艾塞那肽对健康女性联合口服避孕药药代动力学的影响:一项开放标签、随机、交叉试验

Prajakti A Kothare, Mary E Seger, Justin Northrup, Kenneth Mace, Malcolm I Mitchell, Helle Linnebjerg
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引用次数: 22

摘要

背景:艾塞那肽,一种治疗2型糖尿病的注射药物,与其对胃排空的作用一致,可能会减慢同时给药的口服药物的吸收速度,导致最大浓度(Cmax)的降低。本研究评估了艾塞那肽与口服避孕药联合使用时的药物相互作用潜力,考虑到它们可能同时使用。方法:评价艾塞那肽联合给药对联合口服避孕药(乙炔雌二醇[EE] 30 μg,左炔诺孕酮[LV] 150 μg [Microgynon 30®])单剂量和多剂量药代动力学的影响。32名健康女性受试者参加了一项开放标签、随机、交叉试验,共有3个治疗期(单独口服避孕药、使用艾塞那肽前1小时、使用艾塞那肽后30分钟)。受试者在每个月经周期的第8天接受单剂量口服避孕药,并在第10至28天接受QD剂量。在同时使用治疗期间,艾塞那肽在早晚餐前以5 μg BID(第1 - 4天)和10 μg BID(第5 - 22天)皮下给药。评估每个治疗期单剂量(第8天)和多剂量(第22天)的药代动力学特征。结果:艾塞那肽没有改变生物利用度,也没有降低两种口服避孕药成分的日谷浓度。口服避孕药用药前1小时口服避孕药药代动力学无实质性变化。在艾塞那肽后30分钟给予单剂量口服避孕药,EE和LV的平均(90% CI) Cmax分别降低46%(42-51%)和41%(35-47%)。在服用艾塞那肽30分钟后,每日重复口服避孕药可使EE和LV的Cmax分别降低45%(40-50%)和27%(21-33%)。口服避孕药浓度峰值延迟约3至4小时。轻度至中度恶心和呕吐是试验期间观察到的最常见的不良事件。结论:考虑到未改变的口服避孕药生物利用度和谷浓度,观察到的Cmax降低的重要性可能有限;然而,对于依赖于阈值浓度的口服药物,如避孕药和抗生素,应建议患者在注射艾塞那肽前至少1小时服用这些药物。试验注册:ClinicalTrials.gov: NCT00254800。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Effect of exenatide on the pharmacokinetics of a combination oral contraceptive in healthy women: an open-label, randomised, crossover trial.

Background: Consistent with its effect on gastric emptying, exenatide, an injectable treatment for type 2 diabetes, may slow the absorption rate of concomitantly administered oral drugs resulting in a decrease in maximum concentration (Cmax). This study evaluated the drug interaction potential of exenatide when administered adjunctively with oral contraceptives, given their potential concomitant use.

Methods: This trial evaluated the effect of exenatide co-administration on single- and multiple-dose pharmacokinetics of a combination oral contraceptive (ethinyl estradiol [EE] 30 μg, levonorgestrel [LV] 150 μg [Microgynon 30®]). Thirty-two healthy female subjects participated in an open-label, randomised, crossover trial with 3 treatment periods (oral contraceptive alone, 1 hour before exenatide, 30 minutes after exenatide). Subjects received a single dose of oral contraceptive on Day 8 of each period and QD doses on Days 10 through 28. During treatment periods of concomitant usage, exenatide was administered subcutaneously prior to morning and evening meals at 5 μg BID from Days 1 through 4 and at 10 μg BID from Days 5 through 22. Single- (Day 8) and multiple-dose (Day 22) pharmacokinetic profiles were assessed for each treatment period.

Results: Exenatide did not alter the bioavailability nor decrease daily trough concentrations for either oral contraceptive component. No substantive changes in oral contraceptive pharmacokinetics occurred when oral contraceptive was administered 1 hour before exenatide. Single-dose oral contraceptive administration 30 minutes after exenatide resulted in mean (90% CI) Cmax reductions of 46% (42-51%) and 41% (35-47%) for EE and LV, respectively. Repeated daily oral contraceptive administration 30 minutes after exenatide resulted in Cmax reductions of 45% (40-50%) and 27% (21-33%) for EE and LV, respectively. Peak oral contraceptive concentrations were delayed approximately 3 to 4 hours. Mild-to-moderate nausea and vomiting were the most common adverse events observed during the trial.

Conclusions: The observed reduction in Cmax is likely of limited importance given the unaltered oral contraceptive bioavailability and trough concentrations; however, for oral medications that are dependent on threshold concentrations for efficacy, such as contraceptives and antibiotics, patients should be advised to take those drugs at least 1 hour before exenatide injection.

Trial registration: ClinicalTrials.gov: NCT00254800.

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