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评价芬太尼口腔黏膜溶解片在健康志愿者中单剂量和多剂量的药代动力学。

Evaluation of the single- and multiple-dose pharmacokinetics of fentanyl buccal soluble film in normal healthy volunteers.

机构信息

BioDelivery Sciences International, 801 Corporate Center Drive, Suite 210, Raleigh, NC 27607, USA.

出版信息

J Clin Pharmacol. 2010 Jul;50(7):785-91. doi: 10.1177/0091270010361354. Epub 2010 Feb 11.

Abstract

Fentanyl buccal soluble film (FBSF) is a rapidly absorbed transmucosal formulation of fentanyl for the management of breakthrough pain in opioid-tolerant patients with cancer. This open-label, 3-period, sequential dose study evaluated the dose-to-dose reproducibility of the pharmacokinetics of fentanyl following the administration of 600- or 1800-microg doses of FBSF in 12 naltrexone-blocked, healthy adult volunteers. Subjects received 3 study treatments: single doses of 600 microg of FBSF on day 1 and day 4 and three 600-microg doses administered at 1-hour intervals on day 7. Plasma fentanyl concentrations were measured over a 48-hour period after each single dose of FBSF and 72 hours after the 3-dose regimen. Peak plasma concentrations (mean C(max) = 1.08 and 1.01 ng/mL) and overall exposure (mean AUC(0-12) = 6.3 and 6.2 h.ng/mL; mean AUC(inf) = 9.14 and 9.60 h.ng/mL) were nearly identical after the 2 single doses (P >or= .1, all comparisons). C(max) and overall fentanyl exposure (AUC(inf)) increased approximately 3-fold with the 3-dose regimen compared with the single-dose periods. Fentanyl plasma concentrations following single doses of FBSF were reproducible, and 3 doses administered 1 hour apart produced a tripling in exposure and maximal concentration compared with a single dose.

摘要

芬太尼颊膜(FBSF)是一种快速吸收的经粘膜芬太尼配方,用于治疗阿片类药物耐受的癌症患者爆发性疼痛。这项开放性、3 期、序贯剂量研究评估了 600 或 1800 微克 FBSF 剂量后芬太尼药代动力学的剂量重现性,在 12 名纳曲酮阻断的健康成年志愿者中进行。受试者接受了 3 种研究治疗:第 1 天和第 4 天单次给予 600 微克 FBSF,第 7 天每 1 小时给予 3 次 600 微克剂量。在每次单剂量 FBSF 后 48 小时和 3 剂量方案后 72 小时测量芬太尼的血浆浓度。单剂量后(平均 C(max)=1.08 和 1.01ng/ml)和总体暴露(平均 AUC(0-12)=6.3 和 6.2 h.ng/ml;平均 AUC(inf)=9.14 和 9.60 h.ng/ml)几乎相同(P>.1,所有比较)。与单剂量期相比,3 剂量方案后 C(max)和总体芬太尼暴露(AUC(inf))增加了约 3 倍。FBSF 单剂量后的芬太尼血浆浓度具有重现性,3 剂间隔 1 小时给予与单剂量相比,暴露量和最大浓度增加了 3 倍。

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