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Genetics of antipsychotic drug outcome and implications for the clinician: into the limelight

机译:抗精神病药物预后的遗传学及其对临床医生的影响:成为众人瞩目的焦点

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Background and purposeAntipsychotics (APs) are the primary method of treatment for schizophrenia and other psychotic disorders. Unfortunately, lengthy trial-and-error approaches are typically required to find the optimal medication and dosage due to a large interindividual variability with outcome to AP treatment. The literature has shown abundant evidence for a genetic component in individuals’ responses to APs. Pharmacogenetic studies analyze specific genetic markers and their association with symptom improvement and occurrence of side effects with APs. This research aims to optimize AP drug treatment by usage of predictive testing and to personalize medicine.Recent findingsThis review will highlight the most consistent findings in pharmacogenetics of APs and will update the reader on the clinical implications. This will include how genetic variants modulate AP drug levels, side effects, and therapeutic symptom improvement (i.e. response) to AP treatment.SummarySeveral promising findings were obtained implicating gene variants of the dopamine receptor genes in addition to gene variants of serotonin receptors for response and common side effects. Notably, effect sizes appear to be particularly high in the genetics of side effects compared to response. One example is antipsychotic-induced weight gain where the leptin, HTR2C and in particular the melanocortin-4-receptor (MC4R ) genes have been implicated in weight gain in children and adolescents. Consistent findings were also obtained for genes implicated in tardive dyskinesia and agranulocytosis. However, the most clinically relevant findings pertain to genes involved in drug metabolism such as the CYP2D6 and CYP2C19 genes which have been included in the first genetic test kits such as the Amplichip~(?) CYP450 Test and more recently the DMET? Plus Panel, the Genecept? Assay, the Genomas HILOmet PhyzioType? System, and the GeneSight~(?) Test.
机译:背景和目的抗精神病药(APs)是治疗精神分裂症和其他精神病性疾病的主要方法。不幸的是,由于个体间的巨大差异会导致AP治疗的结果,通常需要漫长的反复试验才能找到最佳的药物和剂量。文献已经为个人对AP的反应显示了遗传成分的大量证据。药物遗传学研究分析了特定的遗传标记及其与症状改善和AP副作用的发生相关。这项研究旨在通过使用预测性测试来优化AP药物治疗并个性化药物。最新发现本综述将重点介绍AP药物遗传学上最一致的发现,并向读者介绍其临床意义。这将包括遗传变异体如何调节AP药物水平,副作用和对AP治疗的治疗症状改善(即反应)。常见的副作用。值得注意的是,与反应相比,在副作用的遗传学中效应的大小似乎特别高。一个例子是抗精神病药引起的体重增加,其中瘦素,HTR2C,尤其是黑皮质素-4-受体(MC4R)基因与儿童和青少年的体重增加有关。对于迟发性运动障碍和粒细胞缺乏症的基因也获得了一致的发现。但是,与临床最相关的发现是涉及药物代谢的基因,例如CYP2D6和CYP2C19基因,这些基因已包含在第一批基因检测试剂盒中,例如Amplichip〜(?)CYP450检测还有最近的DMET?加上面板,Genecept?例如,基因组 HILOmet PhyzioType?系统和GeneSight〜(?)测试。

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