新型ALX4基因多态性与抗抑郁治疗反应的关系:来自CO-MED试验的发现

Molecular Neuropsychiatry Pub Date : 2018-06-01 Epub Date: 2018-05-03 DOI:10.1159/000487321
Bharathi S Gadad, Prithvi Raj, Manish K Jha, Thomas Carmody, Igor Dozmorov, Taryn L Mayes, Edward K Wakeland, Madhukar H Trivedi
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引用次数: 9

摘要

全基因组关联研究(GWAS)在CO-MED(联合药物增强抑郁结局)试验的参与者中进行,这是一项随机的,3治疗组的重度抑郁症(MDD)临床试验,旨在确定不同治疗结果(反应和缓解)的标志物。QIDS-SR(抑郁症状快速量表,自我报告版)用于测量第6周的反应(QIDS-SR≤5)和第12周的缓解(最后两次研究访问时QIDS-SR≤6和≤8)。对艾司西酞普兰单药、艾司西酞普兰+安非他酮、文拉法辛+米氮平三个治疗组进行评价。GWAS在白种人11号染色体上的ALX4基因上发现了一个潜在的调控SNP rs10769025,它与对艾司西酞普兰单药治疗的反应有很强的相关性(p值= 9.85925E-08)。此外,对7个ALX4变异的单倍型分析显示,调节单倍型CAAACTG与第6周对艾司西酞普兰单药治疗的反应显著相关(优势比= 3.4,p = 2.00E-04)。本研究中的独创性通路分析表明,ALX4与重度抑郁症的抗抑郁基因通路有间接联系,这可能解释了与治疗结果的遗传关联。功能基因组学研究ALX4在抗抑郁治疗结果中的作用将是一个有趣的未来方向。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Association of Novel ALX4 Gene Polymorphisms with Antidepressant Treatment Response: Findings from the CO-MED Trial.

Association of Novel ALX4 Gene Polymorphisms with Antidepressant Treatment Response: Findings from the CO-MED Trial.

Association of Novel ALX4 Gene Polymorphisms with Antidepressant Treatment Response: Findings from the CO-MED Trial.

Association of Novel ALX4 Gene Polymorphisms with Antidepressant Treatment Response: Findings from the CO-MED Trial.

Genome-wide association studies (GWAS) were conducted in participants of the CO-MED (Combining Medications to Enhance Depression Outcomes) trial, a randomized, 3-treatment arm clinical trial of major depressive disorder (MDD) designed to identify markers of differential treatment outcome (response and remission). The QIDS-SR (Quick Inventory of Depressive Symptomatology, Self-Reported version) was used to measure response at week 6 (QIDS-SR ≤5) and remission at week 12 (QIDS-SR ≤6 and ≤8 at the last two study visits). Three treatment groups (escitalopram monotherapy, escitalopram + bupropion, and venlafaxine + mirtazapine) were evaluated. GWAS identified a potentially regulatory SNP rs10769025 in the ALX4 gene on chromosome 11 with a strong association (p value = 9.85925E-08) with response to escitalopram monotherapy in Caucasians. Further, haplotype analysis on 7 ALX4 variants showed that a regulatory haplotype CAAACTG was significantly associated (odds ratio = 3.4, p = 2.00E-04) with response to escitalopram monotherapy at week 6. Ingenuity pathway analyses in the present study suggest that ALX4 has an indirect connection with antidepressant gene pathways in MDD, which may account for the genetic association with treatment outcome. Functional genomics studies to investigate the role of ALX4 in antidepressant treatment outcome will be an interesting future direction.

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