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核糖体tRNA结合位点:翻译的三位点模型

Ribosomal tRNA binding sites: three-site models of translation.

作者信息

Burkhardt N, Jünemann R, Spahn C M, Nierhaus K H

机构信息

Max-Planck-Institut für Molekulare Genetik, Berlin, Germany.

出版信息

Crit Rev Biochem Mol Biol. 1998;33(2):95-149. doi: 10.1080/10409239891204189.

Abstract

The first models of translation described protein synthesis in terms of two operationally defined tRNA binding sites, the P-site for the donor substrate, the peptidyl-tRNA, and the A-site for the acceptor substrates, the aminoacyl-tRNAs. The discovery and analysis of the third tRNA binding site, the E-site specific for deacylated tRNAs, resulted in the allosteric three-site model, the two major features of which are (1) the reciprocal relationship of A-site and E-site occupation, and (2) simultaneous codon-anticodon interactions of both tRNAs present at the elongating ribosome. However, structural studies do not support the three operationally defined sites in a simple fashion as three topographically fixed entities, thus leading to new concepts of tRNA binding and movement: (1) the hybrid-site model describes the tRNAs' movement through the ribosome in terms of changing binding sites on the 30S and 50S subunits in an alternating fashion. The tRNAs thereby pass through hybrid binding states. (2) The alpha-epsilon model introduces the concept of a movable tRNA-binding domain comprising two binding sites, termed alpha and epsilon. The translocation movement is seen as a result of a conformational change of the ribosome rather than as a diffusion process between fixed binding sites. The alpha-epsilon model reconciles most of the experimental data currently available.

摘要

最早的翻译模型是根据两个在操作上定义的tRNA结合位点来描述蛋白质合成的,供体底物肽基-tRNA的P位点和受体底物氨酰-tRNA的A位点。第三个tRNA结合位点(即脱酰基tRNA特异性的E位点)的发现和分析,产生了变构三位点模型,其两个主要特征是:(1)A位点和E位点占据的相互关系;(2)延伸核糖体上存在的两个tRNA同时进行密码子-反密码子相互作用。然而,结构研究并不简单地支持这三个在操作上定义的位点是三个地形固定的实体,从而产生了tRNA结合和移动的新概念:(1)杂交位点模型根据tRNA在30S和50S亚基上交替变化的结合位点来描述其在核糖体中的移动。tRNA因此经历杂交结合状态。(2)α-ε模型引入了一个可移动的tRNA结合结构域的概念,该结构域包含两个称为α和ε的结合位点。转位运动被视为核糖体构象变化的结果,而不是固定结合位点之间的扩散过程。α-ε模型协调了目前可用的大部分实验数据。

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