Germinal centers (GCs) support high-affinity, long-lived humoral immunity. How memory B cells develop in GCs is not clear. Through the use of a cell-cycle-reporting system, we identified GC-derived memory precursor cells (GC-MP cells) that had quit cycling and reached G0 phase while in the GC, exhibited memory-associated phenotypes with signs of affinity maturation and localized toward the GC border. After being transferred into adoptive hosts, GC-MP cells reconstituted a secondary response like genuine memory B cells. GC-MP cells expressed the interleukin 9 (IL-9) receptor and responded to IL-9. Acute treatment with IL-9 or antibody to IL-9 accelerated or retarded the positioning of GC-MP cells toward the GC edge and exit from the GC, and enhanced or inhibited the development of memory B cells, which required B cell-intrinsic responsiveness to IL-9. Follicular helper T cells (TFH cells) produced IL-9, and deletion of IL-9 from T cells or, more specifically, from GC TFH cells led to impaired memory formation of B cells. Therefore, the GC development of memory B cells is promoted by TFH cell-derived IL-9.

译文

:生殖器中心(GC)支持高亲和力,长寿命的体液免疫。尚不清楚GC中记忆B细胞如何发育。通过使用细胞周期报告系统,我们确定了GC衍生的记忆前体细胞(GC-MP细胞)已经退出循环并达到G0期,而在GC中则表现出与记忆相关的表型,并伴有亲和力成熟和定位于GC边界。在被转移到过继宿主中之后,GC-MP细胞像真正的记忆B细胞一样重新构成了次级反应。 GC-MP细胞表达白介素9(IL-9)受体并对IL-9作出反应。用IL-9或IL-9抗体进行的急性治疗可加速或延迟GC-MP细胞向GC边缘定位并从GC退出,并增强或抑制记忆B细胞的发育,这需要B细胞内在的响应能力IL-9。卵泡辅助性T细胞(TFH细胞)产生IL-9,T细胞或更具体地从GC TFH细胞中删除IL-9导致B细胞记忆形成受损。因此,源自TFH细胞的IL-9促进了记忆B细胞的GC发育。

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