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正粘病毒基质蛋白的晶体结构揭示了其自我聚合和膜结合的机制。

Crystal structure of an orthomyxovirus matrix protein reveals mechanisms for self-polymerization and membrane association.

机构信息

Department of BioSciences, Rice University, Houston, TX 77251.

State Key Laboratory of Agricultural Microbiology, College of Veterinary Medicine, Huazhong Agricultural University, Wuhan 430070, People's Republic of China.

出版信息

Proc Natl Acad Sci U S A. 2017 Aug 8;114(32):8550-8555. doi: 10.1073/pnas.1701747114. Epub 2017 Jul 24.

Abstract

Many enveloped viruses encode a matrix protein. In the influenza A virus, the matrix protein M1 polymerizes into a rigid protein layer underneath the viral envelope to help enforce the shape and structural integrity of intact viruses. The influenza virus M1 is also known to mediate virus budding as well as the nuclear export of the viral nucleocapsids and their subsequent packaging into nascent viral particles. Despite extensive studies on the influenza A virus M1 (FLUA-M1), only crystal structures of its N-terminal domain are available. Here we report the crystal structure of the full-length M1 from another orthomyxovirus that infects fish, the infectious salmon anemia virus (ISAV). The structure of ISAV-M1 assumes the shape of an elbow, with its N domain closely resembling that of the FLUA-M1. The C domain, which is connected to the N domain through a flexible linker, is made of four α-helices packed as a tight bundle. In the crystal, ISAV-M1 monomers form infinite 2D arrays with a network of interactions involving both the N and C domains. Results from liposome flotation assays indicated that ISAV-M1 binds membrane via electrostatic interactions that are primarily mediated by a positively charged surface loop from the N domain. Cryoelectron tomography reconstruction of intact ISA virions identified a matrix protein layer adjacent to the inner leaflet of the viral membrane. The physical dimensions of the virion-associated matrix layer are consistent with the 2D ISAV-M1 crystal lattice, suggesting that the crystal lattice is a valid model for studying M1-M1, M1-membrane, and M1-RNP interactions in the virion.

摘要

许多包膜病毒都编码一种基质蛋白。在甲型流感病毒中,基质蛋白 M1 聚合形成病毒包膜下的刚性蛋白层,以帮助维持完整病毒的形状和结构完整性。流感病毒 M1 也被认为介导病毒出芽以及病毒核衣壳的核输出及其随后包装到新生病毒颗粒中。尽管对甲型流感病毒 M1(FLUA-M1)进行了广泛的研究,但仅获得了其 N 端结构域的晶体结构。在这里,我们报告了另一种感染鱼类的正粘病毒——传染性鲑鱼贫血病毒(ISAV)全长 M1 的晶体结构。ISAV-M1 的结构呈肘状,其 N 结构域与 FLUA-M1 非常相似。通过柔性接头与 N 结构域相连的 C 结构域由四个α-螺旋组成一个紧密的束。在晶体中,ISAV-M1 单体形成无限的 2D 阵列,其网络相互作用涉及 N 和 C 结构域。脂质体浮选分析的结果表明,ISAV-M1 通过主要由 N 结构域的正电荷表面环介导的静电相互作用结合膜。完整 ISA 病毒粒子的冷冻电镜断层重建鉴定了位于病毒膜内叶附近的基质蛋白层。病毒相关基质层的物理尺寸与 2D ISAV-M1 晶格一致,表明晶格是研究病毒粒子中 M1-M1、M1-膜和 M1-RNP 相互作用的有效模型。

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