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做好发现准备:呼肠孤病毒进入中间态的原子分辨率冷冻电镜结构。

Primed for Discovery: Atomic-Resolution Cryo-EM Structure of a Reovirus Entry Intermediate.

机构信息

Laboratory of Infectious Diseases, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, MD 20892, USA.

出版信息

Viruses. 2010 Jun;2(6):1340-1346. doi: 10.3390/v2061340. Epub 2010 Jun 15.

Abstract

A recently solved structure of the aquareovirus virion (Zhang, X; Jin, L.; Fang, Q; Hui, W.H.; Zhou Z.H. 3.3 Å Cryo-EM Structure of a Nonenveloped Virus Reveals a Priming Mechanism for Cell Entry. Cell2010, 141, 472-482 [1]) provides new insights into the order of entry events, as well as confirming and refining several aspects of the entry mechanism, for aquareovirus and the related orthoreovirus. In particular, the structure provides evidence of a defined order for the progressive proteolytic cleavages of myristoylated penetration protein VP5 that prime the virion for membrane penetration. These observations reinforce the concept that, much like enveloped viruses, nonenveloped virions often undergo priming events that lead to a meta-stable state, preparing the virus for membrane penetration under the appropriate circumstances. In addition, this and other recent studies highlight the increasing power of electron cryomicroscopy to analyze large, geometrically regular structures, such as icosahedral viruses, at atomic resolution.

摘要

最近解决的 aquareovirus 病毒粒子结构(Zhang, X; Jin, L.; Fang, Q; Hui, W.H.; Zhou Z.H. 3.3 Å Cryo-EM Structure of a Nonenveloped Virus Reveals a Priming Mechanism for Cell Entry. Cell2010, 141, 472-482 [1])为 aquareovirus 和相关的 orthoreovirus 的进入事件的顺序提供了新的见解,同时也证实和完善了进入机制的几个方面。特别是,该结构提供了证据表明,myristoylated penetration protein VP5 的逐步蛋白水解切割具有明确的顺序,使病毒粒子为膜穿透做好准备。这些观察结果强化了这样的概念,即与包膜病毒类似,无包膜病毒通常会经历引发事件,导致亚稳定状态,为在适当的情况下进行膜穿透做好准备。此外,这项研究和其他最近的研究强调了电子低温显微镜在分析大型、几何规则结构(如二十面体病毒)方面的日益强大的能力,可以达到原子分辨率。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8d73/3185709/eb9170d17ef3/viruses-02-01340f1.jpg

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