首页> 外文期刊>Immunology: An Official Journal of the British Society for Immunology >Presentation of high antigen-dose by splenic B220(lo) B cells fosters a feedback loop between T helper type 2 memory and antibody isotype switching
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Presentation of high antigen-dose by splenic B220(lo) B cells fosters a feedback loop between T helper type 2 memory and antibody isotype switching

机译:脾脏B220(lo)B细胞呈递高抗原剂量可促进T辅助2型记忆与抗体同种型转换之间的反馈回路

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摘要

Effective humoral immunity ensues when antigen presentation by B cells culminates in productive cooperation with T lymphocytes. This collaboration, however, remains ill-defined because naive antigen-specific B cells are rare and difficult to track in vivo. Herein, we used a defined transfer model to examine how B lymphocytes, as antigen-presenting cells, shape the development of T-cell memory suitable for generation of relevant antibody responses. Specifically, we examined how B cells presenting different doses of antigen during the initial priming phase shape the development of CD4 T-cell memory and its influence on humoral immunity. The findings indicate that B cells presenting low dose of antigen favour the development of T helper type 1 (Th1) type memory, while those presenting a high antigen dose yielded better Th2 memory cells. The memory Th2 cells supported the production of antibodies by effector B cells and promoted isotype switching to IgG1. Moreover, among the B-cell subsets tested for induction of Th2 memory, the splenic but not peritoneal B220(lo) cells were most effective in sustaining Th2 memory development as well as immunoglobulin isotype switching, and this function involved a tight control by programmed death 1-programmed death ligand 2 interactions.
机译:当B细胞的抗原呈递达到与T淋巴细胞的生产性合作的最高峰时,便会产生有效的体液免疫。但是,这种合作仍然不确定,因为幼稚的抗原特异性B细胞很少见,并且很难在体内追踪。在这里,我们使用定义的转移模型来检查B淋巴细胞作为抗原呈递细胞如何塑造适合于产生相关抗体反应的T细胞记忆的发育。具体来说,我们检查了在初始启动阶段B细胞呈现不同剂量抗原的方式如何影响CD4 T细胞记忆的发展及其对体液免疫的影响。这些发现表明,低剂量抗原的B细胞有利于T辅助1型(Th1)型记忆的发展,而高抗原剂量的B细胞产生更好的Th2记忆细胞。记忆Th2细胞支持效应B细胞产生抗体,并促进同种型转换为IgG1。此外,在经测试可诱导Th2记忆的B细胞亚群中,脾脏而非腹膜B220(lo)细胞在维持Th2记忆发展以及免疫球蛋白同种型转换方面最有效,该功能涉及通过程序性死亡进行严格控制1-编程的死亡配体2相互作用。

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