Compound K modulates fatty acid‐induced lipid droplet formation and expression of proteins involved in lipid metabolism in hepatocytes

脂质代谢 脂滴 脂肪变性 安普克 脂肪肝 过氧化物酶体增殖物激活受体 过氧化物酶体 化学 内分泌学 内科学 脂肪酸 β氧化 生物化学 生物 受体 磷酸化 蛋白激酶A 医学 疾病
作者
Moon‐Sun Kim,Kyoungtae Lee,Tristan J. Iseli,Andrew J. Hoy,Jacob George,Thomas Grewal,Basil D. Roufogalis
出处
期刊:Liver International [Wiley]
卷期号:33 (10): 1583-1593 被引量:28
标识
DOI:10.1111/liv.12287
摘要

Abstract Background & Aims A key factor in the development of type 2 diabetes and non‐alcoholic fatty liver disease ( NAFLD ) is hepatic steatosis. Incubation of human hepatic cells with free fatty acids ( FFA s) causes accumulation of neutral lipids in lipid droplets ( LD s) and serves as a model for hepatic steatosis. Ginsenosides, active constituents of ginsengs, have demonstrated beneficial effects in various pharmacological areas, including diabetes, however their effect on lipid accumulation in hepatocytes remains unclear. Here, we examine the effect of compound K (ComK), an active metabolite of ginsenosides, on the regulation of LD formation and on the expression of proteins involved in lipid homeostasis in hepatocytes. Methods HuH7 cells were pretreated with ComK, followed by lipid loading with FFA . LD s were visualized using Oil Red O staining and immunohistochemistry for the LD ‐related protein PLIN 2. Triglyceride levels were determined in isolated LD s. The expression of proteins involved in lipid homeostasis was examined by Western blotting. Results Treatment with ComK significantly decreased LD formation in FFA ‐loaded HuH7 cells and increased phosphorylation levels of AMPK , and its substrate ACC . ComK also increased protein expression of peroxisome proliferator‐activated receptor‐α ( PPAR ‐α) and acyl‐CoA oxidase ( ACOX 1) together with elevated activity of a PPAR ‐α response element reporter construct. These effects were inhibited by the PPAR ‐α antagonist MK 886. Conclusions ComK reduced LD formation and TG accumulation in FFA ‐loaded hepatocytes, in part by up‐regulating AMPK activity and PPAR ‐α related pathways. These results suggest that ComK may have efficacy for the treatment of hepatic steatosis and associated diseases.
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