昂丹司琼用于减少具有生物学易感性的酒精性患者饮酒量:一项随机对照试验。
Ondansetron for reduction of drinking among biologically predisposed alcoholic patients: A randomized controlled trial.
作者信息
Johnson B A, Roache J D, Javors M A, DiClemente C C, Cloninger C R, Prihoda T J, Bordnick P S, Ait-Daoud N, Hensler J
机构信息
Department of Psychiatry, University of Texas Health Science Center, 7703 Floyd Curl Dr, Mail Stop 7792, San Antonio, TX 78229-3900, USA.
出版信息
JAMA. 2000;284(8):963-71. doi: 10.1001/jama.284.8.963.
CONTEXT
Early-onset alcoholism differs from late-onset alcoholism by its association with greater serotonergic abnormality and antisocial behaviors. Thus, individuals with early-onset alcoholism may be responsive to treatment with a selective serotonergic agent.
OBJECTIVE
To test the hypothesis that drinking outcomes associated with early vs late-onset alcoholism are differentially improved by the selective 5-HT(3) (serotonin) antagonist ondansetron.
DESIGN
Double-blind, randomized, placebo-controlled clinical trial.
SETTINGS
University of Texas Health Science Center in Houston (April 1995-June 1998) and University of Texas Health Science Center in San Antonio (July 1998-December 1999).
PARTICIPANTS
A total of 321 patients with diagnosed alcoholism (mean age, 40.6 years; 70.5% male; 78.6% white) were enrolled, 271 of whom proceeded to randomization.
INTERVENTIONS
After 1 lead-in week of single-blind placebo, patients were randomly assigned to receive 11 weeks of treatment with ondansetron, 1 microg/kg (n = 67), 4 microg/kg (n = 77), or 16 microg/kg (n = 71) twice per day; or identical placebo (n = 56). All patients also participated in weekly standardized group cognitive behavioral therapy.
MAIN OUTCOME MEASURES
Self-reported alcohol consumption (drinks per day, drinks per drinking day, percentage of days abstinent, and total days abstinent per study week); and plasma carbohydrate deficient transferrin (CDT) level, an objective and sensitive marker of transient alcohol consumption.
RESULTS
Patients with early-onset alcoholism who received ondansetron (1, 4, and 16 microg/kg twice per day) compared with those who were administered placebo, had fewer drinks per day (1.89, 1.56, and 1.87 vs 3.30; P =.03, P =.01, and P =.02, respectively) and drinks per drinking day (4.75, 4.28, and 5.18 vs 6.90; P =.03, P =.004, and P =.03, respectively). Ondansetron, 4 microg/kg twice per day, was superior to placebo in increasing percentage of days abstinent (70.10 vs 50.20; P =.02) and total days abstinent per study week (6.74 vs 5.92; P =.03). Among patients with early-onset alcoholism, there was a significant difference in the mean log CDT ratio between those who received ondansetron (1 and 4 microg/kg twice per day) compared with those who received the placebo (-0.17 and -0.19 vs 0.12; P =.03 and P =.01, respectively).
CONCLUSION
Our results suggest that ondansetron (particularly the 4 microg/kg twice per day dosage) is an effective treatment for patients with early-onset alcoholism, presumably by ameliorating an underlying serotonergic abnormality. JAMA. 2000;284:963-971
背景
早发性酒精中毒与晚发性酒精中毒不同,它与更严重的血清素能异常及反社会行为相关。因此,早发性酒精中毒患者可能对选择性血清素能药物治疗有反应。
目的
检验选择性5-羟色胺(5-HT(3))拮抗剂昂丹司琼对早发性与晚发性酒精中毒相关饮酒结果有不同改善作用的假设。
设计
双盲、随机、安慰剂对照临床试验。
地点
休斯顿德克萨斯大学健康科学中心(1995年4月至1998年6月)和圣安东尼奥德克萨斯大学健康科学中心(1998年7月至1999年12月)。
参与者
共招募了321例确诊酒精中毒患者(平均年龄40.6岁;70.5%为男性;78.6%为白人),其中271例进入随机分组。
干预措施
在单盲安慰剂导入1周后,患者被随机分配接受11周的昂丹司琼治疗,剂量为1微克/千克(n = 67)、4微克/千克(n = 77)或16微克/千克(n = 71),每日2次;或接受相同的安慰剂(n = 56)。所有患者还参加每周的标准化团体认知行为疗法。
主要观察指标
自我报告的饮酒量(每天饮酒量、每次饮酒日饮酒量、戒酒天数百分比以及每研究周的总戒酒天数);以及血浆缺糖转铁蛋白(CDT)水平,这是短暂饮酒的客观且敏感标志物。
结果
与接受安慰剂的早发性酒精中毒患者相比,接受昂丹司琼(每日2次,剂量为1、4和16微克/千克)的患者每天饮酒量更少(分别为1.89、1.56和1.87杯对3.30杯;P = 0.03、P = 0.01和P = 0.02),每次饮酒日饮酒量也更少(分别为4.75、4.28和5.18杯对6.90杯;P = 0.03、P = 0.004和P = 0.03)。每日2次、剂量为4微克/千克的昂丹司琼在提高戒酒天数百分比(70.10对50.20;P = 0.02)和每研究周的总戒酒天数(6.74对5.92;P = 0.03)方面优于安慰剂。在早发性酒精中毒患者中,接受昂丹司琼(每日2次,剂量为1和4微克/千克)的患者与接受安慰剂的患者相比,平均对数CDT比值有显著差异(分别为-0.17和-0.19对0.12;P = 0.03和P = 0.01)。
结论
我们的结果表明,昂丹司琼(特别是每日2次、剂量为4微克/千克)是早发性酒精中毒患者的有效治疗方法,可能是通过改善潜在的血清素能异常起作用。《美国医学会杂志》。2000年;284:963 - 971
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