首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >ATRIP associates with replication protein A-coated ssDNA through multiple interactions
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ATRIP associates with replication protein A-coated ssDNA through multiple interactions

机译:ATRIP通过多种相互作用与复制蛋白A包裹的ssDNA缔合

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摘要

The ATR (ATM- and rad3-related)-mediated checkpoint pathway has a crucial role in regulating the cellular responses to DNA damage and DNA-replication stress. ATRIP (ATR-interacting protein), the regulatory partner of ATR, binds directly to replication protein A (RPA)-coated ssDNA and enables the ATR-ATRIP complex to recognize this DNA damage-induced structure. Here, we show that ATRIP associates with RPA-ssDNA through multiple interactions. Two major RPA-ssDNA-interacting domains of ATRIP were mapped to the regions flanking the conserved coiled-coil domain. In contrast to a recent article, we found that ATRIP mutants lacking the N terminus retained the ability to bind to RPA-ssDNA, suggesting that the multiple interactions between ATRIP and RPA-ssDNA may function redundantly in the recruitment of ATR-ATRIP. Unexpectedly, one internal region of ATRIP exhibited affinity to ssDNA, suggesting that ATRIP may interact with ssDNA in the ATRIP-RPA-ssDNA complex. Also, the N terminus of ATRIP associated with RPA-ssDNA in two distinct ways, indicating a dynamic and regulated association between ATRIP and RPA-ssDNA.
机译:ATR(与ATM和rad3相关)介导的检查点途径在调节细胞对DNA损伤和DNA复制应激的反应中起着至关重要的作用。 ATRI的调节伙伴ATRIP(与ATR相互作用的蛋白)直接结合到复制蛋白A(RPA)包裹的ssDNA上,并使ATR-ATRIP复合物能够识别这种DNA损伤诱导的结构。在这里,我们显示ATRIP通过多种相互作用与RPA-ssDNA缔合。 ATRIP的两个主要RPA-ssDNA相互作用域被映射到保守的卷曲螺旋域的侧翼区域。与最近的文章相反,我们发现缺少N末端的ATRIP突变体保留了与RPA-ssDNA结合的能力,这表明ATRIP和RPA-ssDNA之间的多重相互作用可能在ATR-ATRIP的募集中起冗余作用。出乎意料的是,ATRIP的一个内部区域表现出对ssDNA的亲和力,这表明ATRIP可能与ATRIP-RPA-ssDNA复合物中的ssDNA相互作用。同样,ATRIP的N末端以两种不同的方式与RPA-ssDNA关联,表明ATRIP和RPA-ssDNA之间存在动态和调控的关联。

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