| Literature DB >> 33979623 |
Xiujia Yang1, Minhui Wang2, Jiaqi Wu3, Dianchun Shi4, Yanfang Zhang3, Huikun Zeng5, Yan Zhu3, Chunhong Lan1, Yang Deng6, Shixin Guo7, Lijun Xu8, Cuiyu Ma5, Yanxia Zhang3, Jinxia Ou9, Chu-Jun Liu10, Yuan Chen11, Qilong Wang11, Wenxi Xie2, Junjie Guan2, Jieyu Ding12, Zhi Wang13, Changqing Chang14, Wei Yang15, Huijie Zhang16, Jun Chen17, Lijie Qin8, Hongwei Zhou9, Jin-Xin Bei10, Lai Wei7, Guangwen Cao18, Xueqing Yu19, Zhenhai Zhang20.
Abstract
Antibody repertoire sequencing enables researchers to acquire millions of B cell receptors and investigate these molecules at the single-nucleotide level. This power and resolution in studying humoral responses have led to its wide applications. However, most of these studies were conducted with a limited number of samples. Given the extraordinary diversity, assessment of these key features with a large sample set is demanded. Thus, we collect and systematically analyze 2,152 high-quality heavy-chain antibody repertoires. Our study reveals that 52 core variable genes universally contribute to more than 99% of each individual's repertoire; a distal interspersed preferences characterize V gene recombination; the number of public clones between two repertoires follows a linear model, and the positive selection dominates at RGYW motif in somatic hypermutations. Thus, this population-level analysis resolves some critical features of the antibody repertoire and may have significant value to the large cadre of scientists.Entities:
Keywords: B cell biology; Ig-seq; antibody repertoire; high-throughput sequencing; large-scale analysis
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Year: 2021 PMID: 33979623 DOI: 10.1016/j.celrep.2021.109110
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423