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Publication : PPAR-alpha dependent regulation of vanin-1 mediates hepatic lipid metabolism.

First Author  van Diepen JA Year  2014
Journal  J Hepatol Volume  61
Issue  2 Pages  366-72
PubMed ID  24751833 Mgi Jnum  J:271190
Mgi Id  MGI:6278450 Doi  10.1016/j.jhep.2014.04.013
Citation  van Diepen JA, et al. (2014) PPAR-alpha dependent regulation of vanin-1 mediates hepatic lipid metabolism. J Hepatol 61(2):366-72
abstractText  BACKGROUND & AIMS: Peroxisome proliferator-activated receptor alpha (PPARalpha) is a key regulator of hepatic fat oxidation that serves as an energy source during starvation. Vanin-1 has been described as a putative PPARalpha target gene in liver, but its function in hepatic lipid metabolism is unknown. METHODS: We investigated the regulation of vanin-1, and total vanin activity, by PPARalpha in mice and humans. Furthermore, the function of vanin-1 in the development of hepatic steatosis in response to starvation was examined in Vnn1 deficient mice, and in rats treated with an inhibitor of vanin activity. RESULTS: Liver microarray analyses reveals that Vnn1 is the most prominently regulated gene after modulation of PPARalpha activity. In addition, activation of mouse PPARalpha regulates hepatic- and plasma vanin activity. In humans, consistent with regulation by PPARalpha, plasma vanin activity increases in all subjects after prolonged fasting, as well as after treatment with the PPARalpha agonist fenofibrate. In mice, absence of vanin-1 exacerbates the fasting-induced increase in hepatic triglyceride levels. Similarly, inhibition of vanin activity in rats induces accumulation of hepatic triglycerides upon fasting. Microarray analysis reveal that the absence of vanin-1 associates with gene sets involved in liver steatosis, and reduces pathways involved in oxidative stress and inflammation. CONCLUSIONS: We show that hepatic vanin-1 is under extremely sensitive regulation by PPARalpha and that plasma vanin activity could serve as a readout of changes in PPARalpha activity in human subjects. In addition, our data propose a role for vanin-1 in regulation of hepatic TG levels during fasting.
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