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Predicting the effect of naltrexone and acamprosate in alcohol-dependent patients using genetic indicators.

机译:使用遗传指标预测纳曲酮和阿坎酸在酒精依赖型患者中的作用。

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摘要

Acamprosate and naltrexone are effective medications in the treatment of alcoholism. However, effect sizes are modest. Pharmacogenomics may improve patient-treatment-matching and effect sizes. It is hypothesized that naltrexone exerts its effect through genetic characteristics associated with the dopaminergic/opioidergic positive reinforcement system, whereas acamprosate works through the glutamatergic/GABAergic negative reinforcement system. Alcohol-dependent subjects were randomly assigned to either acamprosate or naltrexone. Subjects participated in a cue-exposure experiment at the day before and at the last day of medication. Reductions in cue-induced craving and physiological cue reactivity were measured. Differential effects of naltrexone and acamprosate on these outcomes were tested for different polymorphisms of the opioid, dopamine, glutamate and GABA-receptors. Significant matching effects were found for polymorphisms at the DRD2, GABRA6 and GABRB2 gene. In addition, a trend was found for the OPRM1 polymorphism. This provides evidence for the matching potential of genotypes. It is expected that more effective treatments can be offered when genetic information is used in patient-treatment-matching.
机译:阿坎酸和纳曲酮是治疗酒精中毒的有效药物。但是,效果大小适中。药物基因组学可以改善患者治疗的匹配度和效果大小。假设纳曲酮通过与多巴胺能/阿片肌营养不良正强化系统相关的遗传特性发挥作用,而阿坎酸则通过谷氨酸/ GABA能负强化系统发挥作用。酒精依赖的受试者被随机分配到阿坎酸或纳曲酮中。受试者在用药的前一天和最后一天参加了提示暴露实验。测量了线索诱导的渴望和生理线索反应性的降低。对于阿片样物质,多巴胺,谷氨酸和GABA受体的不同多态性,测试了纳曲酮和阿坎酸对这些结果的差异作用。发现DRD2,GABRA6和GABRB2基因的多态性具有明显的匹配效应。另外,发现了OPRM1多态性的趋势。这为基因型的匹配潜力提供了证据。预期将遗传信息用于患者治疗匹配时,可以提供更有效的治疗。

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