大麻素受体基因型调节儿童身体虐待对快感缺乏和抑郁的影响。

Arpana Agrawal, Elliot C Nelson, Andrew K Littlefield, Kathleen K Bucholz, Louisa Degenhardt, Anjali K Henders, Pamela A F Madden, Nicholas G Martin, Grant W Montgomery, Michele L Pergadia, Kenneth J Sher, Andrew C Heath, Michael T Lynskey
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引用次数: 81

摘要

背景:在啮齿动物研究中,内源性大麻素系统与应激适应和情绪调节有关,但很少有人类相关研究研究了这些联系,而且重复性有限。目的:研究编码人类内源性大麻素受体(CNR1)的基因外显子4的同义多态性rs1049353是否调节自我报告的童年身体虐待对终生快感缺乏症和抑郁症的影响,并在独立样本中复制这种相互作用。设计、环境和参与者:1041名年轻美国女性的遗传关联研究,并在澳大利亚的1428名海洛因依赖个体作为病例和506名参与者作为邻里对照的独立样本中进行复制。主要结局指标:自我报告的快感缺乏和抑郁(伴快感缺乏)。结果:在这两个样本中,经历过童年身体虐待的个体更有可能报告终生快感缺乏症。然而,在那些有1个或多个rs1049353小等位基因拷贝的人群中,儿童时期身体虐待的致病作用减弱了。因此,在报告童年身体虐待的参与者中,尽管57.1%的主要等位基因纯合子报告了快感缺乏症,但只有28.6%的次要等位基因携带者报告了快感缺乏症(P= 0.01)。rs1049353多态性还能缓冲童年身体虐待对重度抑郁症的影响;然而,这种影响在很大程度上可归因于享乐缺乏性抑郁症。这些影响在一个独立的样本中也被注意到,在这个样本中,少量的等位基因携带者即使受到身体虐待,也有较低的快感缺乏症风险。结论:与临床前研究结果一致,同义的CNR1多态性rs1049353与儿童身体虐待导致的应激对快感缺乏和快感缺乏抑郁症的影响有关。据报道,这种多态性位于外显子剪接增强子附近;因此,未来的研究应仔细研究其对CNR1表达和构象变化的影响,特别是与胁迫适应的关系。
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Cannabinoid receptor genotype moderation of the effects of childhood physical abuse on anhedonia and depression.

Context: The endocannabinoid system has been implicated in stress adaptation and the regulation of mood in rodent studies, but few human association studies have examined these links and replications are limited.

Objectives: To examine whether a synonymous polymorphism, rs1049353, in exon 4 of the gene encoding the human endocannabinoid receptor (CNR1) moderates the effect of self-reported childhood physical abuse on lifetime anhedonia and depression and to replicate this interaction in an independent sample.

Design, setting, and participants: Genetic association study in 1041 young US women with replication in an independent Australian sample of 1428 heroin-dependent individuals as cases and 506 participants as neighborhood controls.

Main outcome measures: Self-reported anhedonia and depression (with anhedonia).

Results: In both samples, individuals who experienced childhood physical abuse were considerably more likely to report lifetime anhedonia. However, in those with 1 or more copies of the minor allele of rs1049353, this pathogenic effect of childhood physical abuse was attenuated. Thus, in participants reporting childhood physical abuse, although 57.1% of those homozygous for the major allele reported anhedonia, only 28.6% of those who were carriers of the minor allele reported it (P=.01). The rs1049353 polymorphism also buffered the effects of childhood physical abuse on major depressive disorder; however, this influence was largely attributable to anhedonic depression. These effects were also noted in an independent sample, in which minor allele carriers were at decreased risk for anhedonia even when exposed to physical abuse.

Conclusions: Consistent with preclinical findings, a synonymous CNR1 polymorphism, rs1049353, is linked to the effects of stress attributable to childhood physical abuse on anhedonia and anhedonic depression. This polymorphism reportedly resides in the neighborhood of an exon splice enhancer; hence, future studies should carefully examine its effect on expression and conformational variation in CNR1, particularly in relation to stress adaptation.

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Archives of general psychiatry
Archives of general psychiatry 医学-精神病学
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