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丁丙诺啡长效注射剂(CAM2038)与氢吗啡酮阻滞对阿片类物质使用障碍患者的影响:一项随机临床试验

Effect of Buprenorphine Weekly Depot (CAM2038) and Hydromorphone Blockade in Individuals With Opioid Use Disorder: A Randomized Clinical Trial.

作者信息

Walsh Sharon L, Comer Sandra D, Lofwall Michelle R, Vince Bradley, Levy-Cooperman Naama, Kelsh Debra, Coe Marion A, Jones Jermaine D, Nuzzo Paul A, Tiberg Fredrik, Sheldon Behshad, Kim Sonnie

机构信息

Center on Drug and Alcohol Research, University of Kentucky, Lexington.

Department of Psychiatry, Columbia University, New York, New York.

出版信息

JAMA Psychiatry. 2017 Sep 1;74(9):894-902. doi: 10.1001/jamapsychiatry.2017.1874.

DOI:10.1001/jamapsychiatry.2017.1874
PMID:28655025
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5710238/
Abstract

IMPORTANCE

Buprenorphine is an efficacious, widely used treatment for opioid use disorder (OUD). Daily oral transmucosal formulations can be associated with misuse, diversion, and nonadherence; these limitations may be obviated by a sustained release formulation.

OBJECTIVE

To evaluate the ability of a novel, weekly, subcutaneous buprenorphine depot formulation, CAM2038, to block euphorigenic opioid effects and suppress opioid withdrawal in non-treatment-seeking individuals with OUD.

DESIGN, SETTING, AND PARTICIPANTS: This multisite, double-blind, randomized within-patient study was conducted at 3 controlled inpatient research facilities. It involved 47 adults with DSM-V moderate-to-severe OUD. The study was conducted from October 12, 2015 (first patient enrolled), to April 21, 2016 (last patient visit).

INTERVENTIONS

A total of five 3-day test sessions evaluated the response to hydromorphone (0, 6, and 18 mg intramuscular in random order; 1 dose/session/day). After the first 3-day session (ie, qualification phase), participants were randomized to either CAM2038 weekly at 24 mg (n = 22) or 32 mg (n = 25); the assigned CAM2038 dose was given twice, 1 week apart (day 0 and 7). Four sets of sessions were conducted after randomization (days 1-3, 4-6, 8-10, and 11-13).

MAIN OUTCOMES AND MEASURES

The primary end point was maximum rating on the visual analog scale for drug liking. Secondary end points included other visual analog scale (eg, high and desire to use), opioid withdrawal scales, and physiological and pharmacokinetic outcomes.

RESULTS

A total of 46 of 47 randomized participants (mean [SD] age, 35.5 [9] years; 76% male [n = 35]) completed the study. Both weekly CAM2038 doses produced immediate and sustained blockade of hydromorphone effects (liking maximum effect, CAM2038, 24 mg: effect size, 0.813; P < .001, and CAM2038, 32 mg: effect size, 0.753; P < .001) and suppression of withdrawal (Clinical Opiate Withdrawal Scale, CAM2038, 24 mg: effect size, 0.617; P < .001, and CAM2038, 32 mg: effect size, 0.751; P < .001). CAM2038 produces a rapid initial rise of buprenorphine in plasma with maximum concentration around 24 hours, with an apparent half-life of 4 to 5 days and approximately 50% accumulation of trough concentration from first to second dose (trough concentration = 0.822 and 1.23 ng/mL for weeks 1 and 2, respectively, with 24 mg; trough concentration = 0.993 and 1.47 ng/mL for weeks 1 and 2, respectively, with 32 mg).

CONCLUSIONS AND RELEVANCE

CAM2038 weekly, 24 and 32 mg, was safely tolerated and produced immediate and sustained opioid blockade and withdrawal suppression. The results support the use of this depot formulation for treatment initiation and stabilization of patients with OUD, with the further benefit of obviating the risk for misuse and diversion of daily buprenorphine while retaining its therapeutic benefits.

TRIAL REGISTRATION

Clinicaltrials.gov Identifier: NCT02611752.

摘要

重要性

丁丙诺啡是一种有效且广泛用于治疗阿片类物质使用障碍(OUD)的药物。每日口服黏膜给药制剂可能会出现滥用、转移和不依从的情况;而缓释制剂或许可以消除这些局限性。

目的

评估一种新型的每周一次皮下注射丁丙诺啡长效注射剂CAM2038,在未寻求治疗的OUD个体中阻断阿片类药物致欣快效应和抑制阿片类物质戒断反应的能力。

设计、地点和参与者:这项多中心、双盲、患者内随机研究在3个受控住院研究机构进行。研究纳入了47名患有DSM-Ⅴ中重度OUD的成年人。研究于2015年10月12日(第一名患者入组)至2016年4月21日(最后一名患者访视)进行。

干预措施

总共进行了5次为期3天的测试疗程,评估对氢吗啡酮(0、6和18mg,随机顺序肌肉注射;每次疗程每日1剂)的反应。在第一个为期3天的疗程(即资格阶段)后,参与者被随机分为每周接受24mg(n = 22)或32mg(n = 25)的CAM2038;指定的CAM2038剂量分两次给药,间隔1周(第0天和第7天)。随机分组后进行了4组疗程(第1 - 3天、第4 - 6天、第8 - 10天和第11 - 13天)。

主要结局和测量指标

主要终点是药物喜好视觉模拟量表的最高评分。次要终点包括其他视觉模拟量表(如兴奋和使用欲望)、阿片类物质戒断量表以及生理和药代动力学结果。

结果

47名随机分组的参与者中有46名(平均[标准差]年龄,35.5[9]岁;76%为男性[n = 35])完成了研究。两种每周剂量的CAM2038均能立即且持续地阻断氢吗啡酮的效应(喜好最大效应,24mg的CAM2038:效应量,0.813;P <.001,32mg的CAM2038:效应量,0.753;P <.001)并抑制戒断反应(临床阿片类物质戒断量表,24mg的CAM2038:效应量,0.617;P <.001,32mg的CAM2038:效应量,0.751;P <.001)。CAM2038使丁丙诺啡在血浆中迅速初始上升,最大浓度出现在约24小时左右,表观半衰期为4至5天,从第一剂到第二剂谷浓度约有50%的蓄积(24mg时,第1周和第2周的谷浓度分别为0.822和1.23ng/mL;32mg时,第1周和第2周的谷浓度分别为0.993和1.47ng/mL)。

结论与相关性

每周24mg和32mg的CAM2038耐受性良好,能立即且持续地阻断阿片类物质并抑制戒断反应。结果支持使用这种长效注射剂用于OUD患者的起始治疗和病情稳定,其进一步的益处是消除了每日丁丙诺啡滥用和转移的风险,同时保留了其治疗效果。

试验注册

Clinicaltrials.gov标识符:NCT02611752。

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