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甲型流感病毒 M2 蛋白将 M1 募集到质膜:荧光波动显微镜研究。

Influenza A M2 recruits M1 to the plasma membrane: A fluorescence fluctuation microscopy study.

机构信息

University of Potsdam, Institute of Biochemistry and Biology, Potsdam, Germany.

University of Rome Tor Vergata, Department of Chemical Science and Technologies, Roma, Italy.

出版信息

Biophys J. 2021 Dec 21;120(24):5478-5490. doi: 10.1016/j.bpj.2021.11.023. Epub 2021 Nov 19.

Abstract

Influenza A virus (IAV) is a respiratory pathogen that causes seasonal epidemics with significant mortality. One of the most abundant proteins in IAV particles is the matrix protein 1 (M1), which is essential for the virus structural stability. M1 organizes virion assembly and budding at the plasma membrane (PM), where it interacts with other viral components. The recruitment of M1 to the PM as well as its interaction with the other viral envelope proteins (hemagglutinin [HA], neuraminidase, matrix protein 2 [M2]) is controversially discussed in previous studies. Therefore, we used fluorescence fluctuation microscopy techniques (i.e., scanning fluorescence cross-correlation spectroscopy and number and brightness) to quantify the oligomeric state of M1 and its interactions with other viral proteins in co-transfected as well as infected cells. Our results indicate that M1 is recruited to the PM by M2, as a consequence of the strong interaction between the two proteins. In contrast, only a weak interaction between M1 and HA was observed. M1-HA interaction occurred only in the event that M1 was already bound to the PM. We therefore conclude that M2 initiates the assembly of IAV by recruiting M1 to the PM, possibly allowing its further interaction with other viral proteins.

摘要

甲型流感病毒(IAV)是一种呼吸道病原体,可导致具有显著死亡率的季节性流行。IAV 粒子中最丰富的蛋白之一是基质蛋白 1(M1),它对病毒结构稳定性至关重要。M1 组织病毒粒子在质膜(PM)处的组装和出芽,在该处它与其他病毒成分相互作用。M1 向 PM 的募集及其与其他病毒包膜蛋白(血凝素 [HA]、神经氨酸酶、基质蛋白 2 [M2])的相互作用在以前的研究中存在争议。因此,我们使用荧光波动显微镜技术(即扫描荧光互相关光谱和数量和亮度)来定量共转染和感染细胞中 M1 的寡聚状态及其与其他病毒蛋白的相互作用。我们的结果表明,M1 被 M2 募集到 PM,这是两种蛋白之间强烈相互作用的结果。相比之下,仅观察到 M1 和 HA 之间的弱相互作用。仅在 M1 已经与 PM 结合的情况下才观察到 M1-HA 相互作用。因此,我们得出结论,M2 通过将 M1 募集到 PM 来启动 IAV 的组装,可能允许其与其他病毒蛋白进一步相互作用。

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