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在非裔美国人中,可卡因使用障碍的GABA能多基因风险与认知控制过程中楔前叶活动呈负相关。

GABAergic polygenic risk for cocaine use disorder is negatively correlated with precuneus activity during cognitive control in African American individuals.

作者信息

Yang Bao-Zhu, Balodis Iris M, Kober Hedy, Worhunsky Patrick D, Lacadie Cheryl M, Gelernter Joel, Potenza Marc N

机构信息

Department of Psychiatry, Yale University School of Medicine, New Haven, CT, USA; VA CT Healthcare Center, West Haven, CT, USA.

Department of Psychiatry, Yale University School of Medicine, New Haven, CT, USA; Peter Boris Centre for Addictions Research, Department of Psychiatry and Behavioural Neurosciences, McMaster University, Hamilton, Ontario, Canada.

出版信息

Addict Behav. 2021 Mar;114:106695. doi: 10.1016/j.addbeh.2020.106695. Epub 2020 Oct 10.

Abstract

Impaired cognitive control has been implicated in cocaine use disorder (CUD). GABAergic treatments have been proposed for CUD. Here we examined relationships between GABAergic genes and neural correlates of cognitive control in CUD. We analyzed two independent African American cohorts: one of >3000 genomewide-genotyped subjects with substance dependence and another of 40 CUD and 22 healthy control (HC) subjects who were exome-array genotyped and completed an fMRI Stroop task. We used five association thresholds to select variants of GABAergic genes in the reference cohort, yielding five polygenic risk scores (i.e., CUD-GABA-PRSs) for the fMRI cohort. At p < 0.005, the CUD-GABA-PRSs, which aggregated relative risks of CUD from 89 variants harboring in 16 genes, differed between CUD and HC individuals in the fMRI sample (p = 0.013). This CUD-GABA-PRS correlated inversely with Stroop-related activity in the left precuneus in CUD (r = -80.58, p < 0.05) but not HC participants. Post-hoc seed-based connectivity analysis of the left precuneus identified reduced functional connectivity to the posterior cingulate cortex (PCC) in CUD compared to HC subjects (p = 0.0062) and the degree of connectivity correlated with CUD-GABA-PRSs in CUD individuals (r = 0.287, p = 0.036). Our findings suggest that the GABAergic genetic risk of CUD in African Americans relates to precuneus/PCC functional connectivity during cognitive control. Identification of these GABAergic processes may be relevant targets in CUD treatment. The novel identification of 16 GABAergic genes may be investigated further to inform treatment development efforts for this condition that currently has no medication with a formal indication for its treatment.

摘要

认知控制受损与可卡因使用障碍(CUD)有关。已有人提出用GABA能治疗方法来治疗CUD。在此,我们研究了GABA能基因与CUD中认知控制的神经相关性之间的关系。我们分析了两个独立的非裔美国人队列:一个队列包含3000多名进行了全基因组基因分型且有物质依赖的受试者,另一个队列有40名CUD受试者和22名健康对照(HC)受试者,这些受试者进行了外显子阵列基因分型并完成了一项功能磁共振成像(fMRI)的斯特鲁普任务。我们使用五个关联阈值在参考队列中选择GABA能基因的变异体,为fMRI队列得出五个多基因风险评分(即CUD - GABA - PRS)。在p < 0.005时,CUD - GABA - PRS在fMRI样本中的CUD个体和HC个体之间存在差异(p = 0.013),该评分汇总了16个基因中89个变异体的CUD相对风险。在CUD患者中,这种CUD - GABA - PRS与左侧楔前叶中与斯特鲁普相关的活动呈负相关(r = -80.58,p < 0.05),但在HC参与者中并非如此。对左侧楔前叶进行基于种子的事后连通性分析发现,与HC受试者相比,CUD患者与后扣带回皮质(PCC)的功能连通性降低(p = 0.0062),并且连通程度与CUD个体中的CUD - GABA - PRS相关(r = 0.287,p = 0.036)。我们的研究结果表明,非裔美国人中CUD的GABA能遗传风险与认知控制过程中楔前叶/PCC的功能连通性有关。确定这些GABA能过程可能是CUD治疗中的相关靶点。这16个GABA能基因的新发现可能需要进一步研究,以为目前尚无正式治疗用药的这种疾病的治疗开发提供信息。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2350/8299472/09a0bb8e7940/nihms-1643364-f0001.jpg

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