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噬菌体P4蛋白Psu与转录终止因子Rho形成复合物所需的相互作用表面。

Interaction surface of bacteriophage P4 protein Psu required for complex formation with the transcription terminator Rho.

作者信息

Pani Bibhusita, Ranjan Amitabh, Sen Ranjan

机构信息

Laboratory of Transcription Biology, Centre for DNA Fingerprinting and Diagnostics, Tuljaguda, Nampally, Hyderabad-500001, India.

出版信息

J Mol Biol. 2009 Jun 19;389(4):647-60. doi: 10.1016/j.jmb.2009.04.052. Epub 2009 May 3.

DOI:10.1016/j.jmb.2009.04.052
PMID:19409394
Abstract

Rho-dependent transcription termination is an essential function in prokaryotes, and the transcription terminator Rho is highly conserved among different species. The bacteriophage P4 capsid-decoration protein, Psu, interacts specifically with and inhibits the function of Escherichia coli Rho. The interaction surface of Psu involved in interacting with Rho is not known, but knowledge of this is important to understand the mechanism of its action and will be useful to design peptide inhibitor(s) for Rho. We have isolated and characterized seven Psu mutants defective in interacting with Rho and in exerting anti-Rho activity. Conformational probing of Psu revealed that the N-terminal region of the protein folds over onto its central part, forming a globular domain and leaving a solvent-exposed "tail" in the C-terminus. The mutations are located in both of these domains. N-terminal mutants are instrumental in disrupting the N- to C-terminal "cross-talk" in Psu that is required for its structural integrity and its function. Site-specific cross-linking experiments showed that the C-terminal tail preferentially cross-links to Rho and this region of Psu is protected from limited proteolysis when bound to Rho. Therefore, the mutations in this region may have affected the direct interaction of Psu with Rho. We propose that the globular N-terminal domain of Psu confers structural integrity to the functionally important C-terminal tail, which interacts directly with the hexameric Rho.

摘要

Rho 依赖性转录终止是原核生物中的一项基本功能,转录终止因子 Rho 在不同物种间高度保守。噬菌体 P4 衣壳装饰蛋白 Psu 可特异性地与大肠杆菌 Rho 相互作用并抑制其功能。目前尚不清楚 Psu 与 Rho 相互作用的表面,但了解这一点对于理解其作用机制很重要,并且对于设计 Rho 的肽抑制剂也将有所帮助。我们已经分离并鉴定了七个在与 Rho 相互作用及发挥抗 Rho 活性方面存在缺陷的 Psu 突变体。对 Psu 的构象探测表明,该蛋白的 N 端区域折叠到其中心部分之上,形成一个球状结构域,并在 C 端留下一个溶剂暴露的“尾巴”。这些突变位于这两个结构域中。N 端突变体有助于破坏 Psu 中 N 端到 C 端的“串扰”,而这种串扰对于其结构完整性和功能是必需的。位点特异性交联实验表明,C 端尾巴优先与 Rho 交联,并且当与 Rho 结合时,Psu 的这个区域可免受有限蛋白酶解的影响。因此,该区域的突变可能影响了 Psu 与 Rho 的直接相互作用。我们提出,Psu 的球状 N 端结构域赋予了对功能重要的 C 端尾巴的结构完整性,该 C 端尾巴直接与六聚体 Rho 相互作用。

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