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GAD1基因分型状态对健康志愿者听觉注意力及急性尼古丁给药的影响。

Effect of GAD1 genotype status on auditory attention and acute nicotine administration in healthy volunteers.

作者信息

Hadjis Efthymios, Hyde Molly, Choueiry Joelle, Jaworska Natalia, Nelson Renee, de la Salle Sara, Smith Dylan, Aidelbaum Rob, Knott Verner

机构信息

Department of Psychiatry, McGill University, Montreal, Quebec, Canada.

University of Ottawa Institute of Mental Health Research, Ottawa, Ontario, Canada.

出版信息

Hum Psychopharmacol. 2019 Jan;34(1):e2684. doi: 10.1002/hup.2684. Epub 2018 Nov 29.

Abstract

OBJECTIVE

The effects of GABA modulating drugs and nicotine, the prototypical nicotinic cholinergic agonist, on attention have been investigated using subcomponents of the P300 event-related potentials (ERP), which index involuntary (P3a) and voluntary attention (P3b). However, investigations into how such pharmacologic effects interact with genetic features in the GABA system remain unclear. This study examined the moderating effects of a single nucleotide polymorphism (rs7557793) in the glutamic acid decarboxylase 67 (GAD1) gene, which is implicated in the conversion of glutamate to GABA, on P300-indices of auditory attentional processing; the influence of nicotine administration was also assessed.

METHODS

The effects of GAD1 genotype (TT/CC/CT) were examined on the P3a/b in response to an auditory selective attention task in healthy, nonsmoking male volunteers (N = 126; 18-40 years). Participants responded to rare target stimuli (P3b-eliciting) and ignored frequent nontarget stimuli as well as rare distractor stimuli (P3a-eliciting). In a subsample (N = 59), P3a/b profiles to acute nicotine (vs. placebo) administration were examined as a function of GAD1 genotype. As a secondary aim, earlier sensory processes were assessed with N200 ERP subcomponents elicited by novel (N2a) and target (N2b) auditory stimuli.

RESULTS

GAD1 allelic variation moderated early sensory processes, enhancing N2a amplitudes in CT versus TT carriers. Further, TT homozygotes exhibited larger P3b amplitudes than CC homozygotes in the placebo versus nicotine condition. Regardless of genotype, nicotine versus placebo moderated the N200 ERP.

CONCLUSION

These findings expand our knowledge regarding the attentional effects of GAD1 genetic variants in relation to nicotine.

摘要

目的

已使用P300事件相关电位(ERP)的子成分研究了γ-氨基丁酸(GABA)调节药物和典型烟碱胆碱能激动剂尼古丁对注意力的影响,这些子成分可指示非自愿性(P3a)和自愿性注意力(P3b)。然而,关于此类药理作用如何与GABA系统中的遗传特征相互作用的研究仍不清楚。本研究考察了谷氨酸脱羧酶67(GAD1)基因中的单核苷酸多态性(rs7557793)对听觉注意力加工的P300指标的调节作用,该基因与谷氨酸向GABA的转化有关;同时还评估了尼古丁给药的影响。

方法

在健康、不吸烟的男性志愿者(N = 126;18 - 40岁)中,研究了GAD1基因型(TT/CC/CT)对听觉选择性注意任务中P3a/b的影响。参与者对罕见的目标刺激(诱发P3b)做出反应,忽略频繁的非目标刺激以及罕见的干扰刺激(诱发P3a)。在一个子样本(N = 59)中,研究了急性尼古丁(与安慰剂相比)给药后P3a/b的特征与GAD1基因型的关系。作为次要目的,用新的(N2a)和目标(N2b)听觉刺激诱发的N200 ERP子成分评估早期感觉过程。

结果

GAD1等位基因变异调节早期感觉过程,CT携带者比TT携带者的N2a波幅增强。此外,在安慰剂与尼古丁条件下,TT纯合子的P3b波幅比CC纯合子大。无论基因型如何,尼古丁与安慰剂相比调节了N200 ERP。

结论

这些发现扩展了我们对GAD1基因变异与尼古丁相关的注意力影响的认识。

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