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In Vivo and in Vitro Study on Drug-Drug Interaction of Lovastatin and Berberine from Pharmacokinetic and HepG2 Cell Metabolism Studies

机译:洛伐他汀和小Ber碱药代动力学和HepG2细胞代谢研究的体内和体外研究

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Background: We assumed that the pharmacokinetics of lovastatin could be changed by the induction effect of berberine. Methods: An UPLC-MS/MS method was developed and validated for the pharmacokinetics tudy of lovastatin to investigate the in vivo drug-drug interactions between lovastatin and berberine. SD male rats were random divided into lovastatin group and berberine induced prior to lovastatin group for the in vivo pharmacokinetic studies. Meanwhile HepG2 cells were induced by berberine for three days to study the metabolism of lovastatin. Results: The AUC (p p in vivo, and the metabolic activity of HepG2 cell ccould be increased by berberine induction in vitro. The metabolism parameters of lovastatin such as CL, Vmax and Km were increased after the induction of berberine. From the pharmacokinetic study of lovastatin induced with berberine, we obtained pharmacokinetic parameters which are compliance with the metabolic parameters of lovastatin in HepG2 cells with berberine induction in vitro. Conclusions: From the in vivo pharmacokinetics study and the HepG2 cell metabolism study in vitro, berberine could be an inducer for the metabolism of lovastatin according to our previous research on berberine induction effects on HepG2 cells, which may be relevant to the fact that berberine possesses induction effects through the CYP 450 3A4 enzyme. View Full-Text
机译:背景:我们认为洛伐他汀的药代动力学可以通过小ber碱的诱导作用而改变。方法:开发了一种UPLC-MS / MS方法并验证了洛伐他汀的药代动力学研究,以研究洛伐他汀与小ber碱之间的体内药物相互作用。将SD雄性大鼠随机分为洛伐他汀组和在洛伐他汀组之前诱导的小ber碱,用于体内药代动力学研究。同时用黄连素诱导HepG2细胞3天,研究洛伐他汀的代谢。结果:黄连素体外诱导可提高体内AUC(pp)和HepG2细胞的代谢活性;黄连素诱导后洛伐他汀的代谢参数如CL,Vmax和Km增加。小ber碱诱导洛伐他汀的体外药理动力学参数与洛伐他汀在小p碱诱导的HepG2细胞中的代谢参数相符。根据我们先前关于小ber碱对HepG2细胞的诱导作用的研究,洛伐他汀的代谢可能与小ber碱通过CYP 450 3A4酶具有诱导作用有关。

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