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Structural basis for broad coronavirus neutralization

  • Maximilian M. Sauer
  • , M. Alejandra Tortorici
  • , Young Jun Park
  • , Alexandra C. Walls
  • , Leah Homad
  • , Oliver J. Acton
  • , John E. Bowen
  • , Chunyan Wang
  • , Xiaoli Xiong
  • , Willem de van der Schueren
  • , Joel Quispe
  • , Benjamin G. Hoffstrom
  • , Berend Jan Bosch
  • , Andrew T. McGuire
  • , David Veesler
  • University of Washington
  • Institut Pasteur, Paris
  • Fred Hutchinson Cancer Research Center
  • Utrecht University
  • CAS - Guangzhou Institute of Biomedicine and Health
  • Bluebird Bio, Inc.

科研成果: 期刊稿件文章同行评审

146 引用 (Scopus)

摘要

Three highly pathogenic β-coronaviruses have crossed the animal-to-human species barrier in the past two decades: SARS-CoV, MERS-CoV and SARS-CoV-2. To evaluate the possibility of identifying antibodies with broad neutralizing activity, we isolated a monoclonal antibody, termed B6, that cross-reacts with eight β-coronavirus spike glycoproteins, including all five human-infecting β-coronaviruses. B6 broadly neutralizes entry of pseudotyped viruses from lineages A and C, but not from lineage B, and the latter includes SARS-CoV and SARS-CoV-2. Cryo-EM, X-ray crystallography and membrane fusion assays reveal that B6 binds to a conserved cryptic epitope located in the fusion machinery. The data indicate that antibody binding sterically interferes with the spike conformational changes leading to membrane fusion. Our data provide a structural framework explaining B6 cross-reactivity with β-coronaviruses from three lineages, along with a proof of concept for antibody-mediated broad coronavirus neutralization elicited through vaccination. This study unveils an unexpected target for next-generation structure-guided design of a pan-β-coronavirus vaccine.

源语言英语
页(从-至)478-486
页数9
期刊Nature Structural and Molecular Biology
28
6
DOI
出版状态已出版 - 6月 2021
已对外发布

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    可持续发展目标 3 良好健康与福祉

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