BCR selection and affinity maturation in Peyer’s patch germinal centres

体细胞突变 生发中心 派尔斑 断点群集区域 B细胞受体 亲和力成熟 生殖系 互补决定区 体细胞 免疫球蛋白重链 遗传学 免疫球蛋白轻链 生物 免疫学 基因 抗体 抗原 B细胞
作者
Huan Chen,Yuxiang Zhang,Adam Yongxin Ye,Zhou Du,Mo Xu,Cheng‐Sheng Lee,Joyce K. Hwang,Nia Kyritsis,Zhaoqing Ba,Donna Neuberg,Dan R. Littman,Frederick W. Alt
出处
期刊:Nature [Springer Nature]
卷期号:582 (7812): 421-425 被引量:99
标识
DOI:10.1038/s41586-020-2262-4
摘要

The antigen-binding variable regions of the B cell receptor (BCR) and of antibodies are encoded by exons that are assembled in developing B cells by V(D)J recombination1. The BCR repertoires of primary B cells are vast owing to mechanisms that create diversity at the junctions of V(D)J gene segments that contribute to complementarity-determining region 3 (CDR3), the region that binds antigen1. Primary B cells undergo antigen-driven BCR affinity maturation through somatic hypermutation and cellular selection in germinal centres (GCs)2,3. Although most GCs are transient3, those in intestinal Peyer's patches (PPs)—which depend on the gut microbiota—are chronic4, and little is known about their BCR repertoires or patterns of somatic hypermutation. Here, using a high-throughput assay that analyses both V(D)J segment usage and somatic hypermutation profiles, we elucidate physiological BCR repertoires in mouse PP GCs. PP GCs from different mice expand public BCR clonotypes (clonotypes that are shared between many mice) that often have canonical CDR3s in the immunoglobulin heavy chain that, owing to junctional biases during V(D)J recombination, appear much more frequently than predicted in naive B cell repertoires. Some public clonotypes are dependent on the gut microbiota and encode antibodies that are reactive to bacterial glycans, whereas others are independent of gut bacteria. Transfer of faeces from specific-pathogen-free mice to germ-free mice restored germ-dependent clonotypes, directly implicating BCR selection. We identified somatic hypermutations that were recurrently selected in such public clonotypes, indicating that affinity maturation occurs in mouse PP GCs under homeostatic conditions. Thus, persistent gut antigens select recurrent BCR clonotypes to seed chronic PP GC responses. An analysis of the immunoglobulin repertoire of B cells in Peyer's patch germinal centres in mice provides evidence for the selection of B cell receptor clonotypes by gut antigens and antigen-driven affinity maturation.
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