在接受阿片类药物使用障碍治疗的门诊患者中,缓释纳曲酮是否优于丁丙诺啡-纳洛酮减少饮酒?CTN X:BOT 试验的二次分析。
Is extended release naltrexone superior to buprenorphine-naloxone to reduce drinking among outpatients receiving treatment for opioid use disorder? A secondary analysis of the CTN X:BOT trial.
机构信息
Division of Alcohol & Drug Addiction, Department of Psychiatry & Behavioral Sciences, University of Texas Health Science Center, San Antonio, Texas, USA.
Biostatistics Department, Mailman School of Public Health, Columbia University, New York City, New York, USA.
出版信息
Alcohol Clin Exp Res. 2021 Dec;45(12):2569-2578. doi: 10.1111/acer.14729. Epub 2021 Nov 23.
BACKGROUND
The comparative effectiveness of extended-release naltrexone versus buprenorphine-naloxone for opioid relapse prevention (X:BOT) trial showed that following induction, treatment with the sublingual agonist (buprenorphine-naloxone, BUP-NX) or injected antagonist (extended release naltrexone, XR-NTX) produced similar reductions in opioid relapse in injection users with opioid use disorder (OUD). Because XR-NTX reduces drinking in alcohol use disorder (AUD), we conducted a secondary analysis of the X:BOT sample of patients successfully inducted onto treatment to determine whether XR-NTX (n = 204) was superior to BUP-NX (n = 270) in reducing drinking or heavy drinking in patients with OUD.
METHODS
Standard drink units consumed were measured using the Timeline Follow-back method. Mixed-models regression was used to examine the monthly frequency of any drinking and heavy drinking over 6 months of treatment. We used a proportional hazard survival analysis to examine the time to first drink.
RESULTS
Both treatment groups reduced drinking from baseline to posttreatment (small to medium effect), but no differences between groups were detected. However, only 29% (n = 136) of the sample had AUD and 19% (n = 26/136) of those were abstinent before treatment. Analysis of a subsample enriched for possible drinking included 136 individuals with an AUD diagnosis plus 43 who did not have AUD, but reported at least one day of heavy drinking prior to the study. However, this subsample reported only 32% of days of any drinking with a median of only 13% of days designated as "heavy." Within this subsample, at baseline, the BUP-NX group reported more mean drinks per drinking day than the XR-NTX group (p = 0.03); however, there were no other significant group differences on drinking observed before, during, or at the end of treatment.
CONCLUSIONS
There was an overall reduction in drinking during treatment of OUD using both agonist and antagonist medications, so that the hypothesis that XR-NTX would be superior to BUP-NX was not supported. The study is limited by low levels of comorbid AUD or heavy drinking observed in X:BOT trial participants seeking treatment for OUD.
背景
扩展释放纳曲酮与丁丙诺啡-纳洛酮相比,用于阿片类药物戒断预防的疗效(X:BOT)试验表明,在诱导后,使用舌下激动剂(丁丙诺啡-纳洛酮,BUP-NX)或注射拮抗剂(扩展释放纳曲酮,XR-NTX)治疗,在有阿片类药物使用障碍(OUD)的注射使用者中,阿片类药物戒断的减少情况相似。由于 XR-NTX 可减少酒精使用障碍(AUD)中的饮酒,因此我们对 X:BOT 成功接受治疗的患者样本进行了二次分析,以确定 XR-NTX(n=204)是否优于 BUP-NX(n=270)在减少 OUD 患者的饮酒或重度饮酒方面。
方法
使用时间线随访法测量标准饮酒单位的消耗量。使用混合模型回归分析在 6 个月的治疗期间检查任何饮酒和重度饮酒的月频率。我们使用比例风险生存分析来检查首次饮酒的时间。
结果
两组治疗均从基线减少到治疗后(小到中等效果),但组间无差异。然而,只有 29%(n=136)的样本患有 AUD,并且 19%(n=26/136)在治疗前已经戒酒。对可能饮酒的样本亚组进行分析,包括 136 名有 AUD 诊断的个体和 43 名没有 AUD 但在研究前报告至少一天重度饮酒的个体。然而,该亚组仅报告了 32%的任何饮酒天数,中位数仅为 13%的天数被指定为“重度”。在该亚组中,基线时,BUP-NX 组报告的每日平均饮酒量多于 XR-NTX 组(p=0.03);然而,在治疗前、治疗中和治疗结束时,都没有观察到其他显著的组间饮酒差异。
结论
在使用激动剂和拮抗剂药物治疗 OUD 期间,饮酒总体减少,因此 XR-NTX 优于 BUP-NX 的假设不成立。该研究受到 X:BOT 试验参与者寻求 OUD 治疗时观察到的合并 AUD 或重度饮酒水平较低的限制。
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