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MutS/MutL crystal structure reveals that the MutS sliding clamp loads MutL onto DNA

机译:MutS / MutL晶体结构显示MutS滑动夹具将MutL加载到DNA上

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摘要

To avoid mutations in the genome, DNA replication is generally followed by DNA mismatch repair (MMR). MMR starts when a MutS homolog recognizes a mismatch and undergoes an ATP-dependent transformation to an elusive sliding clamp state. How this transient state promotes MutL homolog recruitment and activation of repair is unclear. Here we present a crystal structure of the MutS/MutL complex using a site-specifically crosslinked complex and examine how large conformational changes lead to activation of MutL. The structure captures MutS in the sliding clamp conformation, where tilting of the MutS subunits across each other pushes DNA into a new channel, and reorientation of the connector domain creates an interface for MutL with both MutS subunits. Our work explains how the sliding clamp promotes loading of MutL onto DNA, to activate downstream effectors. We thus elucidate a crucial mechanism that ensures that MMR is initiated only after detection of a DNA mismatch.>DOI:
机译:为了避免基因组中的突变,通常在DNA复制后进行DNA错配修复(MMR)。当MutS同源物识别出不匹配并经历ATP依赖性转变为难以捉摸的滑动钳位状态时,MMR开始。这种瞬时状态如何促进MutL同源物募集和修复激活尚不清楚。在这里,我们介绍了使用位点特异性交联的复合物的MutS / MutL复合物的晶体结构,并检查了多大的构象变化导致MutL的激活。该结构捕获了滑动钳构象中的MutS,其中MutS亚基彼此之间的倾斜将DNA推入新的通道,并且连接器域的重新定向为MutL与这两个MutS亚基创建了接口。我们的工作解释了滑动夹具如何促进MutL在DNA上的加载,从而激活下游效应子。因此,我们阐明了一种重要机制,可确保仅在检测到DNA错配后才启动MMR。> DOI:

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