Department of Immunology and Oncology, Centro Nacional de Biotecnología/CSIC, Madrid, Spain.
Institute for Research in Biomedicine (IRB Barcelona), Barcelona Institute of Science and Technology, Barcelona, Spain.
Immunol Cell Biol. 2017 Oct;95(9):814-823. doi: 10.1038/icb.2017.51. Epub 2017 Jun 14.
The p38 mitogen-activated protein kinase (MAPK) pathway is involved in the regulation of immune and inflammatory processes. We used p38α-conditional, p38β-deficient and p38α/β double-null mouse models to address the role of these two p38 MAPK in CD4 T cells, and found that p38α deficiency causes these cells to hyperproliferate. Our studies indicate that both p38α and p38β are dispensable for T helper cell type 1 (Th1) differentiation but, by controlling interferon (IFN)γ and tumor necrosis factor (TNF)α production, are critical for normal Th1 effector function. We found that both p38α and p38β modulate T-cell receptor-induced IFNγ and TNFα production, whereas only p38α regulates cytokine-induced IFNγ production. The lack of p38α and p38β did not affect transcription and mRNA stability of Ifng. However, the absence of p38α in Th1 cells resulted in a decreased MNK1 phosphorylation after cytokine activation, and MNK1 inhibition blocked IFNγ production. Our results indicate that p38α regulates IFNγ secretion through the activation of the MNK1/eIF4E pathway of translation initiation and identify specific functions for p38α and p38β in T-cell proliferation.
p38 丝裂原活化蛋白激酶 (MAPK) 途径参与免疫和炎症过程的调节。我们使用 p38α 条件性敲除、p38β 缺陷和 p38α/β 双敲除小鼠模型来研究这两种 p38 MAPK 在 CD4 T 细胞中的作用,发现 p38α 缺陷导致这些细胞过度增殖。我们的研究表明,p38α 和 p38β 对于辅助性 T 细胞 1(Th1)分化都是可有可无的,但通过控制干扰素(IFN)γ和肿瘤坏死因子(TNF)α的产生,它们对于正常 Th1 效应功能至关重要。我们发现,p38α 和 p38β 都可以调节 T 细胞受体诱导的 IFNγ 和 TNFα 的产生,而只有 p38α 可以调节细胞因子诱导的 IFNγ 的产生。缺乏 p38α 和 p38β 并不影响 Ifng 的转录和 mRNA 稳定性。然而,Th1 细胞中 p38α 的缺失导致细胞因子激活后 MNK1 磷酸化减少,而 MNK1 抑制阻断了 IFNγ 的产生。我们的研究结果表明,p38α 通过激活翻译起始的 MNK1/eIF4E 途径来调节 IFNγ 的分泌,并确定了 p38α 和 p38β 在 T 细胞增殖中的特定功能。
