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核糖体中的各向异性波动决定 tRNA 动力学。

Anisotropic Fluctuations in the Ribosome Determine tRNA Kinetics.

机构信息

Department of Physics, Northeastern University , Dana Research Center 111, 360 Huntington Avenue, Boston, Massachusetts 02115, United States.

Max Delbrück Center for Molecular Medicine , Berlin, Germany.

出版信息

J Phys Chem B. 2017 Nov 30;121(47):10593-10601. doi: 10.1021/acs.jpcb.7b06828. Epub 2017 Oct 2.

DOI:10.1021/acs.jpcb.7b06828
PMID:28910101
Abstract

The ribosome is a large ribonucleoprotein complex that is responsible for the production of proteins in all organisms. Accommodation is the process by which an incoming aminoacyl-tRNA (aa-tRNA) molecule binds the ribosomal A site, and its kinetics has been implicated in the accuracy of tRNA selection. In addition to rearrangements in the aa-tRNA molecule, the L11 stalk can undergo large-scale anisotropic motions during translation. To explore the potential impact of this protruding region on the rate of aa-tRNA accommodation, we used molecular dynamics simulations with a simplified model to evaluate the free energy as a function of aa-tRNA position. Specifically, these calculations describe the transition between A/T and elbow-accommodated (EA) configurations (∼20 Å displacement). We find that the free-energy barrier associated with elbow accommodation is proportional to the degree of mobility exhibited by the L11 stalk. That is, when L11 is more rigid, the free-energy barrier height is decreased. This effect arises from the ability of L11 to confine, and thereby destabilize, the A/T ensemble. In addition, when elongation factor Tu (EF-Tu) is present, the A/T ensemble is further destabilized in an L11-dependent manner. These results provide a framework that suggests how next-generation experiments may precisely control the dynamics of the ribosome.

摘要

核糖体是一种大型的核糖核蛋白复合物,负责所有生物中蛋白质的生成。容纳是指进入的氨酰基-tRNA(aa-tRNA)分子与核糖体 A 位结合的过程,其动力学与 tRNA 选择的准确性有关。除了 aa-tRNA 分子的重排外,L11 茎在翻译过程中还可以进行大规模的各向异性运动。为了探究该突出区域对 aa-tRNA 容纳速率的潜在影响,我们使用简化模型的分子动力学模拟来评估 aa-tRNA 位置的自由能函数。具体来说,这些计算描述了 A/T 和肘容纳(EA)构象之间的转变(约 20Å 位移)。我们发现,与肘容纳相关的自由能障碍与 L11 茎的可移动性程度成正比。也就是说,当 L11 更僵硬时,自由能障碍的高度降低。这种效应源于 L11 限制和因此不稳定 A/T 集合的能力。此外,当延伸因子 Tu(EF-Tu)存在时,A/T 集合以依赖于 L11 的方式进一步不稳定。这些结果提供了一个框架,表明下一代实验如何可以精确地控制核糖体的动力学。

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