Affinity-coupled CCL22 promotes positive selection in germinal centres

生发中心 CCL17型 CD40 趋化因子 亲和力成熟 幼稚B细胞 CCL22型 B细胞 CXCL13型 体细胞突变 细胞生物学 生物 趋化因子受体 抗体 化学 分子生物学 受体 免疫学 细胞毒性T细胞 体外 生物化学
作者
Bo Liu,Yihan Lin,Jiacong Yan,Jiacheng Yao,Dan Liu,Weiwei Ma,Jianbin Wang,Wanli Liu,Chengshuo Wang,Luo Zhang,Hai Qi
出处
期刊:Nature [Springer Nature]
卷期号:592 (7852): 133-137 被引量:47
标识
DOI:10.1038/s41586-021-03239-2
摘要

Antibody affinity maturation depends on positive selection in germinal centres (GCs) of rare B cell clones that acquire higher-affinity B cell receptors via somatic hypermutation, present more antigen to follicular helper T (TFH) cells and, consequently, receive more contact-dependent T cell help1. As these GC B cells and TFH cells do not maintain long-lasting contacts in the chaotic GC environment2–4, it is unclear how sufficient T cell help is cumulatively focused onto those rare clones. Here we show that, upon stimulation of CD40, GC B cells upregulate the chemokine CCL22 and to a lesser extent CCL17. By engaging the chemokine receptor CCR4 on TFH cells, CCL22 and CCL17 can attract multiple helper cells from a distance, thus increasing the chance of productive help. During a GC response, B cells that acquire higher antigen-binding affinities express higher levels of CCL22, which in turn ‘highlight’ these high-affinity GC B cells. Acute increase or blockade of TFH cells helps to rapidly increase or decrease CCL22 expression by GC B cells, respectively. Therefore, a chemokine-based intercellular reaction circuit links the amount of T cell help that individual B cells have received recently to their subsequent ability to attract more help. When CCL22 and CCL17 are ablated in B cells, GCs form but B cells are not affinity-matured efficiently. When competing with wild-type B cells in the same reaction, B cells lacking CCL22 and CCL17 receive less T cell help to maintain GC participation or develop into bone-marrow plasma cells. By uncovering a chemokine-mediated mechanism that highlights affinity-improved B cells for preferential help from TFH cells, our study reveals a principle of spatiotemporal orchestration of GC positive selection. CCL22 promotes positive selection in germinal centres by highlighting affinity-enhanced B cells for helper T cells to sense and seek remotely.
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