 Effect of DNA damage on a BRCA1 complexFoon Wu-Baer and
Richard Baer ()
Nature, 2001, vol. 414, issue 6859, 36-36 Abstract: Abstract The tumour-suppressor protein BRCA1 mediates its biological functions by interacting with cellular factors1,2 such as the CtIP polypeptide3,4, a substrate for the ATM (for 'ataxia telangiectasia mutated') protein kinase5. Li et al.6 report that the BRCA1–CtIP interaction is disrupted by ionizing radiation and by other genotoxic stresses that induce phosphorylation of CtIP by ATM kinase, and that this dissociation of the BRCA1–CtIP complex in turn modulates the transcription of DNA-damage-response genes6. We have shown that the BRCA1-binding domain of CtIP (amino-acid residues 133–369) is distal to the sites that are phosphorylated by ATM kinase (residues S664 and S745)7. We now show that the BRCA1–CtIP complex is stable in irradiated cells, and that the phosphorylated isoforms of CtIP that are induced by ionizing radiation still interact in vivo with BRCA1. We conclude that disruption of the BRCA1–CtIP complex cannot account for induction of DNA-damage-response genes in the way proposed by Li et al.6. Date: 2001 Downloads: (external link) Related works: Export reference: BibTeX RIS (EndNote, ProCite, RefMan) HTML/Text Persistent link: https://EconPapers.repec.org/RePEc:nat:nature:v:414:y:2001:i:6859:d:10.1038_35102118 Ordering information: This journal article can be ordered from DOI: 10.1038/35102118 Access Statistics for this article Nature is currently edited by Magdalena Skipper More articles in Nature from Nature |
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