Membrane fusion and immune evasion by the spike protein of SARS-CoV-2 Delta variant | Zendy

Jun Zhang | Zendy; Tianshu Xiao | Zendy; Yongfei Cai | Zendy; Christy L. Lavine | Zendy; Hanqin Peng | Zendy; Haisun Zhu | Zendy; Krishna Anand | Zendy; Pei Tong | Zendy; Avneesh Gautam | Zendy; Megan L. Mayer | Zendy; Richard M. Walsh | Zendy; Sophia RitsVolloch | Zendy; Duane R. Wesemann | Zendy; Wei Yang | Zendy; Michael S. Seaman | Zendy; Jianming Lü | Zendy; Bing Chen | Zendy

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Membrane fusion and immune evasion by the spike protein of SARS-CoV-2 Delta variant

Author(s) -

Jun Zhang,

Tianshu Xiao,

Yongfei Cai,

Christy L. Lavine,

Hanqin Peng,

Haisun Zhu,

Krishna Anand,

Pei Tong,

Avneesh Gautam,

Megan L. Mayer,

Richard M. Walsh,

Sophia RitsVolloch,

Duane R. Wesemann,

Wei Yang,

Michael S. Seaman,

Jianming Lü,

Bing Chen

Publication year - 2021

Publication title -

science

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 12.556

H-Index - 1186

eISSN - 1095-9203

pISSN - 0036-8075

DOI - 10.1126/science.abl9463

Subject(s) - biology , immune system , coronavirus , virology , antibody , spike (software development) , antigen , receptor , immunity , microbiology and biotechnology , computational biology , genetics , covid-19 , medicine , disease , management , pathology , infectious disease (medical specialty) , economics

Delta’s spike Understanding the molecular mechanisms of the increased transmissibility and immune evasion of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) variants is critical to guiding current and future intervention strategies. Zhanget al . determined cryo–electron microscopy structures of the full-length spike protein trimers of the Delta, Kappa, and Gamma variants of SARS-CoV-2 and studied their function and antigenic properties. The Delta spike protein fused membranes more efficiently at low levels of the cellular receptor ACE2, and its pseudotyped viruses infected target cells substantially more rapidly than all other variants tested, possibly at least partly accounting for its heightened transmissibility. Mutations of each variant rearranged the antigenic surface of the N-terminal domain of the spike protein but only caused local changes in the receptor-binding domain, consistent with greater resistance to neutralizing antibodies. These findings elucidate the molecular events that have led these viruses to adapt in human communities and to evade host immunity. —VV

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