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Crystal structure of the UvrB dimer: insights into the nature and functioning of the UvrAB damage engagement and UvrB-DNA complexes

机译:UvrB二聚体的晶体结构:洞悉UvrAB损伤参与和UvrB-DNA复合体的性质和功能

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摘要

UvrB has a central role in the highly conserved UvrABC pathway functioning not only as a damage recognition element but also as an essential component of the lesion tracking machinery. While it has been recently confirmed that the tracking assembly comprises a UvrA2B2 heterotetramer, the configurations of the damage engagement and UvrB–DNA handover complexes remain obscure. Here, we present the first crystal structure of a UvrB dimer whose biological significance has been verified using both chemical cross-linking and electron paramagnetic resonance spectroscopy. We demonstrate that this dimeric species stably associates with UvrA and forms a UvrA2B2–DNA complex. Our studies also illustrate how signals are transduced between the ATP and DNA binding sites to generate the helicase activity pivotal to handover and formation of the UvrB2–DNA complex, providing key insights into the configurations of these important repair intermediates.
机译:UvrB在高度保守的UvrABC通路中起着核心作用,它不仅起损伤识别元件的作用,而且还作为病灶跟踪机制的重要组成部分。尽管最近已确认跟踪组件包含UvrA2B2异四聚体,但损伤接合和UvrB-DNA交接复合物的构型仍然不清楚。在这里,我们介绍了UvrB二聚体的第一个晶体结构,其生物学意义已通过化学交联和电子顺磁共振波谱验证。我们证明了这种二聚体物种与UvrA稳定缔合并形成了UvrA2B2-DNA复合体。我们的研究还说明了如何在ATP和DNA结合位点之间转导信号,以产生对移交和形成UvrB2-DNA复合物至关重要的解旋酶活性,从而为这些重要的修复中间体的结构提供了重要见识。

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