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Analysis of Rab GTPase-Activating Proteins Indicates that Rab1a/b and Rab43 Are Important for Herpes Simplex Virus 1 Secondary Envelopment

机译:Rab GTPase激活蛋白的分析表明Rab1a / b和Rab43对单纯疱疹病毒1次要包膜很重要

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摘要

Assembly of herpes simplex virus 1 (HSV-1) occurs in the cytoplasm, where the capsid and tegument bud into host cell membranes. It is at this point that the viral glycoproteins are incorporated into the virion, as they are located at the assembly site. We investigated the role of the Rab GTPases in coordinating the assembly process by overexpressing 37 human Rab GTPase-activating proteins (GAPs) and assessing infectious titers. Rab GTPases are key cellular regulators of membrane trafficking events that, by their membrane association and binding of effector proteins, ensure the appropriate fusion of membranes. We identified that TBC1D20 and RN-tre and their partner Rabs, Rab1a/b and Rab43, respectively, are important for virion assembly. In the absence of Rab1a/b, the viral glycoproteins are unable to traffic from the endoplasmic reticulum to the assembly compartment, and thus unenveloped particles build up in the cytoplasm. The defect resulting from Rab43 depletion is somewhat more complex, but it appears that the fragmentation and dispersal of the trans-Golgi network and associated membranes render these compartments unable to support secondary envelopment.
机译:单纯疱疹病毒1(HSV-1)的组装在细胞质中发生,在那里衣壳和外皮萌芽进入宿主细胞膜。正是在这一点上,病毒糖蛋白被整合到病毒体中,因为它们位于装配位点。我们调查了Rab GTPases在通过过度表达37个人Rab GTPase激活蛋白(GAP)和评估感染滴度来协调装配过程中的作用。 Rab GTPases是膜运输事件的关键细胞调节剂,通过它们的膜结合和效应蛋白的结合,可确保膜的适当融合。我们确定,TBC1D20和RN-tre及其伙伴Rabs,Rab1a / b和Rab43分别对于病毒体组装很重要。在没有Rab1a / b的情况下,病毒糖蛋白无法从内质网运输到装配室,因此未包被的颗粒会在细胞质中堆积。 Rab43耗竭导致的缺陷有些复杂,但是反式高尔基体网络和相关膜的破碎和分散似乎使这些隔室无法支持次级包膜。

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