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Weaving DNA strands: structural insight on ATP hydrolysis in RecA-induced homologous recombination

机译:编织DNA链:RecA诱导的同源重组中ATP水解的结构见解

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摘要

Homologous recombination is a fundamental process in all living organisms that allows the faithful repair of DNA double strand breaks, through the exchange of DNA strands between homologous regions of the genome. Results of three decades of investigation and recent fruitful observations have unveiled key elements of the reaction mechanism, which proceeds along nucleofilaments of recombinase proteins of the RecA family. Yet, one essential aspect of homologous recombination has largely been overlooked when deciphering the mechanism: while ATP is hydrolyzed in large quantity during the process, how exactly hydrolysis influences the DNA strand exchange reaction at the structural level remains to be elucidated. In this study, we build on a previous geometrical approach that studied the RecA filament variability without bound DNA to examine the putative implication of ATP hydrolysis on the structure, position, and interactions of up to three DNA strands within the RecA nucleofilament. Simulation results on modeled intermediates in the ATP cycle bring important clues about how local distortions in the DNA strand geometries resulting from ATP hydrolysis can aid sequence recognition by promoting local melting of already formed DNA heteroduplex and transient reverse strand exchange in a weaving type of mechanism.
机译:同源重组是所有活生物体的基本过程,通过在基因组同源区域之间交换DNA链,可以忠实修复DNA双链断裂。三十年研究的结果和最近卓有成效的观察结果揭示了反应机理的关键要素,该机理沿着RecA家族重组酶蛋白的核丝进行。然而,在解释该机理时,同源重组的一个基本方面已被大大忽略:尽管在此过程中ATP大量水解,但在结构水平上水解到底如何影响DNA链交换反应尚有待阐明。在这项研究中,我们基于先前的几何方法研究了没有结合DNA的RecA细丝变异性,以检查ATP水解对RecA核丝中最多三条DNA链的结构,位置和相互作用的假定影响。 ATP循环中建模中间体的模拟结果提供了重要线索,说明由ATP水解引起的DNA链几何结构中的局部畸变如何通过编织形式的机制促进已经形成的DNA异源双链的局部融化和瞬时反向链交换,从而有助于序列识别。

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