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轮状病毒感染中通过调控 Argonaute2 实现 RNA 干扰的两相调节。

Biphasic regulation of RNA interference during rotavirus infection by modulation of Argonaute2.

机构信息

Division of Virology, National Institute of Cholera and Enteric Diseases, Kolkata, India.

Department of Biotechnology, GITAM Institute of Science, Visakhapatnam, India.

出版信息

Cell Microbiol. 2019 Dec;21(12):e13101. doi: 10.1111/cmi.13101. Epub 2019 Aug 26.

DOI:10.1111/cmi.13101
PMID:31424151
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7162324/
Abstract

RNA interference (RNAi) is an evolutionary ancient innate immune response in plants, nematodes, and arthropods providing natural protection against viral infection. Viruses have also gained counter-defensive measures by producing virulence determinants called viral-suppressors-of-RNAi (VSRs). Interestingly, in spite of dominance of interferon-based immunity over RNAi in somatic cells of higher vertebrates, recent reports are accumulating in favour of retention of the antiviral nature of RNAi in mammalian cells. The present study focuses on the modulation of intracellular RNAi during infection with rotavirus (RV), an enteric virus with double-stranded RNA genome. Intriguingly, a time point-dependent bimodal regulation of RNAi was observed in RV-infected cells, where short interfering RNA (siRNA)-based RNAi was rendered non-functional during early hours of infection only to be reinstated fully beyond that early infection stage. Subsequent investigations revealed RV nonstructural protein 1 to serve as a putative VSR by associating with and triggering degradation of Argonaute2 (AGO2), the prime effector of siRNA-mediated RNAi, via ubiquitin-proteasome pathway. The proviral significance of AGO2 degradation was further confirmed when ectopic overexpression of AGO2 significantly reduced RV infection. Cumulatively, the current study presents a unique modulation of host RNAi during RV infection, highlighting the importance of antiviral RNAi in mammalian cells.

摘要

RNA 干扰 (RNAi) 是植物、线虫和节肢动物中一种古老的先天免疫反应,为其提供了天然的抗病毒感染保护。病毒也通过产生称为抗病毒 RNAi 抑制子 (VSRs) 的毒力决定因子获得了对抗防御措施。有趣的是,尽管干扰素为基础的免疫在高等脊椎动物的体细胞中占主导地位,但最近的报道越来越多地支持保留 RNAi 在哺乳动物细胞中的抗病毒性质。本研究集中于感染轮状病毒 (RV) 时细胞内 RNAi 的调节,RV 是一种具有双链 RNA 基因组的肠道病毒。有趣的是,在 RV 感染的细胞中观察到 RNAi 的时间依赖性双模态调节,其中 siRNA 为基础的 RNAi 在感染早期仅失去功能,而在早期感染阶段之后完全恢复。随后的研究表明,RV 非结构蛋白 1 作为一种推定的 VSR,通过与 Argonaute2 (AGO2) 结合并通过泛素-蛋白酶体途径触发其降解,从而发挥作用,AGO2 是 siRNA 介导的 RNAi 的主要效应因子。当通过异位过表达 AGO2 显著降低 RV 感染时,AGO2 降解的前病毒意义得到进一步证实。综上所述,本研究提出了 RV 感染过程中宿主 RNAi 的独特调节,突出了抗病毒 RNAi 在哺乳动物细胞中的重要性。

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