Wang Pan-Fen, Yang Yanming, Patel Vishal, Neiner Alicia, Kharasch Evan D
Department of Anesthesiology, Duke University, Durham, North Carolina (P.-F.W., E.D.K.) and Department of Anesthesiology, Washington University in St. Louis, St. Louis, Missouri (Y.Y., V.P., A.N.).
Department of Anesthesiology, Duke University, Durham, North Carolina (P.-F.W., E.D.K.) and Department of Anesthesiology, Washington University in St. Louis, St. Louis, Missouri (Y.Y., V.P., A.N.)
Drug Metab Dispos. 2024 Feb 14;52(3):252-265. doi: 10.1124/dmd.123.001578.
Methadone is cleared predominately by hepatic cytochrome P450 (CYP) 2B6-catalyzed metabolism to inactive metabolites. CYP2B6 also catalyzes the metabolism of several other drugs. Methadone and CYP2B6 are susceptible to pharmacokinetic drug-drug interactions. Use of natural products such as herbals and other botanicals is substantial and growing, and concomitant use of prescription medicines and non-prescription herbals is common and may result in interactions, often precipitated by CYP inhibition. Little is known about herbal product effects on CYP2B6 activity, and CYP2B6-catalyzed methadone metabolism. We screened a family of natural product compounds used in traditional medicines, herbal teas, and synthetic analogs of compounds found in plants, including kavalactones, flavokavains, chalcones and gambogic acid, for inhibition of expressed CYP2B6 activity and specifically inhibition of CYP2B6-mediated methadone metabolism. An initial screen evaluated inhibition of CYP2B6-catalyzed 7-ethoxy-4-(trifluoromethyl) coumarin O-deethylation. Hits were further evaluated for inhibition of racemic methadone metabolism, including mechanism of inhibition and kinetic constants. In order of decreasing potency, the most effective inhibitors of methadone metabolism were dihydromethysticin (competitive, 0.074 M), gambogic acid (noncompetitive, 6 M), and 2,2'-dihydroxychalcone (noncompetitive, 16 M). Molecular modeling of CYP2B6-methadone and inhibitor binding showed substrate and inhibitor binding position and orientation and their interactions with CYP2B6 residues. These results show that CYP2B6 and CYP2B6-catalyzed methadone metabolism are inhibited by certain natural products, at concentrations which may be clinically relevant. SIGNIFICANCE STATEMENT: This investigation identified several natural product constituents which inhibit human recombinant CYP2B6 and CYP2B6-catalyzed N-demethylation of the opioid methadone. The most potent inhibitors ( ) were dihydromethysticin (0.074 µM), gambogic acid (6 µM) and 2,2'-dihydroxychalcone (16 µM). Molecular modeling of ligand interactions with CYP2B6 found that dihydromethysticin and 2,2'-dihydroxychalcone bound at the active site, while gambogic acid interacted with an allosteric site on the CYP2B6 surface. Natural product constituents may inhibit CYP2B6 and methadone metabolism at clinically relevant concentrations.
美沙酮主要通过肝脏细胞色素P450(CYP)2B6催化代谢为无活性代谢产物而清除。CYP2B6还催化其他几种药物的代谢。美沙酮和CYP2B6易发生药代动力学药物-药物相互作用。天然产物如草药和其他植物药的使用广泛且呈增长趋势,处方药与非处方草药同时使用很常见,可能会导致相互作用,这种相互作用通常由CYP抑制引发。关于草药产品对CYP2B6活性和美沙酮代谢的影响知之甚少。我们筛选了一系列用于传统药物、花草茶以及植物中发现的化合物的合成类似物的天然产物化合物,包括卡瓦内酯、黄酮卡瓦因、查耳酮和藤黄酸,以研究它们对表达的CYP2B6活性的抑制作用,特别是对CYP2B6介导的美沙酮代谢的抑制作用。初步筛选评估了对CYP2B6催化的7-乙氧基-4-(三氟甲基)香豆素O-脱乙基作用的抑制情况。对筛选出的活性物质进一步评估其对外消旋美沙酮代谢的抑制作用,包括抑制机制和动力学常数。按效力递减顺序,美沙酮代谢的最有效抑制剂为二氢紫水晶素(竞争性,0.074 μM)、藤黄酸(非竞争性,6 μM)和2,2'-二羟基查耳酮(非竞争性,16 μM)。CYP2B6-美沙酮和抑制剂结合的分子模型显示了底物和抑制剂的结合位置与方向以及它们与CYP2B6残基的相互作用。这些结果表明,某些天然产物在可能具有临床相关性的浓度下可抑制CYP2B6和美沙酮代谢。重要声明:本研究确定了几种天然产物成分可抑制人重组CYP2B6以及CYP2B6催化的阿片类药物美沙酮的N-去甲基化。最有效的抑制剂( )为二氢紫水晶素(0.074 μM)、藤黄酸(6 μM)和2,2'-二羟基查耳酮(16 μM)。配体与CYP2B6相互作用的分子模型发现,二氢紫水晶素和2,2'-二羟基查耳酮结合在活性位点,而藤黄酸与CYP2B6表面的一个别构位点相互作用。天然产物成分可能在临床相关浓度下抑制CYP2B6和美沙酮代谢。
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