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评价含缬草和胡椒碱的提取物对细胞色素 P450 3A 和 P-糖蛋白活性的影响。

Evaluation of the Effects of Extracts Containing Valeriana officinalis and Piper methysticum on the Activities of Cytochrome P450 3A and P-Glycoprotein.

机构信息

Universidade Federal de São João del-Rei, Campus Centro-Oeste Dona Lindu, Chanadour, Divinópolis-MG, Brazil.

Universidade Federal de Minas Gerais, Campus Pampulha, Belo Horizonte-MG, Brazil.

出版信息

Planta Med. 2024 Aug;90(10):792-800. doi: 10.1055/a-2360-4808. Epub 2024 Jul 16.

DOI:10.1055/a-2360-4808
PMID:39013429
Abstract

This work investigated interactions ascribed to the administration of phytomedicines containing and with conventional drugs. The phytomedicines were characterized by HPLC and administered per os to male Wistar rats, either concomitantly or not with the CYP3A substrate midazolam. To distinguish between the presystemic or systemic effect, midazolam was given orally and intravenously. The effects on the P-gp substrate fexofenadine uptake by Caco-2 cells were examined. The valerenic acid content was 1.6 ± 0.1 mg per tablet, whereas kavain was 13.7 ± 0.3 mg/capsule. Valerian and kava-kava extracts increased the maximum plasma concentration (C) of midazolam 2- and 4-fold compared to the control, respectively. The area under the plasma concentrations versus time curve (AUC) was enhanced from 994.3 ± 152.3 ng.h/mL (control) to 3041 ± 398 ng.h/mL (valerian) and 4139 ± 373 ng.h/mL (kava-kava). The half-life of midazolam was not affected. These changes were attributed to the inhibition of midazolam metabolism by the enteric CYP3A since the i. v. pharmacokinetic of midazolam remained unchanged. The kava-kava extract augmented the uptake of fexofenadine by 3.5-fold compared to the control. Although increased the uptake of fexofenadine, it was not statistically significant to that of the control (12.5 ± 3.7 ng/mg protein vs. 5.4 ± 0.3 ng/mg protein, respectively). Therefore, phytomedicines containing or inhibited the intestinal metabolism of midazolam in rats. Conversely, the P-gp-mediated transport of fexofenadine was preferably affected by kava-kava.

摘要

本研究考察了含有缬草根或卡瓦胡椒的植物药与常规药物联合应用时的相互作用。这些植物药通过 HPLC 进行了特征描述,并以口服方式给予雄性 Wistar 大鼠,或与 CYP3A 底物咪达唑仑同时给予,或在其之前给予。为了区分这种相互作用是发生于肠前还是系统,咪达唑仑以口服和静脉内两种方式给予。还研究了这些提取物对 P-糖蛋白底物非索非那定摄取的影响。每片缬草根提取物的缬草酸含量为 1.6±0.1mg,每粒卡瓦胡椒提取物的卡瓦碱含量为 13.7±0.3mg。缬草根和卡瓦胡椒提取物使咪达唑仑的最大血浆浓度(C)分别比对照组增加了 2 倍和 4 倍。与对照组(994.3±152.3ng·h·mL-1)相比,咪达唑仑的血浆浓度-时间曲线下面积(AUC)分别提高到 3041±398ng·h·mL-1(缬草根)和 4139±373ng·h·mL-1(卡瓦胡椒)。咪达唑仑的半衰期没有改变。这些变化归因于肠内 CYP3A 对咪达唑仑代谢的抑制,因为咪达唑仑的静脉内药代动力学没有改变。卡瓦胡椒提取物使非索非那定的摄取增加了 3.5 倍,与对照组相比差异有统计学意义。虽然缬草根增加了非索非那定的摄取,但与对照组相比差异无统计学意义(分别为 12.5±3.7ng/mg 蛋白和 5.4±0.3ng/mg 蛋白)。因此,含有缬草根或卡瓦胡椒的植物药抑制了大鼠中咪达唑仑的肠道代谢。相反,卡瓦胡椒更优先影响非索非那定的 P-糖蛋白介导的转运。

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