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Shared IGHV1-69-encoded neutralizing antibodies contribute to the emergence of L452R substitution in SARS-CoV-2 variants

Emerg Microbes Infect. 2022-12; 
Qihong Yan, Ruitian Hou, Xiaohan Huang, Yanjun Zhang, Ping He, Yudi Zhang, Banghui Liu, Qian Wang, Haiyue Rao, Xianying Chen, Xinwei Zhao, Xuefeng Niu, Jincun Zhao, Xiaoli Xiong, Ling Chen
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Proteins, Expression, Isolation and Analysis The antibody heavy- and light-V genes (VH/VL) were synthesized (Genscript, China) and were cloned into human IgG1 expression vectors using Clone Express II One Step Cloning Kit (Vazyme, China). Supernatants were filtered through 0.22-μm filters (Merck Millipore, Germany) before incubated with Protein A Resin (Genscript, China) at room temperature for 2 h for antibody affinity purification. Get A Quote
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摘要

SARS-CoV-2 variants continue to emerge facing established herd immunity. L452R, previously featured in the Delta variant, quickly emerged in Omicron subvariants, including BA.4/BA.5, implying a continued selection pressure on this residue. The underlying links between spike mutations and their selective pressures remain incompletely understood. Here, by analyzing 221 structurally characterized antibodies, we found that IGHV1-69-encoded antibodies preferentially contact L452 using germline-encoded hydrophobic residues at the tip of HCDR2 loop. Whereas somatic hypermutations or VDJ rearrangements are required to acquire L452-contacting hydrophobic residues for non-IGHV1-69 encoded antibodies. Antibody repertoire ... More

關鍵詞

IGHV1-69, Immune evasion, L452R, SARS-CoV-2, Shared antibody response
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