Structures and distributions of SARS-CoV-2 spike proteins on intact virions

被引:0
|
作者
Zunlong Ke
Joaquin Oton
Kun Qu
Mirko Cortese
Vojtech Zila
Lesley McKeane
Takanori Nakane
Jasenko Zivanov
Christopher J. Neufeldt
Berati Cerikan
John M. Lu
Julia Peukes
Xiaoli Xiong
Hans-Georg Kräusslich
Sjors H. W. Scheres
Ralf Bartenschlager
John A. G. Briggs
机构
[1] Medical Research Council Laboratory of Molecular Biology,Structural Studies Division
[2] Molecular Virology,Department of Infectious Diseases
[3] Heidelberg University,Department of Infectious Diseases
[4] Virology,Visual Aids Department
[5] Heidelberg University,German Center for Infection Research
[6] Medical Research Council Laboratory of Molecular Biology,Division of Virus
[7] Heidelberg Partner Site,Associated Carcinogenesis
[8] German Cancer Research Center (DKFZ),undefined
来源
Nature | 2020年 / 588卷
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摘要
Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) virions are surrounded by a lipid bilayer from which spike (S) protein trimers protrude1. Heavily glycosylated S trimers bind to the angiotensin-converting enzyme 2 receptor and mediate entry of virions into target cells2–6. S exhibits extensive conformational flexibility: it modulates exposure of its receptor-binding site and subsequently undergoes complete structural rearrangement to drive fusion of viral and cellular membranes2,7,8. The structures and conformations of soluble, overexpressed, purified S proteins have been studied in detail using cryo-electron microscopy2,7,9–12, but the structure and distribution of S on the virion surface remain unknown. Here we applied cryo-electron microscopy and tomography to image intact SARS-CoV-2 virions and determine the high-resolution structure, conformational flexibility and distribution of S trimers in situ on the virion surface. These results reveal the conformations of S on the virion, and provide a basis from which to understand interactions between S and neutralizing antibodies during infection or vaccination.
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页码:498 / 502
页数:4
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