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人类多巴胺基因与时间的双重分离。

Double dissociation of dopamine genes and timing in humans.

机构信息

University of Pennsylvania, Philadelphia, PA 19104-6241, USA.

出版信息

J Cogn Neurosci. 2011 Oct;23(10):2811-21. doi: 10.1162/jocn.2011.21626. Epub 2011 Jan 24.

Abstract

A number of lines of evidence implicate dopamine in timing [Rammsayer, T. H. Neuropharmacological approaches to human timing. In S. Grondin (Ed.), Psychology of time (pp. 295-320). Bingley, UK: Emerald, 2008; Meck, W. H. Neuropharmacology of timing and time perception. Brain Research, Cognitive Brain Research, 3, 227-242, 1996]. Two human genetic polymorphisms are known to modulate dopaminergic activity. DRD2/ANKK1-Taq1a is a D(2) receptor polymorphism associated with decreased D(2) density in the striatum [Jönsson, E. G., Nothen, M. M., Grunhage, F., Farde, L., Nakashima, Y., Propping, P., et al. Polymorphisms in the dopamine D(2) receptor gene and their relationships to striatal dopamine receptor density of healthy volunteers. Molecular Psychiatry, 4, 290-296, 1999]; COMT Val158Met is a functional polymorphism associated with increased activity of the COMT enzyme such that catabolism of synaptic dopamine is greater in pFC [Meyer-Lindenberg, A., Kohn, P. D., Kolachana, B., Kippenhan, S., McInerney-Leo, A., Nussbaum, R., et al. Midbrain dopamine and prefrontal function in humans: Interaction and modulation by COMT genotype. Nature Neuroscience, 8, 594-596, 2005]. To investigate the role of dopamine in timing, we genotyped 65 individuals for DRD2/ANKK1-Taq1a, COMT Val158Met, and a third polymorphism, BDNF Val66Met, a functional polymorphism affecting the expression of brain-derived neurotrophic factor [Egan, M. F., Kojima, M., Callicott, J. H., Goldberg, T. E., Kolachana, B. S., Bertolino, A., et al. The BDNF val66met polymorphism affects activity-dependent secretion of BDNF and human memory and hippocampal function. Cell, 112, 257-269, 2003]. Subjects were tested on a temporal discrimination task with sub- and supra-second intervals (500- and 2000-msec standards) as well as a spontaneous motor tempo task. We found a double dissociation for temporal discrimination: the DRD2/ANKK1-Taq1a polymorphism (A1+ allele) was associated with significantly greater variability for the 500-msec duration only, whereas the COMT Val158Met polymorphism (Val/Val homozygotes) was associated with significantly greater variability for the 2000-msec duration only. No differences were detected for the BDNF Vall66Met variant. Additionally, the DRD2/ANKK1-Taq1a polymorphism was associated with a significantly slower preferred motor tempo. These data provide a potential biological basis for the distinctions between sub- and supra-second timing and suggest that BG are integral for the former whereas pFC is implicated in the latter.

摘要

有许多证据表明多巴胺与计时有关[Rammsayer,TH。神经药理学方法在人类计时中的应用。在 S. Grondin(编辑),时间心理学(第 295-320 页)。英国比灵厄姆:翡翠,2008 年; Meck,WH。计时和时间感知的神经药理学。大脑研究,认知大脑研究,3,227-242,1996]。已知两种人类遗传多态性可以调节多巴胺能活性。DRD2/ANKK1-Taq1a 是一种与纹状体中 D(2)受体密度降低相关的 D(2)受体多态性[Jönsson,EG,Nothen,MM,Grunhage,F.,Farde,L.,Nakashima,Y.,Propping,P.,等。多巴胺 D(2)受体基因的多态性及其与健康志愿者纹状体多巴胺受体密度的关系。分子精神病学,4,290-296,1999];COMT Val158Met 是一种功能性多态性,与 COMT 酶的活性增加有关,使得 pFC 中突触多巴胺的代谢增加[Meyer-Lindenberg,A.,Kohn,PD,Kolachana,B.,Kippenhan,S.,McInerney-Leo,A.,Nussbaum,R.,等。人类中脑多巴胺和前额叶功能:COMT 基因型的相互作用和调节。自然神经科学,8,594-596,2005]。为了研究多巴胺在计时中的作用,我们对 65 名个体进行了 DRD2/ANKK1-Taq1a、COMT Val158Met 和第三种多态性 BDNF Val66Met 的基因分型,BDNF Val66Met 是一种影响脑源性神经营养因子表达的功能性多态性[Egan,MF,Kojima,M.,Callicott,JH,Goldberg,TE,Kolachana,BS,Bertolino,A.,等。BDNF val66met 多态性影响 BDNF 的活性依赖性分泌及其与人类记忆和海马功能的关系。细胞,112,257-269,2003]。被试者接受了一个时间辨别任务,包括亚秒和超秒间隔(500-和 2000 毫秒标准)以及一个自发的运动节奏任务。我们发现时间辨别存在双重分离:DRD2/ANKK1-Taq1a 多态性(A1+等位基因)仅与 500 毫秒的持续时间的显著更大变异性相关,而 COMT Val158Met 多态性(Val/Val 纯合子)仅与 2000 毫秒的持续时间的显著更大变异性相关。BDNF Vall66Met 变体没有检测到差异。此外,DRD2/ANKK1-Taq1a 多态性与明显较慢的首选运动节奏有关。这些数据为亚秒和超秒计时之间的区别提供了潜在的生物学基础,并表明 BG 对前者至关重要,而 pFC 则与后者有关。

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