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通过光交联探测核糖体结合的新生多肽与异源寡聚伴侣蛋白TRiC亚基之间的共翻译接触。

The cotranslational contacts between ribosome-bound nascent polypeptides and the subunits of the hetero-oligomeric chaperonin TRiC probed by photocross-linking.

作者信息

Etchells Stephanie A, Meyer Anne S, Yam Alice Y, Roobol Anne, Miao Yiwei, Shao Yuanlong, Carden Martin J, Skach William R, Frydman Judith, Johnson Arthur E

机构信息

Department of Biochemistry and Biophysics, Texas A&M University, College Station, Texas 77843, USA.

出版信息

J Biol Chem. 2005 Jul 29;280(30):28118-26. doi: 10.1074/jbc.M504110200. Epub 2005 May 30.

DOI:10.1074/jbc.M504110200
PMID:15929940
Abstract

The hetero-oligomeric eukaryotic chaperonin TRiC (TCP-1-ring complex, also called CCT) interacts cotranslationally with a diverse subset of newly synthesized proteins, including actin, tubulin, and luciferase, and facilitates their correct folding. A photocross-linking approach has been used to map the contacts between individual chaperonin subunits and ribosome-bound nascent chains of increasing length. Whereas a cryo-EM study suggests that chemically denatured actin interacts with only two TRiC subunits (delta and either beta or epsilon), actin and luciferase chains photocross-link to at least six TRiC subunits (alpha, beta, delta, epsilon, xi, and theta) at different stages of translation. Furthermore, the photocross-linking of actin, but not luciferase, nascent chains to TRiC subunits zeta and theta was length-dependent. In addition, a single photoreactive probe incorporated at a unique site in actin nascent chains of different lengths reacted covalently with multiple TRiC subunits, thereby indicating that the nascent chain samples the polypeptide binding sites of different subunits. We conclude that elongating actin and luciferase nascent chains contact multiple TRiC subunits upon emerging from the ribosome, and that the TRiC subunits contacted by nascent actin change as it elongates and starts to fold.

摘要

异源寡聚真核伴侣蛋白TRiC(TCP-1环复合物,也称为CCT)在共翻译过程中与多种新合成的蛋白质相互作用,包括肌动蛋白、微管蛋白和荧光素酶,并促进它们正确折叠。一种光交联方法已被用于绘制单个伴侣蛋白亚基与核糖体结合的长度不断增加的新生链之间的接触位点。虽然一项冷冻电镜研究表明化学变性的肌动蛋白仅与两个TRiC亚基(δ和β或ε)相互作用,但肌动蛋白和荧光素酶链在翻译的不同阶段与至少六个TRiC亚基(α、β、δ、ε、ξ和θ)发生光交联。此外,肌动蛋白新生链而非荧光素酶新生链与TRiC亚基ζ和θ的光交联是长度依赖性的。另外,在不同长度的肌动蛋白新生链的独特位点掺入的单个光反应性探针与多个TRiC亚基发生共价反应,从而表明新生链对不同亚基的多肽结合位点进行了采样。我们得出结论,正在延长的肌动蛋白和荧光素酶新生链从核糖体出现时会与多个TRiC亚基接触,并且新生肌动蛋白接触的TRiC亚基会随着其延长和开始折叠而发生变化。

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