1. Oleoylethanolamide, an endogenous PPAR-α agonist, lowers body weight and hyperlipidemia in obese rats
- Author
-
Fu, Jin, Oveisi, Fariba, Gaetani, Silvana, Lin, Edward, and Piomelli, Daniele
- Subjects
Obesity ,Nutrition ,Stroke ,Cardiovascular ,Oral and gastrointestinal ,Metabolic and endocrine ,Animals ,Body Weight ,Butyrates ,CD36 Antigens ,Cholesterol ,Coenzyme A Ligases ,Eating ,Endocannabinoids ,Fatty Acid-Binding Proteins ,Hepatocytes ,Hyperlipidemias ,Ion Channels ,Liver ,Male ,Mice ,Mice ,Inbred C57BL ,Mice ,Knockout ,Mitochondrial Proteins ,Oleic Acids ,PPAR alpha ,Phenylurea Compounds ,Pyrimidines ,RNA ,Messenger ,Rats ,Rats ,Inbred WF ,Rats ,Zucker ,Thiazoles ,Thiazolidinediones ,Triglycerides ,Uncoupling Protein 2 ,oleoylethanolamine ,peroxisome proliferator-activated receptor-alpha ,obesity ,Zucker rat ,lipid metabolism ,Neurosciences ,Pharmacology and Pharmaceutical Sciences ,Psychology ,Neurology & Neurosurgery - Abstract
The fatty-acid ethanolamide, oleoylethanolamide (OEA), is a naturally occurring lipid that regulates feeding and body weight [Rodriguez de Fonseca, F., Navarro, M., Gomez, R., Escuredo, L., Nava, F., Fu, J., Murillo-Rodriguez, E., Giuffrida, A., LoVerme, J., Gaetani, S., Kathuria, S., Gall, C., Piomelli, D., 2001. An anorexic lipid mediator regulated by feeding. Nature 414, 209-212], and serves as an endogenous agonist of peroxisome proliferator-activated receptor-alpha (PPAR-alpha) [Fu, J., Gaetani, S., Oveisi, F., Lo Verme, J., Serrano, A., Rodriguez De Fonseca, F., Rosengarth., A., Luecke, H., Di Giacomo, B., Tarzia, G., Piomelli, D., 2003. Oleoylethanolamide regulates feeding and body weight through activation of the nuclear receptor PPAR-alpha. Nature 425, 90-93], a ligand-activated transcription factor that regulates several aspects of lipid metabolism [. Peroxisome proliferator-activated receptors: nuclear control of metabolism. Endocr. Rev. 20, 649-688]). OEA reduces food intake in wild-type mice, but not in mice deficient in PPAR-alpha (PPAR-alpha(-/-)), an effect that is also observed with the PPAR-alpha agonists Wy-14643 and GW7647 [Brown, P.J., Chapman, J.M., Oplinger, J.A., Stuart, L.W., Willson, T.M. and Wu, Z., 2000. Chemical compounds as selective activators of PPAR-alpha. PCT Int. Appl., 32; . The PPARs: from orphan receptors to drug discovery. J. Med. Chem. 43, 527-550]. By contrast, specific agonists of PPAR-delta/beta (GW501516) or PPAR-gamma (ciglitazone) have no such effect. In obese Zucker rats, which lack functional leptin receptors, OEA reduces food intake and lowers body-weight gain along with plasma lipid levels. Similar effects are seen in diet-induced obese rats and mice. In the present study, we report that subchronic OEA treatment (5mgkg(-1), intraperitoneally, i.p., once daily for two weeks) in Zucker rats initiates transcription of PPAR-alpha and other PPAR-alpha target genes, including fatty-acid translocase (FAT/CD36), liver fatty-acid binding protein (L-FABP), and uncoupling protein-2 (UCP-2). Moreover, OEA decreases neutral lipid content in hepatocytes, as assessed by Oil red O staining, as well as serum cholesterol and triglyceride levels. The results suggest that OEA regulates lipid metabolism and that this effect may contribute to its anti-obesity properties.
- Published
- 2005