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A non-catalytic role of RecBCD in homology directed gap repair and translesion synthesis

机译:Recbcd在同源性的非催化作用,定向间隙修复和翻塑合成

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摘要

The RecBCD complex is a key factor in DNA metabolism. This protein complex harbors a processive nuclease and two helicases activities that give it the ability to process duplex DNA ends. These enzymatic activities make RecBCD a major player in double strand break repair, conjugational recombination and degradation of linear DNA. In this work, we unravel a new role of the RecBCD complex in the processing of DNA single-strand gaps that are generated at DNA replication-blocking lesions. We show that independently of its nuclease or helicase activities, the entire RecBCD complex is required for recombinational repair of the gap and efficient translesion synthesis. Since none of the catalytic functions of RecBCD are required for those processes, we surmise that the complex acts as a structural element that stabilizes the blocked replication fork, allowing efficient DNA damage tolerance.
机译:RecBCD复合物是DNA代谢的关键因素。 该蛋白质复杂的母语是一种加工核酸酶和两种直升机活性,其使其能够处理双链DNA结束。 这些酶活性使重用双链破裂修复,缀合性重组和线性DNA降解的主要参与者。 在这项工作中,我们在DNA复制阻断病变处产生的DNA单链间隙的处理中,我们在处理DNA单链间隙的处理中解开了RecBCD复合物的新作用。 我们表明,独立于其核酸酶或螺旋酶活性,整个RecBCD复合物是重组修复所需的间隙和有效的翻塑合成所必需的。 由于这些方法需要RecBCD的催化功能,因此我们猜测该复合物作为稳定阻塞复制叉的结构元素,允许有效的DNA损伤耐受性。

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