流感 A 病毒核蛋白的 SUMO 化对于细胞内运输和病毒生长是必需的。
Sumoylation of influenza A virus nucleoprotein is essential for intracellular trafficking and virus growth.
机构信息
Molecular Virology Unit, Key Laboratory of Molecular Virology & Immunology, Institut Pasteur of Shanghai, Shanghai Institutes for Biological Sciences, Chinese Academy of Sciences, Shanghai, China.
Department of Biochemistry, University of Zürich, Zürich, Switzerland.
出版信息
J Virol. 2014 Aug;88(16):9379-90. doi: 10.1128/JVI.00509-14. Epub 2014 Jun 11.
UNLABELLED
Viruses take advantage of host posttranslational modifications for their own benefit. It was recently reported that influenza A virus proteins interact extensively with the host sumoylation system. Thereby, several viral proteins, including NS1 and M1, are sumoylated to facilitate viral replication. However, to what extent sumoylation is exploited by influenza A virus is not fully understood. In this study, we found that influenza A virus nucleoprotein (NP) is a bona fide target of sumoylation in both NP-transfected cells and virus-infected cells. We further found that NP is sumoylated at the two most N-terminal residues, lysines 4 and 7, and that sumoylation at lysine 7 of NP is highly conserved across different influenza A virus subtypes and strains, including the recently emerged human H7N9 virus. While NP stability and polymerase activity are little affected by sumoylation, the NP sumoylation-defective WSN-NPK4,7R virus exhibited early cytoplasmic localization of NP. The growth of the WSN-NPK4,7R virus was highly attenuated compared to that of the wild-type WSN virus, and the lysine residue at position 7 is indispensable for the virus's survival, as illustrated by the rapid emergence of revertant viruses. Thus, sumoylation of influenza A virus NP is essential for intracellular trafficking of NP and for virus growth, illustrating sumoylation as a crucial strategy extensively exploited by influenza A virus for survival in its host.
IMPORTANCE
Host posttranslational modifications are heavily targeted by viruses for their own benefit. We and others previously reported that influenza A virus interacts extensively with the host sumoylation system. However, the functional outcomes of viral sumoylation are not fully understood. Here we found that influenza A virus nucleoprotein (NP), an essential component for virus replication, is a new target of SUMO. This is the first study to find that NP from different influenza A viruses, including recently emerged H7N9, is sumoylated at conserved lysine 7. Our data further illustrated that sumoylation of influenza A virus NP is essential for intracellular trafficking of NP and virus growth, indicating that influenza A virus relies deeply on sumoylation to survive in host cells. Strategies to downregulate viral sumoylation could thus be a potential antiviral treatment.
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病毒利用宿主翻译后修饰来为自己谋利。最近有报道称,甲型流感病毒蛋白与宿主 SUMO 系统广泛相互作用。由此,包括 NS1 和 M1 在内的几种病毒蛋白被 SUMO 化,以促进病毒复制。然而,甲型流感病毒在多大程度上利用 SUMO 化尚不完全清楚。在这项研究中,我们发现甲型流感病毒核蛋白(NP)在 NP 转染细胞和病毒感染细胞中都是 SUMO 化的真正靶标。我们进一步发现,NP 在两个最 N 端残基赖氨酸 4 和 7 处被 SUMO 化,并且 NP 的赖氨酸 7 的 SUMO 化在不同的甲型流感病毒亚型和株系中高度保守,包括最近出现的人 H7N9 病毒。虽然 NP 的稳定性和聚合酶活性受 SUMO 化的影响很小,但 NP SUMO 化缺陷的 WSN-NPK4,7R 病毒表现出 NP 的早期细胞质定位。与野生型 WSN 病毒相比,WSN-NPK4,7R 病毒的生长受到高度抑制,并且位置 7 的赖氨酸残基对于病毒的存活是必不可少的,正如回复病毒的快速出现所说明的那样。因此,甲型流感病毒 NP 的 SUMO 化对于 NP 的细胞内运输和病毒生长至关重要,这表明 SUMO 化是甲型流感病毒在宿主中生存所广泛利用的关键策略。
重要性
宿主翻译后修饰被病毒大量靶向以谋取自身利益。我们和其他人之前曾报道过甲型流感病毒与宿主 SUMO 系统广泛相互作用。然而,病毒 SUMO 化的功能结果尚不完全清楚。在这里,我们发现甲型流感病毒核蛋白(NP),一种病毒复制所必需的重要成分,是 SUMO 的一个新靶标。这是第一项发现不同甲型流感病毒(包括最近出现的 H7N9)的 NP 在保守赖氨酸 7 处被 SUMO 化的研究。我们的数据进一步表明,甲型流感病毒 NP 的 SUMO 化对于 NP 的细胞内运输和病毒生长至关重要,这表明甲型流感病毒严重依赖 SUMO 化在宿主细胞中生存。因此,下调病毒 SUMO 化的策略可能是一种潜在的抗病毒治疗方法。
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