The<i>C. elegans</i>Hand gene controls embryogenesis and early gonadogenesis

Mathies, Laura D.; Henderson, Samuel T.; Kimble, Judith

doi:10.1242/dev.00483

Cited by 50 publications

(94 citation statements)

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“…Interestingly, a synthetic lethal analysis using RNA interference (RNAi) and available mutants identified unc-120 interactions with both hlh-1 and hnd-1, suggesting these three factors might define a "muscle module" (Baugh et al 2005b). However, bodywall muscle development was not assayed in this study, and genetic studies failed to find interactions between hlh-1 and hnd-1 mutants affecting bodywall myogenesis (Mathies et al 2003). This suggested that the synthetic lethality observed between hlh-1 and hnd-1 in the RNAi screen may be due, in part or in whole, to defects in nonmuscle lineages.…”

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confidence: 87%

“…Previous studies of hnd-1 have described its expression and mutant phenotypes (Mathies et al 2003). Reporter gene studies showed a very dynamic pattern of hnd-1 expression in early embryos, including transient expression in most, if not all, bodywall muscle lineages.…”

Section: Hnd-1 Genetically Interacts With Both Hlh-1 and Unc-120mentioning

confidence: 99%

“…For hnd-1, a deletion null allele had been previously characterized (Mathies et al 2003). Genetically defined nulls (all point mutants) have also been previously characterized for hlh-1 (Chen et al 1992.…”

Section: Identifying Deletion Alleles For Unc-120 and Hlh-1mentioning

confidence: 99%

“…In vertebrates, the HAND factors are best known for their role in cardiac ventricle development Srivastava et al 1995), although studies also demonstrate more widespread functions in embryonic and extraembryonic tissue development (for review, see Firulli 2003). In C. elegans, the hnd-1 gene was first identified as a regulator of somatic gonad precursor (SGP) cell development (Mathies et al 2003). Interestingly, reporter gene studies suggested that hnd-1 was also expressed in early embryonic blastomeres, including those that exclusively give rise to bodywall muscle cells.…”

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confidence: 99%

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Defining the transcriptional redundancy of early bodywall muscle development in C. elegans: evidence for a unified theory of animal muscle development

Fukushige¹,

Brodigan²,

Schriefer³

et al. 2006

Genes Dev.

164

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Myogenic regulatory factors (MRFs) are required for mammalian skeletal myogenesis. In contrast, bodywall muscle is readily detectable in Caenorhabditis elegans embryos lacking activity of the lone MRF ortholog HLH-1, indicating that additional myogenic factors must function in the nematode. We find that two additional C. elegans proteins, UNC-120/SRF and HND-1/HAND, can convert naïve blastomeres to muscle when overproduced ectopically in the embryo. In addition, we have used genetic null mutants to demonstrate that both of these factors act in concert with HLH-1 to regulate myogenesis. Loss of all three factors results in embryos that lack detectable bodywall muscle differentiation, identifying this trio as a set that is both necessary and sufficient for bodywall myogenesis in C. elegans. In mammals, SRF and HAND play prominent roles in regulating smooth and cardiac muscle development. That C. elegans bodywall muscle development is dependent on transcription factors that are associated with all three types of mammalian muscle supports a theory that all animal muscle types are derived from a common ancestral contractile cell type.[Keywords: Myogenesis; MyoD; SRF; HAND] Supplemental material is avaliable at http://www.genesdev.org.

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mentioning

confidence: 87%

Section: Hnd-1 Genetically Interacts With Both Hlh-1 and Unc-120mentioning

confidence: 99%

Section: Identifying Deletion Alleles For Unc-120 and Hlh-1mentioning

confidence: 99%

mentioning

confidence: 99%

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Defining the transcriptional redundancy of early bodywall muscle development in C. elegans: evidence for a unified theory of animal muscle development

Fukushige¹,

Brodigan²,

Schriefer³

et al. 2006

Genes Dev.

164

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“…Using KpnI and XbaI, the FLP recombinase cDNA fragment was excised from pGC92 and ligated to KpnI/NheI-digested pPD118.26 or pPD118.28 (A. Fire, S. Xu, J. Fleenor, J. Ahnn and G. Seydoux, personal communication; http lag-2-promoter driven FLP recombinase plasmid pGC158 [P lag-2 T FLPTlet-858(39)]: We created a lag-2-driven FLP, pGC158, by replacing GFPTunc-54(39) from pJK590 (Blelloch et al 1999;Mathies et al 2003) between XmaI and ApaI with the FLPTlet-858(39) fragment cut from pGC94 with the same restriction enzymes.…”

Section: Vector Constructionmentioning

confidence: 99%

A “FLP-Out” System for Controlled Gene Expression in Caenorhabditis elegans

Voutev

Hubbard

2008

Genetics

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We present a two-part system for conditional FLP-out of FRT-flanked sequences in Caenorhabditis elegans to control gene activity in a spatially and/or temporally regulated manner. Using reporters, we assess the system for efficacy and demonstrate its use as a cell lineage marking tool. In addition, we construct and test a dominant-negative form of hlh-12, a gene that encodes a basic helix-loop-helix (bHLH) transcription factor required for proper distal tip cell (DTC) migration. We show that this allele can be conditionally expressed from a heat-inducible FLP recombinase and can interfere with DTC migration. Using the same DTC assay, we conditionally express an hlh-12 RNAi-hairpin and induce the DTC migration defect. Finally, we introduce a set of traditional and Gateway-compatible vectors to facilitate construction of plasmids for this technology using any promoter, reporter, and gene/hairpin of interest.T WO-COMPONENT gene expression systems are indispensable tools to probe molecular mechanisms underlying development. Because control can be exerted by each component independently, exquisite temporal and spatial control of gene activation or repression can be achieved. Using different promoter combinations to drive each component of these systems, additional control can be obtained beyond that afforded by heat-inducible or tissue-specific promoters alone. Site-specific recombination systems such as the FLP/FRT system have been used to control gene expression by ''FLP-out'': a recombinase-catalyzed intramolecular excision of spacer DNA that lies between tandemly oriented FRT sites. The spacer includes a transcriptional stop so that prior to activation of the FLP recombinase (and subsequent FLP-out) the gene downstream of the spacer is not transcribed (Golic and Lindquist 1989;Struhl and Basler 1993; Figure 1A). After the FRT-containing cassette is excised by the FLP recombinase, the downstream gene is brought into proximity to the promoter and is expressed (reporter 2 in Figure 1A). This system and related systems have proven quite powerful and flexible in model organisms including Drosophila and mouse (see Branda and Dymecki 2004, for review;McGuire et al. 2004). However, prior to our study presented here, and a recently published study (Davis et al. 2008), these systems had not been developed for use in Caenorhabditis elegans.An ideal FLP-out system provides the means to generate both loss-and gain-of-function effects in a spatially and temporally controlled manner. In addition, wild-type gene expression can be turned on in particular cells at particular times in an otherwise mutant background. In organisms where transgenes can be reliably inserted in single copy, FLP-out can also be used to eliminate wild-type gene expression by excision of an FRT-flanked wild-type cassette in a mutant background. In C. elegans, the most common methods for generating transgenic C. elegans introduce multiple copies of transgenes on extrachromosomal arrays (Stinchcomb et al. 1985;Mello et al. 1991;Kelly et al. 1997). ...

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Endomesoderm specification in Caenorhabditis elegans and other nematodes

Maduro

2006

BioEssays

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The endomesoderm gene regulatory network (GRN) of C. elegans is a rich resource for studying the properties of cell-fate-specification pathways. This GRN contains both cell-autonomous and cell non-autonomous mechanisms, includes network motifs found in other GRNs, and ties maternal factors to terminal differentiation genes through a regulatory cascade. In most cases, upstream regulators and their direct downstream targets are known. With the availability of resources to study close and distant relatives of C. elegans, the molecular evolution of this network can now be examined. Within Caenorhabditis, components of the endomesoderm GRN are well conserved. A cursory examination of the preliminary genome sequences of two parasitic nematodes, Haemonchus contortus and Brugia malayi, suggests that evolution in this GRN is occurring most rapidly for the zygotic genes that specify blastomere identity.

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TheC. elegansHand gene controls embryogenesis and early gonadogenesis

Cited by 50 publications

References 68 publications

Defining the transcriptional redundancy of early bodywall muscle development in C. elegans: evidence for a unified theory of animal muscle development

Defining the transcriptional redundancy of early bodywall muscle development in C. elegans: evidence for a unified theory of animal muscle development

A “FLP-Out” System for Controlled Gene Expression in Caenorhabditis elegans

Endomesoderm specification in Caenorhabditis elegans and other nematodes

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