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TGF-β 敏感性通过增强对 IL-7 和 IL-15 的敏感性来抑制 CD8+ T 细胞的稳态增殖。

TGF-β sensitivity restrains CD8+ T cell homeostatic proliferation by enforcing sensitivity to IL-7 and IL-15.

机构信息

Lab Medicine and Pathology, Center for Immunology, University of Minnesota, Minneapolis, Minnesota, United States of America.

出版信息

PLoS One. 2012;7(8):e42268. doi: 10.1371/journal.pone.0042268. Epub 2012 Aug 6.

Abstract

The pleiotropic cytokine TGF-β has been implicated in the regulation of numerous aspects of the immune response, including naïve T cell homeostasis. Previous studies found that impairing TGF-β responsiveness (through expression of a dominant-negative TGF-β RII [DNRII] transgene) leads to accumulation of memory phenotype CD8 T cells, and it was proposed that this resulted from enhanced IL-15 sensitivity. Here we show naïve DNRII CD8 T cells exhibit enhanced lymphopenia-driven proliferation and generation of "homeostatic" memory cells. However, this enhanced response occurred in the absence of IL-15 and, unexpectedly, even in the combined absence of IL-7 and IL-15, which were thought essential for CD8 T cell homeostatic expansion. DNRII transgenic CD8 T cells still require access to self Class I MHC for homeostatic proliferation, arguing against generalized dysregulation of homeostatic cues. These findings suggest TGF-β responsiveness is critical for enforcing sensitivity to homeostatic cytokines that limit maintenance and composition of the CD8 T cell pool. (154 words).

摘要

多功能细胞因子 TGF-β 被认为参与了免疫反应的许多方面的调节,包括幼稚 T 细胞的稳态。先前的研究发现,抑制 TGF-β 的反应性(通过表达显性负 TGF-β RII [DNRII] 转基因)会导致记忆表型 CD8 T 细胞的积累,并且据推测这是由于增强了 IL-15 的敏感性所致。在这里,我们发现幼稚的 DNRII CD8 T 细胞表现出增强的淋巴细胞减少驱动的增殖和“稳态”记忆细胞的生成。然而,这种增强的反应发生在没有 IL-15 的情况下,而且出乎意料的是,甚至在没有 IL-7 和 IL-15 的联合情况下也会发生,这被认为是 CD8 T 细胞稳态扩张所必需的。DNRII 转基因 CD8 T 细胞仍然需要获得自身的 Class I MHC 以进行稳态增殖,这表明对稳态细胞因子的敏感性受到限制,从而限制了 CD8 T 细胞库的维持和组成。(154 个单词)。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a7ab/3412850/e5430d8b1c0f/pone.0042268.g001.jpg

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