Effect modification in therapeutic impact of nalmefene on alcohol dependence by ADH1B polymorphism: A secondary analysis of a Japanese randomized clinical trial.

IF 5.3 1区医学 Q1 PSYCHIATRY

Addiction Pub Date : 2025-08-08 DOI:10.1111/add.70160

Nozomu Hashimoto, Manabu Takaki, Yoshitsugu Kojima, Izuru Nakamura, Daisuke D Ikeda, Shinji Sakamoto, Yuko Okahisa, Soshi Takao, Keitaro Matsuo

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引用次数: 0

Abstract

Background and aims: The association between alcohol-metabolizing enzyme polymorphisms and treatment response to nalmefene for alcohol dependence has not been studied. We aimed to determine whether alcohol-metabolizing enzyme polymorphisms, specifically ADH1B rs1229984 and ALDH2 rs671, modify the treatment response to nalmefene for alcohol dependence.

Design: Secondary analysis of a Japanese randomized clinical trial, in which participants were randomly assigned (4:3:4) to placebo, 10 mg nalmefene or 20 mg nalmefene groups for 24 weeks, accompanied by a brief psychosocial intervention.

Setting: 80 addiction outpatient clinics across Japan.

Participants: A subset of 531 individuals (mean age 49.2 years, standard deviation 11.5; 69.9% male), including 196 in the placebo group and 335 in the nalmefene group, who agreed to DNA preservation and had available DNA data between February 2015 and July 2016.

Measurements: Genotyping was performed to determine ADH1B rs1229984 polymorphism (AA, AG, GG) and ALDH2 rs671 polymorphism (GG, GA, AA) in participants. Primary endpoint was change from baseline in monthly heavy drinking days (HDD, days/month) over the 24 treatment weeks. The key secondary endpoint was change from baseline in daily total alcohol consumption (TAC, g/day) over the 24 treatment weeks.

Findings: A mixed-effects model for repeated measures analyses showed a statistically significant gene-treatment interaction with ADH1B rs1229984 for TAC [10.71 (95% confidence interval = 4.03-17.39) g/day, P = 0.002], but not for HDD [1.65 (-0.38 to 3.67) days/month, P = 0.110]: as the G allele of rs1229984 increased, the efficacy regarding TAC decreased. In contrast, no statistically significant gene-treatment interaction was seen with ALDH2 rs671 for either TAC [4.46 (-7.88 to 16.80) g/day, P = 0.478] or HDD [-0.91 (-4.60 to 2.78) days/month, P = 0.630]. In the ADH1B rs1229984 variant, the number needed to treat for two category shifts in drinking risk level, as defined by the World Health Organization, was 3.7 for AA carriers, 6.6 for AG carriers and 18.5 for GG carriers.

Conclusions: The ADH1B rs1229984 polymorphism appears to moderate the response to nalmefene in Japanese patients with alcohol dependence. Specifically, nalmefene appears to show efficacy in individuals with the ADH1B rs1229984 AA genotype.

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通过ADH1B多态性改变纳美芬对酒精依赖的治疗效果：一项日本随机临床试验的二次分析

背景和目的：酒精代谢酶多态性与纳美芬治疗酒精依赖反应之间的关系尚未得到研究。我们的目的是确定酒精代谢酶多态性，特别是ADH1B rs1229984和ALDH2 rs671，是否会改变纳美芬对酒精依赖的治疗反应。设计：对一项日本随机临床试验进行二次分析，在该试验中，参与者被随机分配（4:3:4）到安慰剂、10mg纳美芬或20mg纳美芬组，为期24周，并伴随短暂的社会心理干预。设置：日本各地有80家成瘾门诊诊所。参与者：531人(平均年龄49.2岁，标准差11.5；69.9%的男性)，其中安慰剂组196人，纳美芬组335人，他们同意进行DNA保存，并在2015年2月至2016年7月期间拥有可用的DNA数据。测量方法：对受试者进行基因分型，确定ADH1B rs1229984多态性（AA、AG、GG）和ALDH2 rs671多态性（GG、GA、AA）。主要终点是在24个治疗周内每月重度饮酒天数（HDD，天/月）与基线的变化。关键的次要终点是在24个治疗周内每日总酒精摄入量（TAC， g/天）与基线的变化。结果：用于重复测量分析的混合效应模型显示，ADH1B rs1229984对TAC有统计学意义的基因治疗相互作用[10.71(95%可信区间= 4.03-17.39)g/天，P = 0.002]，但对HDD无统计学意义[1.65（-0.38至3.67）天/月，P = 0.110]：随着rs1229984 g等位基因的增加，TAC的疗效下降。相比之下，TAC[4.46(-7.88至16.80)g/天，P = 0.478]或HDD[-0.91（-4.60至2.78）天/月，P = 0.630]与ALDH2 rs671的基因治疗相互作用均无统计学意义。根据世界卫生组织的定义，在ADH1B rs1229984变体中，AA携带者需要治疗的人数为3.7人，AG携带者为6.6人，GG携带者为18.5人。结论：ADH1B rs1229984多态性似乎可以调节日本酒精依赖患者对纳美芬的反应。具体来说，纳美芬似乎对ADH1B rs1229984 AA基因型的个体有效。

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来源期刊

Addiction 医学-精神病学

CiteScore

10.80

自引率

6.70%

发文量

319

审稿时长

3 months

期刊介绍： Addiction publishes peer-reviewed research reports on pharmacological and behavioural addictions, bringing together research conducted within many different disciplines. Its goal is to serve international and interdisciplinary scientific and clinical communication, to strengthen links between science and policy, and to stimulate and enhance the quality of debate. We seek submissions that are not only technically competent but are also original and contain information or ideas of fresh interest to our international readership. We seek to serve low- and middle-income (LAMI) countries as well as more economically developed countries. Addiction’s scope spans human experimental, epidemiological, social science, historical, clinical and policy research relating to addiction, primarily but not exclusively in the areas of psychoactive substance use and/or gambling. In addition to original research, the journal features editorials, commentaries, reviews, letters, and book reviews.