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Pharmacogenetic study of antipsychotic induced acute extrapyramidal symptoms in a first episode psychosis cohort: role of dopamine, serotonin and glutamate candidate genes

机译:在首发性精神病队列中抗精神病药诱发的急性锥体外系症状的药物遗传学研究:多巴胺,5-羟色胺和谷氨酸候选基因的作用

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摘要

This study investigated whether the risk of presenting antipsychotic (AP)-induced extrapyramidal symptoms (EPS) could be related to single-nucleotide polymorphisms (SNPs) in a naturalistic cohort of first episode psychosis (FEP) patients. Two hundred and two SNPs in 31 candidate genes (involved in dopamine, serotonin and glutamate pathways) were analyzed in the present study. One hundred and thirteen FEP patients (43 presenting EPS and 70 non-presenting EPS) treated with high-potency AP (amisulpride, paliperidone, risperidone and ziprasidone) were included in the analysis. The statistical analysis was adjusted by age, gender, AP dosage, AP combinations and concomitant treatments as covariates. Four SNPs in different genes (DRD2, SLC18A2, HTR2A and GRIK3) contributed significantly to the risk of EPS after correction for multiple testing (P <1 x 10(-4)). These findings support the involvement of dopamine, serotonin and glutamate pathways in AP-induced EPS.
机译:这项研究调查了在首发性精神病(FEP)患者的自然队列中出现抗精神病药(AP)引起的锥体外系症状(EPS)的风险是否可能与单核苷酸多态性(SNP)相关。在本研究中分析了31个候选基因(涉及多巴胺,5-羟色胺和谷氨酸途径)中的202个SNP。分析包括113例接受高效AP(阿米普利,帕潘立酮,利培酮和齐拉西酮)治疗的FEP患者(43例EPS和70例非EPS)。根据年龄,性别,AP剂量,AP组合和伴随治疗作为协变量调整统计分析。校正多个测试后,不同基因中的四个SNP(DRD2,SLC18A2,HTR2A和GRIK3)显着增加了EPS的风险(P <1 x 10(-4))。这些发现支持多巴胺,5-羟色胺和谷氨酸途径参与AP诱导的EPS。

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