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A skipping rope translocation mechanism in a widespread family of DNA repair helicases

机译:一种跨越横跨DNA修复螺旋酶系列的跳绳机制

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摘要

Mitomycin repair factor A represents a family of DNA helicases that harbor a domain of unknown function (DUF1998) and support repair of mitomycin C-induced DNA damage by presently unknown molecular mechanisms. We determined crystal structures of Bacillus subtilis Mitomycin repair factor A alone and in complex with an ATP analog and/or DNA and conducted structure-informed functional analyses. Our results reveal a unique set of auxiliary domains appended to a dual-RecA domain core. Upon DNA binding, a Zn2+-binding domain, encompassing the domain of unknown function, acts like a drum that rolls out a canopy of helicase-associated domains, entrapping the substrate and tautening an inter-domain linker across the loading strand. Quantification of DNA binding, stimulated ATPase and helicase activities in the wild type and mutant enzyme variants in conjunction with the mode of coordination of the ATP analog suggest that Mitomycin repair factor A employs similar ATPase-driven conformational changes to translocate on DNA, with the linker ratcheting through the nucleotides like a ‘skipping rope’. The electrostatic surface topology outlines a likely path for the displaced DNA strand. Our results reveal unique molecular mechanisms in a widespread family of DNA repair helicases linked to bacterial antibiotics resistance.
机译:丝霉素修复因子A代表了一种DNA螺旋酶的系列,其涉及未知功能(DUF1998)的域,并通过目前未知的分子机制来支持丝霉素C诱导的DNA损伤的修复。我们确定枯草芽孢杆菌丝霉素修复因子A的晶体结构,并与ATP模拟和/或DNA复合物,并进行了结构信息的功能分析。我们的结果揭示了一组附加到双Reca域核心的独特辅助域。在DNA结合时,包括未知功能的域的Zn2 + - 桥接结构域,类似于滚动螺旋酶相关域的冠层的滚筒,突出基板和跨越装载股的域间连接器。与ATP模拟的协调模式结合野生型和突变酶变体中的DNA结合,刺激的ATP酶和螺旋酶活性的定量表明,丝霉素修复因子A采用类似的ATP酶驱动的构象变化,用接头在DNA上转移通过像“跳绳”这样的核苷酸棘轮。静电表面拓扑概述了移位的DNA链的可能路径。我们的结果揭示了与细菌抗生素抗性有关的广泛系列DNA修复螺旋酶中的独特分子机制。

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