| Literature DB >> 35773398 |
Xiaoyu Sun1, Chunyan Yi1, Yuanfei Zhu2, Longfei Ding3, Shuai Xia2, Xingchen Chen1, Mu Liu2, Chenjian Gu2, Xiao Lu1, Yadong Fu1, Shuangfeng Chen1,4, Tianlong Zhang5, Yaguang Zhang1, Zhuo Yang1, Liyan Ma1, Wangpeng Gu1, Gaowei Hu2, Shujuan Du2, Renhong Yan6, Weihui Fu3, Songhua Yuan3, Chenli Qiu3, Chen Zhao3, Xiaoyan Zhang3, Yonghui He1, Aidong Qu7, Xu Zhou7, Xiuling Li7, Gary Wong8, Qiang Deng2, Qiang Zhou6, Hongzhou Lu3, Zhiyang Ling9, Jianping Ding10, Lu Lu11,12, Jianqing Xu13, Youhua Xie14,15, Bing Sun16,17.
Abstract
Frequent outbreaks of coronaviruses underscore the need for antivirals and vaccines that can counter a broad range of coronavirus types. We isolated a human antibody named 76E1 from a COVID-19 convalescent patient, and report that it has broad-range neutralizing activity against multiple α- and β-coronaviruses, including the SARS-CoV-2 variants. 76E1 also binds its epitope in peptides from γ- and δ-coronaviruses. 76E1 cross-protects against SARS-CoV-2 and HCoV-OC43 infection in both prophylactic and therapeutic murine animal models. Structural and functional studies revealed that 76E1 targets a unique epitope within the spike protein that comprises the highly conserved S2' site and the fusion peptide. The epitope that 76E1 binds is partially buried in the structure of the SARS-CoV-2 spike trimer in the prefusion state, but is exposed when the spike protein binds to ACE2. This observation suggests that 76E1 binds to the epitope at an intermediate state of the spike trimer during the transition from the prefusion to the postfusion state, thereby blocking membrane fusion and viral entry. We hope that the identification of this crucial epitope, which can be recognized by 76E1, will guide epitope-based design of next-generation pan-coronavirus vaccines and antivirals.Entities:
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Year: 2022 PMID: 35773398 DOI: 10.1038/s41564-022-01155-3
Source DB: PubMed Journal: Nat Microbiol ISSN: 2058-5276 Impact factor: 30.964