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SARS-CoV-2 breakthrough infections induce somatically hypermutated broadly neutralizing antibodies against heterologous variants (preprint)
Xiaoli Xiong; Haisheng Yu; Yaping Wang; Jingrong Shi; Chengqian Feng; Guofang Tang; Jiaojiao Li; Fengyu Hu; Liliangzi Guo; Feng Li; Xiaoping Tang; Banghui Liu; Qiuluan Chen; Zimu Li; Mengzhen Su; Qihong Yan; Xinwen Chen; Rongjuan Pei; Yudi ZHANG; Qian Wang; Peiyu HU; Pingqian Zheng; Ling Chen; Xijie Gao; Jun He; Haitao Xiang; Caixia Xie; Quan Shi; Longqi Liu; Xiaopan Liu; Xiumei Lin; Chuanyu Liu; Yalin Huang; Naibo Yang; Meiniang Wang; Xiaofang Peng; Dan Liang; Bixia Ke; Changwen Ke.
researchsquare; 2022.
Preprint in English | PREPRINT-RESEARCHSQUARE | ID: ppzbmed-10.21203.rs.3.rs-1739426.v1

ABSTRACT

Currently circulating SARS-CoV-2 Omicron variants feature highly mutated spike proteins with extraordinary abilities in evading acute-infection-induced germline antibodies isolated earlier in the pandemic. We identified that memory B cells from Delta variant breakthrough-infection patients expressed antibodies with more extensive somatic hypermutations (SHMs) allowing isolation of a number of broadly neutralizing antibodies with activities against heterologous variants of concerns (VOCs) including Omicron variant. Structural studies identified that SHM introduced altered amino acids and highly unusual HCDR2 insertions respectively in two representative broadly neutralizing antibodies - YB9-258 and YB13-292. Previously, insertion/deletion were rarely reported for antiviral antibodies except for those induced by HIV-1 chronic infections. Identified SHMs involved heavily in epitope recognition, they broadened neutralization breadth by rendering antibodies resistant to VOC mutations highly detrimental to previously isolated antibodies targeting similar epitopes. These data provide molecular mechanisms for enhanced immunity to heterologous SARS-CoV-2 variants after repeated antigen exposures with implications for future vaccination strategy.

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