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轮状病毒装配-复制中间体的电子显微镜分析

Electron microscopic analysis of rotavirus assembly-replication intermediates.

作者信息

Boudreaux Crystal E, Kelly Deborah F, McDonald Sarah M

机构信息

Virginia Tech Carilion School of Medicine and Research Institute, Roanoke, VA, USA.

Virginia Tech Carilion School of Medicine and Research Institute, Roanoke, VA, USA; Department of Biomedical Sciences and Pathobiology, Virginia-Maryland Regional College of Veterinary Medicine, Blacksburg, VA, USA.

出版信息

Virology. 2015 Mar;477:32-41. doi: 10.1016/j.virol.2015.01.003. Epub 2015 Jan 28.

Abstract

Rotaviruses (RVs) replicate their segmented, double-stranded RNA genomes in tandem with early virion assembly. In this study, we sought to gain insight into the ultrastructure of RV assembly-replication intermediates (RIs) using transmission electron microscopy (EM). Specifically, we examined a replicase-competent, subcellular fraction that contains all known RV RIs. Three never-before-seen complexes were visualized in this fraction. Using in vitro reconstitution, we showed that ~15-nm doughnut-shaped proteins in strings were nonstructural protein 2 (NSP2) bound to viral RNA transcripts. Moreover, using immunoaffinity-capture EM, we revealed that ~20-nm pebble-shaped complexes contain the viral RNA polymerase (VP1) and RNA capping enzyme (VP3). Finally, using a gel purification method, we demonstrated that ~30-70-nm electron-dense, particle-shaped complexes represent replicase-competent core RIs, containing VP1, VP3, and NSP2 as well as capsid proteins VP2 and VP6. The results of this study raise new questions about the interactions among viral proteins and RNA during the concerted assembly-replicase process.

摘要

轮状病毒(RVs)在早期病毒体组装的同时复制其分段的双链RNA基因组。在本研究中,我们试图通过透射电子显微镜(EM)深入了解RV组装-复制中间体(RIs)的超微结构。具体而言,我们检查了一个具有复制酶活性的亚细胞组分,其中包含所有已知的RV RIs。在该组分中观察到三种前所未见的复合物。通过体外重组,我们表明成串的约15纳米甜甜圈状蛋白质是与病毒RNA转录本结合的非结构蛋白2(NSP2)。此外,通过免疫亲和捕获EM,我们发现约20纳米卵石状复合物包含病毒RNA聚合酶(VP1)和RNA加帽酶(VP3)。最后,通过凝胶纯化方法,我们证明约30-70纳米电子致密的颗粒状复合物代表具有复制酶活性的核心RIs,包含VP1、VP3和NSP2以及衣壳蛋白VP2和VP6。本研究结果对协同组装-复制酶过程中病毒蛋白与RNA之间的相互作用提出了新问题。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/71fc/4359669/def52c8d1e62/nihms661110f1.jpg

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