Hypoxia-mediated Na-K-ATPase degradation requires von Hippel Lindau protein

doi:10.1096/fj.07-8369com

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Published as doi: 10.1096/fj.07-8369com.
(The FASEB Journal. 2008;22:1335-1342.)
© 2008 FASEB

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Hypoxia-mediated Na-K-ATPase degradation requires von Hippel Lindau protein

Guofei Zhou^*, Laura A. Dada^*, Navdeep S. Chandel^*, Kazuhiro Iwai, Emilia Lecuona^*, Aaron Ciechanover and Jacob I. Sznajder^*^,1

^* Division of Pulmonary and Critical Care Medicine, Feinberg School of Medicine, Northwestern University, Chicago, Illinois, USA;

Department of Molecular Cell Biology, Graduate School of Medicine, Osaka City University, Abeno-Ku, Osaka, Japan; and

Vascular and Tumor Biology Research Center, Faculty of Medicine, Technion-Israel Institute of Technology, Haifa, Israel

¹Correspondence: Pulmonary and Critical Care Medicine, Feinberg School of Medicine, Northwestern University, 240 E. Huron, McGaw Pavilion M-300, Chicago, IL 60611, USA. E-mail: j-sznajder{at}northwestern.edu

Hypoxia inhibits Na-K-ATPase activity and leads to its degradationin mammalian cells. Von Hippel Lindau protein (pVHL) and hypoxiainducible factor (HIF) are key mediators in cellular adaptationto hypoxia; thus, we set out to investigate whether pVHL andHIF participate in the hypoxia-mediated degradation of plasmamembrane Na-K-ATPase. We found that in the presence of pVHLhypoxia decreased Na-K-ATPase activity and promoted the degradationof plasma membrane Na-K-ATPase. In pVHL-deficient cells, hypoxiadid not decrease the Na-K-ATPase activity and the degradationof plasma membrane Na-K-ATPase was prevented. pVHL-mediateddegradation of Na-K-ATPase required the functional pVHL E3 ligaseand Ubc5 since pVHL mutants and dominant-negative Ubc5 preventedNa-K-ATPase from degradation. The generation of reactive oxygenspecies was necessary for pVHL-mediated Na-K-ATPase degradationduring hypoxia. Desferrioxamine, which stabilizes HIF1/2 ${alpha}$ , didnot affect the half-life of plasma membrane Na-K-ATPase. Inaddition, stabilizing HIF1/2 ${alpha}$ by infecting mammalian cells withadenoviruses containing the oxygen-dependent degradation domainof HIF1 ${alpha}$ did not affect the plasma membrane Na-K-ATPase degradation.In cells with suppression of pVHL by short hairpin RNA, theNa-K-ATPase was not degraded during hypoxia, whereas cells withknockdown of HIF1/2 ${alpha}$ retained the ability to degrade plasma membraneNa-K-ATPase. These findings suggest that pVHL participates inthe hypoxia-mediated degradation of plasma membrane Na-K-ATPasein a HIF-independent manner.—Zhou, G., Dada, L. A., Chandel,N. S., Iwai, K., Lecuona, E., Ciechanover, A., Sznajder, J.I. Hypoxia-mediated Na-K-ATPase degradation requires von HippelLindau protein.

Key Words: hypoxia inducible factor • pVHL