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单链RNA病毒中基因组及基因组传递装置的原位结构

In situ structures of the genome and genome-delivery apparatus in a single-stranded RNA virus.

作者信息

Dai Xinghong, Li Zhihai, Lai Mason, Shu Sara, Du Yushen, Zhou Z Hong, Sun Ren

机构信息

Department of Molecular and Medical Pharmacology, University of California, Los Angeles (UCLA), Los Angeles, California 90095, USA.

The California NanoSystems Institute (CNSI), UCLA, Los Angeles, California 90095, USA.

出版信息

Nature. 2017 Jan 5;541(7635):112-116. doi: 10.1038/nature20589. Epub 2016 Dec 19.

Abstract

Packaging of the genome into a protein capsid and its subsequent delivery into a host cell are two fundamental processes in the life cycle of a virus. Unlike double-stranded DNA viruses, which pump their genome into a preformed capsid, single-stranded RNA (ssRNA) viruses, such as bacteriophage MS2, co-assemble their capsid with the genome; however, the structural basis of this co-assembly is poorly understood. MS2 infects Escherichia coli via the host 'sex pilus' (F-pilus); it was the first fully sequenced organism and is a model system for studies of translational gene regulation, RNA-protein interactions, and RNA virus assembly. Its positive-sense ssRNA genome of 3,569 bases is enclosed in a capsid with one maturation protein monomer and 89 coat protein dimers arranged in a T = 3 icosahedral lattice. The maturation protein is responsible for attaching the virus to an F-pilus and delivering the viral genome into the host during infection, but how the genome is organized and delivered is not known. Here we describe the MS2 structure at 3.6 Å resolution, determined by electron-counting cryo-electron microscopy (cryoEM) and asymmetric reconstruction. We traced approximately 80% of the backbone of the viral genome, built atomic models for 16 RNA stem-loops, and identified three conserved motifs of RNA-coat protein interactions among 15 of these stem-loops with diverse sequences. The stem-loop at the 3' end of the genome interacts extensively with the maturation protein, which, with just a six-helix bundle and a six-stranded β-sheet, forms a genome-delivery apparatus and joins 89 coat protein dimers to form a capsid. This atomic description of genome-capsid interactions in a spherical ssRNA virus provides insight into genome delivery via the host sex pilus and mechanisms underlying ssRNA-capsid co-assembly, and inspires speculation about the links between nucleoprotein complexes and the origins of viruses.

摘要

将基因组包装到蛋白质衣壳中并随后将其递送至宿主细胞是病毒生命周期中的两个基本过程。与将基因组泵入预先形成的衣壳中的双链DNA病毒不同,单链RNA(ssRNA)病毒,如噬菌体MS2,会将其衣壳与基因组共同组装;然而,这种共同组装的结构基础却知之甚少。MS2通过宿主的“性菌毛”(F菌毛)感染大肠杆菌;它是第一个被完全测序的生物体,是研究翻译基因调控、RNA-蛋白质相互作用和RNA病毒组装的模型系统。其由3569个碱基组成的正链ssRNA基因组被包裹在一个衣壳中,该衣壳由一个成熟蛋白单体和89个衣壳蛋白二聚体排列成T = 3二十面体晶格。成熟蛋白负责在感染期间将病毒附着到F菌毛上并将病毒基因组递送至宿主,但基因组是如何组织和递送的尚不清楚。在这里,我们描述了通过电子计数冷冻电子显微镜(cryoEM)和不对称重建确定的分辨率为3.6 Å的MS2结构。我们追踪了病毒基因组约80%的主链,为16个RNA茎环构建了原子模型,并在这些具有不同序列的15个茎环中鉴定出RNA-衣壳蛋白相互作用的三个保守基序。基因组3'端的茎环与成熟蛋白广泛相互作用,成熟蛋白仅由一个六螺旋束和一个六链β折叠形成一个基因组递送装置,并连接89个衣壳蛋白二聚体形成一个衣壳。这种对球形ssRNA病毒中基因组-衣壳相互作用的原子描述为通过宿主性菌毛进行基因组递送以及ssRNA-衣壳共同组装的潜在机制提供了见解,并引发了对核蛋白复合物与病毒起源之间联系的推测。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a638/5701785/7a1b653e9625/nihms825899f6.jpg

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