Rational development of a human antibody cocktail that deploys multiple functions to confer Pan-SARS-CoVs protection

Author:

Yao HangpingORCID,Sun Yao,Deng Yong-Qiang,Wang Nan,Tan Yongcong,Zhang Na-Na,Li Xiao-Feng,Kong Chao,Xu Yan-PengORCID,Chen Qi,Cao Tian-Shu,Zhao Hui,Yan Xintian,Cao Lei,Lv Zhe,Zhu Dandan,Feng Rui,Wu Nanping,Zhang Wenhai,Hu Yuhao,Chen Keda,Zhang Rong-Rong,Lv Qingyu,Sun Shihui,Zhou Yunhua,Yan Run,Yang Guan,Sun Xinglu,Liu Chanjuan,Lu Xiangyun,Cheng Linfang,Qiu Hongying,Huang Xing-Yao,Weng Tianhao,Shi Danrong,Jiang Weidong,Shao Junbin,Wang Lei,Zhang Jie,Jiang Tao,Lang Guojun,Qin Cheng-FengORCID,Li Lanjuan,Wang XiangxiORCID

Abstract

AbstractStructural principles underlying the composition and synergistic mechanisms of protective monoclonal antibody cocktails are poorly defined. Here, we exploited antibody cooperativity to develop a therapeutic antibody cocktail against SARS-CoV-2. On the basis of our previously identified humanized cross-neutralizing antibody H014, we systematically analyzed a fully human naive antibody library and rationally identified a potent neutralizing antibody partner, P17, which confers effective protection in animal model. Cryo-EM studies dissected the nature of the P17 epitope, which is SARS-CoV-2 specific and distinctly different from that of H014. High-resolution structure of the SARS-CoV-2 spike in complex with H014 and P17, together with functional investigations revealed that in a two-antibody cocktail, synergistic neutralization was achieved by S1 shielding and conformational locking, thereby blocking receptor attachment and viral membrane fusion, conferring high potency as well as robustness against viral mutation escape. Furthermore, cluster analysis identified a hypothetical 3rd antibody partner for further reinforcing the cocktail as pan-SARS-CoVs therapeutics.

Publisher

Springer Science and Business Media LLC

Subject

Cell Biology,Molecular Biology

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