in ASH neurons and found that ablation of AWA neurons enhanced the calcium response of ASH neurons, indicating that AWA maybe involved in an inhibitory circuit with ASH."
Remark	"ENTITY:WBbt:0005665(ASH)|CHEBI:29108(calcium(2+))|GO:0050801(ion homeostasis)|PATO:0000077(response to)|PATO:0001159(concentrated)|CHEBI:16583(diacetyl)"
Remark	"QUALITY:PATO:0001997(decrease amount)"
Remark	"Genotype \"Ex[Podr-10::mCap1]\""
Reference	"WBPaper00045214"


Anatomy_function : "WBbtf0923"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001048"	Autonomous
Gene	"WBGene00005526"
Involved	"WBbt:0005665"	Sufficient
Remark	"ENTITY:WBbt:0005665(ASH)|CHEBI:29108(calcium(2+))|GO:0050801(ion homeostasis)|PATO:0000077(response to)|PATO:0001159(concentrated)|CHEBI:16583(diacetyl)"
Remark	"QUALITY:PATO:0001997(decrease amount) NOT"
Remark	"Genotype \"sri-14(ok2865); Ex[Psra-6::sri-14]\""
Remark	"Published_as sri-14"
Remark	"We observed normal Ca2+ dynamics that were evoked by a high concentration of diacetyl in ASH neurons in odr-10 mutants, but significantly decreased responses in ASH neurons in sri-14 mutants. This defect of sri-14 mutants in response to diacetyl in ASH was rescued by ASH-specific expression of the wild-type sri-14 gene."
Reference	"WBPaper00045214"


Anatomy_function : "WBbtf0924"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001048"	Autonomous
Gene	"WBGene00005526"
Involved	"WBbt:0005665"	Necessary
Remark	"ENTITY:WBbt:0005665(ASH)|CHEBI:29108(calcium(2+))|GO:0050801(ion homeostasis)|PATO:0000077(response to)|PATO:0001159(concentrated)|CHEBI:16583(diacetyl)"
Remark	"QUALITY:PATO:0001997(decrease amount)"
Remark	"Genotype \"Ex[Psra-6::sri-14RNAi]\""
Remark	"Published_as sri-14"
Remark	"We observed normal Ca2+ dynamics that were evoked by a high concentration of diacetyl in ASH neurons in odr-10 mutants, but significantly decreased responses in ASH neurons in sri-14 mutants. ASH-specific sri-14 knockdown in wild-type animals decreased ASH Ca2+ responses to a high concentration of diacetyl."
Reference	"WBPaper00045214"


Anatomy_function : "WBbtf0925"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000736"
Involved	"WBbt:0005784"	Necessary
Remark	"ENTITY:WBbt:0005792(intestinal cell)|WBbt:0005753(seam cell)|GO:0006914(autophagy)"
Remark	"QUALITY:PATO:0002051(increased occurrence)"
Remark	"Genotype \"glp-1(e2141)\""
Remark	"We observed a dramatic increase in autophagosomes as well as in autolysosomes in intestinal and hypodermal seam cells in glp-1(e2141) mutants compared to N2 wild-type animals."
Reference	"WBPaper00040180"


Anatomy_function : "WBbtf0926"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001785"
Gene	"WBGene00003423"
Involved	"WBbt:0005842"	Sufficient
Involved	"WBbt:0006819"	Sufficient
Involved	"WBbt:0006818"	Sufficient
Involved	"WBbt:0005835"	Sufficient
Involved	"WBbt:0003850"	Sufficient
Involved	"WBbt:0004823"	Sufficient
Involved	"WBbt:0005840"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0007613(memory)|GO:0008306(associative learning)|GO:0042595(behavioral response to starvation)|GO:0006935(chemotaxis)|CHEBI:16583(diacetyl)"
Remark	"QUALITY:PATO:0000498(increased duration) NOT"
Remark	"Genotype \"msi-1(os1); utrEx61[pnmr-1::msi-1cDNA::MYC-tag::3'UTR, psur-5::mDsRed]\""
Remark	"In order to de&amp;#64257;ne the cellular requirement for MSI-1, we performed tissue-speci&amp;#64257;c rescue experiments by expressing the msi-1 cDNA under the control of the endogenous, nmr-1, lim-4, rig-3, or the unc-47 promoters in the msi-1(lf) mutant. In the STAM (short-term associative memory) test, the endogenous promoter as well as the Pnmr-1- and Prig-3-driven msi-1 cDNA rescued the memory phenotype of msi-1(lf) mutants, whereas no rescue was observed when using Plim-4 or Punc-47."
Remark	"Published_as msi-1"
Reference	"WBPaper00045009"


Anatomy_function : "WBbtf0927"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001785"
Gene	"WBGene00003423"
Involved	"WBbt:0005842"	Sufficient
Involved	"WBbt:0003649"	Sufficient
Involved	"WBbt:0004741"	Sufficient
Involved	"WBbt:0004467"	Sufficient
Involved	"WBbt:0003666"	Sufficient
Involved	"WBbt:0004070"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0007613(memory)|GO:0008306(associative learning)|GO:0042595(behavioral response to starvation)|GO:0006935(chemotaxis)|CHEBI:16583(diacetyl)"
Remark	"QUALITY:PATO:0000498(increased duration) NOT"
Remark	"Genotype \"msi-1(os1); utrEx60[prig-3::msi-1cDNA::MYC-tag::3'UTR, psur-5::mDsRed]\""
Remark	"In order to de&amp;#64257;ne the cellular requirement for MSI-1, we performed tissue-speci&amp;#64257;c rescue experiments by expressing the msi-1 cDNA under the control of the endogenous, nmr-1, lim-4, rig-3, or the unc-47 promoters in the msi-1(lf) mutant. In the STAM (short-term associative memory) test, the endogenous promoter as well as the Pnmr-1- and Prig-3-driven msi-1 cDNA rescued the memory phenotype of msi-1(lf) mutants, whereas no rescue was observed when using Plim-4 or Punc-47."
Remark	"Published_as msi-1"
Reference	"WBPaper00045009"


Anatomy_function : "WBbtf0928"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001785"
Gene	"WBGene00003423"
Not_involved	"WBbt:0005671"	Insufficient
Not_involved	"WBbt:0005021"	Insufficient
Not_involved	"WBbt:0005400"	Insufficient
Not_involved	"WBbt:0003938"	Insufficient
Not_involved	"WBbt:0006839"	Insufficient
Not_involved	"WBbt:0005397"	Insufficient
Not_involved	"WBbt:0005361"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0007613(memory)|GO:0008306(associative learning)|GO:0042595(behavioral response to starvation)|GO:0006935(chemotaxis)|CHEBI:16583(diacetyl)"
Remark	"QUALITY:PATO:0000498(increased duration)"
Remark	"Genotype \"msi-1(os1); utrEx59[plim-4::msi-1cDNA::MYC-tag::3'UTR, psur-5::mDsRed]\""
Remark	"In order to de&amp;#64257;ne the cellular requirement for MSI-1, we performed tissue-speci&amp;#64257;c rescue experiments by expressing the msi-1 cDNA under the control of the endogenous, nmr-1, lim-4, rig-3, or the unc-47 promoters in the msi-1(lf) mutant. In the STAM (short-term associative memory) test, the endogenous promoter as well as the Pnmr-1- and Prig-3-driven msi-1 cDNA rescued the memory phenotype of msi-1(lf) mutants, whereas no rescue was observed when using Plim-4 or Punc-47."
Remark	"Published_as msi-1"
Reference	"WBPaper00045009"


Anatomy_function : "WBbtf0929"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001785"
Gene	"WBGene00003423"
Not_involved	"WBbt:0005399"	Insufficient
Not_involved	"WBbt:0003843"	Insufficient
Not_involved	"WBbt:0005045"	Insufficient
Not_involved	"WBbt:0004070"	Insufficient
Not_involved	"WBbt:0004822"	Insufficient
Not_involved	"WBbt:0005270"	Insufficient
Not_involved	"WBbt:0005303"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0007613(memory)|GO:0008306(associative learning)|GO:0042595(behavioral response to starvation)|GO:0006935(chemotaxis)|CHEBI:16583(diacetyl)"
Remark	"QUALITY:PATO:0000498(increased duration)"
Remark	"Genotype \"msi-1(os1); utrEx70[punc-47::msi-1cDNA::MYC-tag::3'UTR, psur-5::mDsRed]\""
Remark	"In order to de&amp;#64257;ne the cellular requirement for MSI-1, we performed tissue-speci&amp;#64257;c rescue experiments by expressing the msi-1 cDNA under the control of the endogenous, nmr-1, lim-4, rig-3, or the unc-47 promoters in the msi-1(lf) mutant. In the STAM (short-term associative memory) test, the endogenous promoter as well as the Pnmr-1- and Prig-3-driven msi-1 cDNA rescued the memory phenotype of msi-1(lf) mutants, whereas no rescue was observed when using Plim-4 or Punc-47."
Remark	"Published_as msi-1"
Reference	"WBPaper00045009"


Anatomy_function : "WBbtf0930"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001785"
Involved	"WBbt:0005842"	Sufficient
Involved	"WBbt:0003649"	Sufficient
Involved	"WBbt:0004741"	Sufficient
Involved	"WBbt:0004467"	Sufficient
Involved	"WBbt:0003666"	Sufficient
Involved	"WBbt:0004070"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0007613(memory)|GO:0008306(associative learning)|GO:0042595(behavioral response to starvation)|GO:0006935(chemotaxis)|CHEBI:16583(diacetyl)"
Remark	"QUALITY:PATO:0000498(increased duration) NOT"
Remark	"Genotype \"utrEx62[prig-3::wsp-1VCA::3'UTR, psur-5::mDsRed]\""
Remark	"To overactivate the Arp2/3 complex, we expressed the WSP-1 VCA fragment under the control of the nmr-1 or rig-3 promoters in wild-type worms. In accord with our hypothesis, expression of the WSP-1 VCA fragment under the nmr-1 or rig-3 promoters increased memory retention in wild-type worms similar to msi-1 deletion. This result shows that increased activity of the Arp2/3 complex in the AVA neuron is sufficient to inhibit memory loss."
Reference	"WBPaper00045009"


Anatomy_function : "WBbtf0931"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001785"
Involved	"WBbt:0005842"	Sufficient
Involved	"WBbt:0006819"	Sufficient
Involved	"WBbt:0006818"	Sufficient
Involved	"WBbt:0005835"	Sufficient
Involved	"WBbt:0003850"	Sufficient
Involved	"WBbt:0004823"	Sufficient
Involved	"WBbt:0005840"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0007613(memory)|GO:0008306(associative learning)|GO:0042595(behavioral response to starvation)|GO:0006935(chemotaxis)|CHEBI:16583(diacetyl)"
Remark	"QUALITY:PATO:0000498(increased duration) NOT"
Remark	"Genotype \"utrEx63[pnmr-1::wsp-1VCA::3'UTR, psur-5::mDsRed]\""
Remark	"To overactivate the Arp2/3 complex, we expressed the WSP-1 VCA fragment under the control of the nmr-1 or rig-3 promoters in wild-type worms. In accord with our hypothesis, expression of the WSP-1 VCA fragment under the nmr-1 or rig-3 promoters increased memory retention in wild-type worms similar to msi-1 deletion. This result shows that increased activity of the Arp2/3 complex in the AVA neuron is sufficient to inhibit memory loss."
Reference	"WBPaper00045009"


Anatomy_function : "WBbtf0932"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001681"
Involved	"WBbt:0008609"	Necessary
Remark	"ENTITY:WBbt:0006874(Psub1)|"
Remark	"QUALITY:"
Remark	"We directly tested the role of the MBR (midbody remnant) in spindle rotation by specifically ablating the MBR alone with the use of a focused, pulsed UV laser. MBR ablation before rotation of the nucleus-centrosome complex started in P1 leads to a loss of nucleus-centrosome complex and spindle rotation onto the AP axis."
Reference	"WBPaper00044848"


Anatomy_function : "WBbtf0933"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001681"
Involved	"WBbt:0008609"	Necessary
Remark	"ENTITY:WBbt:0006874(Psub1)|GO:0072686(mitotic spindle)|PATO:0001599(rotation)"
Remark	"QUALITY:PATO:0000381(decreased frequency)"
Remark	"We directly tested the role of the MBR (midbody remnant, of first cell division) in spindle rotation by specifically ablating the MBR alone with the use of a focused, pulsed UV laser. MBR ablation before rotation of the nucleus-centrosome complex started in P1 leads to a loss of nucleus-centrosome complex and spindle rotation onto the AP axis."
Reference	"WBPaper00044848"


Anatomy_function : "WBbtf0934"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001897"
Involved	"WBbt:0003645"	Necessary
Remark	"ENTITY:WBbt:0003681(pharynx)|GO:0043050(pharyngeal pumping)|PATO:0000381(reduced frequency)|GO:0009416(response to light stimulus)|PATO:0001424(violet)"
Remark	"QUALITY:PATO:0000502(delayed)"
Remark	"To test whether either of these pharyngeal neuron classes might function in the response to light, we used laser microsurgery to kill the pair of I2 neurons and the I4 neuron. We found that killing the I2 neuron pair delayed the acute response, indicating that the I2 neurons promote acute response speed."
Reference	"WBPaper00046411"


Anatomy_function : "WBbtf0935"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001897"
Not_involved	"WBbt:0004741"	Unnecessary
Remark	"ENTITY:WBbt:0003681(pharynx)|GO:0043050(pharyngeal pumping)|PATO:0000381(reduced frequency)|GO:0009416(response to light stimulus)|PATO:0001424(violet)"
Remark	"QUALITY:PATO:0000502(delayed) NOT"
Remark	"To test whether either of these pharyngeal neuron classes might function in the response to light, we used laser microsurgery to kill the pair of I2 neurons and the I4 neuron. We found that killing the I2 neuron pair delayed the acute response, indicating that the I2 neurons promote acute response speed. By contrast, we observed no effect of ablating the I4 neuron."
Reference	"WBPaper00046411"


Anatomy_function : "WBbtf0936"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0001897"
Involved	"WBbt:0003645"	Necessary
Remark	"ENTITY:WBbt:0003681(pharynx)|GO:0043050(pharyngeal pumping)|PATO:0000381(reduced frequency)|GO:0009416(response to light stimulus)|PATO:0001424(violet)"
Remark	"QUALITY:PATO:0000502(delayed)"
Remark	"To test whether either of these pharyngeal neuron classes might function in the response to light, we used laser microsurgery to kill the pair of I2 neurons and the I4 neuron. We found that killing the I2 neuron pair delayed the acute response, indicating that the I2 neurons promote acute response speed. Cell-specific genetic ablation of the I2 neurons using the caspase CSP-1B confirmed these findings."
Reference	"WBPaper00046411"


Anatomy_function : "WBbtf0937"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001897"
Gene	"WBGene00001804"
Involved	"WBbt:0003645"	Sufficient
Remark	"ENTITY:WBbt:0003681(pharynx)|GO:0043050(pharyngeal pumping)|PATO:0000381(reduced frequency)|GO:0009416(response to light stimulus)|PATO:0001424(violet)"
Remark	"QUALITY:PATO:0000502(delayed) NOT"
Remark	"Genotype \"gur-3(ok2245) lin-15(n765); nEx2144[flp-15prom::mCherry::gur-3, lin-15(+)]\""
Remark	"Published_as gur-3"
Remark	"To test whether gur-3 acts in the I2 neurons for the pumping response to light, we generated a transgenic strain (flp-15prom::mCherry::gur-3) that expressed a fluorescence-tagged GUR-3 protein using a promoter that expresses specifically in the I2s and PHAs, a pair of neurons in the tail (flp-15prom). Expression of gur-3 using this promoter rescued the acute response defect of gur-3 mutants."
Reference	"WBPaper00046411"


Anatomy_function : "WBbtf0938"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001897"	Autonomous
Gene	"WBGene00001804"
Involved	"WBbt:0003645"	Sufficient
Remark	"ENTITY:WBbt:0003645(I2 neuron)|PATO:0001162(increased concentration)|CHEBI:29108(calcium(2+))||GO:0009416(response to light stimulus)|PATO:0001424(violet)"
Remark	"QUALITY:PATO:0000297(abolished) NOT"
Remark	"Published_as gur-3"
Remark	"We found that gur-3 mutants completely lacked the I2 calcium response to light and that this response was restored by I2-specific expression of gur-3."
Reference	"WBPaper00046411"


Anatomy_function : "WBbtf0939"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001897"
Gene	"WBGene00006434"
Involved	"WBbt:0003645"	Sufficient
Remark	"ENTITY:WBbt:0003681(pharynx)|GO:0043050(pharyngeal pumping)|PATO:0000381(reduced frequency)|GO:0009416(response to light stimulus)|PATO:0001424(violet)"
Remark	"QUALITY:PATO:0000502(delayed) NOT"
Remark	"Genotype \"prdx-2(gk169); lin-15(n765); nEx2155[flp-15prom::prdx-2 cDNA, lin-15(+)]\""
Remark	"Published_as prdx-2"
Remark	"To test whether prdx-2 acts in the I2 neurons for the pumping response to light, we generated a transgenic strain that expresses prdx-2 cDNA specifically in the I2s (flp-15prom::prdx-2 cDNA). I2-specific expression of prdx-2 rescued the acute response defect of prdx-2 mutants, indicating that prdx-2 functions in I2 for the pumping response to light."
Reference	"WBPaper00046411"


Anatomy_function : "WBbtf0940"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001897"	Autonomous
Gene	"WBGene00006434"
Involved	"WBbt:0003645"	Sufficient
Remark	"ENTITY:WBbt:0003645(I2 neuron)|PATO:0001162(increased concentration)|CHEBI:29108(calcium(2+))||GO:0009416(response to light stimulus)|PATO:0001424(violet)"
Remark	"QUALITY:PATO:0000297(abolished) NOT"
Remark	"Published_as prdx-2"
Remark	"We found that prdx-2 mutants completely lacked the I2 calcium response to light and that this response was restored by I2-specific expression of prdx-2."
Reference	"WBPaper00046411"


Anatomy_function : "WBbtf0941"
Assay	"Optogenetic"
Phenotype	"WBPhenotype:0000436"
Involved	"WBbt:0005662"	Sufficient
Remark	"ENTITY:WBbt:0006796(germ cell)|WP:CE22380(HSF-1)|GO:0051179(localization)|GO:0005634(nucleus)|PATO:0001629(aggregate)"
Remark	"QUALITY:PATO:0000470(present in greater numbers in organism)"
Remark	"Light stimulation of the AFD thermosensory neurons (carrying AFD::ChR2) resulted in the formation of HSF1::GFP puncta (in gonadal nuclei) in 78.4% of the experimental animals grown on ATR."
Reference	"WBPaper00046292"


Anatomy_function : "WBbtf0942"
Assay	"Optogenetic"
Phenotype	"WBPhenotype:0001006"
Involved	"WBbt:0005662"	Sufficient
Remark	"ENTITY:WBbt:0003681(pharynx)|GO:0043050(pharyngeal pumping)|PATO:0000161(rate)"
Remark	"QUALITY:PATO:0000380(increased frequency)"
Remark	"Optogenetic excitation of the AFD thermosensory neurons caused an increase in pharyngeal pumping within the first minute of light exposure."
Reference	"WBPaper00046292"


Anatomy_function : "WBbtf0943"
Assay	"Optogenetic"
Phenotype	"WBPhenotype:0000436"
Involved	"WBbt:0005662"	Sufficient
Remark	"ENTITY:WBbt:0006796(germ cell)|WP:CE22380(HSF-1)|GO:0051179(localization)|GO:0005634(nucleus)|PATO:0001629(aggregate)"
Remark	"QUALITY:PATO:0000470(present in greater numbers in organism)"
Remark	"Light stimulation of the AFD thermosensory neurons (carrying AFD::ChR2) resulted in the formation of HSF1::GFP puncta (in gonadal nuclei) in 78.4% of the experimental animals grown on ATR."
Reference	"WBPaper00046292"


Anatomy_function : "WBbtf0944"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000991"
Involved	"WBbt:0003666"	Necessary
Involved	"WBbt:0005660"	Necessary
Remark	"ENTITY:WBbt:0005739(head)|GO:0005576(extracellular region)|CHEBI:28790(serotonin)|GO:0001820(serotonin secretion)|GO:0034605(cellular response to heat)"
Remark	"QUALITY:PATO:0000470(present in greater numbers in organism) NOT"
Remark	"Genotype \"olaEx75 [Ptph-1::caspase-3(p12)::nz; Ptph-1::cz::caspase3(p17);Punc-122::mCherry]\""
Remark	"We then investigated which of the serotonergic neurons were responsible for the temperature-dependent serotonin release by genetically ablating specific serotonergic neurons. Genetic ablation of the NSM and ADF neurons only, achieved by directing the expression of a split caspase to these cells, resulted in the loss of serotonin relocalization following heat shock."
Reference	"WBPaper00046292"


Anatomy_function : "WBbtf0945"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0001273"
Involved	"WBbt:0003666"	Necessary
Involved	"WBbt:0005660"	Necessary
Remark	"Animals lacking serotonergic ADF and NSM neurons showed significant decreases in hsp70 mRNA accumulation upon heat shock compared to wild-type animals."
Remark	"ENTITY:WBbt:0007833(organism)|WBGene00002026(hsp-70)|GO:0010467(gene expression)|GO:0034605(cellular response to heat)"
Remark	"QUALITY:PATO:0000470(present in greater numbers in organism) NOT"
Remark	"Genotype \"olaEx75 [Ptph-1::caspase-3(p12)::nz; Ptph-1::cz::caspase3(p17);Punc-122::mCherry]\""
Reference	"WBPaper00046292"


Anatomy_function : "WBbtf0946"
Assay	"Optogenetic"
Phenotype	"WBPhenotype:0000991"
Involved	"WBbt:0003666"	Sufficient
Involved	"WBbt:0005660"	Necessary
Remark	"ENTITY:WBbt:0005739(head)|GO:0005576(extracellular region)|CHEBI:28790(serotonin)|GO:0001820(serotonin secretion)|GO:0034605(cellular response to heat)"
Remark	"QUALITY:PATO:0000470(present in greater numbers in organism) NOT"
Remark	"Genotype \"lite-1(ce314) X; ljIs102\""
Remark	"We used optogenetics to stimulate only the NSM and ADF neurons while maintaining animals at 20C. It was done by locally illuminating the NSM and ADF neurons in a previously characterized transgenic strain lite-1(ce314) X; ljIs102, which expresses ChR2 only in these neurons. We confirmed that the optogenetic activation of these serotonergic neurons caused the relocalization of serotonin into areas outside serotonergic neuronal cell bodies, as observed upon heat shock."
Reference	"WBPaper00046292"


Anatomy_function : "WBbtf0947"
Assay	"Optogenetic"
Phenotype	"WBPhenotype:0004023"
Involved	"WBbt:0003666"	Sufficient
Involved	"WBbt:0005660"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0031987(locomotion involved in locomotory behavior)"
Remark	"QUALITY:PATO:0001997(present in fewer numbers in organism)"
Remark	"Genotype \"lite-1(ce314) X; ljIs102\""
Remark	"We used optogenetics to stimulate only the NSM and ADF neurons while maintaining animals at 20C. It was done by locally illuminating the NSM and ADF neurons in a previously characterized transgenic strain lite-1(ce314) X; ljIs102, which expresses ChR2 only in these neurons. We also confirmed that, as previously reported, optogenetic excitation of serotonergic neurons decreased locomotory rates (number of body bends) and increased pharyngeal pumping rates."
Reference	"WBPaper00046292"


Anatomy_function : "WBbtf0948"
Assay	"Optogenetic"
Phenotype	"WBPhenotype:0001006"
Involved	"WBbt:0003666"	Sufficient
Involved	"WBbt:0005660"	Sufficient
Remark	"ENTITY:WBbt:0003681(pharynx)|GO:0006936(muscle contraction)|GO:0043050(pharyngeal pumping)"
Remark	"QUALITY:PATO:0000912(increased rate)"
Remark	"Genotype \"lite-1(ce314) X; ljIs102\""
Remark	"We used optogenetics to stimulate only the NSM and ADF neurons while maintaining animals at 20C. It was done by locally illuminating the NSM and ADF neurons in a previously characterized transgenic strain lite-1(ce314) X; ljIs102, which expresses ChR2 only in these neurons. We also confirmed that, as previously reported, optogenetic excitation of serotonergic neurons decreased locomotory rates (number of body bends) and increased pharyngeal pumping rates."
Reference	"WBPaper00046292"


Anatomy_function : "WBbtf0949"
Assay	"Optogenetic"
Phenotype	"WBPhenotype:0000436"
Involved	"WBbt:0003666"	Sufficient
Involved	"WBbt:0005660"	Sufficient
Remark	"ENTITY:WBbt:0006796(germ cell)|WP:CE22380(HSF-1)|GO:0051179(localization)|GO:0005634(nucleus)|PATO:0001629(aggregate)"
Remark	"QUALITY:PATO:0000470(present in greater numbers in organism)"
Remark	"Genotype \"lite-1(ce314) X; ljIs102\""
Remark	"Optogenetic activation of the ADF and NSM neurons caused 64% (n = 44) of the experimental animals grown on ATR to exhibit relocalization of HSF1::GFP into nuclear stress granules within 10-20 min post light activation."
Reference	"WBPaper00046292"


Anatomy_function : "WBbtf0950"
Assay	"Optogenetic"
Phenotype	"WBPhenotype:0000436"
Involved	"WBbt:0003666"	Sufficient
Remark	"ENTITY:WBbt:0006796(germ cell)|WP:CE22380(HSF-1)|GO:0051179(localization)|GO:0005634(nucleus)|PATO:0001629(aggregate)"
Remark	"QUALITY:PATO:0000470(present in greater numbers in organism)"
Remark	"Genotype \"lite-1(ce314) X; ljIs102\""
Remark	"Optogenetic stimulation of either the ADF or the NSM neurons was effective in activating HSF1, although the ADF neurons appeared more effective (75% versus 33.3%)."
Reference	"WBPaper00046292"


Anatomy_function : "WBbtf0951"
Assay	"Optogenetic"
Phenotype	"WBPhenotype:0000436"
Involved	"WBbt:0005660"	Sufficient
Remark	"ENTITY:WBbt:0006796(germ cell)|WP:CE22380(HSF-1)|GO:0051179(localization)|GO:0005634(nucleus)|PATO:0001629(aggregate)"
Remark	"QUALITY:PATO:0000470(present in greater numbers in organism)"
Remark	"Genotype \"lite-1(ce314) X; ljIs102\""
Remark	"Optogenetic stimulation of either the ADF or the NSM neurons was effective in activating HSF1, although the ADF neurons appeared more effective (75% versus 33.3%)."
Reference	"WBPaper00046292"


Anatomy_function : "WBbtf0952"
Assay	"Optogenetic"
Phenotype	"WBPhenotype:0001273"
Involved	"WBbt:0003666"	Sufficient
Involved	"WBbt:0005660"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|WBGene00002026(hsp-70)|GO:0010467(gene expression)"
Remark	"QUALITY:PATO:0000470(present in greater numbers in organism)"
Remark	"Genotype \"lite-1(ce314) X; ljIs102\""
Remark	"Stimulation of the ADF and NSM neurons resulted in a 5- to 8-fold induction of hsp70 mRNA."
Reference	"WBPaper00046292"


Anatomy_function : "WBbtf0953"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000750"
Gene	"WBGene00020490"
Involved	"WBbt:0003675"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|WBls:0000023(larva Ce)|GO:0021700(developmental maturation)|BTO:0001091(axenic)|CHEBI:33290(food)"
Remark	"QUALITY:PATO:0000912(increased rate) NOT"
Remark	"Genotype \"tmc-1(ok1859); Ex[Plev-11:tmc-1]\""
Remark	"Published_as tmc-1"
Remark	"To localize further the tmc-1 cell-specific function, we introduced tmc-1 cDNA with with Punc-17(3.7k), Punc-17(10k) and Plev-11(3.5k) promoters into the tmc-1(ok1859) mutant. Strains expressing either the unc-17 or the lev-11 promoter constructs suppressed the tmc-1 phenotype (faster larval development on Ce maintenance medium), although the muscle-expressing transgene was less effective."
Reference	"WBPaper00046467"


Anatomy_function : "WBbtf0954"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000750"
Gene	"WBGene00020490"
Involved	"WBbt:0006840"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|WBls:0000023(larva Ce)|GO:0021700(developmental maturation)|BTO:0001091(axenic)|CHEBI:33290(food)"
Remark	"QUALITY:PATO:0000912(increased rate) NOT"
Remark	"Genotype \"tmc-1(ok1859); Ex[Punc-17:tmc-1]\""
Remark	"Published_as tmc-1"
Remark	"To localize further the tmc-1 cell-specific function, we introduced tmc-1 cDNA with with Punc-17(3.7k), Punc-17(10k) and Plev-11(3.5k) promoters into the tmc-1(ok1859) mutant. Strains expressing either the unc-17 or the lev-11 promoter constructs suppressed the tmc-1 phenotype (faster larval development on Ce maintenance medium), although the muscle-expressing transgene was less effective. We found that expression from either Punc-17(3.7k) or Punc-17(10k) promoters partially suppress the tmc-1(ok1859) phenotype."
Reference	"WBPaper00046467"


Anatomy_function : "WBbtf0955"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000750"
Involved	"WBbt:0003638"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|WBls:0000023(larva Ce)|GO:0021700(developmental maturation)|BTO:0001091(axenic)|CHEBI:33290(food)"
Remark	"QUALITY:PATO:0000912(increased rate) NOT"
Remark	"To assess if the tmc-1-expressing MC neurons attenuated growth on CeMM, we laser ablated these bilateral cells in wild-type L1 larvae. CeMM-fed operated animals (27%) developed into adults by 5 d.p.h. and most developed into adults by 8 d.p.h. Thus, removal of both wild-type MC neurons mimics the mutant's phenotype, suggesting they attenuate growth in the axenic media."
Reference	"WBPaper00046467"


Anatomy_function : "WBbtf0956"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000750"
Gene	"WBGene00020490"
Not_involved	"WBbt:0005661"	Insufficient
Not_involved	"WBbt:0005660"	Insufficient
Not_involved	"WBbt:0005670"	Insufficient
Not_involved	"WBbt:0005665"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|WBls:0000023(larva Ce)|GO:0021700(developmental maturation)|BTO:0001091(axenic)|CHEBI:33290(food)"
Remark	"QUALITY:PATO:0000912(increased rate)"
Remark	"Genotype \"tmc-1(ok1859); Ex[Pocr-2::tmc-1]\""
Remark	"However, the  transgenic  expression  of  TMC-1  in  the  chemosensory neurons ADL, ADF, AWA and ASH, using the ocr-2 promoter, did not restore a wild-type developmental rate to the tmc-1 mutant."
Remark	"Published_as tmc-1"
Reference	"WBPaper00046467"


Anatomy_function : "WBbtf0957"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000750"
Not_involved	"WBbt:0005661"	Unnecessary
Not_involved	"WBbt:0005660"	Unnecessary
Not_involved	"WBbt:0005670"	Unnecessary
Not_involved	"WBbt:0005665"	Unnecessary
Remark	"ENTITY:WBbt:0007833(organism)|WBls:0000023(larva Ce)|GO:0021700(developmental maturation)|BTO:0001091(axenic)|CHEBI:33290(food)"
Remark	"QUALITY:PATO:0000912(increased rate) NOT"
Remark	"Genotype \"Ex[Pocr-2::unc-103(gf)]\""
Remark	"To test the contributions of these neurons in an alternative way, we hyperpolarized the above sensory neurons in wild-type animals, using a gain-of-function mutant unc-103 voltage-gated K+ channel expressed from the ocr-2 promoter. But unlike crippling the MC neurons, we did not detect accelerated development on CeMM of the unc-103(gf) transgenic line."
Reference	"WBPaper00046467"


Anatomy_function : "WBbtf0958"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001524"
Gene	"WBGene00003760"
Involved	"WBbt:0006833"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|WBls:0000023(larva Ce)|GO:0030431(sleep)"
Remark	"QUALITY:PATO:0001997(decreased amount)"
Remark	"Genotype \"sid-1(pk3321)V qnIs157[glr-3:nlp-22(RNAi);myo-2:mCherry;unc-119(+)]\""
Remark	"Published_as nlp-22"
Remark	"To test for the functional relevance of the observed RIA gene reporter expression, we expressed nlp-22 double-stranded RNA (dsRNA) to knockdown nlp-22 mRNA specifically in RIA, and, as a control, in the hypodermis. Expression in the RIA neurons but not in the hypodermis reduced lethargus quiescence."
Reference	"WBPaper00044546"


Anatomy_function : "WBbtf0959"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001524"
Gene	"WBGene00003760"
Not_involved	"WBbt:0007846"	Unnecessary
Remark	"ENTITY:WBbt:0007833(organism)|WBls:0000023(larva Ce)|GO:0030431(sleep)"
Remark	"QUALITY:PATO:0001997(decreased amount) NOT"
Remark	"Genotype \"sid-1(pk3321)V qnIs137[dpy-7:nlp-22(RNAi);myo-2:mCherry;unc-119(+)]\""
Remark	"Published_as nlp-22"
Remark	"To test for the functional relevance of the observed RIA gene reporter expression, we expressed nlp-22 double-stranded RNA (dsRNA) to knockdown nlp-22 mRNA specifically in RIA, and, as a control, in the hypodermis. Expression in the RIA neurons but not in the hypodermis reduced lethargus quiescence."
Reference	"WBPaper00044546"


Anatomy_function : "WBbtf0960"
Assay	"Optogenetic"
Phenotype	"WBPhenotype:0001524"
Involved	"WBbt:0006833"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|WBls:0000023(larva Ce)|GO:0030431(sleep)"
Remark	"QUALITY:PATO:0001997(decreased amount)"
Remark	"We made transgenic animals expressing the blue light-activated cation channel channelrhosopsin-2 (ChR2) in the RIA neurons. We optogenetically depolarized the RIA neurons during the active L4 stage as well as during L4 lethargus. Stimulating the RIA neurons during the active L4 stage caused no induction in behavioural quiescence. In contrast, optogenetic depolarization of the RIA neurons during L4 lethargus had a locomotion-stimulating effect."
Reference	"WBPaper00044546"


Anatomy_function : "WBbtf0961"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0001524"
Involved	"WBbt:0006833"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|WBls:0000023(larva Ce)|GO:0030431(sleep)"
Remark	"QUALITY:PATO:0001997(decreased amount)"
Remark	"Genotype \"lin-15(n765ts)X; akEx211[Pglr-3:gfp;Pglr-3:ICE;lin-15(+)]\""
Remark	"We used the strain VM1345, which expresses the cell death gene ICE in the RIA neurons. There was a significant reduction in lethargus quiescence in animals lacking both RIA neurons.  Animals lacking only one of the RIA neurons also showed a small but significant reduction in L4 lethargus quiescence compared with control transgenic animals."
Reference	"WBPaper00044546"


Anatomy_function : "WBbtf0962"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001801"
Gene	"WBGene00003397"
Involved	"WBbt:0005237"	Sufficient
Remark	"A transgene containing a mom-5 cDNA driven from the mec-3 promoter that expresses MOM-5 in mechanosensory neurons partially rescued the ALM defects of the cwn-1; mom-5(gm409) double mutant, indicating that MOM-5 acts in the neurons."
Remark	"ENTITY:WBbt:0005406(ALM)|GO:0033564(anterior/posterior axon guidance)"
Remark	"QUALITY:PATO:0001507(disrupted) NOT"
Remark	"Genotype \"mom-5(gm409); cwn-1(ok456); Ex[Pmec-3::mom-5]\""
Remark	"Published_as mom-5"


Anatomy_function : "WBbtf0963"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001801"	Autonomous
Gene	"WBGene00000289"
Involved	"WBbt:0005406"	Sufficient
Remark	"ENTITY:WBbt:0005406(ALM)|GO:0033564(anterior/posterior axon guidance)"
Remark	"QUALITY:PATO:0001507(disrupted) NOT"
Remark	"Genotype \"cam-1(gm122);Ex[Punc-18::cam-1]\""
Remark	"Published_as cam-1"
Remark	"To test whether CAM functions in the ALM, we expressed a cam-1 cDNA under the control of the unc-86 promoter, which is expressed in many neurons including the ALMs, but not in non-neuronal cells.  This transgene partially rescued the ALM defects in both cam-1 single and cwn-1 cam-1 double mutants, suggesting that CAM-1 can act in the ALM to regulate its polarity."


Anatomy_function : "WBbtf0964"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001801"	Autonomous
Gene	"WBGene00000289"
Involved	"WBbt:0005406"	Sufficient
Remark	"ENTITY:WBbt:0005406(ALM)|GO:0033564(anterior/posterior axon guidance)"
Remark	"QUALITY:PATO:0001507(disrupted) NOT"
Remark	"Genotype \"cam-1(gm122);ncl-1(e1865);gmEx188[Pcam-1::cam-1; ncl-1(+); pRF4[rol-6(su1006)]]\""
Remark	"Published_as cam-1"
Remark	"To further test the autonomous role for CAM-1 in ALM polarity, we generated animals that were mosaic for cam-1 function. We started with a strain that was mutant for cam-1 and ncl-1. The strain also bore an extra-chromosomal transgenic array that contained the wild-type cam-1 and ncl-1 genes as well as a dominant allele of the rol-6 gene that causes animals to roll. Approximately 45% of the Ncl ALMs displayed a polarity defect, but none of the 459 ALMs with wild-type nucleoli displayed a polarity defect.  These observations strongly support the hypothesis that cam-1 acts in the ALM to promote normal polarity"


Anatomy_function : "WBbtf0965"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001801"	Nonautonomous
Gene	"WBGene00000289"
Involved	"WBbt:0007810"	Sufficient
Remark	"ENTITY:WBbt:0005406(ALM)|GO:0033564(anterior/posterior axon guidance)"
Remark	"QUALITY:PATO:0001507(disrupted)"
Remark	"Genotype \"cam-1(gm122);Ex[Pmyo-3::cam-1]\""
Remark	"One interesting finding from this experiment is that the mosaic animals with Ncl ALMs have a higher frequency of reversed ALMs than cam-1; ncl-1 mutants that do not carry the transgenic array, which we interpret as an enhancement of the ALM defect. One explanation for this effect is that CAM-1 has antagonistic activities in ALM polarity: an autonomous function as a Wnt receptor that promotes normal polarity, and a nonautonomous function that antagonizes Wnt function. To test this hypothesis further, we expressed CAM-1 from the myo-3 promoter in muscle cells. This expression resulted in a strong ALM polarity defect in a cam-1 mutant background, consistent with our hypothesis that CAM-1 has antagonistic functions."
Remark	"Published_as cam-1"


Anatomy_function : "WBbtf0966"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000039"
Involved	"WBbt:0005666"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0008340(determination of adult lifespan)|PATO:0001152(susceptible toward)|CHEBI:28201(rotenone)"
Remark	"QUALITY:PATO:0001550(decreased sensitivity)"
Remark	"To further elucidate which neuronal subsets may be involved into mtROS-mediated lifespan extension we laser-ablated selectively ASI neurons in wild-type nematodes. Notably, rotenone did not extend lifespan in the absence of ASI neurons."
Reference	"WBPaper00044426"


Anatomy_function : "WBbtf0967"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000039"
Gene	"WBGene00004804"
Involved	"WBbt:0005666"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0008340(determination of adult lifespan)|PATO:0001152(susceptible toward)|CHEBI:28201(rotenone)"
Remark	"QUALITY:PATO:0001550(decreased sensitivity) NOT"
Remark	"Genotype \"skn-1(zu67)\""
Remark	"Published_as skn-1"
Remark	"To further support this hypothesis we analyzed worms that were deficient for only two of the three SKN-1 isoforms, named skn-1(zu67). Notably, the neuronal SKN-1 isoform is functional in these worms. Consistent with neuronal ROS signaling both rotenone as well as piericidin A extended lifespan in this isoform-specific mutant."
Reference	"WBPaper00044426"


Anatomy_function : "WBbtf0968"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000039"
Gene	"WBGene00004804"
Involved	"WBbt:0005666"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0008340(determination of adult lifespan)|PATO:0001152(susceptible toward)|(piericidin A)"
Remark	"QUALITY:PATO:0001550(decreased sensitivity) NOT"
Remark	"Genotype \"skn-1(zu67)\""
Remark	"Published_as skn-1"
Remark	"To further support this hypothesis we analyzed worms that were deficient for only two of the three SKN-1 isoforms, named skn-1(zu67). Notably, the neuronal SKN-1 isoform is functional in these worms. Consistent with neuronal ROS signaling both rotenone as well as piericidin A extended lifespan in this isoform-specific mutant."
Reference	"WBPaper00044426"


Anatomy_function : "WBbtf0969"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0002154"
Not_involved	"WBbt:0005784"	Unnecessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0005844(polysome)|(profile)"
Remark	"QUALITY:PATO:0000460(abnormal) NOT"
Remark	"Polyribosome profiling experiments were performed in germline-ablated nematodes. To this end, daf-2(e1370) and N2 nematodes were fed siRNA against GLP-1, a germline-specific GLP-/Notch receptor. Interestingly, polyribosome profiles of N2 nematodes did not markedly differ upon abrogation of GLP-1."
Reference	"WBPaper00042552"


Anatomy_function : "WBbtf0970"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0002171"
Involved	"WBbt:0003904"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0010446(response to alkaline pH)|GO:0006935(chemotaxis)"
Remark	"QUALITY:PATO:0002303(decreased object quality)"
Remark	"We examined which sensory neuron serves as a sensor for alkaline pH by analyzing wild-type animals whose ASEL and/or ASER had been ablated by laser microsurgery. Animals lacking ASEL distributed almost equally to both higher and lower pH regions, whereas animals lacking ASER moved toward higher pH just as intact wild-type animals do."
Reference	"WBPaper00042397"


Anatomy_function : "WBbtf0971"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0002171"
Not_involved	"WBbt:0003903"	Unnecessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0010446(response to alkaline pH)|GO:0006935(chemotaxis)"
Remark	"QUALITY:PATO:0002303(decreased object quality) NOT"
Remark	"We examined which sensory neuron serves as a sensor for alkaline pH by analyzing wild-type animals whose ASEL and/or ASER had been ablated by laser microsurgery. Animals lacking ASEL distributed almost equally to both higher and lower pH regions, whereas animals lacking ASER moved toward higher pH just as intact wild-type animals do."
Reference	"WBPaper00042397"


Anatomy_function : "WBbtf0972"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0002171"
Gene	"WBGene00001119"
Involved	"WBbt:0003904"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0010446(response to alkaline pH)|GO:0006935(chemotaxis)"
Remark	"QUALITY:PATO:0002303(decreased object quality) NOT"
Remark	"Furthermore, the chemotactic defect of dyf-3 mutants was reversed by specific expression of the wild-type dyf-3 gene in ASEL, whereas specific expression of dyf-3 in ASER did not."
Remark	"Genotype \"dyf-3(m185); ixEx91[pgcy-7p::dyf-3cDNA; pmyo-3p::venus]\""
Remark	"Published_as dyf-3"
Reference	"WBPaper00042397"


Anatomy_function : "WBbtf0973"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0002171"
Gene	"WBGene00001119"
Not_involved	"WBbt:0003903"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0010446(response to alkaline pH)|GO:0006935(chemotaxis)"
Remark	"QUALITY:PATO:0002303(decreased object quality)"
Remark	"Furthermore, the chemotactic defect of dyf-3 mutants was reversed by specific expression of the wild-type dyf-3 gene in ASEL, whereas specific expression of dyf-3 in ASER did not."
Remark	"Genotype \"dyf-3(m185); ixEx91[pgcy-5p::dyf-3cDNA; pmyo-3p::venus]\""
Remark	"Published_as dyf-3"
Reference	"WBPaper00042397"


Anatomy_function : "WBbtf0974"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0002171"
Gene	"WBGene00006526"
Involved	"WBbt:0003904"	Sufficient
Remark	"ASEL-specific expression of TAX-4 in tax-4 mutants completely reversed the alkaline pH chemotaxis defect."
Remark	"ENTITY:WBbt:0007833(organism)|GO:0010446(response to alkaline pH)|GO:0006935(chemotaxis)"
Remark	"QUALITY:PATO:0002303(decreased object quality) NOT"
Remark	"Genotype \"tax-4(p678); ixEx183[pgcy-7p::tax-4gDNA; pmyo-3p::venus]\""
Remark	"Published_as tax-4"
Reference	"WBPaper00042397"


Anatomy_function : "WBbtf0975"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0002171"
Gene	"WBGene00006526"
Not_involved	"WBbt:0003903"	Insufficient
Remark	"ASEL-specific (but not ASER-specific) expression of TAX-4 in tax-4 mutants completely reversed the alkaline pH chemotaxis defect."
Remark	"ENTITY:WBbt:0007833(organism)|GO:0010446(response to alkaline pH)|GO:0006935(chemotaxis)"
Remark	"QUALITY:PATO:0002303(decreased object quality)"
Remark	"Genotype \"tax-4(p678); ixEx183[pgcy-5p::tax-4gDNA; pmyo-3p::venus]\""
Remark	"Published_as tax-4"
Reference	"WBPaper00042397"


Anatomy_function : "WBbtf0976"
Assay	"Optogenetic"
Phenotype	"WBPhenotype:0002171"	Autonomous
Involved	"WBbt:0003904"	Sufficient
Remark	"ENTITY:WBbt:0003904(ASEL)|GO:0071469(cellular response to alkaline pH)|GO:0070588(calcium ion transmembrane transport)"
Remark	"QUALITY:PATO:0002305(increased object quality)"
Remark	"To analyze alkaline pH sensitivity of ASE neurons in living animals, we carried out in vivo Ca2+ imaging by specifically expressing GCaMP3, a genetically encoded Ca2+ indicator in ASE. ASEL was activated by elevation of pH and was slightly inactivated by lowering of pH. When the pH was elevated from 6.8 to 10.0, ASEL of both unc-13 and snb-1 mutants was activated to levels similar to those observed in wild-type animals. These results demonstrate that ASEL functions as the primary, direct sensor of environmental alkalinity in C. elegans."
Reference	"WBPaper00042397"


Anatomy_function : "WBbtf0977"
Assay	"Optogenetic"
Phenotype	"WBPhenotype:0002171"	Nonautonomous
Not_involved	"WBbt:0003903"
Remark	"ENTITY:WBbt:0003903(ASER)|GO:0071469(cellular response to alkaline pH)|GO:0070588(calcium ion transmembrane transport)"
Remark	"QUALITY:PATO:0002305(increased object quality)"
Reference	"WBPaper00042397"


Anatomy_function : "WBbtf0978"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0004006"
Involved	"WBbt:0004062"	Necessary
Remark	"ENTITY:WBbt:0007850(male)|GO:0034606(response to hermaphrodite contact)|GO:0043057(backward locomotion)|"
Remark	"QUALITY:PATO:0002052(decreased occurrence)"
Remark	"In males where only PVY was ablated, contact response efficiency and scanning speed were significantly reduced compared to control males."
Reference	"WBPaper00042229"


Anatomy_function : "WBbtf0979"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0004006"
Involved	"WBbt:0004062"	Necessary
Remark	"ENTITY:WBbt:0007850(male)|GO:0034606(response to hermaphrodite contact)|GO:0043057(backward locomotion)|PATO:0000008(speed)"
Remark	"QUALITY:PATO:0002302(decreased process quality)"
Remark	"In males where only PVY was ablated, contact response efficiency and scanning speed were significantly reduced compared to control males."
Reference	"WBPaper00042229"


Anatomy_function : "WBbtf0980"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0004006"
Involved	"WBbt:0005842"	Necessary
Remark	"ENTITY:WBbt:0007850(male)|GO:0034606(response to hermaphrodite contact)|GO:0043057(backward locomotion)|PATO:0000008(speed)"
Remark	"QUALITY:PATO:0002302(decreased process quality)"
Remark	"When scanning was initiated successfully, the scanning speed of AVA-ablated males was significantly slower than that of control males."
Reference	"WBPaper00042229"


Anatomy_function : "WBbtf0981"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0004006"
Involved	"WBbt:0005842"	Necessary
Remark	"AVA-ablated males lost tail contact during scanning at a significantly higher rate than controls, possibly because the uncoordinated phenotype resulting from AVA ablation interferes with tail apposition."
Remark	"ENTITY:WBbt:0007850(male)|GO:0034606(response to hermaphrodite contact)|GO:0043057(backward locomotion)|WBbt:0005741(tail)|PATO:0001961(in contact with)|WBbt:0007849(hermaphrodite)"
Remark	"QUALITY:PATO:0002302(decreased process quality)"
Reference	"WBPaper00042229"


Anatomy_function : "WBbtf0982"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0004006"
Involved	"WBbt:0004062"	Necessary
Remark	"ENTITY:WBbt:0007850(male)|GO:0034606(response to hermaphrodite contact)|GO:0043057(backward locomotion)|WBbt:0005741(tail)|PATO:0001961(in contact with)|WBbt:0007849(hermaphrodite)"
Remark	"QUALITY:PATO:0002302(decreased process quality)"
Remark	"PVY-ablated males also lost tail contact at a significantly higher frequency than control males during the search."
Reference	"WBPaper00042229"


Anatomy_function : "WBbtf0983"
Assay	"Optogenetic"
Phenotype	"WBPhenotype:0001702"
Involved	"WBbt:0004063"	Sufficient
Involved	"WBbt:0004062"	Sufficient
Remark	"ENTITY:WBbt:0007850(male)|GO:0043057(backward locomotion)"
Remark	"QUALITY:PATO:0002051(increased occurrence)"
Remark	"Genotype \"lite-1(ce314); Ex[Pnlp-14(PVY+PVX)::ChR2-YFP+Punc-122::GFP]\""
Remark	"When exposed to the light flash, 90% of Pnlp-14::ChR2-YFP males immediately reversed and traveled a median distance of -5 micrometer, with the negative value indicating that they reversed away from their position at the time of the flash. Through a series of control experiments we determined that this reversal response was specifically due to activation of male-specific interneurons PVY and PVX."
Reference	"WBPaper00042229"


Anatomy_function : "WBbtf0984"
Assay	"Optogenetic"
Phenotype	"WBPhenotype:0001702"
Involved	"WBbt:0004063"	Necessary
Involved	"WBbt:0004062"	Necessary
Remark	"ENTITY:WBbt:0007850(male)|GO:0034606(response to hermaphrodite contact)|GO:0043057(backward locomotion)"
Remark	"QUALITY:PATO:0000499(decreased duration)"
Remark	"Genotype \"lite-1(ce314); Ex[Pnlp-14(PVY+PVX)::NpHR-EYFP+pha-1(+)]\""
Remark	"We activated NpHR during scanning by exposing the male to a 500 msec flash of yellow light (540/25 nm wavelength) at 5, evenly spaced, time intervals and counted the number of times pausing coincided with a pulse. Pnlp-14::NpHR-EYFP males, grown in the presence of ATR, paused in response to 4 out of 5 flashes, on average."
Reference	"WBPaper00042229"


Anatomy_function : "WBbtf0985"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001702"
Involved	"WBbt:0005842"	Necessary
Remark	"ENTITY:WBbt:0007850(male)|WBbt:0004063(PVX)|WBbt:0004062(PYV)|GO:0051899(membrane depolarization)|GO:0043057(backward locomotion)"
Remark	"QUALITY:PATO:0002052(decreased occurrence)"
Remark	"Genotype \"lite-1(ce314); Ex[Pnlp-14(PVY+PVX)::ChR2-YFP+Punc-122::GFP]\""
Remark	"When exposed to a 500 msec flash of blue light, Pnlp-14::ChR2-YFP AVA-ablated males were severely impaired in reversal behavior with a significant proportion either pausing, unable to reverse (25%), or reversing a median distance of ~1 micrometer (56%). Thus, PVY+PVX-induced reversal is dependent on AVA function."
Reference	"WBPaper00042229"


Anatomy_function : "WBbtf0986"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001702"
Gene	"WBGene00000057"
Involved	"WBbt:0005842"	Sufficient
Involved	"WBbt:0006818"	Sufficient
Involved	"WBbt:0006819"	Sufficient
Involved	"WBbt:0003850"	Sufficient
Involved	"WBbt:0005835"	Sufficient
Involved	"WBbt:0005840"	Sufficient
Remark	"ENTITY:WBbt:0007850(male)|WBbt:0004063(PVX)|WBbt:0004062(PYV)|GO:0051899(membrane depolarization)|GO:0043057(backward locomotion)"
Remark	"QUALITY:PATO:0002052(decreased occurrence) NOT"
Remark	"Published_as acr-18"
Remark	"We placed a promoterless fragment of the wild type acr-18 gene (a cDNA::genomic hybrid gene and its 39 UTR) under the control of the nmr-1 gene promoter, which is expressed in backward command cells AVA, AVD, AVE and in AVG, RIM and PVC. We observed that the presence of the acr-18(+) transgene in the nmr-1-expressing cells was sufficient to rescue the acr-18 mutant defect."
Remark	"We placed a promoterless fragment of the wild type acr-18 gene (a cDNA::genomic hybrid gene and its 39 UTR) under the control of the nmr-1 gene promoter, which is expressed in backward command cells AVA, AVD, AVE and in AVG, RIM and PVC. We observed that the presence of the acr-18(+) transgene in the nmr-1-expressing cells was sufficient to rescue the acr-18 mutant defect."
Reference	"WBPaper00042229"


Anatomy_function : "WBbtf0987"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001702"
Gene	"WBGene00006765"
Involved	"WBbt:0005842"	Sufficient
Involved	"WBbt:0006818"	Sufficient
Involved	"WBbt:0006819"	Sufficient
Involved	"WBbt:0003850"	Sufficient
Involved	"WBbt:0005835"	Sufficient
Involved	"WBbt:0005840"	Sufficient
Remark	"ENTITY:WBbt:0007850(male)|WBbt:0004063(PVX)|WBbt:0004062(PYV)|GO:0051899(membrane depolarization)|GO:0043057(backward locomotion)"
Remark	"QUALITY:PATO:0002052(decreased occurrence) NOT"
Remark	"Published_as unc-29"
Remark	"To test whether the absence of unc-29 function from AVA might be responsible for the reversal defect of unc-29; acr-16 males, we performed tissue-specific rescue experiments, targeting expression of unc-29(+) to AVA. This was achieved using an unc-29(+)::SL2::GFP transgene placed under the control of the Pnmr-1 promoter. In ChR2-mediated PVY+PVX activation assays, unc-29; acr-16 males expressing unc-29(+) in AVA (indicated by GFP expression in AVA) were rescued, reversing at frequencies comparable to acr-16 single mutants and wild type males (83%)."
Remark	"To test whether the absence of unc-29 function from AVA might be responsible for the reversal defect of unc-29; acr-16 males, we performed tissue-specific rescue experiments, targeting expression of unc-29(+) to AVA. This was achieved using an unc-29(+)::SL2::GFP transgene placed under the control of the Pnmr-1 promoter. In ChR2-mediated PVY+PVX activation assays, unc-29; acr-16 males expressing unc-29(+) in AVA (indicated by GFP expression in AVA) were rescued, reversing at frequencies comparable to acr-16 single mutants and wild type males (83%)."
Reference	"WBPaper00042229"


Anatomy_function : "WBbtf0988"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000644"
Gene	"WBGene00004777"
Involved	"WBbt:0005190"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0040011(locomotion)|PATO:0000763(paralysed)|GO:0042221(response to chemical)|CHEBI:15760(tyramine)"
Remark	"QUALITY:PATO:0002302(decreased process quality) NOT"
Remark	"Genotype \"[Punc-47::SER-2, lin-15(+)]; ser-2(pk1357) lin-15(n765ts)\""
Remark	"Published_as ser-2"
Remark	"SER-2 is specifically expressed in the GABAergic VD motor neurons. No other promoters have been described that specifically drive expression in the GABAergic VD neurons. We therefore expressed ser-2 cDNA in all GABAergic neurons using the unc-47 promoter (Punc-47::SER-2). ser-2 expression in GABAergic neurons of ser-2 mutants restored normal sensitivity to exogenous tyramine."
Reference	"WBPaper00042221"


Anatomy_function : "WBbtf0989"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000644"
Gene	"WBGene00001648"
Involved	"WBbt:0005190"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0040011(locomotion)|PATO:0000763(paralysed)|GO:0042221(response to chemical)|CHEBI:15760(tyramine)"
Remark	"QUALITY:PATO:0002302(decreased process quality) NOT"
Remark	"Genotype \"[Punc-47::GOA-1::SL2::mCherry, unc-122::GFP]; goa-1(sa734)\""
Remark	"Published_as goa-1"
Remark	"goa-1 expression in GABAergic neurons (Punc-47::GOA-1) of goa-1 mutants largely restored sensitivity to exogenous tyramine."
Reference	"WBPaper00042221"


Anatomy_function : "WBbtf0990"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000644"
Gene	"WBGene00001145"
Involved	"WBbt:0005190"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0040011(locomotion)|PATO:0000763(paralysed)|GO:0042221(response to chemical)|CHEBI:15760(tyramine)"
Remark	"QUALITY:PATO:0002302(decreased process quality) NOT"
Remark	"Genotype \" [Punc-47::EAT-16::SL2::mCherry, unc-122::GFP]; eat-16(sa609)\""
Remark	"Published_as eat-16"
Remark	"Similarly, rescue expression of eat-16 in GABAergic neurons partly restores sensitivity to exogenous tyramine."
Reference	"WBPaper00042221"


Anatomy_function : "WBbtf0991"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001703"
Involved	"WBbt:0005303"	Necessary
Remark	"Animals in which only the VD neurons were ablated still propagated a sinusoidal wave along the anterior-posterior axis, but displayed deeper ventral than dorsal flexures. As a consequence VD ablated animals moved in ventrally directed circles."
Remark	"ENTITY:WBbt:0007833(organism)|GO:0040011(locomotion)|WBbt:0005740(midbody)|PATO:0002501(ventrally directed)|PATO:0000617(bent)"
Remark	"QUALITY:PATO:0002017(increased magnitude)"
Reference	"WBPaper00042221"


Anatomy_function : "WBbtf0992"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001703"
Involved	"WBbt:0005270"	Necessary
Remark	"Conversely, animals in which the DD neurons were ablated exhibited deeper dorsal than ventral flexures and moved in dorsally directed circles."
Remark	"ENTITY:WBbt:0007833(organism)|GO:0040011(locomotion)|WBbt:0005740(midbody)|PATO:0002495(dorsally directed)|PATO:0000617(bent)"
Remark	"QUALITY:PATO:0002017(increased magnitude)"
Reference	"WBPaper00042221"


Anatomy_function : "WBbtf0993"
Assay	"Optogenetic"
Phenotype	"WBPhenotype:0001703"
Involved	"WBbt:0005270"	Sufficient
Remark	"ENTITY:WBbt:0007833(organism)|GO:0040011(locomotion)|WBbt:0005740(midbody)|PATO:0002501(ventrally directed)|PATO:0000617(bent)"
Remark	"QUALITY:PATO:0002017(increased magnitude)"
Remark	"To test whether the differential activity of the VD and DD motor neurons can induce bending, we generated transgenic animals that co-expressed the light-activated cation channel Channelrhodopsin-2 (ChR2) and light-activated chloride pump Halorhodopsin (NpHR) in the six GABAergic DD motor neurons that synapse onto the dorsal muscles (Pflp-13::ChR2; Pflp-13::NpHR). ChR2 is activated by blue light and depolarizes neurons, while NpHR is activated by green light and hyperpolarizes neurons. We found that blue light activation induced a deep ventral turn."
Reference	"WBPaper00042221"


Anatomy_function : "WBbtf0994"
Assay	"Optogenetic"
Phenotype	"WBPhenotype:0001703"
Involved	"WBbt:0005270"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0040011(locomotion)|WBbt:0005740(midbody)|PATO:0002495(dorsally directed)|PATO:0000617(bent)"
Remark	"QUALITY:PATO:0002017(increased magnitude)"
Remark	"To test whether the differential activity of the VD and DD motor neurons can induce bending, we generated transgenic animals that co-expressed the light-activated cation channel Channelrhodopsin-2 (ChR2) and light-activated chloride pump Halorhodopsin (NpHR) in the six GABAergic DD motor neurons that synapse onto the dorsal muscles (Pflp-13::ChR2; Pflp-13::NpHR). ChR2 is activated by blue light and depolarizes neurons, while NpHR is activated by green light and hyperpolarizes neurons. We found that blue light activation induced a deep ventral turn. In contrast, green light inhibition induced a deep dorsal turn."
Reference	"WBPaper00042221"


Anatomy_function : "WBbtf0995"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000551"
Involved	"WBbt:0005270"	Necessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0040011(locomotion)|WBbt:0005740(midbody)|PATO:0002501(ventrally directed)|PATO:0000617(bent)"
Remark	"QUALITY:PATO:0002018(decreased magnitude)"
Remark	"In response to touch, animals in which the GABAergic DD neurons were ablated initiated omega turns with a deep ventral head bend, but often their head failed to touch the ventral side of the body to close the omega turn. Animals with ablated GABAergic VD neurons did not have a defect in the execution of closed omega turns."
Reference	"WBPaper00042221"


Anatomy_function : "WBbtf0996"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000551"
Not_involved	"WBbt:0005303"	Unnecessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0040011(locomotion)|WBbt:0005740(midbody)|PATO:0002501(ventrally directed)|PATO:0000617(bent)"
Remark	"QUALITY:PATO:0002018(decreased magnitude) NOT"
Remark	"In response to touch, animals in which the GABAergic DD neurons were ablated initiated omega turns with a deep ventral head bend, but often their head failed to touch the ventral side of the body to close the omega turn. Animals with ablated GABAergic VD neurons did not have a defect in the execution of closed omega turns."
Reference	"WBPaper00042221"


Anatomy_function : "WBbtf0997"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000399"
Not_involved	"WBbt:0004574"	Unnecessary
Remark	"ENTITY:WBbt:0004577(Z1)|GO:0016477(cell migration)"
Remark	"QUALITY:PATO:0000461(normal)"
Remark	"We killed the ancestor of one SGP by laser-irradiation and observed the behavior of the remaining SGP using transgenes to mark the SGP and PGC surfaces. We found that the remaining SGP always migrated to the normal location, and eventually wrapped entirely around that PGC.  In laser-irradiated embryos, we never observed the single SGP significantly over- or under-migrate, or wrap around the contralateral PGC. We conclude that even though the two SGPs undergo mirror-symmetric and synchronous morphogenetic movements, Z1 and Z4 are not dependent on each other for their posterior migration, extension of projections, or wrapping behaviors."
Reference	"WBPaper00042220"


Anatomy_function : "WBbtf0998"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000399"
Not_involved	"WBbt:0004577"	Unnecessary
Remark	"ENTITY:WBbt:0004574(Z4)|GO:0016477(cell migration)"
Remark	"QUALITY:PATO:0000461(normal)"
Remark	"We killed the ancestor of one SGP by laser-irradiation and observed the behavior of the remaining SGP using transgenes to mark the SGP and PGC surfaces. We found that the remaining SGP always migrated to the normal location, and eventually wrapped entirely around that PGC.  In laser-irradiated embryos, we never observed the single SGP significantly over- or under-migrate, or wrap around the contralateral PGC. We conclude that even though the two SGPs undergo mirror-symmetric and synchronous morphogenetic movements, Z1 and Z4 are not dependent on each other for their posterior migration, extension of projections, or wrapping behaviors."
Reference	"WBPaper00042220"


Anatomy_function : "WBbtf0999"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000399"
Not_involved	"WBbt:0004574"	Unnecessary
Remark	"ENTITY:WBbt:0004577(Z1)|GO:0030030(cell projection organization)"
Remark	"QUALITY:PATO:0000461(normal)"
Remark	"We killed the ancestor of one SGP by laser-irradiation and observed the behavior of the remaining SGP using transgenes to mark the SGP and PGC surfaces. We found that the remaining SGP always migrated to the normal location, and eventually wrapped entirely around that PGC.  In laser-irradiated embryos, we never observed the single SGP significantly over- or under-migrate, or wrap around the contralateral PGC. We conclude that even though the two SGPs undergo mirror-symmetric and synchronous morphogenetic movements, Z1 and Z4 are not dependent on each other for their posterior migration, extension of projections, or wrapping behaviors."
Reference	"WBPaper00042220"


Anatomy_function : "WBbtf1000"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000399"
Not_involved	"WBbt:0004577"	Unnecessary
Remark	"ENTITY:WBbt:0004574(Z4)|GO:0030030(cell projection organization)"
Remark	"QUALITY:PATO:0000461(normal)"
Remark	"We killed the ancestor of one SGP by laser-irradiation and observed the behavior of the remaining SGP using transgenes to mark the SGP and PGC surfaces. We found that the remaining SGP always migrated to the normal location, and eventually wrapped entirely around that PGC.  In laser-irradiated embryos, we never observed the single SGP significantly over- or under-migrate, or wrap around the contralateral PGC. We conclude that even though the two SGPs undergo mirror-symmetric and synchronous morphogenetic movements, Z1 and Z4 are not dependent on each other for their posterior migration, extension of projections, or wrapping behaviors."
Reference	"WBPaper00042220"


Anatomy_function : "WBbtf1001"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000399"
Involved	"WBbt:0006849"	Necessary
Remark	"ENTITY:WBbt:0007854(somatic gonad precursor)|GO:0016477(cell migration)"
Remark	"QUALITY:PATO:0000461(normal) NOT"
Remark	"In mes-1 (RNAi) embryos (PGCs are transformed into muscle-like cells), the SGPs were born at the same location as wild-type embryos. The SGPs still migrated posteriorly along the lateral edges of the endoderm in mes-1(RNAi) embryos (Fig. 4A and B), and they remained lateral to the endoderm but ceased migrating at a slightly more anterior position. We conclude that PGCs are dispensable for SGP posterior migration but are required for the precise positioning of SGPs at the end of their migration."
Reference	"WBPaper00042220"


Anatomy_function : "WBbtf1002"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000399"
Involved	"WBbt:0006849"	Necessary
Remark	"ENTITY:WBbt:0007854(somatic gonad precursor)|GO:0030030(cell projection organization)"
Remark	"QUALITY:PATO:0000461(normal) NOT"
Remark	"In mes-1 (RNAi) embryos (PGCs are transformed into muscle-like cells), the SGPs extended projections that were abnormal in shape and orientation compared to those in wild-type embryos. We conclude while PGCs are not needed to initiate formation of SGP projections, PGCs are essential for the morphology and behavior of the SGP projections and for the wrapping behavior of the SGPs."
Reference	"WBPaper00042220"


Anatomy_function : "WBbtf1003"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000399"
Involved	"WBbt:0005208"	Necessary
Remark	"ENTITY:WBbt:0007854(somatic gonad precursor)|GO:0016477(cell migration)"
Remark	"QUALITY:PATO:0000461(normal) NOT"
Remark	"In end-1 end-3 mutant embryos, the endodermal cell lineage is transformed to adopt epidermal- and muscle-like cell fates. We observed that the SGPs were born in approximately the normal location in end-1 end-3 embryos. However, while the SGPs still migrated posteriorly in the absence of endoderm, they stopped migrating at a more anterior position."
Reference	"WBPaper00042220"


Anatomy_function : "WBbtf1004"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000399"
Involved	"WBbt:0005208"	Necessary
Remark	"ENTITY:WBbt:0007854(somatic gonad precursor)|GO:0030030(cell projection organization)"
Remark	"QUALITY:PATO:0000461(normal) NOT"
Remark	"In end-1 end-3 mutant embryos, the endodermal cell lineage is transformed to adopt epidermal- and muscle-like cell fates. In the end-1 end-3 embryos in which the PGCs failed to ingress, the SGPs extended short dynamic projections in various directions but did not migrate to the external PGCs nor wrap around any other cell. In the end-1 end-3 embryos in which one or both PGCs had ingressed, the SGPs always extended projections around the PGCs they contacted, but these projections were often shorter and thicker than in wild type. ... We conclude that endoderm is not required for SGPs to migrate posteriorly, extend projections, or wrap around the PGCs. However, endoderm is required for the normal morphology of the SGP projections, for SGPs to reach their regular final position just posterior to the PGCs, and to prevent SGPs from shifting medially and contacting the contralateral SGP and/or PGC."
Reference	"WBPaper00042220"


Anatomy_function : "WBbtf1005"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000184"	Autonomous
Gene	"WBGene00000417"
Involved	"WBbt:0006925"	Sufficient
Involved	"WBbt:0006925"	Necessary
Remark	"Five obviously mosaic animals are described in categories 1 and 2 of Table 2. The category 1 mosaics are semi-Dpy and Unc. These animals were found to have cell death survivors only among cells generated from the ABp lineage. The category 2 mosaic, with an apparent ABa loss, was semiDpy and non-Unc (although this animal moved more slowly than does a wild-type animal). These results again indicate that ced-3 is cell autonomous and reveal that unc-26, like unc-30, acts in the ABp lineage."
Remark	"Genotype \"ced-3(n717) unc-26(e205) dpy-4(e1166); nDp3(IV,V;f)\""
Remark	"Published_as ced-3"
Remark	"Strain used for ced-3 mosaic analysis"
Reference	"WBPaper00001254"


Anatomy_function : "WBbtf1006"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000102"
Not_involved	"WBbt:0005821"	Unnecessary
Not_involved	"WBbt:0005304"	Unnecessary
Remark	"ENTITY:WBbt:0004758(HSNL)|GO:0008021(synaptic vesicle)|GO:0051179(localization) QUALITY:PATO:0000461(normal)"
Remark	"Genotype \"kyIs235(unc-86::snb-1::yfp);lin-39(n709ts)\""
Remark	"The two postsynaptic targets of HSNL were eliminated during the L1 stage by killing the M cell, the precursor to all vulval muscles, in lin-39(n709ts) mutant animals, in which the VC neurons undergo programmed cell death in the L1 stage, the position and intensity of HSNL SNB-1-labeled synaptic vesicles were indistinguishable from those of wild-type animals."
Reference	"WBPaper00005760"


Anatomy_function : "WBbtf1007"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001837"
Gene	"WBGene00004758"
Involved	"WBbt:0005772"	Sufficient
Remark	"Curated by Fernando Bolio."
Remark	"DR longevity was fully rescued by expression of SEK-1 from its own promoter (Figure S1K), and was rescued by intestinal SEK-1 partially (Figure 1J) but less robustly than pathogen resistance (Shivers et al., 2009)."
Remark	"Genotype \"sek-1(km4);qdEx4[ges-1p::sek-1(cDNA)::GFP::unc-54-3 0 UTR + myo-2p::mStrawberry::unc-54-3 0 UTR]\""
Remark	"Published_as sek-1"
Reference	"WBPaper00056443"


Anatomy_function : "WBbtf1008"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001234"
Gene	"WBGene00000897"
Not_involved	"WBbt:0005759"	Insufficient
Remark	"Expressing either the genomic DNA fragment of daf-1 or the daf-1 cDNA selectively in the interneurons RIM and RIC (Pdaf-1::daf-1 or pRIM/RIC::daf-1; [70, 72]) fully rescued the defect in the daf-1(m40) mutant animals (Fig 4B and 4C), while expressing daf-1 in sensory neurons (Pbbs-1::daf-1 or Posm-6::daf-1; [70]) was not sufficient to rescue (Figs 4D and S3)."
Remark	"Genotype \"daf-1(m40)IV; ftEx70[Pbbs-1::daf-1::gfp; Podr-1::dsRed]\""
Remark	"Published_as daf-1"
Reference	"WBPaper00056328"


Anatomy_function : "WBbtf1009"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001837"
Gene	"WBGene00004758"
Involved	"WBbt:0003679"	Sufficient
Remark	"Curated by Fernando Bolio."
Remark	"DR longevity was also partially rescued by neuronal SEK-1 (Figures 1K and 1L), although the pathogen avoidance response itself was not essential (Figure 1I)."
Remark	"Genotype \"sek-1(km4);qdEx8[unc-119p::sek-1(cDNA)::GFP::unc-54-3 0 UTR + myo-2p::mStrawberry::unc-54-3 0 UTR]\""
Remark	"Published_as sek-1"
Reference	"WBPaper00056443"


Anatomy_function : "WBbtf1010"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001234"
Gene	"WBGene00000897"
Not_involved	"WBbt:0005759"	Insufficient
Remark	"Expressing either the genomic DNA fragment of daf-1 or the daf-1 cDNA selectively in the interneurons RIM and RIC (Pdaf-1::daf-1 or pRIM/RIC::daf-1; [70, 72]) fully rescued the defect in the daf-1(m40) mutant animals (Fig 4B and 4C), while expressing daf-1 in sensory neurons (Pbbs-1::daf-1 or Posm-6::daf-1; [70]) was not sufficient to rescue (Figs 4D and S3)."
Remark	"Genotype \"daf-1(m40)IV;ftEx83[osm-6p::daf-1]\""
Remark	"Published_as daf-1"
Reference	"WBPaper00056328"


Anatomy_function : "WBbtf1011"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0002241"
Gene	"WBGene00000912"
Involved	"WBbt:0005772"	Sufficient
Remark	"Curated by Fernando Bolio."
Remark	"Genotype \" daf-16(mu86); daf-2(e1370); muIs142[ges-1p::GFP::daf-16 + odr-1p::RFP\""
Remark	"Published_as daf-16"
Remark	"The reduction in food consumption induced by rIIS was rescued slightly by neuronal DAF-16 expression, but intestinal DAF-16 provided a more robust rescue (Figure 6B)."
Reference	"WBPaper00056443"


Anatomy_function : "WBbtf1012"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0002241"
Gene	"WBGene00000912"
Involved	"WBbt:0003679"	Sufficient
Remark	"Curated by Fernando Bolio."
Remark	"Genotype \" daf-16(mu86); daf-2(e1370); muIs131[unc-119p::GFP::daf-16 + rol-6(su1006)]\""
Remark	"Published_as daf-16"
Remark	"The reduction in food consumption induced by rIIS was rescued slightly by neuronal DAF-16 expression, but intestinal DAF-16 provided a more robust rescue (Figure 6B)"
Reference	"WBPaper00056443"


Anatomy_function : "WBbtf1013"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0001234"
Involved	"WBbt:0005671"	Necessary
Remark	"Curated by Fernando Bolio."
Remark	"Consistently, we found that the transgenic animals that selectively expressed a hyperactive form of an amiloride-sensitive sodium channel MEC-4 that generated necrosis of AWB [42, 46] did not leave the OP50 lawn when 2-nonanone was present (Fig 2A) and that many of the worms remained diffusely distributed on the food lawn by the end of the assay."
Remark	"Genotype \"kyIs102V;kyIs104[Pstr-1::mec-4(d);Pstr-1::gfp]\""
Remark	"Published_as mec-4"
Reference	"WBPaper00056328"


Anatomy_function : "WBbtf1014"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0001234"
Involved	"WBbt:0005671"	Necessary
Remark	"Curated by Fernando Bolio."
Remark	"Genotype \"kyIs102V;kyIs104[Pstr-1::mec-4(d);Pstr-1::gfp]\""
Remark	"Published_as mec-4"
Remark	"These transgenic animals were defective in avoiding 2-nonanone in the standard chemotaxis assay (Table 1 and S1 Fig), consistent with previous findings [42]."
Reference	"WBPaper00056328"


Anatomy_function : "WBbtf1015"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0002545"
Involved	"WBbt:0005668"	Necessary
Involved	"WBbt:0005668"	Remark
Remark	"Curated by Fernando Bolio."
Remark	"Genotype \"qrIs2[Psra-9::mCasp1; Psra-9::gfp; Pelt-2::gfp]\""
Remark	"Published_as twk-18"
Remark	"The transgenic animals that contained genetically-killed ASK left the OP50 lawn significantly faster than wild type (Fig 2B-2D and Table 4)."
Remark	"We also transgenic animals selectively express a cell-death inducing caspase, or twk-18(gf) that encodes a constitutively active form of the potassium channel TWK-18 [57], or tetanus toxin that eliminates the synaptic release [58] in the ASI, AWC, ASJ, ADL, or ASK neurons [48, 54, 59-63]."
Reference	"WBPaper00056328"


Anatomy_function : "WBbtf1016"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0002545"
Involved	"WBbt:0005666"	Necessary
Remark	"Curated by Fernando Bolio."
Remark	"Genotype \"oyls84[Pgpa-4::TU813; Pgcy-27::TU814; Pgcy-27::gfp; Punc-122::dsRed]\""
Remark	"Published_as twk-18"
Remark	"The transgenic animals that contained genetically-killed ASI or expressed the tetanus toxin in ADL left the OP50 lawn significantly more slowly than wild type (Fig 2B-2D and Table 4)."
Reference	"WBPaper00056328"


Anatomy_function : "WBbtf1017"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0002545"
Involved	"WBbt:0005661"	Necessary
Remark	"Curated by Fernando Bolio."
Remark	"Genotype \" CX12330 Ex[Psre-1::TeTx::mCherry; Punc-122:RFP]\""
Remark	"Published_as twk-18"
Remark	"The transgenic animals that contained genetically-killed ASI or expressed the tetanus toxin in ADL left the OP50 lawn significantly more slowly than wild type (Fig 2B-2D and Table 4)."
Reference	"WBPaper00056328"


Anatomy_function : "WBbtf1018"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001234"
Gene	"WBGene00000903"
Involved	"WBbt:0005415"	Sufficient
Remark	"Curated by Fernando Bolio."
Remark	"Genotype \"Pcat-2::daf-7\""
Remark	"Published_as daf-7"
Remark	"We found that expressing daf-7 selectively in ASI (Pstr-3::daf-7[70]) did not rescue the defects in the integrated response; but expressing daf-7 in ADE (Pcat-2::daf-7) or OLQ (Pocr-4::daf-7) sensory neurons using cell-selective promoters [83-85] rescued the delayed leaving phenotype in the daf-7(e1372) mutant animals (Fig 3K-3M)"
Reference	"WBPaper00056328"


Anatomy_function : "WBbtf1019"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001234"
Gene	"WBGene00000903"
Involved	"WBbt:0006848"	Sufficient
Remark	"Curated by Fernando Bolio."
Remark	"Genotype \"Pocr-4::daf-7\""
Remark	"Published_as daf-7"
Remark	"We found that expressing daf-7 selectively in ASI (Pstr-3::daf-7[70]) did not rescue the defects in the integrated response; but expressing daf-7 in ADE (Pcat-2::daf-7) or OLQ (Pocr-4::daf-7) sensory neurons using cell-selective promoters [83-85] rescued the delayed leaving phenotype in the daf-7(e1372) mutant animals (Fig 3K-3M)"
Reference	"WBPaper00056328"


Anatomy_function : "WBbtf1020"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001234"
Gene	"WBGene00000897"
Involved	"WBbt:0005835"	Sufficient
Involved	"WBbt:0006834"	Sufficient
Remark	"Curated by Fernando Bolio."
Remark	"Expressing either the genomic DNA fragment of daf-1 or the daf-1 cDNA selectively in the interneurons RIM and RIC (Pdaf-1::daf-1 or pRIM/RIC::daf-1; [70, 72]) fully rescued the defect in the daf-1(m40) mutant animals (Fig 4B and 4C)."
Remark	"Genotype \"daf-1(m40)IV; ftEx205[Ptdc-1::daf-1::gfp; Podr-1::dsRed],\""
Remark	"Published_as daf-1"
Reference	"WBPaper00056328"


Anatomy_function : "WBbtf1021"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000633"
Gene	"WBGene00016611"
Not_involved	"WBbt:0006804"	Insufficient
Remark	"ENTITY:WBbt:0006831(PVD)|(tertiary)|GO:0044307(dendritic branch)|GO:0048856(anatomical structure development) QUALITY:PATO:0000584(hypertrophy) NOT"
Remark	"Genotype \"bicd-1(ok2731); otIs138[ser2prom3::GFP];Ex[bicd-1(+);myo-3prom::RFP;mec-7prom::GFP]\""
Remark	"Published_as bicd-1"
Remark	"genetic mosaic analyses revealed that animals that retained wild-type bicd-1 in the AB.p lineage (which gives rise to the PVD neurons) but not the P1 lineage (which gives rise to 94 out of 95 body wall muscles) exhibited partial rescue of the enhanced-branching bicd-1(ok2731) mutant phenotype."
Reference	"WBPaper00037977"


Anatomy_function : "WBbtf1022"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001446"
Gene	"WBGene00001681"
Not_involved	"WBbt:0005663"	Insufficient
Remark	"NaCl gustatory plasticity defective"
Remark	"gpc-1 mutant, expression of GPC-1 in ASE neurons did not restore gustatory plasticity."
Reference	"WBPaper00027029"


Anatomy_function : "WBbtf1023"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000992"
Gene	"WBGene00003850"
Not_involved	"WBbt:0005660"	Insufficient
Remark	"ADF specific expression of odr-3 did not restore avoidance of 1M NaCl."
Remark	"avoidance of 1M NaCl"
Reference	"WBPaper00027029"


Anatomy_function : "WBbtf1024"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001446"
Gene	"WBGene00003850"
Not_involved	"WBbt:0005665"	Insufficient
Remark	"NaCl avoidance after pre-exposure was not restored by expressing odr-3 in ASH neurons."
Remark	"NaCl gustatory plasticity defective"
Reference	"WBPaper00027029"


Anatomy_function : "WBbtf1025"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001084"
Gene	"WBGene00001709"
Not_involved	"WBbt:0005842"	Insufficient
Not_involved	"WBbt:0005841"
Not_involved	"WBbt:0006818"
Not_involved	"WBbt:0006819"
Not_involved	"WBbt:0005840"
Not_involved	"WBbt:0006813"
Not_involved	"WBbt:0005400"
Not_involved	"WBbt:0005835"
Not_involved	"WBbt:0005353"
Not_involved	"WBbt:0003850"
Not_involved	"WBbt:0006976"
Not_involved	"WBbt:0005346"
Not_involved	"WBbt:0006822"
Not_involved	"WBbt:0004821"
Not_involved	"WBbt:0006836"
Not_involved	"WBbt:0005045"
Not_involved	"WBbt:0005399"
Remark	"attractive response to NaCl defective"
Remark	"expression of GRK-2 using a glr-1::grk-2 construct did not restore NaCl chemotaxis."
Reference	"WBPaper00027029"


Anatomy_function : "WBbtf1026"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001084"
Gene	"WBGene00001709"
Not_involved	"WBbt:0005842"	Insufficient
Not_involved	"WBbt:0005841"	Insufficient
Not_involved	"WBbt:0006818"	Insufficient
Not_involved	"WBbt:0006819"	Insufficient
Not_involved	"WBbt:0005840"	Insufficient
Not_involved	"WBbt:0006813"	Insufficient
Not_involved	"WBbt:0005400"	Insufficient
Not_involved	"WBbt:0005835"	Insufficient
Not_involved	"WBbt:0005353"	Insufficient
Not_involved	"WBbt:0003850"	Insufficient
Not_involved	"WBbt:0006976"	Insufficient
Not_involved	"WBbt:0005346"	Insufficient
Not_involved	"WBbt:0006822"	Insufficient
Not_involved	"WBbt:0004821"	Insufficient
Not_involved	"WBbt:0006836"	Insufficient
Not_involved	"WBbt:0005045"	Insufficient
Not_involved	"WBbt:0005399"	Insufficient
Remark	"attractive response to NaCl defective"
Remark	"expression of GRK-2 using a glr-1::grk-2 construct did not restore NaCl chemotaxis."
Reference	"WBPaper00027029"


Anatomy_function : "WBbtf1027"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000254"
Not_involved	"WBbt:0003904"	Unnecessary
Remark	"chloride chemotaxis was unaffected by ablation of ASEL."
Reference	"WBPaper00004609"


Anatomy_function : "WBbtf1028"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0001058"
Not_involved	"WBbt:0003904"	Unnecessary
Remark	"potassium chemotaxis was unaffected by ablation of ASEL."
Reference	"WBPaper00004609"


Anatomy_function : "WBbtf1029"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000265"
Not_involved	"WBbt:0005832"	Unnecessary
Remark	"ablation of AWC-on did not affect chemotaxis to 2,3-pentanedione."
Remark	"chemotaxis towards 2,3-pentanedione abnormal."
Reference	"WBPaper00004610"


Anatomy_function : "WBbtf1030"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000265"
Not_involved	"WBbt:0005832"	Unnecessary
Remark	"ablation of AWC-on did not cause defects in butanone/benzaldehyde discrimination."
Remark	"discrimination of benzaldehyde from butanone abnormal."
Reference	"WBPaper00004610"


Anatomy_function : "WBbtf1031"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000117"
Gene	"WBGene00000035"
Not_involved	"WBbt:0003679"	Unnecessary
Remark	"Genotype \"ace-2 I; ace-3 II; unc-3 daf-6 ace-1 X; mnDp14(X,f)\""
Remark	"ace-2 ace-3 animals also lacking ace-1(+) in all cells of the AB lineage (which includes most of the cells making up the nervous system) are viable and fertile."
Remark	"multiple strains were used for mosaic analysis"
Reference	"WBPaper00001039"


Anatomy_function : "WBbtf1032"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000646"
Gene	"WBGene00000035"
Not_involved	"WBbt:0003679"	Unnecessary
Remark	"Ace-Unc"
Remark	"Genotype \"ace-2 I; daf-6 ace-1 X; mnDp14(X;f)\""
Remark	"animals showed wild-type movement despite having lost ace-1+ at ABp or AB."
Remark	"two different genotypes were used separately"
Reference	"WBPaper00000761"


Anatomy_function : "WBbtf1033"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000177"
Gene	"WBGene00000035"
Not_involved	"WBbt:0003679"	Unnecessary
Remark	"Genotype \"ace-2 I; daf-6 ace-1 X; mnDp14(X;f)\""
Remark	"acetylcholinesterase activity, histochemically staining, reduced."
Remark	"animals showed normal acetylcholinesterase histochemical staining in nerve ring and nerve cords, despite having lost ace-1+ at ABp or AB."
Remark	"two different genotypes were used separately"
Reference	"WBPaper00000761"


Anatomy_function : "WBbtf1034"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000061"
Gene	"WBGene00000912"
Not_involved	"WBbt:0003675"	Insufficient
Remark	"Genotype \"daf-16(mu86); daf-2(e1370)\""
Remark	"expressing daf-16 specifically in muscles (with a myo-3 promoter) produced no lifespan extension."
Reference	"WBPaper00006226"


Anatomy_function : "WBbtf1035"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000013"
Gene	"WBGene00000912"
Not_involved	"WBbt:0003675"	Insufficient
Remark	"Genotype \"daf-16(mu86); daf-2(e1370)\""
Remark	"expressing daf-16::gfp specifically in muscles (with a myo-3 promoter) did not rescue dauer formation."
Reference	"WBPaper00006226"


Anatomy_function : "WBbtf1036"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000061"
Gene	"WBGene00000912"
Not_involved	"WBbt:0003675"	Insufficient
Not_involved	"WBbt:0003679"	Insufficient
Remark	"Genotype \"daf-16(mu86); mes-1(bn7)\""
Remark	"expressing daf-16 specifically in muscles (with a myo-3 promoter) had little or no effect on lifespan of daf-16(-); mes-1(bn7) mutants."
Remark	"neuronal (unc-119 promoter-driven) daf-16 expression had little or no effect on lifespan of daf-16(-); mes-1(bn7) mutants."
Reference	"WBPaper00006226"


Anatomy_function : "WBbtf1037"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000245"
Not_involved	"WBbt:0005784"	Unnecessary
Remark	"Z2 and Z3 ablated animals showed normal SM migration in unc-53(ay10) mutants."
Reference	"WBPaper00004362"


Anatomy_function : "WBbtf1038"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000220"
Not_involved	"WBbt:0006893"	Unnecessary
Not_involved	"WBbt:0006895"	Unnecessary
Not_involved	"WBbt:0006780"	Unnecessary
Remark	"ablation of P5.p and P7.p does not affect zmp-1::GFP expression in P6.pxxx during L4 lethargus."
Remark	"ablation of VU precursors before VPCs divide does not affect zmp-1::GFP expression in P6.pxxx during L4 lethargus."
Remark	"vulval primary lineage patterning (P6.pxx, vulE vs. vulF fates) defective."
Reference	"WBPaper00004362"


Anatomy_function : "WBbtf1039"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000220"
Not_involved	"WBbt:0006893"	Unnecessary
Not_involved	"WBbt:0006895"	Unnecessary
Not_involved	"WBbt:0006780"	Unnecessary
Remark	"ablation of P5.p and P7.p does not affect zmp-1::GFP expression in P6.pxxx during L4 lethargus."
Remark	"ablation of VU precursors before VPCs divide does not affect zmp-1::GFP expression in P6.pxxx during L4 lethargus."
Remark	"vulval primary lineage patterning (P6.pxx, vulE vs. vulF fates) defective."
Reference	"WBPaper00004481"


Anatomy_function : "WBbtf1040"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000885"
Not_involved	"WBbt:0006925"	Remark
Remark	"Genotype \"dpy-17(e164) ced-6(n1813) mec-14(u55) ncl-1(e1865) unc-36(e251)III; sDp3\""
Remark	"mosaic analysis demonstrates that ced-6 acts within the engulfing gonadal sheath cells rather than the germline apoptotic cells."
Reference	"WBPaper00003090"


Anatomy_function : "WBbtf1041"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000707"
Not_involved	"WBbt:0006699"
Not_involved	"WBbt:0006142"
Remark	"specific defect: anterior pharyngeal extension abnormal."
Reference	"WBPaper00004707"


Anatomy_function : "WBbtf1042"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0004026"
Gene	"WBGene00001172"
Not_involved	"WBbt:0005665"	Insufficient
Remark	"Genotype \"glr-1(n2461);egl-3(nu349)\""
Remark	"expression of egl-3 in ASH (using the osm-10 promoter) failed to rescue the glr-1 (nose touch defective) suppression defect."
Remark	"glr-1 single mutants are nose-touch insensitive, whereas glr-1;egl-3 double mutants are nose-touch sensitive."
Reference	"WBPaper00004977"


Anatomy_function : "WBbtf1043"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000643"
Not_involved	"WBbt:0005665"	Unnecessary
Remark	"specific defect: execution of the egg-laying motor program correlates with two changes in locomotive behavior: an increased propensity for forward locomotion before egg-laying, and an increased propensity for directional changes, in particular reversals, during and after an egg-laying event."
Reference	"WBPaper00004978"


Anatomy_function : "WBbtf1044"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000643"
Not_involved	"WBbt:0005665"	Unnecessary
Remark	"We also examined the effect of ablating the ASH neurons, another set of neurons that receive synaptic input from the HSNs and have synaptic output to the command interneurons. In contrast to the results of AVF ablation experiment, ablation of the ASH neurons did not cause a significant change in either the general pattern of locomotion (Table 1) or the velocity and reversal bursts around egg-laying [Fig. 5(a) and (b)]."
Remark	"specific defect: execution of the egg-laying motor program correlates with two changes in locomotive behavior: an increased propensity for forward locomotion before egg-laying, and an increased propensity for directional changes, in particular reversals, during and after an egg-laying event."
Reference	"WBPaper00004978"


Anatomy_function : "WBbtf1045"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0004007"
Not_involved	"WBbt:0006862"	Unnecessary
Not_involved	"WBbt:0006862"	Unnecessary
Not_involved	"WBbt:0006862"	Unnecessary
Not_involved	"WBbt:0006862"	Unnecessary
Not_involved	"WBbt:0007805"	Unnecessary
Not_involved	"WBbt:0007805"	Unnecessary
Not_involved	"WBbt:0007805"	Unnecessary
Not_involved	"WBbt:0007805"	Unnecessary
Not_involved	"WBbt:0006861"	Unnecessary
Remark	"Ablation of SPD and SPV neurons (n=14 males) at early L4 stage or damage"
Remark	"to their sensory endings via laser cauterization of the spicule tips at"
Remark	"adult stage (n=10 animals) did not interfere with males' ability to prod"
Remark	"or insert their spicules into hermaphrodites."
Remark	"When SPC-ablated males (n=10) were mated to easily penetrable 96 hr unc-31 adult hermaphrodites, they did not extend their spicules through the vulva, but continuously prodded the vulval slit. Therefore, SPC neurons are required for prolonged protractor contraction but not for initiating or sustaining periodic contractions."
Reference	"WBPaper00005027"


Anatomy_function : "WBbtf1046"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000279"
Not_involved	"WBbt:0006862"	Unnecessary
Not_involved	"WBbt:0007805"	Unnecessary
Remark	"When SPC-ablated males (n=10) were mated to easily penetrable 96 hr unc-31 adult hermaphrodites, they did not extend their spicules through the vulva, but continuously prodded the vulval slit. Therefore, SPC neurons are required for prolonged protractor contraction but not for initiating or sustaining periodic contractions."
Reference	"WBPaper00005027"


Anatomy_function : "WBbtf1047"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000279"
Not_involved	"WBbt:0006862"	Unnecessary
Not_involved	"WBbt:0007805"	Unnecessary
Remark	"When SPC-ablated males (n=10) were mated to easily penetrable 96 hr unc-31 adult hermaphrodites, they did not extend their spicules through the vulva, but continuously prodded the vulval slit. Therefore, SPC neurons are required for prolonged protractor contraction but not for initiating or sustaining periodic contractions."
Reference	"WBPaper00005027"


Anatomy_function : "WBbtf1048"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001291"
Gene	"WBGene00003839"
Not_involved	"WBbt:0005660"	Insufficient
Not_involved	"WBbt:0005670"	Insufficient
Remark	"Genotype \"ocr-2(ak47) IV; npr-1(ad609) lin-15(n765ts)\""
Remark	"expression of ocr-2 in the ADF or AWA neurons does not restore aggregation behavior to ocr-2;npr-1 mutant animals."
Remark	"strain name CX4827"
Reference	"WBPaper00005511"


Anatomy_function : "WBbtf1049"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0001291"
Gene	"WBGene00003851"
Not_involved	"WBbt:0005660"	Insufficient
Not_involved	"WBbt:0005670"	Insufficient
Not_involved	"WBbt:0005671"
Not_involved	"WBbt:0005666"
Not_involved	"WBbt:0005668"
Remark	"Genotype \"odr-4(n2144) III; npr-1(ad609) lin-15(n765ts) X\""
Remark	"odr-4 expression in ADF does not restore social behavior to odr-4; npr-1 mutant animals."
Remark	"odr-4 expression in AWA, AWB, ASI, and ASK neurons also fails to restore aggregation behavior to odr-4; npr-1 animals."
Remark	"strain name AX215"
Reference	"WBPaper00005511"


Anatomy_function : "WBbtf1050"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000047"
Gene	"WBGene00004215"
Not_involved	"WBbt:0003672"	Insufficient
Remark	"Genotype \"vab-1(e2) ptp-3(op147)\""
Remark	"expression of PTP-3 using epidermal promoter (jam-1) gave partial rescue of the lethality of vab-1 ptp-3 double mutants that was not statistically significant."
Reference	"WBPaper00005259"


Anatomy_function : "WBbtf1051"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000195"
Gene	"WBGene00003254"
Not_involved	"WBbt:0006876"	Unnecessary
Not_involved	"WBbt:0004015"	Unnecessary
Not_involved	"WBbt:0006875"	Unnecessary
Remark	"ENTITY:WBbt:0006865(DTC)|GO:0016477(cell migration)|PATO:0001233(dorsal to)|WBbt:0005753(seam cell) QUALITY:PATO:0000468(reduced)"
Remark	"Genotype \"mig-23(k180); ncl-1(e1865); Ex[mig-23(+),sur-5::GFP,ncl-1(+)]\""
Remark	"genetic mosaic analysis revealed that MIG-23 is required in the C lineage and NOT required in the AB, EMS and P3 lineages."
Reference	"WBPaper00006309"


Anatomy_function : "WBbtf1052"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000565"
Gene	"WBGene00006845"
Not_involved	"WBbt:0003679"	Insufficient
Remark	"ENTITY:WBbt:0005740(midbody) QUALITY:PATO:0000404(coiled)"
Remark	"ENTITY:WBbt:0007833(organism)|GO:0040011(locomotion) QUALITY:PATO:0000770(uncoordinated)"
Remark	"Genotype \"unc-122(e2520);Ex[unc-122,myo-3::gfp,ttx-3::gfp]\""
Remark	"Published_as unc-122"
Remark	"mosaic animals in which AB cell descendants retained the unc-122-rescuing transgene but not P cell descendants showed coiling mutant phenotype, indicating that loss of unc-122 in muscle cell lineages affects locomotory behavior."
Reference	"WBPaper00006427"


Anatomy_function : "WBbtf1053"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000565"
Gene	"WBGene00006845"
Not_involved	"WBbt:0003679"	Unnecessary
Remark	"ENTITY:WBbt:0005740(midbody) QUALITY:PATO:0000404(coiled)"
Remark	"ENTITY:WBbt:0007833(organism)|GO:0040011(locomotion) QUALITY:PATO:0000770(uncoordinated)"
Remark	"Genotype \"unc-122(e2520);Ex[unc-122,myo-3::gfp,ttx-3::gfp]\""
Remark	"Published_as unc-122"
Remark	"mosaic animals in which P cell descendants retained the unc-122-rescuing transgene but not AB cell descendants showed rescue of the coiling mutant phenotype, indicating that loss of unc-122 in neuronal lineages has no impact on locomotory behavior."
Reference	"WBPaper00006427"


Anatomy_function : "WBbtf1054"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000012"	Nonautonomous
Gene	"WBGene00000905"
Not_involved	"WBbt:0007855"	Unnecessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0055115(diapause) QUALITY:PATO:0000760(hyperactive) NOT"
Remark	"ENTITY:WBbt:0006865(DTC)|GO:0016477(cell migration) QUALITY:PATO:0000692(heterochronic) NOT"
Remark	"ENTITY:WBbt:0007833(organism)|GO:0000003(reproduction) QUALITY:PATO:0001997(reduced) NOT"
Remark	"Genotype \"daf-9(dh6); dhEx66[daf-9::gfp]\""
Remark	"Mosaics arise spontaneously from transgenic lines of daf-9(dh6) containing extrachromosamal array of genomic daf-9::gfp (dhEx66). Mosaics expressing daf-9 in the hypodermis (but not XXX cells) bypassed diapause, had normal gonadal development and were fertile."
Remark	"Published_as daf-9"
Reference	"WBPaper00013396"


Anatomy_function : "WBbtf1055"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001010"
Gene	"WBGene00003401"
Not_involved	"WBbt:0004015"	Unnecessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050878(regulation of body fluid levels) QUALITY:PATO:0001507(disrupted)"
Remark	"Genotype \"clr-1(e1745ts); mpk-1 ncl-1 unc-36; sDp3\""
Remark	"Mosaic animals with sDp3 losses in AB descendants when shifted to the restrictive temperature displayed the Clr phenotype, suggesting that loss of mpk-1 activity in the AB lineage is not sufficient to suppress the Clr phenotype. Therefore, mpk-1(+) activity within P1 descendants can function to prevent the Soc phenotype."
Remark	"Published_as mpk-1"
Reference	"WBPaper00024207"


Anatomy_function : "WBbtf1056"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001010"
Gene	"WBGene00003401"
Not_involved	"WBbt:0006874"	Unnecessary
Remark	"ENTITY:WBbt:0007833(organism)|GO:0050878(regulation of body fluid levels) QUALITY:PATO:0001507(disrupted)"
Remark	"Mosaic animals with sDp3 losses in P1 descendants when shifted to the restrictive temperature displayed the Clr phenotype, suggesting that loss of mpk-1 activity in the P1 lineage is also not sufficient to suppress the Clr phenotype. Therefore, mpk-1(+) activity within the AB lineage can function to prevent the Soc phenotype."
Remark	"Published_as mpk-1"
Reference	"WBPaper00024207"


Anatomy_function : "WBbtf1057"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000054"
Gene	"WBGene00002881"
Not_involved	"WBbt:0004015"	Unnecessary
Remark	"ENTITY:WBbt:0007833(organism)|WBls:0000023(larva)|GO:0040007(growth) QUALITY:PATO:0000297(arrested) NOT"
Remark	"Genotype \"dpy-17 let-756 ncl-1 unc-36; sDp3\""
Remark	"Published_as let-756"
Remark	"descendants in the AB.p lineage. Besides being Unc, these mosaic animals were completely wild type, suggesting that lack of let-756(+) expression in the AB lineage is not essential for viability."
Reference	"WBPaper00024207"


Anatomy_function : "WBbtf1058"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000054"
Gene	"WBGene00002881"
Not_involved	"WBbt:0004015"	Insufficient
Remark	"ENTITY:WBbt:0007833(organism)|WBls:0000023(larva)|GO:0040007(growth) QUALITY:PATO:0000297(arrested)"
Remark	"Genotype \"dpy-17 let-756 ncl-1 unc-36; sDp3\""
Remark	"Published_as let-756"
Remark	"We screened dpy-17 let-756 ncl-1 unc-36; sDp3 animals for mosaic animals. Dpy non-Unc animals were extremely rare, and the few Dpy non-Unc animals identified turned out to result from the breakdown of the free duplication. This striking finding suggests that the cellular focus of let-756 is not easily separable from that of dpy-17. DPY-17 is thought to be required in the P1 lineage."
Reference	"WBPaper00024207"


Anatomy_function : "WBbtf1059"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000102"
Gene	"WBGene00001499"
Not_involved	"WBbt:0006874"	Unnecessary
Remark	"ENTITY:WBbt:0005190(GABAergic neuron)|GO:0031594(neuromuscular junction)|GO:0008021(synaptic vesicle) QUALITY:PATO:0000628(mislocalized) NOT"
Remark	"Eight out of eight mosaic animals expressing FSN-1(+) only in the AB lineage (not in P1 lineage) were wild-type for juIs1 synaptic marker."
Remark	"Genotype \"fsn-1(hp1);juIs1; Ex[sur-5::GFP, fsn-1(+)]\""
Remark	"Published_as fsn-1"
Reference	"WBPaper00024212"


Anatomy_function : "WBbtf1060"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000102"
Gene	"WBGene00001499"
Not_involved	"WBbt:0006874"	Insufficient
Remark	"All twelve animals that express FSN-1(+) only in the P1 lineage (not in AB lineage) displayed fsn-1-like juIs1 defects."
Remark	"ENTITY:WBbt:0005190(GABAergic neuron)|GO:0031594(neuromuscular junction)|GO:0008021(synaptic vesicle) QUALITY:PATO:0000628(mislocalized)"
Remark	"Genotype \"fsn-1(hp1);juIs1; Ex[sur-5::GFP, fsn-1(+)]\""
Remark	"Published_as fsn-1"
Reference	"WBPaper00024212"


Anatomy_function : "WBbtf1061"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000107"
Gene	"WBGene00007772"
Not_involved	"WBbt:0005784"	Unnecessary
Remark	"Although we were not able to find any animals that lost the transgene only in the germline precursor P2, we did find one animal that lost the transgene in P2 but had a second loss later in the E lineage. This animal exhibited a wild-type phenotype, suggesting that egrh-1 function is not required in the germline."
Remark	"ENTITY:WBbt:0007849(hermaphrodite)|GO:0030728(ovulation) QUALITY:PATO:0000694(premature)"
Remark	"Genotype \"egrh-1(tm1736); CuEx531[egrh-1(+) sur-5::gfp]\""
Remark	"Published_as egrh-1"
Reference	"WBPaper00037082"


Anatomy_function : "WBbtf1062"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001661"
Gene	"WBGene00003822"
Not_involved	"WBbt:0005671"	Insufficient
Remark	"Because the odr-3 promoter is reproducibly expressed in both AWC and AWB neurons, it is possible that nsy-1 expression in AWB rescues AWC cell fate. To rule out this possibility, we examined mosaic animals that expressed odr-3::NSY-1 in the AWB neurons but not the AWC neurons. Mosaic animals arose through the random loss of extrachromosomal arrays containing both odr-3::NSY-1 and the marker odr-1::RFP in a nsy-1 mutant background. str-2::GFP asymmetry was rescued when the arrays were present in AWC neurons, but not when they were present only in AWB neurons."
Remark	"ENTITY:WBbt:0005832(AWC-ON)|GO:0009855(determination of bilateral asymmetry)"
Remark	"QUALITY:PATO:0002051(increased occurrence)"
Remark	"Genotype \"nsy-1(n397); Ex[odr-3::NSY-1 elt-2::GFP odr-1::RFP]\""
Remark	"Published_as nsy-1"
Reference	"WBPaper00004669"


Anatomy_function : "WBbtf1063"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001661"
Gene	"WBGene00006779"
Not_involved	"WBbt:0005671"	Insufficient
Remark	"Because the odr-3 promoter is reproducibly expressed in both AWC and AWB neurons, it is possible that unc-43 expression in AWB rescues AWC cell fate. To rule out this possibility, we examined mosaic animals that expressed odr-3::UNC-43 in the AWB neurons but not the AWC neurons. Mosaic animals arose through the random loss of extrachromosomal arrays containing both odr-3::UNC-43 and the marker odr-1::RFP in a unc-43 mutant background. str-2::GFP asymmetry was rescued when the arrays were present in AWC neurons, but not when they were present only in AWB neurons."
Remark	"ENTITY:WBbt:0005832(AWC-ON)|GO:0009855(determination of bilateral asymmetry)"
Remark	"QUALITY:PATO:0002051(increased occurrence)"
Remark	"Genotype \"unc-43(n1186); Ex[odr-3::UNC-43 elt-2::GFP odr-1::RFP]\""
Remark	"Published_as unc-43"
Reference	"WBPaper00004669"


Anatomy_function : "WBbtf1064"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0001038"
Gene	"WBGene00002196"
Not_involved	"WBbt:0007815"	Unnecessary
Remark	"ENTITY:WBbt:0005784(germ line)|GO:0008283(cell proliferation)"
Remark	"QUALITY:PATO:0001997(reduced)"
Remark	"Genotype \"kin-10(ok1751);glp-1(ar202gf); ugEx27[kin-10::FLAG]\""
Remark	"Published_as kin-10"
Remark	"To determine in which tissue KIN-10 functions to inhibit the proliferative fate, we performed mosaic analysis using kin-10(ok1751); glp-1(ar202gf); ugEx27[kin-10::FLAG] animals. In mosaic gonads that have no expression in the somatic gonad (including the DTC), expression in the germline is suf&amp;#64257;cient to suppress the tumorous phenotype of the kin-10(ok1751); glp-1(ar202gf) double mutant. Although we did not recover animals with speci&amp;#64257;c loss of the ugEx27 array in the germ line, gonads with robust somatic gonad KIN-10 expression, but very limited expression in the germ line, maintain over-proliferation in regions where KIN-10 expression is low or absent."
Reference	"WBPaper00045273"


Anatomy_function : "WBbtf1065"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000625"
Gene	"WBGene00004047"
Not_involved	"WBbt:0004858"	Unnecessary
Remark	"ENTITY:WBbt:0004858(DA8)|WBbt:0004857(DA9)|GO:0045202(synapse)|GO:0003002(regionalization)|GO:0048859(formation of anatomical boundary)|GO:0060386(synapse assembly involved in innervation)"
Remark	"QUALIFY:PATO:0001507(disrupted) NOT"
Remark	"Genotype \"plx-1(nc36); Ex[Pmig-13::plx-1]\""
Remark	"Published_as plx-1"
Remark	"We used a truncated unc-4 promoter (unc-4c) for expression the plx-1 cDNA in the DA motor neurons including both DA8 and DA9. The synaptic tiling phenotype in plx-1 mutants was almost completely rescued. Utilizing the mosaicism of the extrachromosomal array, we conducted genetic mosaic experiments with the Punc-4c::plx-1 transgene to clarify in which DA neurons PLX-1 functions. We found that mosaic animals that lost the rescuing array in DA9 did not rescue the plx-1 mutant phenotype, suggesting that PLX-1 is required in DA9. Consistent with these observations, PLX-1 expression in DA9, but not DA8 (Pmig-13), was also sufficient to rescue the plx-1 phenotype."
Reference	"WBPaper00042107"


Anatomy_function : "WBbtf1066"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000625"
Gene	"WBGene00004889"
Not_involved	"WBbt:0004858"	Unnecessary
Remark	"ENTITY:WBbt:0004858(DA8)|WBbt:0004857(DA9)|GO:0045202(synapse)|GO:0003002(regionalization)|GO:0048859(formation of anatomical boundary)|GO:0060386(synapse assembly involved in innervation)"
Remark	"QUALIFY:PATO:0001507(disrupted) NOT"
Remark	"Genotype \"smp-1; smp-2; Ex[Pmig-13::smp-1]\""
Remark	"Published_as smp-1"
Remark	"We used a truncated unc-4 promoter (unc-4c) for expression the smp-1 cDNA in the DA motor neurons including both DA8 and DA9. The synaptic tiling phenotype in smp-1;smp-2 double mutants was almost completely rescued. Utilizing the mosaicism of the extrachromosomal array, we conducted genetic mosaic experiments with the Punc-4c::smp-1 transgene to clarify in which DA neurons SMP-1 functions. We found that mosaic animals that lost the rescuing array in DA9 did not rescue the mutant phenotype, suggesting that SMP-1 is required in DA9. Consistent with these observations, SMP-1 expression in DA9, but not DA8 (Pmig-13), was also sufficient to rescue the smp-1; smp-2 phenotype."
Reference	"WBPaper00042107"


Anatomy_function : "WBbtf1067"
Assay	"Genetic_mosaic"
Phenotype	"WBPhenotype:0000105"
Gene	"WBGene00002189"
Not_involved	"WBbt:0007816"	Insufficient
Not_involved	"WBbt:0007816"	Unnecessary
Remark	"ENTITY:WBbt:0006797(oocyte)|GO:0001556(oocyte maturation)"
Remark	"QUALIFY:PATO:0002052(decreased occurance)"
Remark	"Genotype \"kin-1(ok338); nEx109[kin-1(+) sur-5::gfp]\""
Remark	"Published_as kin-1"
Remark	"We conducted genetic mosaic analysis using the kin-1(ok338) deletion allele. We sought array losses in the MS lineage, which gives rise to the somatic cells of the gonad. kin-1(+) somatic gonad-loss mosaics exhibit sterility because oocytes fail to undergo meiotic maturation, ovulation, and fertilization, Complex losses found within the sheath-spermathecal lineages suggest that kin-1 is needed in the gonadal sheath cells, not in the spermatheca, for meiotic maturation."
Reference	"WBPaper00041364"


Anatomy_function : "WBbtf1068"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0001048"
Not_involved	"WBbt:0005836"	Unnecessary
Remark	"ENTITY:WBbt:0005665(ASH)|CHEBI:29108(calcium(2+))|GO:0050801(ion homeostasis)|PATO:0000077(response to)|PATO:0001159(concentrated)|CHEBI:16583(diacetyl)"
Remark	"QUALITY:PATO:0001997(decrease amount)"
Remark	"Genotype \"Ex[Podr-10::mCap1]\""
Remark	"In contrast, with the exception of AIY, attraction to low concentrations (1,000X dilution) of diacetyl was unaffected by inhibition of these interneurons (AIA, AIB, AIY or AIZ)."
Reference	"WBPaper00045214"


Anatomy_function : "WBbtf1069"
Assay	"Chemogenetics"
Phenotype	"WBPhenotype:0002545"
Not_involved	"WBbt:0005835"	Unnecessary
Not_involved	"WBbt:0006834"	Unnecessary
Remark	"Genotype \"kyEx5464[Ptdc-1::HisCl1::SL2mCherry]\""
Remark	"To further interrogate the role of the RIM/RIC neurons in multisensory integration, we examined the transgenic animals that expressed a histamine-gated chloride channel in the RIM and RIC neurons under the histamine-treated condition [86] or the transgenic animals that expressed tetanus toxin [58] in RIM and RIC. We found that these transgenic animals were normal in leaving the OP50 lawn when 2-nonanone was present (Fig 4E and 4F)."
Reference	"WBPaper00056328"


Anatomy_function : "WBbtf1070"
Assay	"Neuronal_genetics"
Phenotype	"WBPhenotype:0002545"
Not_involved	"WBbt:0005835"	Unnecessary
Not_involved	"WBbt:0006834"	Unnecessary
Remark	"Genotype \"kyEx4962[Ptdc-1::TeTx::mCherry]\""
Remark	"To further interrogate the role of the RIM/RIC neurons in multisensory integration, we examined the transgenic animals that expressed a histamine-gated chloride channel in the RIM and RIC neurons under the histamine-treated condition [86] or the transgenic animals that expressed tetanus toxin [58] in RIM and RIC. We found that these transgenic animals were normal in leaving the OP50 lawn when 2-nonanone was present (Fig 4E and 4F)."
Reference	"WBPaper00056328"


Anatomy_function : "WBbtf1071"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0002545"
Involved	"WBbt:0005413"	Necessary
Remark	"Genotype \"ttx-3(mg158)\""
Remark	"To disrupt the function of AIY, we selectively expressed in AIY a gain-of-function isoform of a potassium channel TWK-18 [57] to inhibit the activity of AIY (Pttx-3::twk-18(gf)) or the tetanus toxin (Pttx-3::TeTx) to block the synaptic release. We also tested the ttx-3(mg158) mutants that fail to develop AIY interneurons [88]. All three mutations delayed the decision to leave the lawn (Fig 5A*5C)."
Reference	"WBPaper00056328"


Anatomy_function : "WBbtf1072"
Assay	"Neuronal_genetics"
Phenotype	"WBPhenotype:0002545"
Involved	"WBbt:0005413"	Necessary
Remark	"Genotype \"yxEx1248[Pttx-3::twk18(gf)::mCherry;Punc-122::RFP]\""
Remark	"To disrupt the function of AIY, we selectively expressed in AIY a gain-of-function isoform of a potassium channel TWK-18 [57] to inhibit the activity of AIY (Pttx-3::twk-18(gf)) or the tetanus toxin (Pttx-3::TeTx) to block the synaptic release. We also tested the ttx-3(mg158) mutants that fail to develop AIY interneurons [88]. All three mutations delayed the decision to leave the lawn (Fig 5A*5C)."
Reference	"WBPaper00056328"


Anatomy_function : "WBbtf1073"
Assay	"Neuronal_genetics"
Phenotype	"WBPhenotype:0002545"
Involved	"WBbt:0005413"	Necessary
Remark	"Genotype \"yxIs25[Pttx-3::TeTx::mCherry;Punc-122::gfp]\""
Remark	"To disrupt the function of AIY, we selectively expressed in AIY a gain-of-function isoform of a potassium channel TWK-18 [57] to inhibit the activity of AIY (Pttx-3::twk-18(gf)) or the tetanus toxin (Pttx-3::TeTx) to block the synaptic release. We also tested the ttx-3(mg158) mutants that fail to develop AIY interneurons [88]. All three mutations delayed the decision to leave the lawn (Fig 5A*5C)."
Reference	"WBPaper00056328"


Anatomy_function : "WBbtf1074"
Assay	"Neuronal_genetics"
Phenotype	"WBPhenotype:0002545"
Not_involved	"WBbt:0006813"	Unnecessary
Remark	"Genotype \"kyEx4779[Pinx-1::TeTx::mCherry;Punc-122::gfp]\""
Remark	"In contrast, selectively expressing the tetanus toxin in the AIB interneurons or treating the transgenic animals expressing the histamine-gated chloride channel in AIB with histamine did not significantly alter the decision to leave the OP50 lawn that was paired with 2-nanonone (Fig 5D and 5E)."
Reference	"WBPaper00056328"


Anatomy_function : "WBbtf1075"
Assay	"Chemogenetics"
Phenotype	"WBPhenotype:0002545"
Not_involved	"WBbt:0006813"	Unnecessary
Remark	"Genotype \"kyEx4866[Pinx-1::HisCl1::SL2mCherry;Punc-122::dsRed]\""
Remark	"In contrast, selectively expressing the tetanus toxin in the AIB interneurons or treating the transgenic animals expressing the histamine-gated chloride channel in AIB with histamine did not significantly alter the decision to leave the OP50 lawn that was paired with 2-nanonone (Fig 5D and 5E)."
Reference	"WBPaper00056328"


Anatomy_function : "WBbtf1076"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000012"
Involved	"WBbt:0005667"	Necessary
Involved	"WBbt:0005666"	Necessary
Involved	"WBbt:0005664"	Necessary
Involved	"WBbt:0005660"	Necessary
Remark	"Noctua Model \"gomodel:5fa76ad400000494\""
Remark	"Author Statement \"When the amphid cells ADF, ASG, ASI, and ASJ were all killed in single animals, 30 of 37 animals became dauer larvae (Table 1).\""
Reference	"WBPaper00001393"


Anatomy_function : "WBbtf1077"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000012"
Involved	"WBbt:0005666"	Sufficient
Remark	"Author Statement \"The killing of combinations of three of the four cell types ADF, ASG, ASI, and ASJ revealed functional differences among these cells. The deaths of ADF and ASI were crucial to the formation of dauer larvae. If either ADF or ASI neurons were alive, the aminals developed to adulthood exactly as did mock-ablated controls.\""
Reference	"WBPaper00001393"


Anatomy_function : "WBbtf1078"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000012"
Involved	"WBbt:0005660"	Sufficient
Remark	"Author Statement \"The killing of combinations of three of the four cell types ADF, ASG, ASI, and ASJ revealed functional differences among these cells. The deaths of ADF and ASI were crucial to the formation of dauer larvae. If either ADF or ASI neurons were alive, the aminals developed to adulthood exactly as did mock-ablated controls.\""
Reference	"WBPaper00001393"


Anatomy_function : "WBbtf1079"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000408"
Involved	"WBbt:0005667"	Sufficient
Remark	"Author Statement \"When the other three cell types were killed but ASJ was left intact, the animals passed through a dauer stage transiently (Table 1). Unlike similar dauer larvae that formed after ADF, ASG, ASI, and ASJ were killed, the animals in which ADF, ASG, and ASI were killed recovered from the dauer stage after less than 1 day and developed to adulthood.\""
Reference	"WBPaper00001393"


Anatomy_function : "WBbtf1080"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000408"
Involved	"WBbt:0005667"	Necessary
Remark	"Author Statement \"However, after the ASJ cells were killed, recovery from the dauer stage was inefficient (Table 2); many animals were unable to recover, and those that could did so more slowly than unoperated controls.\""
Reference	"WBPaper00001393"


Anatomy_function : "WBbtf1081"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000847"	Autonomous
Gene	"WBGene00003980"
Involved	"WBbt:0005413"	Sufficient
Remark	"Genotype \"cima-1(wy84);pes-7(gk123);Ex[Pttx-3::pes-7]\""
Remark	"Genotype \"cima-1(wy84);pes-7(gk123);Ex[Pmod-1::pes-7]\""
Remark	"Author Statement \"Next, we expressed cdc-42 or pes-7 cDNA with tissue-specific promoters in the corresponding double mutants. We found that driving either of them expression with its own promoter, the pan-neuronal promoter (Prab-3), or the AIY specific promoters (Pttx-3 or Pmod-1) rescues and restores the ectopic synapses and the intensity of synaptic markers (Figures 3A-3P).\""
Reference	"WBPaper00059357"


Anatomy_function : "WBbtf1082"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000847"	Autonomous
Gene	"WBGene00000390"
Involved	"WBbt:0005413"	Sufficient
Remark	"Genotype \"cima-1(wy84);cdc-42(ok825);Ex[Pmod-1:cdc-42]\""
Remark	"Genotype \"cima-1(wy84);cdc-42(ok825);Ex[Pttx-3-1:cdc-42]\""
Remark	"Author Statement \"Next, we expressed cdc-42 or pes-7 cDNA with tissue-specific promoters in the corresponding double mutants. We found that driving either of them expression with its own promoter, the pan-neuronal promoter (Prab-3), or the AIY specific promoters (Pttx-3 or Pmod-1) rescues and restores the ectopic synapses and the intensity of synaptic markers (Figures 3A-3P)\""
Reference	"WBPaper00059357"


Anatomy_function : "WBbtf1083"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000847"
Gene	"WBGene00000390"
Not_involved	"WBbt:0006804"	Insufficient
Remark	"Genotype \"cima-1(wy84);cdc-42(ok825) ;Ex[Pmyo-3::cdc-42]\""
Remark	"Author Statement \"Next, we expressed cdc-42 or pes-7 cDNA with tissue-specific promoters in the corresponding double mutants. We found that driving either of them expression with its own promoter, the pan-neuronal promoter (Prab-3), or the AIY specific promoters (Pttx-3 or Pmod-1) rescues and restores the ectopic synapses and the intensity of synaptic markers (Figures 3A-3P), while driving cdc-42 or pes-7 under body-wall muscle-, intestine-, or epidermis-specific promoters (Pmyo-3, Pges-1, Pdpy-7 respectively) does not (Figures 3M-3P).\""
Reference	"WBPaper00059357"


Anatomy_function : "WBbtf1084"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000847"
Gene	"WBGene00000390"
Not_involved	"WBbt:0005792"	Insufficient
Remark	"Genotype \"cima-1(wy84);cdc-42(ok825) ;Ex[Pges-1::cdc-42]\""
Remark	"Author Statement \"Next, we expressed cdc-42 or pes-7 cDNA with tissue-specific promoters in the corresponding double mutants. We found that driving either of them expression with its own promoter, the pan-neuronal promoter (Prab-3), or the AIY specific promoters (Pttx-3 or Pmod-1) rescues and restores the ectopic synapses and the intensity of synaptic markers (Figures 3A-3P), while driving cdc-42 or pes-7 under body-wall muscle-, intestine-, or epidermis-specific promoters (Pmyo-3, Pges-1, Pdpy-7 respectively) does not (Figures 3M-3P).\""
Reference	"WBPaper00059357"


Anatomy_function : "WBbtf1085"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000847"
Gene	"WBGene00000390"
Not_involved	"WBbt:0007846"	Insufficient
Remark	"Genotype \"cima-1(wy84);cdc-42(ok825) ;Ex[Pdpy-7::cdc-42]\""
Remark	"Author Statement \"Next, we expressed cdc-42 or pes-7 cDNA with tissue-specific promoters in the corresponding double mutants. We found that driving either of them expression with its own promoter, the pan-neuronal promoter (Prab-3), or the AIY specific promoters (Pttx-3 or Pmod-1) rescues and restores the ectopic synapses and the intensity of synaptic markers (Figures 3A-3P), while driving cdc-42 or pes-7 under body-wall muscle-, intestine-, or epidermis-specific promoters (Pmyo-3, Pges-1, Pdpy-7 respectively) does not (Figures 3M-3P).\""
Reference	"WBPaper00059357"


Anatomy_function : "WBbtf1086"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000847"
Gene	"WBGene00003980"
Not_involved	"WBbt:0006804"	Insufficient
Remark	"Genotype \"cima-1(wy84);pes-7(gk123);Ex[Pmyo-3::pes-7]\""
Remark	"Author Statement \"Next, we expressed cdc-42 or pes-7 cDNA with tissue-specific promoters in the corresponding double mutants. We found that driving either of them expression with its own promoter, the pan-neuronal promoter (Prab-3), or the AIY specific promoters (Pttx-3 or Pmod-1) rescues and restores the ectopic synapses and the intensity of synaptic markers (Figures 3A-3P), while driving cdc-42 or pes-7 under body-wall muscle-, intestine-, or epidermis-specific promoters (Pmyo-3, Pges-1, Pdpy-7 respectively) does not (Figures 3M-3P).\""
Reference	"WBPaper00059357"


Anatomy_function : "WBbtf1087"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000847"
Gene	"WBGene00003980"
Not_involved	"WBbt:0005792"	Insufficient
Remark	"Genotype \"cima-1(wy84);cdc-42(ok825) ;Ex[Pges-1::cdc-42]\""
Remark	"Author Statement \"Next, we expressed cdc-42 or pes-7 cDNA with tissue-specific promoters in the corresponding double mutants. We found that driving either of them expression with its own promoter, the pan-neuronal promoter (Prab-3), or the AIY specific promoters (Pttx-3 or Pmod-1) rescues and restores the ectopic synapses and the intensity of synaptic markers (Figures 3A-3P), while driving cdc-42 or pes-7 under body-wall muscle-, intestine-, or epidermis-specific promoters (Pmyo-3, Pges-1, Pdpy-7 respectively) does not (Figures 3M-3P).\""
Reference	"WBPaper00059357"


Anatomy_function : "WBbtf1088"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000847"
Gene	"WBGene00003980"
Not_involved	"WBbt:0007846"	Insufficient
Remark	"Genotype \"cima-1(wy84);cdc-42(ok825) ;Ex[Pdpy-7::cdc-42]\""
Remark	"Author Statement \"Next, we expressed cdc-42 or pes-7 cDNA with tissue-specific promoters in the corresponding double mutants. We found that driving either of them expression with its own promoter, the pan-neuronal promoter (Prab-3), or the AIY specific promoters (Pttx-3 or Pmod-1) rescues and restores the ectopic synapses and the intensity of synaptic markers (Figures 3A-3P), while driving cdc-42 or pes-7 under body-wall muscle-, intestine-, or epidermis-specific promoters (Pmyo-3, Pges-1, Pdpy-7 respectively) does not (Figures 3M-3P).\""
Reference	"WBPaper00059357"


Anatomy_function : "WBbtf1089"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000386"	Autonomous
Gene	"WBGene00000467"
Involved	"WBbt:0006796"	Sufficient
Involved	"WBbt:0006796"	Necessary
Remark	"GIGA = Gliadin-induced germ cell apoptosis"
Remark	"Author Statement \"cep-1 depletion by RNAi in rrf-1 mutants suppressed GIGA, as observed in cep-1 mutants (Figure 8A and Figure 9A). Conversely, depletion of cep-1 by RNAi in the ppw-1 mutants did not suppress GIGA (Figure 9A). These results clearly indicate that cep-1 is required in the germ line, but not in somatic cells, for normal levels of GIGA.\""
Reference	"WBPaper00058851"


Anatomy_function : "WBbtf1090"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000012"
Gene	"WBGene00003407"
Involved	"WBbt:0005451"	Sufficient
Involved	"WBbt:0003679"	Sufficient
Involved	"WBbt:0005792"	Sufficient
Remark	"Author Statement \"Expression of MRP-1 in only one tissue (neurons, intestinal cells or pharyngeal muscles) rescued the dauer larva formation abnormality only weakly. By contrast, the abnormality was rescued efficiently by expressing MRP-1 in two or three tissues (Fig. 6).\""
Reference	"WBPaper00026626"


Anatomy_function : "WBbtf1091"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000637"
Gene	"WBGene00003508"
Involved	"WBbt:0005661"	Sufficient
Remark	"Rescue observed in high pheromone condition. Annotated by Pranjal Garg."
Remark	"Author Statement \"As predicted, we observed that expression of mut-16::gfp in ADL neurons also resulted in a significant rescue of the mut-16 daf-d phenotype, while expression in AWA neurons resulted in no rescue (Figure 4A).\""
Reference	"WBPaper00050683"


Anatomy_function : "WBbtf1092"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000637"
Gene	"WBGene00003508"
Involved	"WBbt:0005667"	Sufficient
Involved	"WBbt:0005666"	Sufficient
Remark	"Expression of mut-16 in ASI or ASJ is sufficient to rescue mut-1 mutants. Annotated by Pranjal Garg."
Remark	"The rescue is observed in high pheromone environmental condition."
Remark	"Author Statement \"We found that expression of mut-16::gfp in ASI and ASJ neurons in the mut-16(pk710) strain resulted in significantly greater number of dauers compared to mut-16(pk710) without the transgene.\""
Reference	"WBPaper00050683"


Anatomy_function : "WBbtf1093"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0002232"	Autonomous
Gene	"WBGene00004134"
Involved	"WBbt:0005270"	Necessary
Remark	"Annotated by Pranjal Garg"
Remark	"Genotype \"gfp::myrf-1::3xFlag(ybq14) II gfp::myrf-2(ybq46)\""
Remark	"Author Statement \"myrf-1(1-790 GFP) allele, in which a part of the extracellular domain of MYRF was removed, exhibited blocked synaptic rewiring under myrf-2 null background (Figure 6; Figure 6-figure supplements 1-12), a phenotype similarly observed in myrf-1(ybq6).\""
Reference	"WBPaper00061377"


Anatomy_function : "WBbtf1094"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0002232"	Autonomous
Gene	"WBGene00004134"
Involved	"WBbt:0005270"	Necessary
Remark	"This is in contrast to myrf-1 (1-790 GFP) allele, where only a part of extracellular domain of MYRF is removed. This showed blocked synaptic rewiring."
Remark	"Genotype \"gfp::myrf-1::3xFlag(ybq14) II\""
Remark	"Author Statement \"Notably, the precocious dorsal synapses in myrf-11-700 GFP mutants were not uniformly distributed along the dorsal cord, that is in some DDs the remodeling occurred while in the rest the remodeling did not, even though they were in the same animal, implying that the observed precocity in myrf-1 (1-700 GFP) mutants was not a strictly regulated event.\""
Remark	"Author Statement \"In contrast, myrf-1 (1-700 GFP) allele, in which the whole extracellular region of MYRF is lost, exhibited precocious synaptic rewiring, that is clearly detectable synaptic puncta formed in the dorsal processes of DDs at 12, 14 post-hatch hours, time points by which synaptic rewiring has not occurred yet in wild type animals (Figure 6; Figure 6-figure supplements 1-12).\""
Reference	"WBPaper00061377"


Anatomy_function : "WBbtf1095"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000436"	Autonomous
Gene	"WBGene00004134"
Involved	"WBbt:0005270"	Necessary
Remark	"The extracellular domain of both myrf-1 and myrf-2 are necessary for localization of MYRF. Annotated by Pranjal Garg"
Remark	"Genotype \"gfp::myrf-1::3xFlag(ybq14) II gfp::myrf-2(ybq46)\""
Remark	"Author Statement \"We generated an in- frame deletion allele of myrf-11-700 GFP that removed the entire extracellular domain from MYRF-1 (Figure 8A).\""
Remark	"Author Statement \"Importantly, MYRF-1 (1-700 GFP) displayed prominent cytoplasmic signals while its cell-membrane or nuclear localization were not obvious at any viable stages (Figure 8D-F; Figure 8-figure supplement 1), showing that the extracellular domain is required for MYRF's proper localization.\""
Reference	"WBPaper00061377"


Anatomy_function : "WBbtf1096"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0002232"	Autonomous
Gene	"WBGene00003915"
Involved	"WBbt:0005270"	Sufficient
Remark	"Genotype \"Punc-25-mCherry::Rab-3(juIs236)/mT1 II,pan-1(gk142)/mT1 III; Punc-25-pan-1b::gfp(ybqIs131) Punc-25-mCherry::Rab-3(juIs236)/mT1II; pan-1(gk142)/mT1 III; Pflp-13-pan-1b:gfp(ybqEx821)\""
Remark	"Author Statement \"To confirm that loss of pan-1 is responsible for synaptic remodeling defects in pan-1 mutants, we performed rescue experiments by expressing pan-1 in DD neurons (Figure 2A,B;Figure 2-figure supplement 1A,B). Expression of longest isoform pan-1b driven by unc-25pro (expressed in DD and VD) restored the synaptic remodeling defects in pan-1mutants. Furthermore, expression of pan-1 (referring to pan-1b hereafter) driven by flp-13pro (expressed in DD not VD among ventral cord motor neurons) also rescued synaptic rewiring defects in pan-1 mutants (Figure 2-figure supplement 1A).\""
Reference	"WBPaper00061377"


Anatomy_function : "WBbtf1097"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0002232"	Autonomous
Gene	"WBGene00003915"
Involved	"WBbt:0005270"	Sufficient
Remark	"pan-1 has three isoforms- pan 1a, pan 1b, pan-1c Annotated by Pranjal Garg"
Remark	"Genotype \"Punc-25-mCherry::Rab-3(juIs236)/mT1 II, pan-1(gk142)/mT1 III; Punc-25-pan-1a (ybqEx624)\""
Remark	"Author Statement \"Expression of longest isoform pan-1b driven by unc-25pro (expressed in DD and VD) restored the synaptic remodeling defects in pan-1 mutants, while the other two isoforms, pan-1a or pan-1c could not (Figure 2B).\""
Reference	"WBPaper00061377"


Anatomy_function : "WBbtf1098"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000436"	Autonomous
Gene	"WBGene00008999"
Involved	"WBbt:0005270"	Necessary
Remark	"The extracellular domain of both myrf-1 and myrf-2 are necessary for localization of MYRF. Annotated by Pranjal Garg"
Remark	"Genotype \"gfp::myrf-2(ybq46) X\""
Remark	"Author Statement \"	 Using a similar strategy, we analyzed an in-frame deletion allele myrf-2 (1-728 GFP) and found that the extracellular region of MYRF-2 was necessary for MYRF-2's cell membrane localization because MYRF-2 (1-728) was primarily detected in cytoplasm (Figure 8-figure supplement 2).\""
Reference	"WBPaper00061377"


Anatomy_function : "WBbtf1099"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0002232"
Gene	"WBGene00003915"
Not_involved	"WBbt:0005733"	Insufficient
Remark	"The expression of pan-1b in epidermis did not rescue the pan-1 null mutants from synaptic rewiring defects in contrast to expression of pan-1b in DD neurons. Annotated by Pranjal Garg"
Remark	"Genotype \"Punc-25-mCherry::Rab-3(juIs236) /mT1 II, pan-1(gk142)/mT1 III\""
Remark	"Author Statement \"In contrast, specific expression of pan-1 in muscles, epidermis, or intestine did not mitigate the deficient synaptic remodeling in pan-1(0) (Figure 2-figure supplement 1B).\""
Reference	"WBPaper00061377"


Anatomy_function : "WBbtf1100"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0002232"
Gene	"WBGene00003915"
Not_involved	"WBbt:0005772"	Insufficient
Remark	"The expression of pan-1b in intestine did not rescue the pan-1 null mutants from synaptic rewiring defects in contrast to expression of pan-1b in DD neurons. Annotated by Pranjal Garg"
Remark	"Genotype \"Punc-25-mCherry::Rab-3(juIs236) /mT1 II, pan-1(gk142)/mT1 III\""
Remark	"Author Statement \"In contrast, specific expression of pan-1 in muscles, epidermis, or intestine did not mitigate the deficient synaptic remodeling in pan-1(0).\""
Reference	"WBPaper00061377"


Anatomy_function : "WBbtf1101"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000637"
Involved	"WBbt:0005666"	Necessary
Remark	"AM251 is the antagonist of human cannabinoid receptor. Annotated by Pranjal Garg."
Remark	"Author Statement \"Ablation of the ASI neuron strongly reduced the ability of AM251 to promote reproductive growth (Figure 4A), but loss of the ASJ neuron had no effect (Figure 4B). These data show that the effect of AM251 in suppressing dauer entry is mediated via the ASI neuron.\""
Reference	"WBPaper00049436"


Anatomy_function : "WBbtf1102"
Involved	"WBbt:0005667"	Necessary
Remark	"Results show that the signals from cell body and axon promote dauer entry. Annotated by Pranjal Garg"


Anatomy_function : "WBbtf1103"
Not_involved	"WBbt:0005668"	Unnecessary
Not_involved	"WBbt:0006976"	Unnecessary
Remark	"Annotated by Pranjal Garg."


Anatomy_function : "WBbtf1104"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000637"
Involved	"WBbt:0005667"	Necessary
Remark	"Results show that the signals from cell body and axon promote dauer entry. Annotated by Pranjal Garg"
Remark	"Author Statement \"We performed surgeries at 4 hr after hatching on the ASJ cell body, dendrite, and axon to determine their roles in daf-11 dauer entry signaling. When assayed at 25 C, significantly (p < 10?4) lower percentages of L+R whole-cell-ablated and L+R dendrite-cut daf-11 mutants enter dauer compared to mock animals (Figure 3A).\""
Reference	"WBPaper00043943"


Anatomy_function : "WBbtf1105"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000637"
Not_involved	"WBbt:0005668"	Unnecessary
Not_involved	"WBbt:0006976"	Unnecessary
Remark	"Annotated by Pranjal Garg."
Remark	"Author Statement \"Interestingly, surgeries on the ASK or PVQ neurons, the postsynaptic partners of the ASJ, did not significantly change dauer entry, suggesting that the signal might be secreted from the ASJ axon rather than synaptically mediated.\""
Reference	"WBPaper00043943"


Anatomy_function : "WBbtf1106"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000637"
Gene	"WBGene00003970"
Involved	"WBbt:0005666"	Sufficient
Remark	"Annotated by Pranjal Garg"
Remark	"Genotype \"daf-28(sa191);pek-1(ok275)\""
Remark	"Author Statement \"Consistent with this expectation, ASI-specific expression of pek-1 was able to restore the constitutive dauer entry phenotype of the daf-28(sa191);pek-1(ok275) mutant, demonstrating that PEK-1 activation by ER stress in the ASI neuron pair is sufficient to promote entry into dauer diapause.\""
Reference	"WBPaper00044570"


Anatomy_function : "WBbtf1107"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000637"	Autonomous
Gene	"WBGene00021351"
Involved	"WBbt:0005666"	Sufficient
Remark	"Annotated by Pranjal Garg."
Remark	"Genotype \"daf-28(sa191);pek-1(ok275)\""
Remark	"Author Statement \"	 We introduced the ASI-specific phosphomimetic eIF2a(S49D) transgene into the daf-28(sa191);pek-1(ok275) mutant and found that this transgene substantially restored the constitutive dauer entry phenotype of the daf-28(sa191) mutant that was suppressed by pek-1(ok275).\""
Reference	"WBPaper00044570"


Anatomy_function : "WBbtf1108"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000637"	Autonomous
Gene	"WBGene00021351"
Involved	"WBbt:0005666"	Sufficient
Remark	"Annotated by Pranjal Garg"
Remark	"Genotype \"daf-28(sa191)\""
Remark	"Author Statement \"We overexpressed an unphosphorylatable version of eIF2a(S49A) specifically in the ASI neurons of the daf-28(sa191) mutant and observed partial suppression of the constitutive dauer entry phenotype\""
Reference	"WBPaper00044570"


Anatomy_function : "WBbtf1109"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000637"
Involved	"WBbt:0005664"	Sufficient
Involved	"WBbt:0005660"	Sufficient
Involved	"WBbt:0005666"	Sufficient
Remark	"In daf-11(sa195): When all exposed amphid neurons are left intact- number of dauers/ total = 121/126. When exposed amphid neurons left intact are ADF, ASI, ASG- number of dauers/ total = 0/5. In daf-11(m87): When all exposed amphid neurons are left intact- number of dauers/ total = 14/15. When exposed amphid neurons left intact are ADF, ASI, ASG- number of dauers/ total = 1/6. Annotated by Pranjal Garg"
Remark	"Genotype \"daf-11(sa195), daf-11(m87)\""
Remark	"Author Statement \"These neurons were also sufficient to prevent dauer formation in two daf-11 mutants, suggesting that daf-11 does not disrupt ADF, ASI, or ASG function.\""
Remark	"Author Statement \"We killed AFD and all exposed amphid neurons except for ADF, ASI, and ASG in the wild type and in Daf-c mutants and determined whether dauer formation was still repressed (Table 1). Though not exposed to the environment, AFD was included because it regulates response to temperature (22), an important modulator of dauer formation (13). As previously reported (4), we found that isolated ADF, ASI, and ASG neurons were sufficient to prevent dauer formation in the wild type\""
Reference	"WBPaper00002586"


Anatomy_function : "WBbtf1110"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000012"
Involved	"WBbt:0005667"	Necessary
Remark	"Complete suppression of gene expression was not observed. Annotated by Pranjal Garg."
Remark	"Author Statement \"To determine which amphid neurons were responsible for the suppression of daf-11, each neuron class was killed individually in a daf-11 mutant (Figure 3A). Only killing ASJ resulted in statistically significant suppression of the daf-11 Daf-c phenotype (p < 0.0001).\""
Reference	"WBPaper00002586"


Anatomy_function : "WBbtf1111"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000637"
Involved	"WBbt:0005667"	Necessary
Remark	"Annotated by Pranjal Garg"
Remark	"Author Statement \"We killed ASJ in the wild type and exposed the animals to several different concentrations of pheromone. At each pheromone concentration, killing ASJ significantly impaired the ability of wild-type animals to form dauers (Figure 5). We conclude that the activity of ASJ contributes to the activation of dauer formation in the wild type.\""
Reference	"WBPaper00002586"


Anatomy_function : "WBbtf1112"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000637"
Involved	"WBbt:0005667"	Necessary
Remark	"This showed that suppression of daf-c phenotype is not specific to daf-11. Annotated by Pranjal Garg."
Remark	"Author Statement \"Killing ASJ suppressed dauer formation for two additional alleles of daf-11 (m84 and m87), as well as for daf-21(p673), another group 1 Daf-c mutation (Figure 4A).\""
Reference	"WBPaper00002586"


Anatomy_function : "WBbtf1113"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000877"	Autonomous
Gene	"WBGene00006652"
Involved	"WBbt:0006754"	Sufficient
Remark	"Amphid sheath published as AMsh. Annotated by Pranjal Garg"
Remark	"Genotype \"ttx- 1(p767); daf-7(e1372); glia::ttx1 (nsIs219), daf-7(e1372); ttx- 1(p767), daf-7(e1372); ttx-1(oy26)\""
Remark	"Author Statement \"As shown in Fig. 2E, AMsh glia fusion failed to occur in almost all daf-7(e1372); ttx- 1(p767) and daf-7(e1372); ttx-1(oy26) double-mutant dauer animals scored using the cytoplasmic mixing assay\""
Remark	"Author Statement \"Restoring ttx-1 in AMsh glia, however, rescued AMsh glia fusion (Fig. 2E) but not thermotaxis or AFD morphology (see Fig. S4A,D,E,I in the supplementary material).\""
Reference	"WBPaper00038156"


Anatomy_function : "WBbtf1114"
Assay	"Expression_mosaic"
Phenotype	"WBPhenotype:0000135"	Autonomous
Gene	"WBGene00006652"
Involved	"WBbt:0006754"	Sufficient
Remark	"Done in non dauer adult animals. Annotated by Pranjal Garg."
Remark	"Author Statement \"The induction of ver-1 expression by temperature was, however, dependent on ttx-1, as animals containing ttx-1 mutations failed to express the ver-1 promoter::gfp reporter at high temperatures (Fig. 6B). Restoring ttx-1 specifically in glia rescued temperature-dependent ver-1 expression, whereas restoring ttx-1 in AFD neurons did not (Table 1).\""
Reference	"WBPaper00038156"


Anatomy_function : "WBbtf1115"
Assay	"Genetic_ablation"
Phenotype	"WBPhenotype:0000717"	Autonomous
Not_involved	"WBbt:0005662"	Unnecessary
Remark	"Amphid sheath published as AMsh. Annotated by Pranjal Garg"
Remark	"Author Statement \"To determine whether temperature control of ver-1 expression was mediated by the sensory neurons associated with the AMsh glia, we genetically ablated both thermosensory AFD neurons and observed no defect in ver-1 expression (Table 1).\""
Reference	"WBPaper00038156"


Anatomy_function : "WBbtf1116"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000877"
Not_involved	"WBbt:0005672"	Unnecessary
Remark	"Amphid Sheath glial cell fusion is independent of signals from AWC neurons. Annotated by Pranjal Garg."
Remark	"Genotype \"daf-7(e1372); AWC::yfp (oyIs45)\""
Remark	"Author Statement \"we ablated the two AWC neurons using a laser microbeam in first-stage daf-7(e1372) larvae that were mosaic for AMsh glia::gfp expression and that expressed an AWC promoter::yfp reporter (oyIs45). Ablated animals were then induced to become dauers by incubation at 25&deg;C for 48 hours, and glial fusion was monitored using the cytoplasmic mixing assay. We found that mock-ablated animals had a high rate of fusion (89%; n=36), perhaps a result of the strain background. Importantly, in animals where both AWC neurons were ablated, we saw no significant decrease in glial cell fusion (81%; n=26; P=0.47, Fisher's exact test).\""
Reference	"WBPaper00038156"


Anatomy_function : "WBbtf1117"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000127"
Involved	"WBbt:0005118"	Necessary
Remark	"Annotated by Pranjal Garg"
Remark	"Genotype \"daf-7(e1372)\""
Remark	"Author Statement \"Moreover, laser ablation of the IL2 neurons (which express the Notch ligand lag-2) prior to dauer entry in a daf-7(e1372) mutant background also leads to dauer maintenance defects that are comparable to those observed in a daf-7; lag-2 double mutant background (Table 2).\""
Reference	"WBPaper00031997"


Anatomy_function : "WBbtf1118"
Assay	"Laser_ablation"
Phenotype	"WBPhenotype:0000127"
Involved	"WBbt:0005672"	Necessary
Remark	"Annotated by Pranjal Garg"
Remark	"Genotype \"glp-1(e2141) daf-7(e1372)\""
Remark	"Author Statement \"	 These neurons are crucial for dauer recovery, as ablation of the AWC neurons in a glp-1(e2141) daf-7(e1372) mutant background suppressed their premature recovery/dauer maintenance defect (Table 2).\""
Reference	"WBPaper00031997"