生发中心
C-C趋化因子受体6型
20立方厘米
抗原
人口
抗体
细胞生物学
分子生物学
B细胞
生物
化学
趋化因子受体
趋化因子
免疫学
免疫系统
医学
环境卫生
作者
Dorothea Reimer,Adrian Y. S. Lee,Jennifer L. Bannan,Phillip D. Fromm,Ervin E. Kara,Iain Comerford,Shaun R. McColl,Florian Wiede,Dirk Mielenz,Heinrich Körner
摘要
The CC-chemokine receptor 6 (CCR6) can be detected on naive and activated B cells. Counterintuitively, its absence accelerates the appearance of germinal centres (GCs) and increases the production of low-affinity antibodies. The detailed mechanism of CCR6 function during the humoral response has remained elusive, but previously we identified a distinct CCR6high B-cell population in vivo early after antigenic challenge. In this study, we defined this population specifically as early, activated pre-GC B cells. In accordance, we show that CCR6 is upregulated rapidly within hours on the protein or mRNA level after activation in vitro. In addition, only activated B cells migrated specifically towards CCL20, the specific ligand for CCR6. Lack of CCR6 increased the dark zone/light zone ratio of GC and led to decreased antigen-specific IgG1 and IgG2a antibody generation in a B-cell intrinsic manner in mixed bone marrow chimeras. In contrast, antigen-specific IgM responses were normal. Hence, CCR6 negatively regulates entry of activated, antigen-specific pre-GC B cells into the GC reaction.
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