Literature DB >> 9426063

Disruption of the mouse xeroderma pigmentosum group D DNA repair/basal transcription gene results in preimplantation lethality.

J de Boer1, I Donker, J de Wit, J H Hoeijmakers, G Weeda.   

Abstract

The xeroderma pigmentosum (XP) group D (XPD) gene encodes a DNA helicase that is a subunit of the transcription factor IIH complex, involved both in nucleotide excision repair of UV-induced DNA damage and in basal transcription initiation. Point mutations in the XPD gene lead either to the cancer-prone repair syndrome XP, sometimes in combination with a second repair condition; Cockayne syndrome; or the non-cancer-prone brittle-hair disorder trichothiodystrophy. To study the role of XPD in nucleotide excision repair and transcription and its implication in human disorders, we isolated the mouse XPD gene and generated a null allele via homologous recombination in embryonic stem cells by deleting XPD helicase domains IV-VI. Heterozygous cells and mice are normal without any obvious defect. However, when intercrossing heterozygotes, homozygous XPD mutant mice were selectively absent from the offspring. Furthermore, we could not detect XPD-/- embryos at day 7.5 of development. In vitro growth experiments with preimplantation-stage embryos obtained from heterozygous intercrosses showed a significantly higher fraction of embryos that died at the two-cell stage, compared to wild-type embryos. These results establish the essential function of the XPD protein in mammals and in cellular viability and are consistent with the notion that only subtle XPD mutations are found in XP, XP/Cockayne syndrome, and trichothiodystrophy patients.

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Year:  1998        PMID: 9426063

Source DB:  PubMed          Journal:  Cancer Res        ISSN: 0008-5472            Impact factor:   12.701


  30 in total

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Review 2.  Disorders of nucleotide excision repair: the genetic and molecular basis of heterogeneity.

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4.  Optical Control of DNA Helicase Function through Genetic Code Expansion.

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5.  Postnatal growth failure, short life span, and early onset of cellular senescence and subsequent immortalization in mice lacking the xeroderma pigmentosum group G gene.

Authors:  Y N Harada; N Shiomi; M Koike; M Ikawa; M Okabe; S Hirota; Y Kitamura; M Kitagawa; T Matsunaga; O Nikaido; T Shiomi
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6.  DNA repair and transcriptional effects of mutations in TFIIH in Drosophila development.

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8.  An Xpb mouse model for combined xeroderma pigmentosum and cockayne syndrome reveals progeroid features upon further attenuation of DNA repair.

Authors:  Jaan-Olle Andressoo; Geert Weeda; Jan de Wit; James R Mitchell; Rudolf B Beems; Harry van Steeg; Gijsbertus T J van der Horst; Jan H Hoeijmakers
Journal:  Mol Cell Biol       Date:  2008-12-29       Impact factor: 4.272

9.  Cdk8 is essential for preimplantation mouse development.

Authors:  Thomas Westerling; Emilia Kuuluvainen; Tomi P Mäkelä
Journal:  Mol Cell Biol       Date:  2007-07-09       Impact factor: 4.272

10.  Male infertility and DNA damage in Doppel knockout and prion protein/Doppel double-knockout mice.

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Journal:  Am J Pathol       Date:  2004-06       Impact factor: 4.307

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