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首页> 外文期刊>DNA repair >Bi-directional routing of DNA mismatch repair protein human exonuclease 1 to replication foci and DNA double strand breaks.
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Bi-directional routing of DNA mismatch repair protein human exonuclease 1 to replication foci and DNA double strand breaks.

机译:DNA错配修复蛋白人类核酸外切酶1双向复制复制灶和DNA双链断裂。

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摘要

Human exonuclease 1 (hEXO1) is implicated in DNA metabolism, including replication, recombination and repair, substantiated by its interactions with PCNA, DNA helicases BLM and WRN, and several DNA mismatch repair (MMR) proteins. We investigated the sub-nuclear localization of hEXO1 during S-phase progression and in response to laser-induced DNA double strand breaks (DSBs). We show that hEXO1 and PCNA co-localize in replication foci. This apparent interaction is sustained throughout S-phase. We also demonstrate that hEXO1 is rapidly recruited to DNA DSBs. We have identified a PCNA interacting protein (PIP-box) region on hEXO1 located in its COOH-terminal ((788)QIKLNELW(795)). This motif is essential for PCNA binding and co-localization during S-phase. Recruitment of hEXO1 to DNA DSB sites is dependent on the MMR protein hMLH1. We show that two distinct hMLH1 interaction regions of hEXO1 (residues 390-490 and 787-846) are required to direct the protein to the DNA damage site. Our results reveal that protein domains in hEXO1 in conjunction with specific protein interactions control bi-directional routing of hEXO1 between on-going DNA replication and repair processes in living cells.
机译:人核酸外切酶1(hEXO1)参与DNA代谢,包括复制,重组和修复,其与PCNA,DNA解旋酶BLM和WRN以及几种DNA错配修复(MMR)蛋白质相互作用证实了这一点。我们调查了hEXO1在S期进展过程中以及响应激光诱导的DNA双链断裂(DSBs)的亚核定位。我们显示,hEXO1和PCNA在复制灶中共定位。这种明显的相互作用在整个S阶段持续存在。我们还证明了hEXO1被迅速招募到DNA DSB。我们在hEXO1的COOH末端((788)QIKLNELW(795))中发现了PCNA相互作用蛋白(PIP-box)区。该基序对于PCNA结合和S期共定位至关重要。 hEXO1招募至DNA DSB位点取决于MMR蛋白hMLH1。我们显示,hEXO1的两个不同的hMLH1相互作用区域(残基390-490和787-846)需要将蛋白质引导至DNA损伤位点。我们的结果表明,hEXO1中的蛋白质结构域与特定的蛋白质相互作用共同控制着hEXO1在活细胞中正在进行的DNA复制和修复过程之间的双向路由。

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