油酰乙醇胺,一种内源性过氧化物酶体增殖物激活受体α(PPAR-α)激动剂,可降低肥胖大鼠的体重和高脂血症。
Oleoylethanolamide, an endogenous PPAR-alpha agonist, lowers body weight and hyperlipidemia in obese rats.
作者信息
Fu Jin, Oveisi Fariba, Gaetani Silvana, Lin Edward, Piomelli Daniele
机构信息
Department of Psychiatry, University of California, Irvine, CA 92697-4625, USA.
出版信息
Neuropharmacology. 2005 Jun;48(8):1147-53. doi: 10.1016/j.neuropharm.2005.02.013. Epub 2005 Apr 21.
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.
脂肪酸乙醇酰胺,即油酰乙醇酰胺(OEA),是一种天然存在的脂质,可调节进食和体重[罗德里格斯·德·丰塞卡,F.,纳瓦罗,M.,戈麦斯,R.,埃斯库雷多,L.,纳瓦,F.,傅,J.,穆里略 - 罗德里格斯,E.,朱弗里达,A.,洛韦尔梅,J.,加埃塔尼,S.,卡图里亚,S.,加尔,C.,皮奥梅利,D.,2001年。一种受进食调节的厌食性脂质介质。《自然》414,209 - 212],并作为过氧化物酶体增殖物激活受体α(PPAR - α)的内源性激动剂[傅,J.,加埃塔尼,S.,奥韦西,F.,洛·韦尔梅,J.,塞拉诺,A.,罗德里格斯·德·丰塞卡,F.,罗森加斯,A.,吕克,H.,迪·贾科莫,B.,塔尔齐亚,G.,皮奥梅利,D.,2003年。油酰乙醇酰胺通过激活核受体PPAR - α调节进食和体重。《自然》425,90 - 93],PPAR - α是一种配体激活的转录因子,可调节脂质代谢的多个方面[。过氧化物酶体增殖物激活受体:代谢的核控制。《内分泌学评论》20,649 - 688]。OEA可减少野生型小鼠的食物摄入量,但对缺乏PPAR - α(PPAR - α(- / -))基因的小鼠无效,PPAR - α激动剂WY - 14643和GW7647也有类似作用[布朗,P.J.,查普曼,J.M.,奥普林格,J.A.,斯图尔特,L.W.,威尔森,T.M.和吴,Z.,2000年。作为PPAR - α选择性激活剂的化合物。《专利合作条约国际申请》,32;。PPARs:从孤儿受体到药物发现。《药物化学杂志》43,527 - 550]。相比之下,PPAR - δ/β(GW501516)或PPAR - γ(吡格列酮)的特异性激动剂则没有这种作用。在缺乏功能性瘦素受体的肥胖 Zucker 大鼠中,OEA 可减少食物摄入量,并降低体重增加以及血浆脂质水平。在饮食诱导肥胖的大鼠和小鼠中也观察到类似效果。在本研究中,我们报告,对 Zucker 大鼠进行亚慢性 OEA 治疗(5mgkg(-1),腹腔注射,每天一次,持续两周)可启动 PPAR - α及其他 PPAR - α靶基因的转录,这些靶基因包括脂肪酸转运蛋白(FAT/CD36)、肝脏脂肪酸结合蛋白(L - FABP)和解偶联蛋白 - 2(UCP - 2)。此外,通过油红 O 染色评估,OEA 可降低肝细胞中的中性脂质含量以及血清胆固醇和甘油三酯水平。结果表明,OEA 可调节脂质代谢,且这种作用可能有助于其抗肥胖特性。
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