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活化的人 B 细胞产生的白细胞介素-10 可调节体外 CD4(+)T 细胞的活化。

IL-10 produced by activated human B cells regulates CD4(+) T-cell activation in vitro.

机构信息

INSERM U976, Saint Louis Hospital, Skin Research Center, Paris, France.

出版信息

Eur J Immunol. 2010 Oct;40(10):2686-91. doi: 10.1002/eji.201040673.

Abstract

IL-10-producing regulatory B cells have been identified in mice and shown to downregulate inflammation, making them potentially important for maintenance of tolerance. In this study, we isolated B cells from human blood and spleen, and showed that after a short period of ex vivo stimulation a number of these cells produced IL-10. The IL-10-producing B cells did not fall within a single clearly defined subpopulation, but were enriched in both the memory (CD27(+)) and the transitional (CD38(high)) B-cell compartments. Combined CpG-B+anti-Ig stimulation was the most potent IL-10 stimulus tested. B cells stimulated in this way inhibited CD4(+)CD25(-) T-cell proliferation in vitro by a partially IL-10-dependent mechanism. These findings imply that manipulating IL-10 production by human B cells could be a useful therapeutic strategy for modulating immune responses in humans.

摘要

IL-10 产生的调节性 B 细胞在小鼠中被鉴定出来,并被证明可以下调炎症反应,因此它们对于维持耐受可能非常重要。在这项研究中,我们从人血液和脾脏中分离出 B 细胞,并表明这些细胞中的许多在体外短时间刺激后会产生 IL-10。产生 IL-10 的 B 细胞并不属于单个明确的亚群,而是在记忆 (CD27(+)) 和过渡 (CD38(high)) B 细胞区室中富集。CpG-B+抗 Ig 联合刺激是测试的最有效的 IL-10 刺激物。以这种方式刺激的 B 细胞通过部分依赖 IL-10 的机制抑制体外 CD4(+)CD25(-)T 细胞增殖。这些发现表明,通过人 B 细胞操纵 IL-10 产生可能是调节人类免疫反应的一种有用的治疗策略。

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