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复制蛋白A主要单链DNA结合结构域的结构表明了一种DNA结合的动态机制。

Structure of the major single-stranded DNA-binding domain of replication protein A suggests a dynamic mechanism for DNA binding.

作者信息

Bochkareva E, Belegu V, Korolev S, Bochkarev A

机构信息

Department of Biochemistry and Molecular Biology, The University of Oklahoma Health Sciences Center, 975 NE 10th Street, BRC-466, Oklahoma City, OK 73190, USA.

出版信息

EMBO J. 2001 Feb 1;20(3):612-8. doi: 10.1093/emboj/20.3.612.

Abstract

Although structures of single-stranded (ss)DNA-binding proteins (SSBs) have been reported with and without ssDNA, the mechanism of ssDNA binding in eukarya remains speculative. Here we report a 2.5 Angstroms structure of the ssDNA-binding domain of human replication protein A (RPA) (eukaryotic SSB), for which we previously reported a structure in complex with ssDNA. A comparison of free and bound forms of RPA revealed that ssDNA binding is associated with a major reorientation between, and significant conformational changes within, the structural modules--OB-folds--which comprise the DNA-binding domain. Two OB-folds, whose tandem orientation was stabilized by the presence of DNA, adopted multiple orientations in its absence. Within the OB-folds, extended loops implicated in DNA binding significantly changed conformation in the absence of DNA. Analysis of intermolecular contacts suggested the possibility that other RPA molecules and/or other proteins could compete with DNA for the same binding site. Using this mechanism, protein-protein interactions can regulate, and/or be regulated by DNA binding. Combined with available biochemical data, this structure also suggested a dynamic model for the DNA-binding mechanism.

摘要

尽管已有单链(ss)DNA结合蛋白(SSB)结合和未结合ssDNA时的结构报道,但真核生物中ssDNA结合的机制仍属推测。在此,我们报道了人类复制蛋白A(RPA)(真核生物SSB)的ssDNA结合结构域的2.5埃结构,我们之前曾报道过其与ssDNA复合物的结构。RPA游离形式和结合形式的比较表明,ssDNA结合与构成DNA结合结构域的结构模块——OB折叠之间的主要重新定向以及其内部的显著构象变化相关。两个OB折叠,其串联方向在有DNA时得以稳定,在无DNA时则呈现多种方向。在OB折叠内部,与DNA结合相关的延伸环在无DNA时显著改变构象。分子间相互作用分析表明,其他RPA分子和/或其他蛋白质可能与DNA竞争相同结合位点。利用这一机制,蛋白质-蛋白质相互作用可以调控DNA结合,和/或受DNA结合调控。结合现有的生化数据,该结构还提出了一个DNA结合机制的动态模型。

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