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真核生物 60S 核糖体亚基与起始因子 6 复合物的晶体结构。

Crystal structure of the eukaryotic 60S ribosomal subunit in complex with initiation factor 6.

机构信息

Institute of Molecular Biology and Biophysics, ETH Zürich, Zürich, Switzerland.

出版信息

Science. 2011 Nov 18;334(6058):941-8. doi: 10.1126/science.1211204. Epub 2011 Nov 3.

Abstract

Protein synthesis in all organisms is catalyzed by ribosomes. In comparison to their prokaryotic counterparts, eukaryotic ribosomes are considerably larger and are subject to more complex regulation. The large ribosomal subunit (60S) catalyzes peptide bond formation and contains the nascent polypeptide exit tunnel. We present the structure of the 60S ribosomal subunit from Tetrahymena thermophila in complex with eukaryotic initiation factor 6 (eIF6), cocrystallized with the antibiotic cycloheximide (a eukaryotic-specific inhibitor of protein synthesis), at a resolution of 3.5 angstroms. The structure illustrates the complex functional architecture of the eukaryotic 60S subunit, which comprises an intricate network of interactions between eukaryotic-specific ribosomal protein features and RNA expansion segments. It reveals the roles of eukaryotic ribosomal protein elements in the stabilization of the active site and the extent of eukaryotic-specific differences in other functional regions of the subunit. Furthermore, it elucidates the molecular basis of the interaction with eIF6 and provides a structural framework for further studies of ribosome-associated diseases and the role of the 60S subunit in the initiation of protein synthesis.

摘要

所有生物体中的蛋白质合成都由核糖体催化。与原核生物相比,真核生物的核糖体要大得多,并且受到更复杂的调控。大亚基(60S)催化肽键的形成,并包含新生多肽出口隧道。我们展示了嗜热四膜虫的 60S 核糖体亚基与真核起始因子 6(eIF6)复合物的结构,该复合物与抗生素环己酰亚胺(一种真核生物中蛋白质合成的特异性抑制剂)共结晶,分辨率为 3.5 埃。该结构说明了真核生物 60S 亚基复杂的功能结构,它由真核生物核糖体蛋白特征和 RNA 扩展片段之间的复杂相互作用网络组成。它揭示了真核核糖体蛋白元件在稳定活性位点以及亚基其他功能区域中真核生物特异性差异程度方面的作用。此外,它阐明了与 eIF6 相互作用的分子基础,并为核糖体相关疾病的研究以及 60S 亚基在蛋白质合成起始中的作用提供了结构框架。

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