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Pharmacogenetic approaches in the treatment of alcohol use disorders: addressing clinical utility and implementation thresholds

机译:治疗酒精使用障碍的药物遗传学方法:解决临床效用和实施门槛

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摘要

Despite advances in characterizing genetic influences on addiction liability and treatment response, clinical applications of these efforts have been slow to evolve. Although challenges to clinical translation remain, stakeholders already face decisions about evidentiary thresholds for the uptake of pharmacogenetic tests in practice. There is optimism about potential pharmacogenetic applications for the treatment of alcohol use disorders, with particular interest in the OPRM1 A118G polymorphism as a moderator of naltrexone response. Findings from human and animal studies suggest preliminary evidence for the clinical validity of this association; on this basis, arguments for clinical implementation can be made in accordance with existing frameworks for the uptake of genomic applications. However, generating evidence-based guidelines requires evaluating the clinical utility of pharmacogenetic tests. This goal will remain challenging, largely due to minimal data to inform clinical utility estimates. The pace of genomic discovery highlights the need for clinical utility and implementation research to inform future translation efforts. Near-term implementation of promising pharmacogenetic tests can help expedite this goal, generating an evidence base to enable efficient translation as additional gene-drug associations are discovered.
机译:尽管在表征对成瘾倾向和治疗反应的遗传影响方面取得了进展,但是这些努力的临床应用进展缓慢。尽管对临床翻译的挑战仍然存在,但是利益相关者已经面临着有关在实践中采用药物遗传学测试的证据阈值的决定。人们对潜在的药物遗传学治疗酒精使用障碍的疾病抱有乐观的态度,尤其对OPRM1 A118G多态性作为纳曲酮反应的调节剂特别感兴趣。人类和动物研究的发现为这种关联的临床有效性提供了初步证据。在此基础上,可以根据现有的基因组应用框架对临床实施进行论证。但是,生成基于证据的指南需要评估药物遗传学测试的临床效用。这个目标将仍然具有挑战性,主要是因为仅有很少的数据可用于临床效用估算。基因组发现的步伐突显了对临床实用性和实施​​研究的需求,以为未来的翻译工作提供信息。近期实施有前途的药物遗传学检测可以帮助加快这一目标,并为发现更多的基因-药物关联提供证据基础,以实现有效的翻译。

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