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白细胞介素-7 通过诱导 T 细胞表达 B 细胞激活因子和 CD70 来调节 B 细胞的存活和激活。

IL-7 modulates B cells survival and activation by inducing BAFF and CD70 expression in T cells.

机构信息

Department of Microbiology, Tumor and Cell Biology, Karolinska Institutet, Nobels väg 16, Stockholm 17177, Sweden.

出版信息

J Autoimmun. 2012 Jun;38(4):304-14. doi: 10.1016/j.jaut.2012.01.012. Epub 2012 Feb 15.

Abstract

Interleukin-7 (IL-7) promotes the maintenance and activation of peripheral T cells, whereas it does not act directly on mature B cells due to the lack of IL-7Rα expression on these. We report here that, in spite of the insensitivity of B cells to IL-7, high concentration of IL-7 can lead to increased B cell survival and antibody production in the presence of T cells, without the use of any further B cell stimulatory signal. IL-7 promoted B cell activation through inducing CD70 expression on resting T cells, particularly on CD4+ memory cells. The interaction of CD70 molecules with the B cell costimulatory receptor CD27 led to B cell proliferation, the accumulation of CD38 + CD20- plasmablasts and antibody production. In addition, IL-7 treatment induced BAFF secretion from resting peripheral T cells thereby promoting B cell survival. IL-7 levels can increase in lymphopenic conditions, in autoimmune diseases or in patients receiving T cell regenerative IL-7 therapy. Based on our findings high IL-7 levels can lead to increased B cell activation by inducing the B cell regulatory proteins CD70 and BAFF in resting T cells. Such activity might be beneficial in short term immune-stimulatory IL-7 therapies; permanently increased IL-7 levels, on the other hand, can contribute to impaired B cell tolerance.

摘要

白细胞介素-7(IL-7)促进外周 T 细胞的维持和激活,而由于成熟 B 细胞缺乏 IL-7Rα表达,IL-7 对其不起直接作用。我们在这里报告,尽管 B 细胞对 IL-7 不敏感,但在 T 细胞存在的情况下,高浓度的 IL-7 可以导致 B 细胞存活和抗体产生增加,而无需使用任何其他 B 细胞刺激信号。IL-7 通过诱导静止 T 细胞(特别是 CD4+记忆细胞)上的 CD70 表达来促进 B 细胞激活。CD70 分子与 B 细胞共刺激受体 CD27 的相互作用导致 B 细胞增殖、CD38+CD20-浆母细胞的积累和抗体产生。此外,IL-7 处理诱导静止外周 T 细胞分泌 BAFF,从而促进 B 细胞存活。在淋巴细胞减少症、自身免疫性疾病或接受 T 细胞再生 IL-7 治疗的患者中,IL-7 水平可以增加。基于我们的发现,高 IL-7 水平可以通过诱导静止 T 细胞中的 B 细胞调节蛋白 CD70 和 BAFF 来导致 B 细胞激活增加。这种活性在短期免疫刺激 IL-7 治疗中可能是有益的;另一方面,永久性增加 IL-7 水平可能导致 B 细胞耐受受损。

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