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首页> 外文期刊>Nucleic acids research >Structure of an ‘open' clamp type II topoisomerase-DNA complex provides a mechanism for DNA capture and transport
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Structure of an ‘open' clamp type II topoisomerase-DNA complex provides a mechanism for DNA capture and transport

机译:“开放式” II型钳位拓扑异构酶-DNA复合物的结构为DNA捕获和运输提供了一种机制

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Type II topoisomerases regulate DNA supercoiling and chromosome segregation. They act as ATP-operated clamps that capture a DNA duplex and pass it through a transient DNA break in a second DNA segment via the sequential opening and closure of ATPase-, G-DNA- and C-gates. Here, we present the first ‘open clamp' structures of a 3-gate topoisomerase II-DNA complex, the seminal complex engaged in DNA recognition and capture. A high-resolution structure was solved for a (full-length ParE-ParC55)2 dimer of Streptococcus pneumoniae topoisomerase IV bound to two DNA molecules: a closed DNA gate in a B-A-B form double-helical conformation and a second B-form duplex associated with closed C-gate helices at a novel site neighbouring the catalytically important β-pinwheel DNA-binding domain. The protein N gate is present in an ‘arms-wide-open' state with the undimerized N-terminal ParE ATPase domains connected to TOPRIM domains via a flexible joint and folded back allowing ready access both for gate and transported DNA segments and cleavage-stabilizing antibacterial drugs. The structure shows the molecular conformations of all three gates at 3.7 ?, the highest resolution achieved for the full complex to date, and illuminates the mechanism of DNA capture and transport by a type II topoisomerase.
机译:II型拓扑异构酶调节DNA超螺旋和染色体分离。它们充当ATP操作的夹具,捕获DNA双链体,并通过依次打开和关闭ATPase-,G-DNA-和C-门的方式,使它通过第二个DNA片段中的瞬时DNA断裂。在这里,我们介绍了3门拓扑异构酶II-DNA复合物的第一个“开放钳位”结构,该复合物参与DNA识别和捕获。解决了高分辨率结构的肺炎链球菌拓扑异构酶IV(全长ParE-ParC55) 2 二聚体与两个DNA分子结合的问题:BAB中的封闭DNA门形成双螺旋构象,第二个B型双链体,与邻近催化重要的β-风车DNA结合域的新位点上的闭合C-门螺旋相关。蛋白质N门以“全臂开放”状态存在,未二聚的N末端ParE ATPase域通过柔性接头连接到TOPRIM域并折回,从而可以方便地进入门和运输的DNA片段并进行切割稳定抗菌药物。该结构显示了三个门在3.7?处的分子构象,这是迄今为止完整复合物实现的最高分辨率,并阐明了II型拓扑异构酶捕获和转运DNA的机制。

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