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芬太尼口腔崩解片在健康志愿者中的单剂量及稳态药代动力学

Single-dose and steady-state pharmacokinetics of fentanyl buccal tablet in healthy volunteers.

作者信息

Darwish Mona, Kirby Mary, Robertson Philmore, Hellriegel Edward, Jiang John G

机构信息

Clinical Pharmacology, Cephalon, Inc., Frazer, Pennsylvania, USA.

出版信息

J Clin Pharmacol. 2007 Jan;47(1):56-63. doi: 10.1177/0091270006294129.

Abstract

This study evaluated the single-dose and steady-state pharmacokinetics of fentanyl buccal tablet 400 microg in healthy adult volunteers. After receiving naltrexone 50 mg to block opioid receptor-mediated effects of fentanyl, subjects received fentanyl buccal tablet 400 microg on day 1, then every 6 hours from day 4 to day 9 (21 doses). Naltrexone 50 mg was administered every 12 hours throughout the study. Plasma fentanyl concentrations were determined for 72 hours after administration of fentanyl buccal tablet 400 microg on day 1 and the last dose of fentanyl buccal tablet 400 microg on day 9. Following single- and multiple-dose administration of fentanyl buccal tablet, the median time to maximum concentration (tmax) was 52.2 and 49.8 minutes, respectively. Peak plasma concentration of fentanyl (Cmax) was 0.88 ng/mL for the single-dose regimen and 1.77 ng/mL for the multiple-dose regimen. Steady state was reached within 5 days, consistent with the observed median half-life of approximately 22 hours following multiple doses. Observed accumulation of fentanyl after multiple doses of fentanyl buccal tablet was slightly greater than would be expected based on the single-dose data. This was attributed to the redistribution of fentanyl from a deep tissue compartment into the plasma. This study indicates that fentanyl buccal tablet has predictable pharmacokinetics following multiple-dose administration.

摘要

本研究评估了400微克芬太尼口腔含片在健康成年志愿者中的单剂量和稳态药代动力学。在接受50毫克纳曲酮以阻断芬太尼的阿片受体介导作用后,受试者在第1天接受400微克芬太尼口腔含片,然后从第4天到第9天每6小时给药一次(共21剂)。在整个研究过程中,每12小时给予50毫克纳曲酮。在第1天给予400微克芬太尼口腔含片后以及第9天给予最后一剂400微克芬太尼口腔含片后72小时测定血浆芬太尼浓度。单剂量和多剂量给予芬太尼口腔含片后,达到最大浓度的中位时间(tmax)分别为52.2分钟和49.8分钟。单剂量给药方案的芬太尼血浆峰浓度(Cmax)为0.88纳克/毫升,多剂量给药方案为1.77纳克/毫升。在5天内达到稳态,这与多次给药后观察到的中位半衰期约22小时一致。多次给予芬太尼口腔含片后观察到的芬太尼蓄积略大于基于单剂量数据的预期。这归因于芬太尼从深部组织隔室重新分布到血浆中。本研究表明,多次给药后芬太尼口腔含片具有可预测的药代动力学。

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