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首页> 外文期刊>Molecular and Cellular Endocrinology >Genistein enhances expression of genes involved in fatty acid catabolism through activation of PPARalpha.
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Genistein enhances expression of genes involved in fatty acid catabolism through activation of PPARalpha.

机译:金雀异黄素通过激活PPARalpha增强与脂肪酸分解代谢有关的基因的表达。

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Although evidences are emerging that dietary isoflavones have beneficial effects in treatment of hyperlipidemia and cardiovascular diseases, the underlying molecular mechanism has not yet been extensively characterized. In this report, we showed that genistein, one of the major isoflavones, increased expression of genes involved in lipid catabolism such as carnitine palmitoyltransferase 1, liver form (CPT1L) in HepG2 cells, when assayed by real-time reverse-transcriptase polymerase chain reactions as well as Western blotting analysis. The increase in mRNA-level of CPT1L after genistein treatment was not changed in the presence of ICI182780, a potent inhibitor of estrogen receptor, suggesting that this effect of genistein was estrogen receptor-independent. Since these genes involved in fatty acid catabolism are considered putative downstream target genes of peroxisome proliferators-activated receptor alpha (PPARalpha), we examined whether expression of PPARalpha was modulated by genistein treatment. Interestingly, genistein induced expression of PPARalpha at both mRNA- and protein-level. Further, genistein activated transcriptional activity of PPARalpha, when determined by reporter gene analysis, suggesting genistein as a potential ligand for PPARalpha. Taken together, this study provides a picture of the regulatory action of genistein, as an activator of PPARalpha in fatty acid catabolism and potential use of genistein as lipid-lowering agent.
机译:尽管有证据表明饮食中的异黄酮对高脂血症和心血管疾病具有有益的作用,但其潜在的分子机制尚未得到广泛表征。在本报告中,我们显示,通过实时逆转录酶聚合酶链反应测定,染料木黄酮(一种主要的异黄酮)在HepG2细胞中增加了参与脂质分解代谢的基因(如肉碱棕榈酰转移酶1,肝脏形式(CPT1L))的表达。以及蛋白质印迹分析。金雀异黄素处理后CPT1L mRNA水平的增加在ICI182780(一种有效的雌激素受体抑制剂)的存在下没有改变,这表明金雀异黄素的这种作用与雌激素受体无关。由于这些参与脂肪酸分解代谢的基因被认为是过氧化物酶体增殖物激活的受体α(PPARalpha)的假定下游靶基因,因此我们检查了染料木黄酮对PPARalpha的表达是否有所调节。有趣的是,金雀异黄素诱导了mRNA和蛋白质水平的PPARα表达。此外,当通过报告基因分析确定染料木黄酮激活了PPARα的转录活性时,表明染料木黄酮是PPARα的潜在配体。两者合计,这项研究提供了染料木黄酮作为脂肪酸分解代谢中PPARα的活化剂的调控作用以及染料木黄酮作为降脂剂的潜在用途的图片。

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