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α-1 肾上腺素能拮抗剂多沙唑嗪治疗可卡因依赖:一项初步研究。

The alpha-1 adrenergic antagonist doxazosin for treatment of cocaine dependence: A pilot study.

机构信息

The Menninger Department of Psychiatry and Behavioral Sciences, Baylor College of Medicine, and Michael E. DeBakey V.A. Medical Center, Houston, TX, United States.

出版信息

Drug Alcohol Depend. 2013 Jul 1;131(1-2):66-70. doi: 10.1016/j.drugalcdep.2012.11.021. Epub 2013 Jan 8.

Abstract

BACKGROUND

Medications decreasing central noradrenergic activity have been associated with attenuation of cocaine effects.

AIMS

This pilot study examined the efficacy of doxazosin versus placebo for reducing cocaine use in treatment-seeking cocaine dependent persons.

METHODS

We screened 108 cocaine dependent subjects and assigned 35 participants to receive either doxazosin (8mg/day) or placebo for 13 weeks. Participants were titrated on the study medication according to two different schedules. During the initial phase of the study, patients were titrated onto the study medication over an 8-week period (DOX-slow). After reviewing data from our human laboratory study, a second phase was initiated, wherein titration was accelerated to a 4-week period (DOX-fast). All participants received weekly cognitive behavioral therapy. Urine toxicology was performed thrice weekly.

RESULTS

Baseline subject characteristics were comparable. Thirty subjects entered the study: 8 subjects in DOX-slow, 9 subjects in DOX-fast, and 13 subjects in placebo. Total number of cocaine-negative urines was significantly increased in the DOX-fast group; and percentage of total cocaine-negative urines by group were 10% for DOX-slow group, 35% for DOX-fast group, and 14% for placebo (χ(2)=36.3, df=2, p<0.0001). The percentage of participants achieving two or more consecutive weeks of abstinence by group was 0% for DOX-slow group, 44% for DOX-fast group, and 7% for placebo (χ(2)=7.35, df=2, p<0.023).

CONCLUSIONS

This pilot study suggests the potential efficacy of doxazosin when rapidly titrated in reducing cocaine use.

摘要

背景

降低中枢去甲肾上腺素活性的药物已被证明可减弱可卡因的作用。

目的

本研究旨在评估多沙唑嗪与安慰剂治疗可卡因依赖者减少可卡因使用的疗效。

方法

我们对 108 例可卡因依赖者进行了筛查,并将 35 例参与者随机分为多沙唑嗪(8mg/天)或安慰剂组,治疗 13 周。根据两种不同的方案对参与者进行研究药物滴定。在研究的初始阶段,患者在 8 周的时间内滴定至研究药物(DOX-slow)。在回顾了我们的人体实验室研究数据后,启动了第二阶段,其中滴定加速至 4 周(DOX-fast)。所有参与者均接受每周认知行为疗法。每周进行三次尿液毒理学检查。

结果

基线受试者特征具有可比性。30 名受试者进入研究:8 名在 DOX-slow 组,9 名在 DOX-fast 组,13 名在安慰剂组。DOX-fast 组的可卡因阴性尿液总数明显增加;按组计算的可卡因阴性尿液百分比分别为 DOX-slow 组 10%,DOX-fast 组 35%,安慰剂组 14%(χ²=36.3,df=2,p<0.0001)。按组计算,连续两周或以上戒断的参与者百分比分别为 DOX-slow 组 0%,DOX-fast 组 44%,安慰剂组 7%(χ²=7.35,df=2,p<0.023)。

结论

本研究初步表明,快速滴定多沙唑嗪可能具有减少可卡因使用的效果。

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