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负链病毒酶学机制的结构与调控。

Architecture and regulation of negative-strand viral enzymatic machinery.

机构信息

Department of Microbiology & Immunobiology, Harvard Medical School, Boston, MA, USA.

出版信息

RNA Biol. 2012 Jul;9(7):941-8. doi: 10.4161/rna.20345. Epub 2012 Jul 1.

Abstract

Negative-strand (NS) RNA viruses initiate infection with a unique polymerase complex that mediates both mRNA transcription and subsequent genomic RNA replication. For nearly all NS RNA viruses, distinct enzymatic domains catalyzing RNA polymerization and multiple steps of 5' mRNA cap formation are contained within a single large polymerase protein (L). While NS RNA viruses include a variety of emerging human and agricultural pathogens, the enzymatic machinery driving viral replication and gene expression remains poorly understood. Recent insights with Machupo virus and vesicular stomatitis virus have provided the first structural information of viral L proteins, and revealed how the various enzymatic domains are arranged into a conserved architecture shared by both segmented and nonsegmented NS RNA viruses. In vitro systems reconstituting RNA synthesis from purified components provide new tools to understand the viral replicative machinery, and demonstrate the arenavirus matrix protein regulates RNA synthesis by locking a polymerase-template complex. Inhibition of gene expression by the viral matrix protein is a distinctive feature also shared with influenza A virus and nonsegmented NS RNA viruses, possibly illuminating a conserved mechanism for coordination of viral transcription and polymerase packaging.

摘要

负链 (NS) RNA 病毒以独特的聚合酶复合物起始感染,该复合物介导 mRNA 转录和随后的基因组 RNA 复制。对于几乎所有的 NS RNA 病毒,催化 RNA 聚合和 5' mRNA 帽形成的多个步骤的不同酶结构域都包含在单个大聚合酶蛋白 (L) 内。虽然 NS RNA 病毒包括多种新兴的人类和农业病原体,但驱动病毒复制和基因表达的酶机制仍知之甚少。最近对马丘波病毒和水疱性口炎病毒的研究提供了病毒 L 蛋白的第一个结构信息,并揭示了各种酶结构域如何排列成一个由有节段和无节段 NS RNA 病毒共享的保守结构。从纯化成分中重新组装 RNA 合成的体外系统提供了新的工具来理解病毒复制机制,并证明了沙粒病毒的基质蛋白通过锁定聚合酶-模板复合物来调节 RNA 合成。病毒基质蛋白对基因表达的抑制是流感 A 病毒和无节段 NS RNA 病毒的共同特征,这可能阐明了病毒转录和聚合酶包装协调的保守机制。

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