KLF2
白细胞介素-7受体
生物
C-C趋化因子受体7型
转录因子
福克斯O1
细胞生物学
CXCR4型
趋化因子受体
免疫学
趋化因子
白细胞介素2受体
T细胞
信号转导
炎症
免疫系统
遗传学
蛋白激酶B
基因
作者
Yann M. Kerdiles,Daniel R. Beisner,Roberto Tinoco,Anne S. Dejean,Diego H. Castrillón,Ronald A. DePinho,Stephen Μ. Hedrick
摘要
Foxo transcription factors have a conserved role in the adaptation of cells and organisms to nutrient and growth factor availability. Here we show that Foxo1 has a crucial, nonredundant role in T cells. In naive T cells, Foxo1 controlled the expression of the adhesion molecule L-selectin, the chemokine receptor CCR7 and the transcription factor Klf2, and its deletion was sufficient to alter lymphocyte trafficking. Furthermore, Foxo1 deficiency resulted in a severe defect in interleukin 7 receptor alpha-chain (IL-7Ralpha) expression associated with its ability to bind an Il7r enhancer. Finally, growth factor withdrawal induced a Foxo1-dependent increase in Sell, Klf2 and Il7r expression. These data suggest that Foxo1 regulates the homeostasis and life span of naive T cells by sensing growth factor availability and regulating homing and survival signals.
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