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人类Ku70蛋白C端DNA结合结构域的三维结构

The three-dimensional structure of the C-terminal DNA-binding domain of human Ku70.

作者信息

Zhang Z, Zhu L, Lin D, Chen F, Chen D J, Chen Y

机构信息

Division of Immunology, Beckman Research Institute of the City of Hope, Duarte, California 91010, USA.

出版信息

J Biol Chem. 2001 Oct 12;276(41):38231-6. doi: 10.1074/jbc.M105238200. Epub 2001 Jul 16.

Abstract

The proteins Ku70 (69.8 kDa) and Ku80 (82.7 kDa) form a heterodimeric complex that is an essential component of the nonhomologous end joining DNA double-strand break repair pathway in mammalian cells. Interaction of Ku with DNA is central for the functions of Ku. Ku70, which is mainly responsible for the DNA binding activity of the Ku heterodimer, contains two DNA-binding domains. We have solved the solution structure of the Ku80-independent DNA-binding domain of Ku70 encompassing residues 536-609 using nuclear magnetic resonance spectroscopy. Residues 536-560 are highly flexible and have a random structure but form specific interactions with DNA. Residues 561-609 of Ku70 form a well defined structure with 3 alpha-helices and also interact with DNA. The three-dimensional structure indicates that all conserved hydrophobic residues are in the hydrophobic core and therefore may be important for structural integrity. Most of the conserved positively charged residues are likely to be critical for DNA recognition. The C-terminal DNA-binding domain of Ku70 contains a helix-extended strand-helix motif, which occurs in other nucleic acid-binding proteins and may represent a common nucleic acid binding motif.

摘要

蛋白质Ku70(69.8 kDa)和Ku80(82.7 kDa)形成一种异源二聚体复合物,它是哺乳动物细胞中非同源末端连接DNA双链断裂修复途径的重要组成部分。Ku与DNA的相互作用对Ku的功能至关重要。主要负责Ku异源二聚体DNA结合活性的Ku70包含两个DNA结合结构域。我们利用核磁共振光谱法解析了Ku70的不依赖Ku80的DNA结合结构域(包含536 - 609位残基)的溶液结构。536 - 560位残基高度灵活且具有随机结构,但能与DNA形成特定相互作用。Ku70的561 - 609位残基形成一个具有3个α螺旋的明确结构,也与DNA相互作用。三维结构表明所有保守的疏水残基都位于疏水核心,因此可能对结构完整性很重要。大多数保守的带正电荷残基可能对DNA识别至关重要。Ku70的C端DNA结合结构域包含一个螺旋 - 延伸链 - 螺旋基序,该基序存在于其他核酸结合蛋白中,可能代表一种常见的核酸结合基序。

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