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血清素和脑源性神经营养因子基因对与压力相关的成人精神症状的风险及保护作用。

Risk and protective effects of serotonin and BDNF genes on stress-related adult psychiatric symptoms.

作者信息

Nestor Paul G, O'Donovan Keira, Lapp Hannah E, Hasler Victoria Choate, Boodai Sara B, Hunter Richard

机构信息

Department of Psychology, University of Massachusetts Boston, Boston, MA, 02125, USA.

出版信息

Neurobiol Stress. 2019 Jul 26;11:100186. doi: 10.1016/j.ynstr.2019.100186. eCollection 2019 Nov.

Abstract

We focused on individual risk by examining childhood adversity and current psychiatric symptoms in a sample of 100 college students genotyped for both the serotonin transporter (5-HTTLPR) and the brain-derived neurotrophic factor (BDNF). Naturally occurring allelic variation in 5-HTTLPR (short/long) and BDNF (valine/methionine) have been strongly implicated in stress-related psychiatric risk, but the combined effects of these alleles on psychological functioning have yet to be fully elucidated. Univariate analysis revealed gene-environment correlations linking heightened psychiatric risk with past childhood adversity for short but not long 5-HTTLPR allelic carriers and for valine (Val) but not methionine (Met) BDNF allelic carriers. Multivariate analyses revealed a significant gene x gene interaction with results showing that risk varied systematically depending on both 5-HTTLPR and BDNF alleles, independent of childhood adversity. Hierarchical regression analyses indicated that approximately 11% of the variance in symptoms of depression could be specifically accounted for by the epistatic interaction of 5-HTTLPR and BDNF val66Met polymorphisms. Allelic group analyses indicated lowest risk, as measured by depression and anxiety, for allelic carriers of 5-HTTLPR-short and BDNF Met, followed by 5-HTTLPR-long and BDNF-Val, 5-HTTLPR-short and BDNF-Val, and 5-HTTLPR-long and BDNF-Met. Results suggest that protective or risk-enhancing effects on stress-related psychiatric functioning may depend on specific allelic combinations of 5-HTTLPR and BDNF.

摘要

我们通过研究100名对血清素转运体(5-HTTLPR)和脑源性神经营养因子(BDNF)进行基因分型的大学生样本中的童年逆境和当前精神症状,来关注个体风险。5-HTTLPR(短/长)和BDNF(缬氨酸/蛋氨酸)中自然发生的等位基因变异与应激相关的精神风险密切相关,但这些等位基因对心理功能的综合影响尚未完全阐明。单变量分析显示,对于携带5-HTTLPR短等位基因而非长等位基因的个体,以及携带BDNF缬氨酸(Val)等位基因而非蛋氨酸(Met)等位基因的个体,基因-环境相关性将更高的精神风险与过去的童年逆境联系起来。多变量分析显示存在显著的基因×基因相互作用,结果表明风险根据5-HTTLPR和BDNF等位基因而系统性变化,与童年逆境无关。分层回归分析表明,抑郁症状约11%的变异可由5-HTTLPR和BDNF val66Met多态性的上位相互作用具体解释。等位基因组分析表明,以抑郁和焦虑衡量,5-HTTLPR短等位基因和BDNF Met等位基因携带者的风险最低,其次是5-HTTLPR长等位基因和BDNF-Val、5-HTTLPR短等位基因和BDNF-Val,以及5-HTTLPR长等位基因和BDNF-Met。结果表明,对与应激相关的精神功能的保护或风险增强作用可能取决于5-HTTLPR和BDNF的特定等位基因组合。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c713/6700400/c70a8652a1c7/gr1.jpg

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