Zika virus remodels and hijacks IGF2BP2 ribonucleoprotein complex to promote viral replication organelle biogenesis.

IF 6.4 1区 生物学 Q1 BIOLOGY
eLife Pub Date : 2024-11-20 DOI:10.7554/eLife.94347
Clément Mazeaud, Stefan Pfister, Jonathan E Owen, Higor Sette Pereira, Flavie Charbonneau, Zachary E Robinson, Anaïs Anton, Cheyanne L Bemis, Aïssatou Aïcha Sow, Trushar R Patel, Christopher J Neufeldt, Pietro Scaturro, Laurent Chatel-Chaix
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引用次数: 0

Abstract

Zika virus (ZIKV) infection causes significant human disease that, with no approved treatment or vaccine, constitutes a major public health concern. Its life cycle entirely relies on the cytoplasmic fate of the viral RNA genome (vRNA) through a fine-tuned equilibrium between vRNA translation, replication, and packaging into new virions, all within virus-induced replication organelles (vROs). In this study, with an RNA interference (RNAi) mini-screening and subsequent functional characterization, we have identified insulin-like growth factor 2 mRNA-binding protein 2 (IGF2BP2) as a new host dependency factor that regulates vRNA synthesis. In infected cells, IGF2BP2 associates with viral NS5 polymerase and redistributes to the perinuclear viral replication compartment. Combined fluorescence in situ hybridization-based confocal imaging, in vitro binding assays, and immunoprecipitation coupled to RT-qPCR showed that IGF2BP2 directly interacts with ZIKV vRNA 3' nontranslated region. Using ZIKV sub-genomic replicons and a replication-independent vRO induction system, we demonstrated that IGF2BP2 knockdown impairs de novo vRO biogenesis and, consistently, vRNA synthesis. Finally, the analysis of immunopurified IGF2BP2 complex using quantitative mass spectrometry and RT-qPCR revealed that ZIKV infection alters the protein and RNA interactomes of IGF2BP2. Altogether, our data support that ZIKV hijacks and remodels the IGF2BP2 ribonucleoprotein complex to regulate vRO biogenesis and vRNA neosynthesis.

寨卡病毒重塑并劫持 IGF2BP2 核糖核蛋白复合物,促进病毒复制细胞器的生物生成。
寨卡病毒(ZIKV)感染会导致严重的人类疾病,由于没有获得批准的治疗方法或疫苗,它已成为一个重大的公共卫生问题。寨卡病毒的生命周期完全依赖于病毒 RNA 基因组(vRNA)在细胞质中的命运,通过 vRNA 翻译、复制和包装成新病毒之间的微调平衡,所有这些都在病毒诱导的复制细胞器(vROs)中进行。在这项研究中,通过 RNA 干扰(RNAi)微型筛选和随后的功能鉴定,我们发现胰岛素样生长因子 2 mRNA 结合蛋白 2(IGF2BP2)是一种调节 vRNA 合成的新宿主依赖因子。在感染细胞中,IGF2BP2 与病毒 NS5 聚合酶结合,并重新分布到核周病毒复制区。基于荧光原位杂交的共聚焦成像、体外结合试验和免疫沉淀与 RT-qPCR 的结合显示,IGF2BP2 直接与 ZIKV vRNA 3' 非翻译区相互作用。利用 ZIKV 亚基因组复制子和复制无关的 vRO 诱导系统,我们证明了 IGF2BP2 基因敲除会损害 vRO 的从头生物生成,并持续影响 vRNA 的合成。最后,使用定量质谱法和 RT-qPCR 分析免疫纯化的 IGF2BP2 复合物发现,ZIKV 感染改变了 IGF2BP2 的蛋白质和 RNA 相互作用组。总之,我们的数据支持 ZIKV 劫持并重塑 IGF2BP2 核糖核蛋白复合物,以调控 vRO 的生物发生和 vRNA 的新合成。
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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来源期刊
eLife
eLife BIOLOGY-
CiteScore
12.90
自引率
3.90%
发文量
3122
审稿时长
17 weeks
期刊介绍: eLife is a distinguished, not-for-profit, peer-reviewed open access scientific journal that specializes in the fields of biomedical and life sciences. eLife is known for its selective publication process, which includes a variety of article types such as: Research Articles: Detailed reports of original research findings. Short Reports: Concise presentations of significant findings that do not warrant a full-length research article. Tools and Resources: Descriptions of new tools, technologies, or resources that facilitate scientific research. Research Advances: Brief reports on significant scientific advancements that have immediate implications for the field. Scientific Correspondence: Short communications that comment on or provide additional information related to published articles. Review Articles: Comprehensive overviews of a specific topic or field within the life sciences.
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