Effect of exportin 1/XPO1 nuclear export pathway inhibition on coronavirus replication.

Masmudur M Rahman, Bereket Estifanos, Honor L Glenn, Ami D Gutierrez-Jensen, Karen Kibler, Yize Li, Bertram Jacobs, Grant McFadden, Brenda G Hogue
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Abstract

Nucleocytoplasmic transport of proteins using XPO1 (exportin 1) plays a vital role in cell proliferation and survival. Many viruses also exploit this pathway to promote infection and replication. Thus, inhibiting the XPO1-mediated nuclear export pathway with selective inhibitors has a diverse effect on virus replication by regulating antiviral, proviral, and anti-inflammatory pathways. The XPO1 inhibitor, Selinexor, is an FDA-approved anticancer drug predicted to have antiviral or proviral functions against viruses. Here, we observed that pretreatment of cultured cell lines from human or mouse origin with nuclear export inhibitor Selinexor significantly enhanced protein expression and replication of Mouse Hepatitis Virus (MHV), a mouse coronavirus. Knockdown of cellular XPO1 protein expression also significantly enhanced the replication of MHV in human cells. However, for SARS-CoV-2, selinexor treatment had diverse effects on virus replication in different cell lines. These results indicate that XPO1-mediated nuclear export pathway inhibition might affect coronavirus replication depending on cell types and virus origin.

输出蛋白1/XPO1核输出通路抑制对冠状病毒复制的影响
利用输出蛋白1 (XPO1)的核质转运在细胞增殖和存活中起着至关重要的作用。许多病毒也利用这一途径促进感染和复制。因此,用选择性抑制剂抑制xpo1介导的核输出途径通过调节抗病毒、前病毒和抗炎途径对病毒复制产生多种影响。XPO1抑制剂Selinexor是fda批准的抗癌药物,预计对病毒具有抗病毒或抗病毒功能。本研究发现,用核输出抑制剂Selinexor对培养的人或小鼠细胞系进行预处理,可显著提高小鼠肝炎病毒(MHV)(一种小鼠冠状病毒)的蛋白表达和复制。敲低细胞XPO1蛋白表达也显著增强人细胞中MHV的复制。然而,对于SARS-CoV-2, selinexor处理对不同细胞系的病毒复制有不同的影响。这些结果表明,xpo1介导的核输出通路抑制可能影响冠状病毒的复制,这取决于细胞类型和病毒来源。
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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