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A genome-wide association study of antidepressant response in Koreans

机译:韩国人抗抑郁反应的全基因组关联研究

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摘要

We conducted a three-stage genome-wide association study (GWAS) of response to antidepressant drugs in an ethnically homogeneous sample of Korean patients in untreated episodes of nonpsychotic unipolar depression, mostly of mature onset. Strict quality control was maintained in case selection, diagnosis, verification of adherence and outcome assessments. Analyzed cases completed 6 weeks of treatment with adequate plasma drug concentrations. The overall successful completion rate was 85.5%. Four candidate single-nucleotide polymorphisms (SNPs) on three chromosomes were identified by genome-wide search in the discovery sample of 481 patients who received one of four allowed selective serotonin reuptake inhibitor (SSRI) antidepressant drugs (Stage 1). In a focused replication study of 230 SSRI-treated patients, two of these four SNP candidates were confirmed (Stage 2). Analysis of the Stage 1 and Stage 2 samples combined (n=711) revealed GWAS significance (P=1.60 × 10-8) for these two SNP candidates, which were in perfect linkage disequilibrium. These two significant SNPs were confirmed also in a focused cross-replication study of 159 patients treated with the non-SSRI antidepressant drug mirtazapine (Stage 3). Analysis of the Stage 1, Stage 2 and Stage 3 samples combined (n=870) also revealed GWAS significance for these two SNPs, which was sustained after controlling for gender, age, number of previous episodes, age at onset and baseline severity (P=3.57 × 10-8). For each SNP, the response rate decreased (odds ratio=0.31, 95% confidence interval: 0.20–0.47) as a function of the number of minor alleles (non-response alleles). The two SNPs significantly associated with antidepressant response are rs7785360 and rs12698828 of the AUTS2 gene, located on chromosome 7 in 7q11.22. This gene has multiple known linkages to human psychological functions and neurobehavioral disorders. Rigorous replication efforts in other ethnic populations are recommended.
机译:我们进行了一个三阶段全基因组关联研究(GWAS),该研究在未经治疗的非精神病性单相抑郁发作(主要是成熟的发作)中,从韩国患者的种族同质样本中对抗抑郁药的反应进行。在病例选择,诊断,依从性验证和结果评估中保持严格的质量控制。分析的病例用适当的血浆药物浓度完成了6周的治疗。总体成功完成率为85.5%。通过在481名患者的发现样本中通过全基因组搜索鉴定了三个染色体上的四个候选单核苷酸多态性(SNP),这些患者接受了四种允许的选择性5-羟色胺再摄取抑制剂(SSRI)抗抑郁药之一(阶段1)。在一项针对230名接受SSRI治疗的患者的集中复制研究中,确认了这四个SNP候选者中的两个(第2阶段)。对第一阶段和第二阶段样本(n = 711)的分析表明,这两个处于理想连锁不平衡状态的SNP候选者的GWAS显着性(P = 1.60×10 -8 )。这两项重要的SNP也已在针对159例接受非SSRI抗抑郁药米氮平治疗的患者的交叉复制研究中得到证实(第3阶段)。对第1阶段,第2阶段和第3阶段样本的合并分析(n = 870)还显示了这两个SNP的GWAS重要性,在控制了性别,年龄,以前发作的次数,发病年龄和基线严重程度后,PGA持续存在(P = 3.57×10 -8 )。对于每个单核苷酸多态性,其应答率随次要等位基因(无应答等位基因)数量的下降而降低(几率= 0.31,95%置信区间:0.20–0.47)。与抗抑郁反应显着相关的两个SNP是位于7q11.22中7号染色体上的AUTS2基因的rs7785360和rs12698828。该基因与人类心理功能和神经行为异常有多种已知的联系。建议在其他种族人群中进行严格的复制工作。

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