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一个 CRHR1 单倍型调节了逆境童年经历对非裔美国女性一生中发生重度抑郁发作的风险的影响。

A CRHR1 haplotype moderates the effect of adverse childhood experiences on lifetime risk of major depressive episode in African-American women.

机构信息

Department of Psychiatry, University of Pennsylvania, Philadelphia, Pennsylvania 19104, USA.

出版信息

Am J Med Genet B Neuropsychiatr Genet. 2011 Dec;156B(8):960-8. doi: 10.1002/ajmg.b.31243. Epub 2011 Oct 13.

Abstract

Adverse childhood experiences (ACEs) increase the risk for adult depression and substance dependence, possibly mediated by the corticotropin-releasing hormone type 1 receptor (CRHR1). In some studies, a three-SNP "T-A-T" haplotype in CRHR1, which encodes CRHR1, exerted a protective moderating effect on risk of depression in adults with ACEs. Other studies have shown a main or moderating effect of SNPs in CRHR1 on alcohol consumption. We tested the moderating effects of the three-SNP haplotype on lifetime risk of a major depressive episode (MDE) and alcohol dependence (AD) in 1,211 European-Americans (EAs) and 1,869 African-Americans (AAs), most of whom had a lifetime substance use disorder. There were no significant main or interaction effects of the TAT haplotype on AD. There was a significant interaction of ACE by TAT on risk of depression only in AA women (P = 0.005); each copy of the TAT haplotype reduced the odds of MDE by almost 40% (OR = 0.63). In AA women without an ACE and two TAT haplotypes, the risk of MDE was increased (OR = 1.51 for each copy). Our findings in relation to the TAT haplotype of CRHR1 extend those obtained in other populations to a largely substance-dependent one. The complex structure of CRHR1 may help to explain why some variants in the gene moderate the effects of an ACE only on depression risk while others moderate the effect of an ACE only on AD risk.

摘要

不良童年经历 (ACEs) 会增加成年后患抑郁症和物质依赖的风险,这可能是通过促肾上腺皮质激素释放激素 1 型受体 (CRHR1) 介导的。在一些研究中,CRHR1 中的三个单核苷酸多态性 (SNP)“T-A-T” 单倍型编码 CRHR1,对 ACE 后成年抑郁症风险具有保护调节作用。其他研究表明,CRHR1 中的 SNP 对酒精消费具有主要或调节作用。我们测试了三个 SNP 单倍型对 1211 名欧洲裔美国人 (EA) 和 1869 名非裔美国人 (AA) 一生中发生重度抑郁发作 (MDE) 和酒精依赖 (AD) 的风险的调节作用,其中大多数人患有终身物质使用障碍。TAT 单倍型对 AD 没有显著的主要或交互作用。只有在 AA 女性中,ACE 与 TAT 的相互作用对抑郁风险才有显著影响 (P = 0.005);TAT 单倍型的每一个拷贝都会使 MDE 的几率降低近 40%(OR = 0.63)。在没有 ACE 和两个 TAT 单倍型的 AA 女性中,MDE 的风险增加了(每增加一个拷贝,OR = 1.51)。我们关于 CRHR1 的 TAT 单倍型的发现将其他人群的研究结果扩展到了主要依赖物质的人群。CRHR1 的复杂结构可能有助于解释为什么该基因中的某些变体仅调节 ACE 对抑郁风险的影响,而其他变体仅调节 ACE 对 AD 风险的影响。

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