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Double-check probing of DNA bending and unwinding by XPA-RPA: an architectural function in DNA repair.

机译:仔细检查探索DNA弯曲和解除XPA-RPA:建筑功能的DNA修复。

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摘要

The multiprotein factor composed of XPA and replication protein A (RPA) is an essential subunit of the mammalian nucleotide excision repair system. Although XPA-RPA has been implicated in damage recognition, its activity in the DNA repair pathway remains controversial. By replacing DNA adducts with mispaired bases or non-hybridizing analogues, we found that the weak preference of XPA and RPA for damaged substrates is entirely mediated by indirect readout of DNA helix conformations. Further screening with artificially distorted substrates revealed that XPA binds most efficiently to rigidly bent duplexes but not to single-stranded DNA. Conversely, RPA recognizes single-stranded sites but not backbone bending. Thus, the association of XPA with RPA generates a double-check sensor that detects, simultaneously, backbone and base pair distortion of DNA. The affinity of XPA for sharply bent duplexes, characteristic of architectural proteins, is not compatible with a direct function during recognition of nucleotide lesions. Instead, XPA in conjunction with RPA may constitute a regulatory factor that monitors DNA bending and unwinding to verify the damage-specific localization of repair complexes or control their correct three-dimensional assembly.
机译:multiprotein因素XPA和组成复制(战)是一种重要的蛋白质亚基的哺乳动物核苷酸切除修复系统。与损伤识别,它的活动DNA修复途径仍然是有争议的。用mispaired基地或取代DNA加合物non-hybridizing类似物,我们发现弱偏好的XPA和战受损的基质完全是由间接读出DNA螺旋构象。人为地扭曲的基板显示XPA结合最高效严格的倾向工器而不是单链DNA。相反,则识别单链网站但不是骨干弯曲。战的XPA生成一个仔细检查传感器检测,同时,支柱和基础对失真的DNA。大幅弯曲工器的特点架构的蛋白质,不兼容直接在核苷酸的识别功能病变。显示器DNA构成监管因素弯曲和解除验证damage-specific本地化修复复合物或控制正确的三维组装。

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