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细菌核糖体中核糖体蛋白S7和S11之间的功能相互作用。

A functional interaction between ribosomal proteins S7 and S11 within the bacterial ribosome.

作者信息

Robert Francis, Brakier-Gingras Léa

机构信息

Département de Biochimie, Université de Montréal, Montréal, Québec H3C 3J7, Canada.

出版信息

J Biol Chem. 2003 Nov 7;278(45):44913-20. doi: 10.1074/jbc.M306534200. Epub 2003 Aug 22.

Abstract

In this study, we used site-directed mutagenesis to disrupt an interaction that had been detected between ribosomal proteins S7 and S11 in the crystal structure of the bacterial 30 S subunit. This interaction, which is located in the E site, connects the head of the 30 S subunit to the platform and is involved in the formation of the exit channel through which passes the 30 S-bound messenger RNA. Neither mutations in S7 nor mutations in S11 prevented the incorporation of the proteins into the 30 S subunits but they perturbed the function of the ribosome. In vivo assays showed that ribosomes with either mutated S7 or S11 were altered in the control of translational fidelity, having an increased capacity for frameshifting, readthrough of a nonsense codon and codon misreading. Toeprinting and filter-binding assays showed that 30 S subunits with either mutated S7 or S11 have an enhanced capacity to bind mRNA. The effects of the S7 and S11 mutations can be related to an increased flexibility of the head of the 30 S, to an opening of the mRNA exit channel and to a perturbation of the proposed allosteric coupling between the A and E sites. Altogether, our results demonstrate that S7 and S11 interact in a functional manner and support the notion that protein-protein interactions contribute to the dynamics of the ribosome.

摘要

在本研究中,我们利用定点诱变来破坏细菌30 S亚基晶体结构中核糖体蛋白S7和S11之间已检测到的相互作用。这种位于E位点的相互作用,将30 S亚基的头部与平台相连,并参与了30 S结合的信使核糖核酸(mRNA)通过的出口通道的形成。S7或S11的突变均未阻止这些蛋白质掺入30 S亚基,但它们扰乱了核糖体的功能。体内试验表明,带有突变S7或S11的核糖体在翻译保真度控制方面发生了改变,移码、无义密码子通读和密码子错读的能力增强。足迹法和滤膜结合试验表明,带有突变S7或S11的30 S亚基结合mRNA的能力增强。S7和S11突变的影响可能与30 S头部增加的灵活性、mRNA出口通道的开放以及A位点和E位点之间假定的变构偶联的扰动有关。总之,我们的结果表明S7和S11以功能相关的方式相互作用,并支持蛋白质 - 蛋白质相互作用有助于核糖体动态变化的观点。

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