Regulation of iron homeostasis by the hypoxia-inducible transcription factors (HIFs)

Carole Peyssonnaux; Annelies S. Zinkernagel; Reto A. Schuepbach; Erinn B. Rankin; Sophie Vaulont; Volker H. Haase; Victor Nizet; Randall S. Johnson

doi:10.1172/jci31370

Regulation of iron homeostasis by the hypoxia-inducible transcription factors (HIFs)

Carole Peyssonnaux(University of California, San Diego), Annelies S. Zinkernagel(University of California, San Diego), Reto A. Schuepbach(Scripps Research Institute), Erinn B. Rankin(University of Pennsylvania), Sophie Vaulont(Inserm), Volker H. Haase(University of Pennsylvania), Victor Nizet(University of California, San Diego), Randall S. Johnson

Journal of Clinical Investigation

June 7, 2007

10.1172/jci31370

Cited by 631Open Access

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Abstract

Iron is essential for many biological processes, including oxygen delivery, and its supply is tightly regulated. Hepcidin, a small peptide synthesized in the liver, is a key regulator of iron absorption and homeostasis in mammals. Hepcidin production is increased by iron overload and decreased by anemia and hypoxia; but the molecular mechanisms that govern the hepcidin response to these stimuli are not known. Here we establish that the von Hippel-Lindau/hypoxia-inducible transcription factor (VHL/HIF) pathway is an essential link between iron homeostasis and hepcidin regulation in vivo. Through coordinate downregulation of hepcidin and upregulation of erythropoietin and ferroportin, the VHL-HIF pathway mobilizes iron to support erythrocyte production.

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