An ancestral SARS-CoV-2 vaccine induces anti-Omicron variants antibodies by hypermutation

Author:

Park SeoryeongORCID,Choi Jaewon,Lee Yonghee,Noh Jinsung,Kim Namphil,Lee JinAhORCID,Cho GeummiORCID,Kim Sujeong,Yoo Duck KyunORCID,Kang Chang Kyung,Choe Pyoeng Gyun,Kim Nam Joong,Park Wan BeomORCID,Kim SeungtaekORCID,Oh Myoung-donORCID,Kwon SunghoonORCID,Chung JunhoORCID

Abstract

AbstractThe immune escape of Omicron variants significantly subsides by the third dose of an mRNA vaccine. However, it is unclear how Omicron variant-neutralizing antibodies develop under repeated vaccination. We analyze blood samples from 41 BNT162b2 vaccinees following the course of three injections and analyze their B-cell receptor (BCR) repertoires at six time points in total. The concomitant reactivity to both ancestral and Omicron receptor-binding domain (RBD) is achieved by a limited number of BCR clonotypes depending on the accumulation of somatic hypermutation (SHM) after the third dose. Our findings suggest that SHM accumulation in the BCR space to broaden its specificity for unseen antigens is a counterprotective mechanism against virus variant immune escape.

Publisher

Springer Science and Business Media LLC

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