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DRD4 外显子 III VNTR、安非他酮与前瞻性戒断的关联。

The DRD4 exon III VNTR, bupropion, and associations with prospective abstinence.

机构信息

Center for Health Sciences, SRI International, Menlo Park, CA 94025, USA.

出版信息

Nicotine Tob Res. 2013 Jul;15(7):1190-200. doi: 10.1093/ntr/nts245. Epub 2012 Dec 3.

Abstract

INTRODUCTION

DRD4 Exon III Variable Number of Tandem Repeat (VNTR) variation was found to interact with bupropion to influence prospective smoking abstinence, in a recently published longitudinal analyses of N = 331 individuals from a randomized double-blind placebo-controlled trial of bupropion and intensive cognitive-behavioral mood management therapy.

METHODS

We used univariate, multivariate, and longitudinal logistic regression to evaluate gene, treatment, time, and interaction effects on point prevalence and continuous abstinence at end of treatment, 6 months, and 12 months, respectively, in N = 416 European ancestry participants in a double-blind pharmacogenetic efficacy trial randomizing participants to active or placebo bupropion. Participants received 10 weeks of pharmacotherapy and 7 sessions of behavioral therapy, with a target quit date 2 weeks after initiating both therapies. VNTR genotypes were coded with the long allele dominant resulting in 4 analysis categories. Covariates included demographics, dependence measures, depressive symptoms, and genetic ancestry. We also performed genotype-stratified secondary analyses.

RESULTS

We observed significant effects of time in longitudinal analyses of both abstinence outcomes, of treatment in individuals with VNTR long allele genotypes for both abstinence outcomes, and of covariates in some analyses. We observed non-significantly larger differences in active versus placebo effect sizes in individuals with VNTR long allele genotypes than in individuals without the VNTR long allele, in the directions previously reported.

CONCLUSIONS

VNTR by treatment interaction differences between these and previous analyses may be attributable to insufficient size of the replication sample. Analyses of multiple randomized clinical trials will enable identification and validation of factors mediating treatment response.

摘要

介绍

DRD4 外显子 III 可变数串联重复(VNTR)变异与安非他酮相互作用,影响前瞻性戒烟,这是最近发表的一项对来自安非他酮和强化认知行为情绪管理治疗随机双盲安慰剂对照试验的 331 名个体的纵向分析结果。

方法

我们使用单变量、多变量和纵向逻辑回归分别评估基因、治疗、时间和相互作用对终点时、治疗结束后 6 个月和 12 个月时的点患病率和连续戒烟的影响,在双盲药物遗传学疗效试验的 416 名欧洲血统参与者中,参与者被随机分配接受活性或安慰剂安非他酮。参与者接受 10 周的药物治疗和 7 次行为治疗,目标戒烟日期为启动两种治疗后 2 周。VNTR 基因型用长等位基因显性编码,产生 4 种分析类别。协变量包括人口统计学、依赖程度、抑郁症状和遗传祖先。我们还进行了基因型分层的次要分析。

结果

我们在两个戒烟结果的纵向分析中观察到时间的显著影响,在 VNTR 长等位基因基因型个体的治疗中观察到两个戒烟结果的显著影响,以及在一些分析中观察到协变量的显著影响。我们观察到在具有 VNTR 长等位基因基因型的个体中,与安慰剂相比,活性药物的效应大小在具有 VNTR 长等位基因的个体中比在没有 VNTR 长等位基因的个体中差异更大,但差异无统计学意义,方向与之前报道的一致。

结论

这些与之前分析的 VNTR 与治疗的相互作用差异可能归因于复制样本的大小不足。对多个随机临床试验的分析将能够识别和验证介导治疗反应的因素。

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