Article by Kerdiles Y.M. et al. Nature Immunology, 2009

نویسندگان

  • Yann M Kerdiles
  • Daniel R Beisner
  • Roberto Tinoco
  • Anne S Dejean
  • Diego H Castrillon
  • Ronald A DePinho
  • Stephen M Hedrick
چکیده

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 a-chain (IL-7Ra) 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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تاریخ انتشار 2009