A Rad26-Def1 complex coordinates repair and RNA pol II proteolysis in response to DNA damage Journal Article


Authors: Woudstra, E. C.; Gilbert, C.; Fellows, J.; Jansen, L.; Brouwer, J.; Erdjument-Bromage, H.; Tempst, P.; Svejstrup, J. Q.
Article Title: A Rad26-Def1 complex coordinates repair and RNA pol II proteolysis in response to DNA damage
Abstract: Eukaryotic cells use multiple, highly conserved mechanisms to contend with ultraviolet-light-induced DNA damage(1). One important response mechanism is transcription-coupled repair (TCR), during which DNA lesions in the transcribed strand of an active gene are repaired much faster than in the genome overall(2). In mammalian cells, defective TCR gives rise to the severe human disorder Cockayne's syndrome (CS)(3). The best-studied CS gene, CSB, codes for a Swi/Snf-like DNA-dependent ATPase, whose yeast homologue is called Rad26 (ref. 4). Here we identify a yeast protein, termed Def1, which forms a complex with Rad26 in chromatin. The phenotypes of cells lacking DEF1 are consistent with a role for this factor in the DNA damage response, but Def1 is not required for TCR. Rather, def1 cells are compromised for transcript elongation, and are unable to degrade RNA polymerase II (RNAPII) in response to DNA damage. Our data suggest that RNAPII stalled at a DNA lesion triggers a coordinated rescue mechanism that requires the Rad26-Def1 complex, and that Def1 enables ubiquitination and proteolysis of RNAPII when the lesion cannot be rapidly removed by Rad26-promoted DNA repair.
Keywords: saccharomyces-cerevisiae; cells; polymerase-ii; degradation; nucleotide excision-repair; cockayne-syndrome; large subunit; transcription-coupled repair; elongation-factor tfiis; induced ubiquitination
Journal Title: Nature
Volume: 415
Issue: 6874
ISSN: 0028-0836
Publisher: Nature Publishing Group  
Date Published: 2002-02-21
Start Page: 929
End Page: 933
Language: English
ACCESSION: WOS:000173941000050
DOI: 10.1038/415929a
PROVIDER: wos
PUBMED: 11859374
Notes: Article -- Source: Wos
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  1. Paul J Tempst
    324 Tempst