Biometrics, Lotus Labs, Bangalore, India.
Eur J Clin Pharmacol. 2010 Sep;66(9):879-87. doi: 10.1007/s00228-010-0829-y. Epub 2010 May 6.
Venlafaxine (VEN), a well accepted anti-depressant, is metabolized through the cytochrome P 450 (CYP) 2D6 isozyme to form O-desmethyvenlafaxine (ODV). Due to the involvement of CYP2D6, the formation of ODV is influenced by genetic polymorphism. We used standard tools of assessment to explore the phenotypic distribution in a retrospective manner using the pharmacokinetic (PK) data of VEN and ODV obtained from several bioavailability/bioequivalence (BA/BE) studies in healthy subjects using the reference formulation.
Four single oral dose, open-label, randomized crossover BA/BE studies of VEN (doses: 37.5-150 mg) were performed in 141 healthy subjects. Plasma samples were collected over a period 72 h post VEN administration. The samples were analyzed for VEN and ODV using a validated LC/MS/MS assay with a limit of quantification 2.073 ng/mL for VEN and 3.973 ng/mL for ODV. PK parameters (C(max), T(max), AUC (0-t), AUC(0-infinity), t(1/2)) were computed using the noncompartmental approach. AUC metabolic ratios of VEN/ODV and ODV/VEN were computed for all subjects and were subjected to normality test procedures to tease out phenotypic distribution.
ODV/VEN and VEN/ODV AUC metabolic ratios were evaluated for standard normal distribution and outliers to determine phenotypic distribution. Use of the VEN/ODV AUC metabolic ratio, arranged in a rank order, resulted in a distribution that distinguished poor metabolizers (PM) and extensive metabolizers (EM). The application of the ODV/VEN AUC metabolic ratio showed a unique distribution that distinguished ultra metabolizers (UM) and extensive metabolizers. By using both metabolic ratios, 141 healthy subjects were classified as follows: PMs = 18, EMs = 118, UMs = 5. Regardless of the formulation or dose size used, the plasma concentration-time profiles for both VEN and ODV were distinct amongst the three phenotypes identified in this work.
The use of VEN/ODV and ODV/VEN AUC metabolic ratios suggested quantitative differences. The data support the use of ODV/VEN but not VEN/ODV metabolic ratio for the identification of UM phenotypes of VEN. The derived metabolic ratios of ODV/VEN from this work were in line with other studies that used both phenotypic and genotypic correlation strategies for VEN.
文拉法辛(VEN)是一种被广泛认可的抗抑郁药,通过细胞色素 P450(CYP)2D6 同工酶代谢生成 O-去甲文拉法辛(ODV)。由于涉及 CYP2D6,ODV 的形成受到遗传多态性的影响。我们使用标准评估工具,回顾性地使用参考制剂获得的来自健康受试者的几种生物利用度/生物等效性(BA/BE)研究的 VEN 和 ODV 的药代动力学(PK)数据,来探索表型分布。
对 141 名健康受试者进行了 4 项单口服剂量、开放标签、随机交叉 BA/BE 研究。VEN 的剂量分别为 37.5-150mg。在 VEN 给药后 72 小时内采集血样。使用具有定量下限为 2.073ng/mL 的 VEN 和 3.973ng/mL 的 ODV 的 LC/MS/MS 验证分析方法对 VEN 和 ODV 进行分析。使用非房室模型计算 PK 参数(Cmax、Tmax、AUC(0-t)、AUC(0-无穷大)、t1/2)。计算了所有受试者的 VEN/ODV 和 ODV/VEN 的 AUC 代谢比值,并进行正态性检验程序,以确定表型分布。
对 VEN/ODV 和 ODV/VEN AUC 代谢比值进行了正态分布和离群值检验,以确定表型分布。使用 VEN/ODV AUC 代谢比值进行排序,结果表明存在代谢慢型(PM)和代谢快型(EM)。应用 ODV/VEN AUC 代谢比值可显示独特的分布,可区分超快代谢者(UM)和代谢快型。通过使用这两种代谢比值,将 141 名健康受试者分为以下几类:PMs=18,EMs=118,UMs=5。无论使用哪种制剂或剂量,本研究中确定的三种表型的 VEN 和 ODV 血浆浓度-时间曲线均存在明显差异。
VEN/ODV 和 ODV/VEN AUC 代谢比值的使用表明存在定量差异。数据支持使用 ODV/VEN 而不是 VEN/ODV 代谢比值来识别 VEN 的 UM 表型。本研究中得出的 ODV/VEN 代谢比值与其他使用表型和基因型相关性策略研究 VEN 的研究一致。
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