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结核分枝杆菌RecA及其与ADP-AlF(4)复合物的晶体结构:对ATP酶活性降低和分子聚集的影响

Crystal structures of Mycobacterium tuberculosis RecA and its complex with ADP-AlF(4): implications for decreased ATPase activity and molecular aggregation.

作者信息

Datta S, Prabu M M, Vaze M B, Ganesh N, Chandra N R, Muniyappa K, Vijayan M

机构信息

Molecular Biophysics Unit, Department of Biochemistry and Bioinformatics Centre, Indian Institute of Science, Bangalore 560 012, India.

出版信息

Nucleic Acids Res. 2000 Dec 15;28(24):4964-73. doi: 10.1093/nar/28.24.4964.

Abstract

Sequencing of the complete genome of Mycobacterium tuberculosis, combined with the rapidly increasing need to improve tuberculosis management through better drugs and vaccines, has initiated extensive research on several key proteins from the pathogen. RecA, a ubiquitous multifunctional protein, is a key component of the processes of homologous genetic recombination and DNA repair. Structural knowledge of MtRecA is imperative for a full understanding of both these activities and any ensuing application. The crystal structure of MtRecA, presented here, has six molecules in the unit cell forming a 6(1) helical filament with a deep groove capable of binding DNA. The observed weakening in the higher order aggregation of filaments into bundles may have implications for recombination in mycobacteria. The structure of the complex reveals the atomic interactions of ADP-AlF(4), an ATP analogue, with the P-loop-containing binding pocket. The structures explain reduced levels of interactions of MtRecA with ATP, despite sharing the same fold, topology and high sequence similarity with EcRecA. The formation of a helical filament with a deep groove appears to be an inherent property of MtRecA. The histidine in loop L1 appears to be positioned appropriately for DNA interaction.

摘要

结核分枝杆菌全基因组测序,加之通过更好的药物和疫苗改善结核病管理的需求迅速增加,引发了对该病原体几种关键蛋白的广泛研究。RecA是一种普遍存在的多功能蛋白,是同源基因重组和DNA修复过程的关键组成部分。了解MtRecA的结构对于全面理解这两种活动以及任何后续应用至关重要。本文介绍的MtRecA晶体结构在单位晶胞中有六个分子,形成一个具有能够结合DNA的深沟的6(1)螺旋丝。观察到的丝束高阶聚集减弱可能对分枝杆菌中的重组有影响。复合物的结构揭示了ATP类似物ADP-AlF(4)与含P环结合口袋的原子相互作用。这些结构解释了尽管MtRecA与EcRecA具有相同的折叠、拓扑结构和高度序列相似性,但与ATP的相互作用水平降低的原因。形成具有深沟的螺旋丝似乎是MtRecA的固有特性。环L1中的组氨酸似乎处于适合与DNA相互作用的位置。

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