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XRCC1 BRCT结构域的结构:一种新型蛋白质-蛋白质相互作用模块。

Structure of an XRCC1 BRCT domain: a new protein-protein interaction module.

作者信息

Zhang X, Moréra S, Bates P A, Whitehead P C, Coffer A I, Hainbucher K, Nash R A, Sternberg M J, Lindahl T, Freemont P S

机构信息

Molecular Structure and Function, Imperial Cancer Research Fund, 44 Lincoln's Inn Fields, London WC2A 3PX, UK.

出版信息

EMBO J. 1998 Nov 2;17(21):6404-11. doi: 10.1093/emboj/17.21.6404.

Abstract

The BRCT domain (BRCA1 C-terminus), first identified in the breast cancer suppressor protein BRCA1, is an evolutionarily conserved protein-protein interaction region of approximately 95 amino acids found in a large number of proteins involved in DNA repair, recombination and cell cycle control. Here we describe the first three-dimensional structure and fold of a BRCT domain determined by X-ray crystallography at 3.2 A resolution. The structure has been obtained from the C-terminal region of the human DNA repair protein XRCC1, and comprises a four-stranded parallel beta-sheet surrounded by three alpha-helices, which form an autonomously folded domain. The compact XRCC1 structure explains the observed sequence homology between different BRCT motifs and provides a framework for modelling other BRCT domains. Furthermore, the established structure of an XRCC1 BRCT homodimer suggests potential protein-protein interaction sites for the complementary BRCT domain in DNA ligase III, since these two domains form a stable heterodimeric complex. Based on the XRCC1 BRCT structure, we have constructed a model for the C-terminal BRCT domain of BRCA1, which frequently is mutated in familial breast and ovarian cancer. The model allows insights into the effects of such mutations on the fold of the BRCT domain.

摘要

BRCT结构域(BRCA1 C末端)最初是在乳腺癌抑制蛋白BRCA1中发现的,是一个进化上保守的蛋白质-蛋白质相互作用区域,约由95个氨基酸组成,存在于大量参与DNA修复、重组和细胞周期调控的蛋白质中。本文我们描述了通过X射线晶体学以3.2埃分辨率测定的BRCT结构域的首个三维结构和折叠情况。该结构取自人类DNA修复蛋白XRCC1的C末端区域,由一个四链平行β折叠片层和围绕其的三个α螺旋组成,形成一个自主折叠的结构域。紧凑的XRCC1结构解释了不同BRCT基序之间观察到的序列同源性,并为其他BRCT结构域的建模提供了框架。此外,已确定的XRCC1 BRCT同二聚体结构表明了DNA连接酶III中互补BRCT结构域潜在的蛋白质-蛋白质相互作用位点,因为这两个结构域形成一个稳定的异二聚体复合物。基于XRCC1 BRCT结构,我们构建了BRCA1 C末端BRCT结构域的模型,该结构域在家族性乳腺癌和卵巢癌中经常发生突变。该模型有助于深入了解此类突变对BRCT结构域折叠的影响。

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