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辅助性T细胞分化过程中整合应激反应的激活。

Activation of the integrated stress response during T helper cell differentiation.

作者信息

Scheu Stefanie, Stetson Daniel B, Reinhardt R Lee, Leber Jess H, Mohrs Markus, Locksley Richard M

机构信息

Howard Hughes Medical Institute, University of California San Francisco, San Francisco, California 94143, USA.

出版信息

Nat Immunol. 2006 Jun;7(6):644-51. doi: 10.1038/ni1338. Epub 2006 May 7.

Abstract

Adaptive immune responses require clonal expansion and differentiation of naive T cells into cytokine-secreting effector cells. After priming via signals through the T cell receptor, naive T helper cells express cytokine mRNA but do not secrete cytokine protein without additional T cell receptor stimulation. Here we show that primed T cells demonstrated phosphorylation of eukaryotic initiation factor 2-alpha (eIF2alpha), a 'collapsed' polysome profile, increased expression of stress-response genes and accumulation of cytoplasmic granules associated with RNA-binding proteins, all features of the integrated stress response. Restimulation of the cells resulted in rapid eIF2alpha dephosphorylation, ribosomal mRNA loading and cytokine secretion. Interference with the function of granule-associated proteins or accumulation of phosphorylated eIF2alpha enhanced release of interleukin 4 during T helper type 2 priming. Therefore, T lymphocytes require components of the integrated stress response to uncouple differentiation from the execution of effector functions.

摘要

适应性免疫反应需要克隆扩增以及初始T细胞分化为分泌细胞因子的效应细胞。在通过T细胞受体信号进行致敏后,初始辅助性T细胞表达细胞因子mRNA,但在没有额外T细胞受体刺激的情况下不会分泌细胞因子蛋白。我们在此表明,致敏的T细胞表现出真核起始因子2α(eIF2α)的磷酸化、“塌陷”的多核糖体图谱、应激反应基因表达增加以及与RNA结合蛋白相关的细胞质颗粒积累,这些都是综合应激反应的特征。再次刺激这些细胞会导致eIF2α迅速去磷酸化、核糖体mRNA加载和细胞因子分泌。干扰颗粒相关蛋白的功能或磷酸化eIF2α的积累会增强2型辅助性T细胞致敏过程中白细胞介素4的释放。因此,T淋巴细胞需要综合应激反应的成分来使分化与效应功能的执行脱钩。

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