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双相障碍易感性基因在重度抑郁症个体中的表型效应。

Phenotypic effects of a bipolar liability gene among individuals with major depressive disorder.

机构信息

Division of Psychiatry, University of Pisa, Pisa, Italy.

出版信息

Am J Med Genet B Neuropsychiatr Genet. 2010 Jan 5;153B(1):303-9. doi: 10.1002/ajmg.b.30962.

Abstract

Variations in voltage-dependent calcium channel L-type, alpha 1C subunit (CACNA1C) gene have been associated with bipolar disorder in a recent meta-analysis of genome-wide association studies [Ferreira et al., 2008]. The impact of these variations on other psychiatric disorders has not been yet investigated. Caucasian non-Hispanic participants in the STAR*D study of treatment for depression for whom DNA was available (N = 1213) were genotyped at two single-nucleotide polymorphisms (SNPs) (rs10848635 and rs1006737) in the CACNA1C gene. We examined putative phenotypic indicators of bipolarity among patients with major depression and elements of longitudinal course suggestive of latent bipolarity. We also considered remission and depression severity following citalopram treatment. The rs10848635 risk allele was significantly associated with lower levels of baseline agitation (P = 0.03; beta = -0.09). The rs1006737 risk allele was significantly associated with lesser baseline depression severity (P = 0.04; beta = -0.4) and decreased likelihood of insomnia (P = 0.047; beta = -0.22). Both markers were associated with an increased risk of citalopram-emergent suicidality (rs10848635: OR = 1.29, P = 0.04; rs1006737: OR = 1.34, P = 0.02). In this exploratory analysis, treatment-emergent suicidality was associated with two risk alleles in a putative bipolar liability gene.

摘要

电压门控钙通道 L 型、α 1C 亚基(CACNA1C)基因的变异与最近的全基因组关联研究荟萃分析中的双相情感障碍有关[Ferreira 等人,2008]。这些变异对其他精神疾病的影响尚未得到研究。有 DNA 可用的 STAR*D 研究治疗抑郁症的高加索非西班牙裔参与者(N = 1213)在 CACNA1C 基因中的两个单核苷酸多态性(SNP)(rs10848635 和 rs1006737)上进行了基因分型。我们在患有重度抑郁症的患者中检查了双相情感障碍的潜在表型指标,以及具有潜在双相情感障碍的纵向病程元素。我们还考虑了西酞普兰治疗后的缓解和抑郁严重程度。rs10848635 风险等位基因与基线激越水平显著相关(P = 0.03;β= -0.09)。rs1006737 风险等位基因与较低的基线抑郁严重程度显著相关(P = 0.04;β= -0.4)和失眠减少的可能性显著相关(P = 0.047;β= -0.22)。这两个标志物都与西酞普兰出现自杀意念的风险增加相关(rs10848635:OR = 1.29,P = 0.04;rs1006737:OR = 1.34,P = 0.02)。在这项探索性分析中,治疗出现的自杀意念与一个潜在的双相情感障碍易感性基因中的两个风险等位基因相关。

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