Predicting Alcoholics' Treatment Responses to an SSRI

预测酗酒者对 SSRI 的治疗反应

• 批准号: 6727030
• 负责人: ROBERT M ANTHENELLI
• 金额: $ 40.93万
• 依托单位: UNIVERSITY OF CINCINNATI
• 依托单位国家: 美国
• 财政年份: 2004
• 资助国家: 美国
• 起止时间: 2004-05-01 至 2009-04-30
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/6727030
• 关键词: alcoholism /alcohol abuse; alcoholism /alcohol abuse therapy; behavior therapy; behavioral /social science research tag; citalopram; clinical research; gel electrophoresis; gene expression; genotype; human subject; motivation; pharmacogenetics; polymerase chain reaction; relapse /recurrence; serotonin inhibitor; serotonin transporter; therapy compliance

DESCRIPTION (provided by applicant): Relapse to alcoholism remains a vexing clinical and national health problem. Efforts to match alcohol dependent patients to specific treatments based on their clinical characteristics have produced mixed results. Pharmacogenetics (the study of genetic influences on therapeutic response to drugs) offers a powerful new tool to match specific elements of an individual patient's complex genetic blueprint with targeted pharmacotherapies to which that individual may optimally respond. The purpose of this proposed research is to apply pharmacogenetic techniques to predict which alcohol dependent patients will respond favorably to a trial of a selective serotonin re-uptake inhibitor (SSRI) for the prevention of alcoholism relapse. Our central hypothesis is that genetic differences affecting serotonin transporter function will influence an alcohol dependent individual's treatment response to the SSRI, citalopram. To test this hypothesis, we will perform a 14-week, randomized, double blind, parallel group comparison of citalopram and placebo in treatment seeking outpatients who meet DSM-IV criteria for alcohol dependence. All subjects will receive a single Motivational Interview and 9 brief sessions of a manual-guided Compliance Enhancement Therapy designed to promote treatment adherence and enhance motivation to quit or cut down on drinking. Post-treatment follow-up assessments will be conducted at 4, 12 and 24 weeks. Subjects' DNA will be genotyped to determine allelic variants in the promoter region of the serotonin transporter gene that have been found to markedly affect serotonin reuptake and influence treatment responsiveness to SSRIs. We predict that individuals who carry two long variant alleles (1/1 homozygotes) of this polymorphism will exhibit a significant reduction in drinking days in response to citalopram compared with patients homozygous for the short variant allele (s/s homozygotes). To our knowledge, this will be the first study conducted in alcohol dependent patients to test whether pharmacogenetic differences in the function of the serotonin transporter (the site of action of these medications) influence the treatment response to a SSRI in nondepressed women and men. The study is designed to maximize the likelihood of finding treatment efficacy for citalopram over placebo by excluding subjects with severe alcohol dependence and marked impulsive traits in which SSRIs have not been found to be effective, controlling the exposure to the concomitant psychosocial intervention to minimize a psychotherapy ceiling effect, and by controlling the potential moderating effects of sex and cigarette smoking. The successful completion of this single center study may lead to future multicenter trials in more heterogeneous populations, and to studies using serotonin receptor subtype-specific medications.

描述（由申请人提供）：酗酒复发仍然是一个令人烦恼的临床和国家健康问题。根据酒精依赖患者的临床特征将其与特定治疗相匹配的努力产生了不同的结果。药物遗传学（研究遗传对药物治疗反应的影响）提供了一种强大的新工具，可以将个体患者复杂遗传蓝图的特定元素与该个体可能产生最佳反应的靶向药物疗法相匹配。这项拟议研究的目的是应用药物遗传学技术来预测哪些酒精依赖患者会对用于预防酒精中毒复发的选择性血清素再摄取抑制剂（SSRI）试验产生良好反应。我们的中心假设是，影响血清素转运蛋白功能的遗传差异将影响酒精依赖个体对 SSRI 西酞普兰的治疗反应。为了检验这一假设，我们将对西酞普兰和安慰剂进行为期 14 周的随机、双盲、平行组比较，以寻找符合 DSM-IV 酒精依赖标准的门诊患者。所有受试者都将接受一次动机访谈和 9 次简短的手动指导的依从性增强治疗，旨在促进治疗依从性并增强戒烟或减少饮酒的动机。治疗后随访评估将在第 4、12 和 24 周进行。将对受试者的 DNA 进行基因分型，以确定血清素转运蛋白基因启动子区域的等位基因变异，这些变异已被发现显着影响血清素再摄取并影响对 SSRI 的治疗反应。我们预测，与短变异等位基因纯合子（s/s 纯合子）的患者相比，携带该多态性的两个长变异等位基因（1/1 纯合子）的个体将表现出响应西酞普兰的饮酒天数显着减少。据我们所知，这将是第一项在酒精依赖患者中进行的研究，旨在测试血清素转运蛋白（这些药物的作用位点）功能的药物遗传学差异是否影响非抑郁症女性和男性对 SSRI 的治疗反应。该研究旨在通过排除具有严重酒精依赖和明显冲动特征（SSRI 尚未被发现有效）的受试者，控制伴随的心理社会干预的暴露，以最大程度地减少心理治疗，从而最大限度地提高西酞普兰治疗效果优于安慰剂的可能性。天花板效应，并通过控制性和吸烟的潜在调节作用。这项单中心研究的成功完成可能会导致未来在更多异质人群中进行多中心试验，以及使用血清素受体亚型特异性药物的研究。