安普克
有机阳离子转运蛋白
运输机
化学
脂肪酸合酶
药理学
生物化学
脂质代谢
天然产物
生物
酶
蛋白激酶A
基因
作者
Yajuan Bi,Li Wang,Lifeng Han,Yiqing Tian,Tongwei Bo,Caiyu Li,Bowen Shi,Chunshan Gui,Youcai Zhang
标识
DOI:10.1021/acs.jnatprod.2c00927
摘要
Organic cation transporter 1 (OCT1) is a liver-specific transporter and plays an essential role in drug disposition and hepatic lipid metabolism. Therefore, inhibition of OCT1 may not only lead to drug–drug interactions but also represent a potential therapy for fatty liver diseases. In this study, we systematically investigated the inhibitory effect of 200 natural products on OCT1-mediated uptake of 4,4-dimethylaminostyryl-N-methylpyridinium (ASP+) and identified 10 potent OCT1 inhibitors. The selectivity of these inhibitors over OCT2 was evaluated using both in vitro uptake assays and in silico molecular docking analyses. Importantly, benzoylpaeoniflorin was identified as the most potent OCT1 inhibitor with the highest selectivity over OCT2. Additionally, benzoylpaeoniflorin prevented lipid accumulation in hepatocytes, with concomitant activation of AMPK and down-regulation of lipogenic genes, such as acetyl-CoA carboxylase (ACC) and fatty acid synthase (FASN). To conclude, our findings are of significant value in understanding OCT1-based natural product–drug interactions and provide a natural source of OCT1 inhibitors which may hold promise for treating fatty liver diseases.
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