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Complex activities of the human Blooms syndrome helicase are encoded in a core region comprising the RecA and Zn-binding domains

机译:人类布卢姆综合症解旋酶的复杂活动在包含RecA和Zn结合域的核心区域编码

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摘要

Bloom's syndrome DNA helicase (BLM), a member of the RecQ family, is a key player in homologous recombination (HR)-based error-free DNA repair processes. During HR, BLM exerts various biochemical activities including single-stranded (ss) DNA translocation, separation and annealing of complementary DNA strands, disruption of complex DNA structures (e.g. displacement loops) and contributes to quality control of HR via clearance of Rad51 nucleoprotein filaments. We performed a quantitative mechanistic analysis of truncated BLM constructs that are shorter than the previously identified minimal functional module. Surprisingly, we found that a BLM construct comprising only the two conserved RecA domains and the Zn2+-binding domain (residues 642–1077) can efficiently perform all mentioned HR-related activities. The results demonstrate that the Zn2+-binding domain is necessary for functional interaction with DNA. We show that the extensions of this core, including the winged-helix domain and the strand separation hairpin identified therein in other RecQ-family helicases, are not required for mechanochemical activity per se and may instead play modulatory roles and mediate protein–protein interactions.
机译:布鲁姆综合症DNA解旋酶(BLM)是RecQ家族的成员,是基于同源重组(HR)的无错DNA修复过程的关键参与者。在HR期间,BLM发挥了各种生化活性,包括单链(ss)DNA易位,互补DNA链的分离和退火,复杂DNA结构的破坏(例如置换环),并通过清除Rad51核蛋白细丝对HR进行质量控制。我们对截短的BLM结构进行了定量的力学分析,该结构比以前确定的最小功能模块要短。令人惊讶的是,我们发现仅包含两个保守的RecA结构域和Zn 2 + 结合结构域(残基642-1077)的BLM构建体可以有效地执行所有上述与HR相关的活动。结果表明,Zn 2 + -结合域对于与DNA的功能相互作用是必需的。我们表明,该核心的延伸,包括在其他RecQ家族解旋酶中鉴定出的翼状螺旋结构域和其中的链分离发夹,并不是机械化学活性本身所必需的,而是可以发挥调节作用并介导蛋白质-蛋白质相互作用。

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