Ribonucleoprotein transport in Negative Strand RNA viruses

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS ACS Applied Bio Materials Pub Date : 2022-10-03 DOI:10.1111/boc.202200059

Cédric Diot, Gina Cosentino, Marie-Anne Rameix-Welti

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引用次数: 2

Abstract

Negative-sense, single-stranded RNA (-ssRNA) viruses comprise some of the deadliest human pathogens (Ebola, rabies, influenza A viruses etc.). Developing therapeutic tools relies on a better understanding of their multiplication cycle. For these viruses, the genome replication and transcription activities most-often segregate in membrane-less environments called inclusion bodies (IBs) or viral factories. These “organelles” usually locate far from the cell surface from where new virions are released, and -ssRNA viruses do not encode for transport factors. The efficient trafficking of the genome progeny toward the cell surface is most often ensured by mechanisms co-opting the cellular machineries.

In this review, for each -ssRNA viral family, we cover the methods employed to characterize these host-virus interactions, the strategies used by the viruses to promote the virus genome transport, and the current gaps in the literature. Finally, we highlight how Rab11 has emerged as a target of choice for the intracellular transport of -ssRNA virus genomes.

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负链RNA病毒中的核糖核蛋白转运

负义单链RNA (-ssRNA)病毒包括一些最致命的人类病原体(埃博拉病毒、狂犬病病毒、甲型流感病毒等)。开发治疗工具依赖于更好地了解它们的增殖周期。对于这些病毒，基因组复制和转录活动通常在称为包涵体(IBs)或病毒工厂的无膜环境中分离。这些“细胞器”通常位于远离新病毒粒子释放的细胞表面的地方，而且-ssRNA病毒不编码转运因子。基因组子代向细胞表面的有效运输通常是通过选择细胞机器的机制来确保的。在这篇综述中，对于每个-ssRNA病毒家族，我们涵盖了用来表征这些宿主-病毒相互作用的方法，病毒用来促进病毒基因组运输的策略，以及目前文献中的空白。最后，我们强调Rab11如何成为-ssRNA病毒基因组胞内转运的首选靶标。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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