SynMuv Genes Redundantly Inhibit lin-3/EGF Expression to Prevent Inappropriate Vulval Induction in C. elegans

Cui, Mingxue; Chen, Jun; Myers, Toshia R.; Hwang, Byung Joon; Sternberg, Paul W.; Greenwald, Iva; Han, Min

doi:10.1016/j.devcel.2006.04.001

Cited by 99 publications

(136 citation statements)

References 39 publications

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“…Adult or L4 worms were used for counting intestinal nuclei in strains containing elt-2::gfp/LacZ reporter. RNAi by feeding was performed as described (7 13-dependent genes that we tested by real-time RT-PCR, sod-3, had an increased expression in unc-13(e1091) background compared with wild type (data not shown). However, its expression was even higher in the lin-35unc-13 strain.…”

Section: Methodsmentioning

confidence: 99%

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RNA interference and retinoblastoma-related genes are required for repression of endogenous siRNA targets in Caenorhabditis elegans

Grishok

Hoersch

Sharp

2008

Proc. Natl. Acad. Sci. U.S.A.

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In Caenorhabditis elegans , a vast number of endogenous short RNAs corresponding to thousands of genes have been discovered recently. This finding suggests that these short interfering RNAs (siRNAs) may contribute to regulation of many developmental and other signaling pathways in addition to silencing viruses and transposons. Here, we present a microarray analysis of gene expression in RNA interference (RNAi)-related mutants rde-4 , zfp-1 , and alg-1 and the retinoblastoma (Rb) mutant lin-35 . We found that a component of Dicer complex RDE-4 and a chromatin-related zinc finger protein ZFP-1, not implicated in endogenous RNAi, regulate overlapping sets of genes. Notably, genes a) up-regulated in the rde-4 and zfp-1 mutants and b) up-regulated in the lin-35 (Rb) mutant, but not the down-regulated genes are highly represented in the set of genes with corresponding endogenous siRNAs (endo-siRNAs). Our study suggests that endogenous siRNAs cooperate with chromatin factors, either C. elegans ortholog of acute lymphoblastic leukemia-1 (ALL-1)-fused gene from chromosome 10 (AF10), ZFP-1, or tumor suppressor Rb, to regulate overlapping sets of genes and predicts a large role for RNAi-based chromatin silencing in control of gene expression in C. elegans .

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Section: Methodsmentioning

confidence: 99%

“…The C. elegans Rb protein LIN-35 represses inappropriate transcription of germline-specific genes (12) and growth factors (13) in differentiated somatic cells and functions redundantly with other transcriptional repressors (14). Also, lin-35 mutants are more sensitive to exogenous RNAi than wild-type worms (11,15).…”

mentioning

confidence: 99%

RNA interference and retinoblastoma-related genes are required for repression of endogenous siRNA targets in Caenorhabditis elegans

Grishok

Hoersch

Sharp

2008

Proc. Natl. Acad. Sci. U.S.A.

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“…In this article, 1 we show that these putative class C synMuv genes are not distinct from and should be considered class B synMuv genes. The gene lin-3, which encodes the EGF-like ligand of the RTK/Ras pathway required for the specification of vulval cell fates (Hill and Sternberg 1992), is an apparent direct or indirect transcriptional target of at least some synMuv genes (Cui et al 2006). Given this observation and the molecular nature of many synMuv proteins, the synMuv proteins likely act as transcriptional repressors to prevent the ectopic expression of the RTK/Ras pathway ligand LIN-3 and in this way prevent ectopic vulval induction.…”

Section: G Lobal Analyses Of Loss-of-function Mutants Havementioning

confidence: 99%

“…The penetrances of synMuv vulval phenotypes correlate with the level of lin-3 mRNA expression: Cui et al (2006) reported that the lin-3 gene, which encodes the EGF ligand of the Ras pathway is a transcriptional target of some synMuv proteins. Three double mutants carrying a class A and a class B synMuv mutation had increased lin-3 EGF mRNA levels.…”

Section: Most Class B-b Double Mutants Do Not Have Muv Phenotypesmentioning

confidence: 99%

Multiple Levels of Redundant Processes InhibitCaenorhabditis elegansVulval Cell Fates

2008

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Many mutations cause obvious abnormalities only when combined with other mutations. Such synthetic interactions can be the result of redundant gene functions. In Caenorhabditis elegans, the synthetic multivulva (synMuv) genes have been grouped into multiple classes that redundantly inhibit vulval cell fates. Animals with one or more mutations of the same class undergo wild-type vulval development, whereas animals with mutations of any two classes have a multivulva phenotype. By varying temperature and genetic background, we determined that mutations in most synMuv genes within a single synMuv class enhance each other. However, in a few cases no enhancement was observed. For example, mutations that affect an Mi2 homolog and a histone methyltransferase are of the same class and do not show enhancement. We suggest that such sets of genes function together in vivo and in at least some cases encode proteins that interact physically. The approach of genetic enhancement can be applied more broadly to identify potential protein complexes as well as redundant processes or pathways. Many synMuv genes are evolutionarily conserved, and the genetic relationships we have identified might define the functions not only of synMuv genes in C. elegans but also of their homologs in other organisms.

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“…Constitutively active Wnt signal transduction causes VPCs that normally adopt the 3°fate to be ''overinduced'' (as assessed by ectopic invaginations), even when EGFR-Ras-MAPK activity is reduced (28). However, a situation in which Wnt signaling is artificially activated may be misleading as an indication of its normal role; a cautionary tale is afforded by the effect of removing SynMuv gene activity, which creates an artificial signaling event (32). In addition, lin-39 activity both prevents fusion and promotes division (4); thus, it is conceivable that abnormally high lin-39 levels in pry-1 mutants (perhaps in combination with other ectopically elevated factors) could cause spurious division so that P4.p or P8.p may divide ectopically without having responded to normal patterning signals.…”

Section: Lin-3/egf Signaling: Maintaining Competence Versus Initiatinmentioning

confidence: 99%

Wnt signal from multiple tissues and lin-3 /EGF signal from the gonad maintain vulval precursor cell competence in Caenorhabditis elegans

Myers¹,

Greenwald

2007

Proc. Natl. Acad. Sci. U.S.A.

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The Caenorhabditis elegans vulva has been a valuable paradigm for defining components of signaling pathways and elucidating how signaling events are coordinated to generate a developmental pattern. Vulval precursor cells (VPCs) are induced to adopt vulval fates in the third larval stage by LIN-3, an EGF-like signal produced by the gonad. Competence to respond to the inductive signal requires that the VPCs do not fuse to the major hypodermal syncytium, hyp7. We found that two Wnt-encoding genes, cwn-1 and egl-20, play a major role in preventing fusion of VPCs with hyp7 in the second larval stage. By using tissue-specific rescue of mig-14/Wntless, which is required for the production of Wnt ligands, we found that Wnt signal produced by multiple tissues, including neurons and muscles, promotes or maintains VPC competence before vulval induction. In addition, through laser ablation and genetic analysis, we provide evidence that LIN-3 signal from the gonad also plays a significant role in preventing VPCs from fusing with hyp7. We propose that Wnt signaling plays a permissive role in preventing VPCs from fusing with hyp7 and reevaluate the roles of Wnt and LIN-3/EGF signaling in competence and induction.

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SynMuv Genes Redundantly Inhibit lin-3/EGF Expression to Prevent Inappropriate Vulval Induction in C. elegans

Cited by 99 publications

References 39 publications

RNA interference and retinoblastoma-related genes are required for repression of endogenous siRNA targets in Caenorhabditis elegans

RNA interference and retinoblastoma-related genes are required for repression of endogenous siRNA targets in Caenorhabditis elegans

Multiple Levels of Redundant Processes InhibitCaenorhabditis elegansVulval Cell Fates

Wnt signal from multiple tissues and lin-3 /EGF signal from the gonad maintain vulval precursor cell competence in Caenorhabditis elegans

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