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核糖体对tRNA的选择需要从开放形式转变为封闭形式。

Selection of tRNA by the ribosome requires a transition from an open to a closed form.

作者信息

Ogle James M, Murphy Frank V, Tarry Michael J, Ramakrishnan V

机构信息

MRC Laboratory of Molecular Biology, Hills Road, CB2 2QH, Cambridge, United Kingdom.

出版信息

Cell. 2002 Nov 27;111(5):721-32. doi: 10.1016/s0092-8674(02)01086-3.

Abstract

A structural and mechanistic explanation for the selection of tRNAs by the ribosome has been elusive. Here, we report crystal structures of the 30S ribosomal subunit with codon and near-cognate tRNA anticodon stem loops bound at the decoding center and compare affinities of equivalent complexes in solution. In ribosomal interactions with near-cognate tRNA, deviation from Watson-Crick geometry results in uncompensated desolvation of hydrogen-bonding partners at the codon-anticodon minor groove. As a result, the transition to a closed form of the 30S induced by cognate tRNA is unfavorable for near-cognate tRNA unless paromomycin induces part of the rearrangement. We conclude that stabilization of a closed 30S conformation is required for tRNA selection, and thereby structurally rationalize much previous data on translational fidelity.

摘要

核糖体对tRNA的选择在结构和机制上的解释一直难以捉摸。在此,我们报告了30S核糖体亚基的晶体结构,其密码子和近同源tRNA反密码子茎环结合在解码中心,并比较了溶液中等效复合物的亲和力。在核糖体与近同源tRNA的相互作用中,偏离沃森-克里克几何结构会导致密码子-反密码子小沟处氢键结合伙伴的去溶剂化无法得到补偿。因此,由同源tRNA诱导的30S向闭合形式的转变对近同源tRNA不利,除非巴龙霉素诱导部分重排。我们得出结论,tRNA选择需要稳定的30S闭合构象,从而在结构上合理化了此前许多关于翻译保真度的数据。

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