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由不同N-糖基化位点的聚糖介导的完全糖基化流感病毒血凝素之间的多价相互作用。

Multivalent interactions between fully glycosylated influenza virus hemagglutinins mediated by glycans at distinct N-glycosylation sites.

作者信息

Li Ruofan, Gao Jingjing, Wang Lin, Gui Miao, Xiang Ye

机构信息

Beijing Frontier Research Center for Biological Structure, Center for Infectious Disease Research, School of Basic Medical Sciences, Tsinghua University, 100084, Beijing, China.

SXMU-Tsinghua Collaborative Innovation Center for Frontier Medicine, Shanxi Medical University, 030001, Taiyuan, Shanxi Province, China.

出版信息

Npj Viruses. 2024 Oct 17;2(1):48. doi: 10.1038/s44298-024-00059-9.

Abstract

The hemagglutinin (HA) glycoprotein of influenza virus binds host cell receptors and mediates viral entry. Here we present cryo-EM structures of fully glycosylated HAs from H5N1 and H5N8 influenza viruses. We find that the H5N1 HA can form filaments that comprise two head-to-head HA trimers. Multivalent interactions between the two HA trimers are mediated by glycans attached to N158. The distal Sia1-Gal2-NAG3 sugar moiety of N158 interacts with the receptor binding site on the opposing HA trimer. Additional interactions are observed between NAG3 and residues K222 and K193. The H5N8 HA lacks the N158 glycosylation site and does not form the filamentous structure. However, the H5N8 HA exhibits an auto-inhibition conformation, where the receptor binding site is occupied by the glycan chain attached to residue N169 from a neighboring protomer. These structures represent native HA-glycan interactions, which may closely mimic the receptor-HA interactions on the cell surface.

摘要

流感病毒的血凝素(HA)糖蛋白可结合宿主细胞受体并介导病毒进入。在此,我们展示了来自H5N1和H5N8流感病毒的完全糖基化HA的冷冻电镜结构。我们发现,H5N1 HA可形成由两个头对头HA三聚体组成的丝状结构。两个HA三聚体之间的多价相互作用由连接在N158上的聚糖介导。N158的远端唾液酸1-半乳糖2-N-乙酰葡糖胺3糖部分与相对HA三聚体上的受体结合位点相互作用。在N-乙酰葡糖胺3与残基K222和K193之间还观察到其他相互作用。H5N8 HA缺乏N158糖基化位点,不形成丝状结构。然而,H5N8 HA呈现出一种自抑制构象,其中受体结合位点被来自相邻原体的连接在残基N169上的糖链占据。这些结构代表了天然的HA-聚糖相互作用,可能紧密模拟了细胞表面的受体-HA相互作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/87a7/11721446/dc563743b82e/44298_2024_59_Fig1_HTML.jpg

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