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人线粒体核糖体与 EF-G1 结合的结构揭示了线粒体翻译延伸的独特特征。

Structures of the human mitochondrial ribosome bound to EF-G1 reveal distinct features of mitochondrial translation elongation.

机构信息

Division of Translational Medicine, Wadsworth Center, New York State Department of Health, Empire State Plaza, Albany, NY, 12201, USA.

Department of Chemistry, Campus Box 3290, University of North Carolina, Chapel Hill, NC, USA.

出版信息

Nat Commun. 2020 Jul 31;11(1):3830. doi: 10.1038/s41467-020-17715-2.

Abstract

The mammalian mitochondrial ribosome (mitoribosome) and its associated translational factors have evolved to accommodate greater participation of proteins in mitochondrial translation. Here we present the 2.68-3.96 Å cryo-EM structures of the human 55S mitoribosome in complex with the human mitochondrial elongation factor G1 (EF-G1) in three distinct conformational states, including an intermediate state and a post-translocational state. These structures reveal the role of several mitochondria-specific (mito-specific) mitoribosomal proteins (MRPs) and a mito-specific segment of EF-G1 in mitochondrial tRNA (tRNA) translocation. In particular, the mito-specific C-terminal extension in EF-G1 is directly involved in translocation of the acceptor arm of the A-site tRNA. In addition to the ratchet-like and independent head-swiveling motions exhibited by the small mitoribosomal subunit, we discover significant conformational changes in MRP mL45 at the nascent polypeptide-exit site within the large mitoribosomal subunit that could be critical for tethering of the elongating mitoribosome onto the inner-mitochondrial membrane.

摘要

哺乳动物线粒体核糖体(mitoribosome)及其相关翻译因子的进化,使其能够更大程度地参与线粒体翻译。在这里,我们展示了人类 55S 线粒体核糖体与人类线粒体延伸因子 G1(EF-G1)在三种不同构象状态下的 2.68-3.96Å 冷冻电镜结构,包括中间状态和翻译后状态。这些结构揭示了几种线粒体特异性(mito-specific)核糖体蛋白(MRP)和 EF-G1 的线粒体特异性片段在线粒体 tRNA(tRNA)转运中的作用。特别是,EF-G1 中的 mito-specific C 末端延伸直接参与 A 位 tRNA 接受臂的移位。除了小线粒体核糖体亚基表现出的棘轮样和独立的头部旋转运动外,我们还发现大线粒体核糖体亚基中新生多肽出口处的 MRP mL45 发生了显著的构象变化,这对于将延伸的线粒体核糖体固定在内质网膜上可能至关重要。

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