Webster Lynn R, Rolleri Robert L, Pixton Glenn C, Sommerville Kenneth W
Lifetree Clinical Research, Salt Lake City, UT, USA.
Salix Pharmaceuticals, Inc., Raleigh, NC, USA ; Pfizer Inc, Cary, NC, USA.
Subst Abuse Rehabil. 2012 Aug 17;3:101-13. doi: 10.2147/SAR.S33080. eCollection 2012.
Abuse-deterrent formulations attempt to address public health and societal concerns regarding opioid abuse. Oxycodone HCl-niacin tablets combine oxycodone HCl with niacin and functional inactive excipients to create potential barriers to oral, intranasal, and intravenous abuse. This study compared the relative abuse potential of oral immediate-release oxycodone HCl-niacin with that of oral immediate-release oxycodone HCl and placebo in nondependent, recreational opioid users.
Forty-nine participants received oxycodone HCl-niacin 40/240 mg and 80/480 mg, oxycodone 40 mg and 80 mg, and placebo in a randomized, double-blind, placebo-controlled and active-controlled, five-way crossover study. Primary endpoints based on a bipolar 100 mm visual analog scale for drug liking were area under effect curve (AUE0-1h, AUE0-2h, AUE0-3h), peak disliking, and effect at 0.5 hours post-dose (E0.5h). Other endpoints included take drug again assessment, overall drug liking, and pupillometry.
There were statistically significant differences between oxycodone HCl-niacin and oxycodone HCl doses for all primary endpoints (P < 0.0001, all comparisons), suggesting reduced abuse potential with oxycodone HCl-niacin. Take drug again and overall drug liking showed greater liking of oxycodone alone. Oxycodone HCl-niacin 80/480 mg had consistently lower liking assessments than oxycodone HCl-niacin 40/240 mg, suggesting a dose-response to the aversive effects of niacin. Opioid-related adverse events were similar for equivalent oxycodone doses. The treatment-emergent adverse events most specifically associated with oxycodone HCl-niacin (ie, skin-burning sensation, warmth, and flushing) were consistent with the expected vasocutaneous effects of niacin. No serious adverse events were reported.
Oxycodone HCl-niacin tablets may, in a dose-dependent manner, decrease the potential for oral abuse of oxycodone without unexpected adverse events or clinically signifi-cant differences in safety parameters compared with oxycodone alone. Although statistically powered, the small size of the study sample and the characteristics of its participants may not be generalizable to the population that abuses prescription opioid medications.
滥用威慑制剂旨在解决公众健康和社会对阿片类药物滥用的担忧。盐酸羟考酮 - 烟酸片将盐酸羟考酮与烟酸及功能性惰性辅料结合,对口服、鼻内和静脉注射滥用形成潜在屏障。本研究比较了口服速释盐酸羟考酮 - 烟酸与口服速释盐酸羟考酮及安慰剂在非依赖的娱乐性阿片类药物使用者中的相对滥用潜力。
49名参与者在一项随机、双盲、安慰剂对照和活性对照的五交叉研究中接受了40/240毫克和80/480毫克的盐酸羟考酮 - 烟酸、40毫克和80毫克的羟考酮以及安慰剂。基于100毫米双极视觉模拟量表对药物喜好程度的主要终点为效应曲线下面积(AUE0 - 1h、AUE0 - 2h、AUE0 - 3h)、最大厌恶程度以及给药后0.5小时的效应(E0.5h)。其他终点包括再次服药评估、总体药物喜好程度以及瞳孔测量。
所有主要终点的盐酸羟考酮 - 烟酸与盐酸羟考酮剂量之间存在统计学显著差异(所有比较,P < 0.0001),表明盐酸羟考酮 - 烟酸的滥用潜力降低。再次服药和总体药物喜好程度显示单独使用羟考酮更受青睐。80/480毫克的盐酸羟考酮 - 烟酸的喜好评估始终低于40/240毫克的盐酸羟考酮 - 烟酸,表明对烟酸厌恶效应存在剂量反应。等效羟考酮剂量的阿片类药物相关不良事件相似。与盐酸羟考酮 - 烟酸最具体相关的治疗中出现的不良事件(即皮肤烧灼感、温热感和潮红)与烟酸预期的血管皮肤效应一致。未报告严重不良事件。
盐酸羟考酮 - 烟酸片可能以剂量依赖方式降低羟考酮的口服滥用潜力,与单独使用羟考酮相比,无意外不良事件或安全参数方面的临床显著差异。尽管该研究样本量小且参与者特征可能无法推广至滥用处方阿片类药物的人群,但研究仍具有统计学效力。
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