氢吗啡酮24小时控释OROS制剂在食物存在和不存在条件下的药动学特征。

Gayatri Sathyan, Emily Xu, John Thipphawong, Suneel K Gupta
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引用次数: 1

摘要

背景:本研究的目的是比较一种新的、每日一次的控释制剂氢吗啡酮(OROS氢吗啡酮)在空腹条件下与健康志愿者在高脂肪早餐后立即的药代动力学特征。阿片拮抗剂纳曲酮对空腹氢吗啡酮药动学的影响也进行了评价。方法:在一项开放标签、三方向、交叉研究中,30名健康志愿者随机接受空腹条件下单剂量16 mg OROS氢吗啡酮、喂养条件下16 mg OROS氢吗啡酮或空腹条件下16 mg OROS氢吗啡酮与纳曲酮50 mg块。在给药前和给药后48小时内定期抽取血浆样本检测氢吗啡酮浓度。对对数变换后的数据进行方差分析;对于平均比率为0.8至1.2(20%),差异被认为是最小的。如果处理平均比率的90%置信区间(CI)在80%至125%之间,则达到生物等效性。结果:饲喂组和禁食组最大血药浓度(Cmax)和浓度-时间曲线下面积(AUC0-t;auc0 -∞)在20%以内。AUC0-t和AUC0-infinity的置信区间在80% ~ 125%之间,但Cmax的置信区间略高(分别为105.9%和133.3%)。纳曲酮阻断组氢吗啡酮Cmax增加39%,终末半衰期缩短4.5 h。Tmax、AUC0-t和AUC0-infinity均无显著变化。结论:标准生物利用度测量表明,食品对OROS氢吗啡酮的生物利用度影响极小。纳曲酮共给药导致吸收率略有增加,但吸收程度没有增加。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Pharmacokinetic profile of a 24-hour controlled-release OROS formulation of hydromorphone in the presence and absence of food.

Pharmacokinetic profile of a 24-hour controlled-release OROS formulation of hydromorphone in the presence and absence of food.

Pharmacokinetic profile of a 24-hour controlled-release OROS formulation of hydromorphone in the presence and absence of food.

Background: The objective of this study was to compare the pharmacokinetic profile of a novel, once-daily, controlled-release formulation of hydromorphone (OROS hydromorphone) under fasting conditions with that immediately after a high-fat breakfast in healthy volunteers. The effect of the opioid antagonist naltrexone on fasting hydromorphone pharmacokinetics also was evaluated.

Methods: In an open-label, three-way, crossover study, 30 healthy volunteers were randomized to receive a single dose of 16 mg OROS hydromorphone under fasting conditions, 16 mg OROS hydromorphone under fed conditions, or 16 mg OROS hydromorphone under fasting conditions with a naltrexone 50-mg block. Plasma samples taken pre-dose and at regular intervals up to 48 hours post-dose were assayed for hydromorphone concentrations. Analysis of variance was performed on log-transformed data; for mean ratios of 0.8 to 1.2 (20%), differences were considered minimal. Bioequivalence was reached if 90% confidence intervals (CI) of treatment mean ratios were between 80% and 125%.

Results: The mean geometric ratios of the fed and fasting treatment groups for maximum plasma concentration (Cmax) and area under the concentration-time curve (AUC0-t; AUC0-infinity) were within 20%. Confidence intervals were within 80% to 125% for AUC0-t and AUC0-infinity but were slightly higher for Cmax (105.9% and 133.3%, respectively). With naltrexone block, the hydromorphone Cmax increased by 39% and the terminal half-life decreased by 4.5 hours. There was no significant change in Tmax, AUC0-t or AUC0-infinity.

Conclusion: Standard bioavailability measures show minimal effect of food on the bioavailability of hydromorphone from OROS hydromorphone. Naltrexone co-administration results in a slight increase in the rate of absorption but not the extent of absorption.

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