| Literature DB >> 33944697 |
Qihong Yan1,2, Ping He1,2, Xiaohan Huang1,2, Kun Luo1,2, Yudi Zhang1,2, Haisu Yi3, Qian Wang1, Feng Li4, Ruitian Hou1,2, Xiaodi Fan5, Pingchao Li1, Xinglong Liu1, Huan Liang4, Yijun Deng4, Zhaoming Chen1, Yunfei Chen1, Xiaoneng Mo4, Xiaoli Xiong1, Liqiang Feng1, Song Li6,7, Jian Han6, Linbing Qu1, Xuefeng Niu3, Ling Chen1,3,4.
Abstract
Monoclonal antibodies (mAbs) encoded by IGHV3-53 (VH3-53) targeting the spike receptor-binding domain (RBD) have been isolated from different COVID-19 patients. However, the existence and prevalence of shared VH3-53-encoded antibodies in the antibody repertoires is not clear. Using antibody repertoire sequencing, we found that the usage of VH3-53 increased after SARS-CoV-2 infection. A highly shared VH3-53-J6 clonotype was identified in 9 out of 13 COVID-19 patients. This clonotype was derived from convergent gene rearrangements with few somatic hypermutations and was evolutionary conserved. We synthesized 34 repertoire-deduced novel VH3-53-J6 heavy chains and paired with a common IGKV1-9 light chain to produce recombinant mAbs. Most of these recombinant mAbs (23/34) possess RBD binding and virus neutralizing activities, and recognize ACE2 binding site via the same molecular interface. Our computational analysis, validated by laboratory experiments, revealed that VH3-53 antibodies targeting RBD are commonly present in COVID-19 patients' antibody repertoires, indicating many people have germline-like precursor sequences to rapidly generate SARS-CoV-2 neutralizing antibodies. Moreover, antigen-specific mAbs can be digitally obtained through antibody repertoire sequencing and computational analysis.Entities:
Year: 2021 PMID: 33944697 DOI: 10.1080/22221751.2021.1925594
Source DB: PubMed Journal: Emerg Microbes Infect ISSN: 2222-1751 Impact factor: 7.163