BDNF、HTR2A、TPH1、SLC6A4和COMT多态性与tDCS和艾司西酞普兰疗效的关联:一项双盲、安慰剂对照试验的辅助分析

A. Brunoni, Á. Carracedo, O. Amigo, A. L. Pellicer, L. Talib, A. Carvalho, P. Lotufo, I. Benseñor, W. Gattaz, C. Cappi
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引用次数: 15

摘要

摘要目的:我们研究了单核苷酸多态性(snp)是否与脑源性神经营养因子(BDNF, rs6265)、5-羟色胺转运蛋白(SLC6A4, rs25531)、色氨酸羟化酶1 (TPH1, rs1800532)、5-羟色胺受体2A (HTR2A, rs6311, rs6313, rs7997012)和儿茶酚- o -甲基转移酶(COMT, rs4680)基因等单胺类神经递质的神经可塑性和活性相关。与经颅直流电刺激(tDCS)治疗重度抑郁症的疗效有关。方法:采用艾司西酞普兰与电流治疗抑郁症临床研究(electric - tdcs)的数据。参与者在基线时无抗抑郁药,并出现急性、中度至重度单相抑郁发作。他们被随机分为艾西酞普兰/tDCS-sham组(n=75)、tDCS/安慰剂-pill组(n=75)或安慰剂-pill/sham-tDCS组(n=45)。一般线性模型评估治疗组和等位基因携带者之间的相互作用。对每组和每个基因型分别进行附加分析。结果:两两组比较(tDCS vs安慰剂,tDCS vs艾司西酞普兰,艾司西酞普兰vs安慰剂)未发现与抑郁改善相关的等位基因。此外,探索性分析也没有发现任何SNP与任何治疗组抑郁症的改善明确相关。结论:需要更大的组合数据集来确定tDCS应答的候选基因。
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Association of BDNF, HTR2A, TPH1, SLC6A4, and COMT polymorphisms with tDCS and escitalopram efficacy: ancillary analysis of a double-blind, placebo-controlled trial
Objective: We investigated whether single nucleotide polymorphisms (SNPs) associated with neuroplasticity and activity of monoamine neurotransmitters, such as the brain-derived neurotrophic factor (BDNF, rs6265), the serotonin transporter (SLC6A4, rs25531), the tryptophan hydroxylase 1 (TPH1, rs1800532), the 5-hydroxytryptamine receptor 2A (HTR2A, rs6311, rs6313, rs7997012), and the catechol-O-methyltransferase (COMT, rs4680) genes, are associated with efficacy of transcranial direct current stimulation (tDCS) in major depression. Methods: Data from the Escitalopram vs. Electrical Current Therapy for Treating Depression Clinical Study (ELECT-TDCS) were used. Participants were antidepressant-free at baseline and presented with an acute, moderate-to-severe unipolar depressive episode. They were randomized to receive escitalopram/tDCS-sham (n=75), tDCS/placebo-pill (n=75), or placebo-pill/sham-tDCS (n=45). General linear models assessed the interaction between treatment group and allele-wise carriers. Additional analyses were performed for each group and each genotype separately. Results: Pairwise group comparisons (tDCS vs. placebo, tDCS vs. escitalopram, and escitalopram vs. placebo) did not identify alleles associated with depression improvement. In addition, exploratory analyses also did not identify any SNP unequivocally associated with improvement of depression in any treatment group. Conclusion: Larger, combined datasets are necessary to identify candidate genes for tDCS response.
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