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Central role for the XRCC1 BRCT I domain in mammalian DNA single-strand break repair

机译:XRCC1 BRCT I结构域在哺乳动物DNa单链断裂修复中的中心作用

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摘要

The DNA single-strand break repair (SSBR) protein XRCC1 is required for genetic stability and for embryonic viability. XRCC1 possesses two BRCA1 carboxyl-terminal (BRCT) protein interaction domains, denoted BRCT I and II. BRCT II is required for SSBR during G1 but is dispensable for this process during S/G2 and consequently for cell survival following DNA alkylation. Little is known about BRCT I, but this domain has attracted considerable interest because it is the site of a genetic polymorphism that epidemiological studies have associated with altered cancer risk. We report that the BRCT I domain comprises the evolutionarily conserved core of XRCC1 and that this domain is required for efficient SSBR during both G1 and S/G2 cell cycle phases and for cell survival following treatment with methyl methanesulfonate. However, the naturally occurring human polymorphism in BRCT I supported XRCC1-dependent SSBR and cell survival after DNA alkylation equally well. We conclude that while the BRCT I domain is critical for XRCC1 to maintain genetic integrity and cell survival, the polymorphism does not impact significantly on this function and therefore is unlikely to impact significantly on susceptibility to cancer.
机译:DNA单链断裂修复(SSBR)蛋白XRCC1是遗传稳定性和胚胎生存能力所必需的。 XRCC1具有两个BRCA1羧基末端(BRCT)蛋白质相互作用域,称为BRCT I和II。 BRCT II对于G1期间的SSBR是必需的,但对于S / G2期间的此过程是必需的,因此对于DNA烷基化后的细胞存活是必不可少的。对BRCT I知之甚少,但由于它是流行病学研究与癌症风险改变相关的遗传多态性的位点,因此引起了人们极大的兴趣。我们报告说,BRCT I结构域包含XRCC1的进化保守核心,并且该结构域对于G1和S / G2细胞周期阶段的有效SSBR以及甲烷甲磺酸甲酯处理后的细胞存活都是必需的。然而,BRCT I中天然存在的人类多态性同样支持XRCC1依赖性SSBR和DNA烷基化后的细胞存活。我们得出的结论是,尽管BRCT I结构域对于XRCC1维持遗传完整性和细胞存活至关重要,但多态性不会对该功能产生重大影响,因此不太可能对癌症的易感性产生明显影响。

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