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首页> 外文期刊>Nucleic acids research >Structural and mechanistic basis of anti-termination of Rho-dependent transcription termination by bacteriophage P4 capsid protein Psu
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Structural and mechanistic basis of anti-termination of Rho-dependent transcription termination by bacteriophage P4 capsid protein Psu

机译:噬菌体P4衣壳蛋白Psu抗Rho依赖性转录终止的结构和机制基础

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The conserved bacterial transcription terminator, Rho, is a potent target for bactericidal agents. Psu, a bacteriophage P4 capsid protein, is capable of inducing anti-termination to the Rho-dependent transcription termination. Knowledge of structural and mechanistic basis of this anti-termination is required to design peptide-inhibitor(s) of Rho from Psu. Using suppressor genetics, cross-linking, protein foot-printing and FRET analyses, we describe a conserved disordered structure, encompassing 139–153 amino acids of Rho, as the primary docking site for Psu. Also a neighbouring helical structure, comprising 347–354 amino acids, lining its central channel, plays a supportive role in the Rho–Psu complex formation. Based on the crystal structure of Psu, its conformation in the capsid of the P4 phage, and its interacting regions on Rho, we build an energy-minimized structural model of the Rho:Psu complex. In this model, a V-shaped dimer of Psu interacts with the two diagonally opposite subunits of a hexameric Rho, enabling Psu to form a ‘lid' on the central channel of the latter. We show that this configuration of Psu makes the central channel of Rho inaccessible, and it causes a mechanical impediment to its translocase activity.
机译:保守的细菌转录终止子Rho是杀菌剂的有效靶标。 Psu是噬菌体的P4衣壳蛋白,能够诱导对Rho依赖性转录终止的抗终止作用。从Psu设计Rho的肽抑制剂需要了解这种抗终止的结构和机理基础。使用抑制基因,交联,蛋白质足迹和FRET分析,我们描述了一个保守的无序结构,包括Rho的139-153个氨基酸,是Psu的主要停靠位点。在其Rho-Psu复合物的形成中,一个相邻的螺旋结构(由347-354个氨基酸组成)位于其中心通道内,起支撑作用。基于Psu的晶体结构,其在P4噬菌体衣壳中的构象及其在Rho上的相互作用区域,我们建立了Rho:Psu配合物的能量最小化结构模型。在该模型中,Psu的V形二聚体与六聚体Rho的两个对角相对的亚基相互作用,从而使Psu可以在后者的中央通道上形成“盖”。我们表明,Psu的这种配置使Rho的中央通道无法访问,并且对其转位酶活性造成了机械障碍。

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