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TrwC介导的位点特异性重组受改变局部DNA拓扑结构的宿主因子控制。

TrwC-mediated site-specific recombination is controlled by host factors altering local DNA topology.

作者信息

César Carolina Elvira, Llosa Matxalen

机构信息

Departamento de Biología Molecular, Universidad de Cantabria, and Instituto de Biomedicina y Biotecnología de Cantabria, Universidad de Cantabria-CSIC-IDICAN, Santander, Spain.

出版信息

J Bacteriol. 2007 Dec;189(24):9037-43. doi: 10.1128/JB.01152-07. Epub 2007 Oct 5.

Abstract

R388 conjugative relaxase TrwC acts as a site-specific recombinase, promoting recombination between two cognate oriTs on double-stranded DNA substrates. The relaxosome component TrwA is also required for efficient recombination. In this work we present data on the in vivo control of this reaction by host proteins that affect local DNA topology. In the absence of TrwA, binding of integration host factor (IHF) to the oriT keeps the recombination levels low, probably by keeping the relaxosome complex, formed at recombination locus 1, in a "closed" conformation. In an IHF-deficient (IHF-) background, the formation of a transcript elongation complex at this locus still hampers recombination. A mutation abating the promoter sequence at locus 1, or repression of transcription by exposure to rifampin, lifts the inhibition imposed on recombination in an IHF- background. We also observe an increase in conjugation efficiency under these conditions. Relieving the inhibition imposed by these host factors allows efficient levels of recombination between short oriT loci in the absence of TrwA. The presence of TrwA counteracts these inhibitory effects. TrwA would then activate both recombination and conjugation by switching the conformation of the relaxosome to an "open" form that exposes single-stranded DNA at the nic site, promoting the initial TrwC nicking reaction.

摘要

R388接合松弛酶TrwC作为一种位点特异性重组酶,促进双链DNA底物上两个同源oriT之间的重组。松弛体组分TrwA对于高效重组也是必需的。在这项工作中,我们展示了关于宿主蛋白对该反应进行体内调控的数据,这些宿主蛋白会影响局部DNA拓扑结构。在没有TrwA的情况下,整合宿主因子(IHF)与oriT的结合使重组水平保持较低,这可能是通过使在重组位点1形成的松弛体复合物处于“封闭”构象来实现的。在IHF缺陷(IHF-)背景下,该位点转录延伸复合物的形成仍然会阻碍重组。使位点1的启动子序列发生突变,或通过暴露于利福平来抑制转录,可解除在IHF-背景下对重组施加的抑制。我们还观察到在这些条件下接合效率有所提高。解除这些宿主因子施加的抑制可使在没有TrwA的情况下短oriT位点之间实现高效水平的重组。TrwA的存在可抵消这些抑制作用。然后,TrwA会通过将松弛体的构象转换为“开放”形式来激活重组和接合,这种开放形式会在切口位点暴露单链DNA,促进最初的TrwC切口反应。

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本文引用的文献

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A new domain of conjugative relaxase TrwC responsible for efficient oriT-specific recombination on minimal target sequences.
Mol Microbiol. 2006 Nov;62(4):984-96. doi: 10.1111/j.1365-2958.2006.05437.x. Epub 2006 Oct 13.
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Site-specific recombinase and integrase activities of a conjugative relaxase in recipient cells.
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