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大蒜-药物相互作用的机制及其体内相关性。

The mechanisms responsible for garlic - drug interactions and their in vivo relevance.

机构信息

Faculty of Pharmacy, Aškerčeva 7, 1000 Ljubljana, Slovenia.

出版信息

Curr Drug Metab. 2013 Jan;14(1):90-101.

PMID:21838705
Abstract

Garlic phytochemicals and garlic supplements influence the pharmacokinetic and pharmacodynamic behavior of concomitantly ingested drugs. In this paper we have summarized the mechanisms responsible for first-pass intestinal pharmacokinetic interactions by investigating the intestinal permeability of some cardiovascular, antiviral drugs, their transport with hepatic transporters and CYP3A4 metabolism. Transporter-enzyme interplay was studied with several in vitro models of varying complexity: rat small intestine and Caco-2 cell monolayers were used in studies of intestinal processes, and hepatic pharmacokinetics was monitored in HepG2 cells, isolated rat hepatocytes and rat liver slices. Garlic phytochemicals from aged garlic extract modified the activities of secretory and absorptive transporters in both intestine and liver and competitively inhibited CYP3A4 enzyme. The increased activities of the most important intestinal efflux (P-glycoprotein - Pgp, Multidrug Resistance Associated Protein 2 - MRP-2, Breast Cancer Resistance Protein - BCRP) and uptake (MonoCarboxylate Transporter 1 - MCT1, Organic Anion Transporting Polypeptide - OATP, Peptide transporter 1 - PepT1) transporters were caused by changes in electrophysiological membrane properties and by allosteric modifications. Because clinical studies investigating interactions between garlic and human immunodeficiency virus protease inhibitors saquinavir and ritonavir have already been performed, we used these in vivo data to evaluate the in vitro results and the reliability of the models employed as screening tools for forecasting the potential of first-pass intestinal metabolism changes. We also assessed the probability of pharmacokinetic interactions with garlic of the novel drug darunavir and other cardiovascular drugs. Finally, selected garlic phytochemicals were tested for their ability to influence P-glycoprotein and CYP3A4 activities.

摘要

大蒜植物化学物质和大蒜补充剂会影响同时摄入的药物的药代动力学和药效学行为。在本文中,我们通过研究一些心血管、抗病毒药物的肠内首过代谢的肠通透性,总结了导致首过肠道药代动力学相互作用的机制。我们使用了几种不同复杂程度的体外模型来研究转运体-酶相互作用:大鼠小肠和 Caco-2 细胞单层用于肠内过程的研究,而 HepG2 细胞、分离的大鼠肝细胞和大鼠肝切片用于监测肝内药代动力学。从陈年大蒜提取物中提取的大蒜植物化学物质改变了肠内和肝内分泌和吸收转运体的活性,并竞争性抑制了 CYP3A4 酶。最重要的肠内流出(P-糖蛋白-Pgp、多药耐药相关蛋白 2-MRP-2、乳腺癌耐药蛋白-BCRP)和摄取(单羧酸转运蛋白 1-MCT1、有机阴离子转运多肽-OATP、肽转运蛋白 1-PepT1)转运体的活性增加是由于膜电生理性质的变化和变构修饰引起的。由于已经进行了大蒜与人类免疫缺陷病毒蛋白酶抑制剂沙奎那韦和利托那韦之间相互作用的临床研究,我们使用这些体内数据来评估体外结果和所使用模型的可靠性,这些模型可作为预测首过肠内代谢变化潜力的筛选工具。我们还评估了新型药物达芦那韦和其他心血管药物与大蒜发生药代动力学相互作用的可能性。最后,测试了选定的大蒜植物化学物质对 P-糖蛋白和 CYP3A4 活性的影响。

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