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An essential role of the Forkhead-box transcription factor Foxo1 in control of T cell homeostasis and tolerance.

机译:叉头盒转录因子Foxo1在控制T细胞稳态和耐受性中的重要作用。

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摘要

Members of the Forkhead box O (Foxo) family of transcription factors are key regulators of cellular responses, but their function in the immune system remains incompletely understood. Here we showed that T cell-specific deletion of Foxo1 gene in mice led to spontaneous T cell activation, effector T cell differentiation, autoantibody production, and the induction of inflammatory bowel disease in a transfer model. In addition, Foxo1 was critical for the maintenance of naive T cells in the peripheral lymphoid organs. Transcriptome analyses of T cells identified Foxo1-regulated genes encoding, among others, cell-surface molecules, signaling proteins, and nuclear factors that control gene expression. Functional studies validated interleukin-7 receptor-alpha as a Foxo1 target gene essential for Foxo1 maintenance of naive T cells. These findings reveal crucial functions of Foxo1-dependent transcription in control of T cell homeostasis and tolerance.
机译:Forkhead box O(Foxo)转录因子家族的成员是细胞反应的关键调节因子,但它们在免疫系统中的功能仍不完全清楚。在这里,我们显示了在转移模型中,小鼠中Foxo1基因的T细胞特异性缺失导致自发性T细胞活化,效应T细胞分化,自身抗体生成以及炎症性肠病的诱导。此外,Foxo1对于维持外周淋巴器官中的幼稚T细胞至关重要。对T细胞的转录组分析确定了Foxo1调控的基因,这些基因编码细胞表面分子,信号蛋白和控制基因表达的核因子。功能研究证实白细胞介素7受体α是Foxo1维持幼稚T细胞所必需的Foxo1靶基因。这些发现揭示了Foxo1依赖性转录在控制T细胞稳态和耐受性中的关键功能。

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