IRS2 signaling in LepR-b neurons suppresses FoxO1 to control energy balance independently of leptin action.

نویسندگان

  • Marianna Sadagurski
  • Rebecca L Leshan
  • Christa Patterson
  • Aldo Rozzo
  • Alexandra Kuznetsova
  • Josh Skorupski
  • Justin C Jones
  • Ronald A Depinho
  • Martin G Myers
  • Morris F White
چکیده

Irs2-mediated insulin/IGF1 signaling in the CNS modulates energy balance and glucose homeostasis; however, the site for Irs2 function is unknown. The hormone leptin mediates energy balance by acting on leptin receptor (LepR-b)-expressing neurons. To determine whether LepR-b neurons mediate the metabolic actions of Irs2 in the brain, we utilized Lepr(cre) together with Irs2(L/L) to ablate Irs2 expression in LepR-b neurons (Lepr(ΔIrs2)). Lepr(ΔIrs2) mice developed obesity, glucose intolerance, and insulin resistance. Leptin action was not altered in young Lepr(ΔIrs2) mice, although insulin-stimulated FoxO1 nuclear exclusion was reduced in Lepr(ΔIrs2) mice. Indeed, deletion of Foxo1 from LepR-b neurons in Lepr(ΔIrs2) mice normalized energy balance, glucose homeostasis, and arcuate nucleus gene expression. Thus, Irs2 signaling in LepR-b neurons plays a crucial role in metabolic sensing and regulation. While not required for leptin action, Irs2 suppresses FoxO1 signaling in LepR-b neurons to promote energy balance and metabolism.

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عنوان ژورنال:
  • Cell metabolism

دوره 15 5  شماره 

صفحات  -

تاریخ انتشار 2012