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A Global Interactome Map of the Dengue Virus NS1 Identifies Virus Restriction and Dependency Host Factors

机译:登革热病毒NS1的全局互乱地图识别病毒限制和依赖宿主因子

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Summary Dengue virus (DENV) infections cause the most prevalent mosquito-borne viral disease worldwide, for which no therapies are available. DENV encodes seven non-structural (NS) proteins that co-assemble and recruit poorly characterized host factors to form the DENV replication complex essential for viral infection. Here, we provide a global proteomic analysis of the human host factors that interact with the?DENV NS1 protein. Combined with a functional RNAi screen, this study reveals a comprehensive network of host cellular processes involved in DENV infection and identifies DENV host restriction and dependency factors. We highlight an important role of RACK1 and the chaperonin TRiC (CCT) and oligosaccharyltransferase (OST) complexes during DENV replication. We further show that the OST complex mediates NS1 and NS4B glycosylation, and pharmacological inhibition of its N-glycosylation function strongly impairs DENV infection. In conclusion, our study provides a global interactome of the DENV NS1 and identifies host factors targetable for antiviral therapies.
机译:摘要登革热病毒(Denv)感染导致全球最普遍的蚊虫病毒疾病,没有任何疗法。 Denv编码七种非结构(NS)蛋白,其共组合和募集特征差的宿主因子,以形成丹佛复制复合物对病毒感染必不可少的复杂性。在这里,我们提供了与αDENV NS1蛋白相互作用的人宿主因子的全局蛋白质组学分析。结合功能性RNAi屏幕,本研究揭示了丹佛感染中涉及的宿主细胞过程综合网络,并确定Denv主机限制和依赖性因素。在DENV复制期间,我们突出了Rack1和伴侣素三(CCT)和寡核苷酸转移酶(OST)复合物的重要作用。我们进一步表明,OST复合物介导NS1和NS4B糖基化,其N-糖基化功能的药理抑制强烈损害DENV感染。总之,我们的研究提供了Denv NS1的全球互联蛋白酶,并识别有针对性抗病毒疗法的宿主因子。

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