Literature DB >> 7982580

The dpy-30 gene encodes an essential component of the Caenorhabditis elegans dosage compensation machinery.

D R Hsu1, B J Meyer.   

Abstract

The need to regulate X chromosome expression in Caenorhabditis elegans arises as a consequence of the primary sex-determining signal, the X/A ratio (the ratio of X chromosomes to sets of autosomes), which directs 1X@A animals to develop as males and 2X/2A animals to develop as hermaphrodites. C. elegans possesses a dosage compensation mechanism that equalizes X chromosome expression between the two sexes despite their disparity in X chromosome dosage. Previous genetic analysis led to the identification of four autosomal genes, dpy-21, dpy-26, dpy-27 and dpy-28, whose products are essential in XX animals for proper dosage compensation, but not for sex determination. We report the identification and characterization of dpy-30, an essential component of the dosage compensation machinery. Putative null mutations in dpy-30 disrupt dosage compensation and cause a severe maternal-effect, XX-specific lethality. Rare survivors of the dpy-30 lethality are dumpy and express their X-linked genes at higher than wild-type levels. These dpy-30 mutant phenotypes superficially resemble those caused by mutations in dpy-26, dpy-27 and dpy-28; however, detailed phenotypic analysis reveals important differences that distinguish dpy-30 from these genes. In contrast to the XX-specific lethality caused by mutations in the other dpy genes, the XX-specific lethality caused by dpy-30 mutations is completely penetrant and temperature sensitive. In addition, unlike the other genes, dpy-30 is required for the normal development of XO animals. Although dpy-30 mutations do not significantly affect the viability of XO animals, they do cause them to be developmentally delayed and to possess numerous morphological and behavioral abnormalities. Finally, dpy-30 mutations can dramatically influence the choice of sexual fate in animals with an ambiguous sexual identity, despite having no apparent effect on the sexual phenotype of otherwise wild-type animals. Paradoxically, depending on the genetic background, dpy-30 mutations cause either masculinization or feminization, thus revealing the complex regulatory relationship between the sex determination and dosage compensation processes. The novel phenotypes caused by dpy-30 mutations suggest that in addition to acting in the dosage compensation process, dpy-30 may play a more general role in the development of both XX and XO animals.

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Year:  1994        PMID: 7982580      PMCID: PMC1206076     

Source DB:  PubMed          Journal:  Genetics        ISSN: 0016-6731            Impact factor:   4.562


  34 in total

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Authors:  T W Cline
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Authors:  A M Villeneuve; B J Meyer
Journal:  Cell       Date:  1987-01-16       Impact factor: 41.582

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Authors:  S W L'Hernault; D C Shakes; S Ward
Journal:  Genetics       Date:  1988-10       Impact factor: 4.562

4.  A second informational suppressor, SUP-7 X, in Caenorhabditis elegans.

Authors:  R H Waterston
Journal:  Genetics       Date:  1981-02       Impact factor: 4.562

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Authors:  R D Klein; B J Meyer
Journal:  Cell       Date:  1993-02-12       Impact factor: 41.582

Review 6.  The Drosophila sex determination signal: how do flies count to two?

Authors:  T W Cline
Journal:  Trends Genet       Date:  1993-11       Impact factor: 11.639

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Journal:  Genetics       Date:  1987-12       Impact factor: 4.562

Review 8.  Molecular genetics of sex determination in C. elegans.

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Journal:  Trends Genet       Date:  1992-05       Impact factor: 11.639

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Authors:  J A Hodgkin; S Brenner
Journal:  Genetics       Date:  1977-06       Impact factor: 4.562

10.  A gene mapping to the sex-determining region of the mouse Y chromosome is a member of a novel family of embryonically expressed genes.

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Journal:  Nature       Date:  1990-07-19       Impact factor: 49.962

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  52 in total

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Journal:  Genetics       Date:  2018-12-05       Impact factor: 4.562

Review 2.  The COMPASS family of histone H3K4 methylases: mechanisms of regulation in development and disease pathogenesis.

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Journal:  Annu Rev Biochem       Date:  2012       Impact factor: 23.643

3.  A ONECUT homeodomain protein communicates X chromosome dose to specify Caenorhabditis elegans sexual fate by repressing a sex switch gene.

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Journal:  Genetics       Date:  2007-08-24       Impact factor: 4.562

Review 4.  C. elegans dosage compensation: a window into mechanisms of domain-scale gene regulation.

Authors:  Sevinc Ercan; Jason D Lieb
Journal:  Chromosome Res       Date:  2009       Impact factor: 5.239

5.  A trithorax-group complex purified from Saccharomyces cerevisiae is required for methylation of histone H3.

Authors:  Peter L Nagy; Joachim Griesenbeck; Roger D Kornberg; Michael L Cleary
Journal:  Proc Natl Acad Sci U S A       Date:  2001-12-18       Impact factor: 11.205

6.  Isolation of dominant XO-feminizing mutations in Caenorhabditis elegans: new regulatory tra alleles and an X chromosome duplication with implications for primary sex determination.

Authors:  J Hodgkin; D G Albertson
Journal:  Genetics       Date:  1995-10       Impact factor: 4.562

7.  An extragenic suppressor of the mitosis-defective bimD6 mutation of Aspergillus nidulans codes for a chromosome scaffold protein.

Authors:  C L Holt; G S May
Journal:  Genetics       Date:  1996-03       Impact factor: 4.562

8.  A screen for genetic loci required for hypodermal cell and glial-like cell development during Caenorhabditis elegans embryogenesis.

Authors:  P Chanal; M Labouesse
Journal:  Genetics       Date:  1997-05       Impact factor: 4.562

9.  Chromosome-wide mechanisms to decouple gene expression from gene dose during sex-chromosome evolution.

Authors:  Bayly S Wheeler; Erika Anderson; Christian Frøkjær-Jensen; Qian Bian; Erik Jorgensen; Barbara J Meyer
Journal:  Elife       Date:  2016-08-30       Impact factor: 8.140

10.  Crystal structure of CRN-4: implications for domain function in apoptotic DNA degradation.

Authors:  Yu-Yuan Hsiao; Akihisa Nakagawa; Zhonghao Shi; Shohei Mitani; Ding Xue; Hanna S Yuan
Journal:  Mol Cell Biol       Date:  2008-11-03       Impact factor: 4.272

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