呼肠孤病毒非结构蛋白μNS将病毒核心表面蛋白和进入核心颗粒募集到工厂样包涵体中。
Reovirus nonstructural protein mu NS recruits viral core surface proteins and entering core particles to factory-like inclusions.
作者信息
Broering Teresa J, Kim Jonghwa, Miller Cathy L, Piggott Caroline D S, Dinoso Jason B, Nibert Max L, Parker John S L
机构信息
Department of Microbiology and Molecular Genetics, Harvard Medical School, Boston, Massachusetts 02115, USA.
出版信息
J Virol. 2004 Feb;78(4):1882-92. doi: 10.1128/jvi.78.4.1882-1892.2004.
Mammalian reoviruses are thought to assemble and replicate within cytoplasmic, nonmembranous structures called viral factories. The viral nonstructural protein mu NS forms factory-like globular inclusions when expressed in the absence of other viral proteins and binds to the surfaces of the viral core particles in vitro. Given these previous observations, we hypothesized that one or more of the core surface proteins may be recruited to viral factories through specific associations with mu NS. We found that all three of these proteins--lambda 1, lambda 2, and sigma 2--localized to factories in infected cells but were diffusely distributed through the cytoplasm and nucleus when each was separately expressed in the absence of other viral proteins. When separately coexpressed with mu NS, on the other hand, each core surface protein colocalized with mu NS in globular inclusions, supporting the initial hypothesis. We also found that lambda 1, lambda 2, and sigma 2 each localized to filamentous inclusions formed upon the coexpression of mu NS and mu 2, a structurally minor core protein that associates with microtubules. The first 40 residues of mu NS, which are required for association with mu 2 and the RNA-binding nonstructural protein sigma NS, were not required for association with any of the three core surface proteins. When coexpressed with mu 2 in the absence of mu NS, each of the core surface proteins was diffusely distributed and displayed only sporadic, weak associations with mu 2 on filaments. Many of the core particles that entered the cytoplasm of cycloheximide-treated cells following entry and partial uncoating were recruited to inclusions of mu NS that had been preformed in those cells, providing evidence that mu NS can bind to the surfaces of cores in vivo. These findings expand a model for how viral and cellular components are recruited to the viral factories in infected cells and provide further evidence for the central but distinct roles of viral proteins mu NS and mu 2 in this process.
哺乳动物呼肠孤病毒被认为在称为病毒工厂的细胞质非膜性结构内组装和复制。病毒非结构蛋白μNS在没有其他病毒蛋白的情况下表达时会形成工厂样球状包涵体,并且在体外与病毒核心颗粒表面结合。基于这些先前的观察结果,我们推测一种或多种核心表面蛋白可能通过与μNS的特异性结合被招募到病毒工厂中。我们发现这三种蛋白——λ1、λ2和σ2——在感染细胞中定位于工厂,但在没有其他病毒蛋白的情况下单独表达时,它们在细胞质和细胞核中呈弥散分布。另一方面,当与μNS分别共表达时,每种核心表面蛋白都与μNS在球状包涵体中共定位,支持了最初的假设。我们还发现,λ1、λ2和σ2各自定位于在μNS和μ2共表达时形成的丝状包涵体,μ2是一种与微管相关的结构上次要的核心蛋白。μNS与μ2和RNA结合非结构蛋白σNS结合所需的前40个残基,对于与三种核心表面蛋白中的任何一种结合不是必需的。在没有μNS的情况下与μ2共表达时,每种核心表面蛋白都呈弥散分布,并且在细丝上仅与μ2有零星、微弱的结合。许多在进入和部分脱壳后进入环己酰亚胺处理细胞细胞质的核心颗粒被招募到那些细胞中预先形成的μNS包涵体中,这证明μNS在体内可以与核心表面结合。这些发现扩展了一个关于病毒和细胞成分如何在感染细胞中被招募到病毒工厂的模型,并为病毒蛋白μNS和μ2在此过程中的核心但不同的作用提供了进一步的证据。
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