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噬菌体 T4 同源重组机制的组装与动态。

Assembly and dynamics of the bacteriophage T4 homologous recombination machinery.

机构信息

Department of Biochemistry, University of Vermont College of Medicine, Burlington, VT 05405, USA.

出版信息

Virol J. 2010 Dec 3;7:357. doi: 10.1186/1743-422X-7-357.

Abstract

Homologous recombination (HR), a process involving the physical exchange of strands between homologous or nearly homologous DNA molecules, is critical for maintaining the genetic diversity and genome stability of species. Bacteriophage T4 is one of the classic systems for studies of homologous recombination. T4 uses HR for high-frequency genetic exchanges, for homology-directed DNA repair (HDR) processes including DNA double-strand break repair, and for the initiation of DNA replication (RDR). T4 recombination proteins are expressed at high levels during T4 infection in E. coli, and share strong sequence, structural, and/or functional conservation with their counterparts in cellular organisms. Biochemical studies of T4 recombination have provided key insights on DNA strand exchange mechanisms, on the structure and function of recombination proteins, and on the coordination of recombination and DNA synthesis activities during RDR and HDR. Recent years have seen the development of detailed biochemical models for the assembly and dynamics of presynaptic filaments in the T4 recombination system, for the atomic structure of T4 UvsX recombinase, and for the roles of DNA helicases in T4 recombination. The goal of this chapter is to review these recent advances and their implications for HR and HDR mechanisms in all organisms.

摘要

同源重组(HR)是指在同源或近乎同源的 DNA 分子之间发生的物理链交换过程,对于维持物种的遗传多样性和基因组稳定性至关重要。噬菌体 T4 是研究同源重组的经典系统之一。T4 利用 HR 实现高频遗传交换,还利用 HDR 过程进行同源定向 DNA 修复,包括 DNA 双链断裂修复,并启动 DNA 复制(RDR)。在大肠杆菌中感染 T4 时,T4 重组蛋白的表达水平很高,并且与细胞生物中的对应蛋白在序列、结构和/或功能上具有很强的保守性。T4 重组的生化研究为 DNA 链交换机制、重组蛋白的结构和功能以及 RDR 和 HDR 期间重组和 DNA 合成活动的协调提供了关键见解。近年来,人们已经建立了 T4 重组系统中预链丝组装和动力学的详细生化模型、T4 UvsX 重组酶的原子结构以及 DNA 解旋酶在 T4 重组中的作用的详细生化模型。本章的目的是回顾这些最新进展及其对所有生物中 HR 和 HDR 机制的影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3fe9/3016280/33fb521e7e70/1743-422X-7-357-1.jpg

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