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儿茶酚-O-甲基转移酶(COMT)基因与多巴胺D2受体基因/ANKK1基因的相互作用可解释γ神经振荡如何重新调整以适应听觉刺激驱动的注意力。

COMT and DRD2/ANKK-1 gene-gene interaction account for resetting of gamma neural oscillations to auditory stimulus-driven attention.

作者信息

Garcia-Garcia Manuel, Via Marc, Zarnowiec Katarzyna, SanMiguel Iria, Escera Carles, Clemente Immaculada C

机构信息

Institute of Neurosciences, University of Barcelona, Barcelona, Spain.

Brainlab-Cognitive Neuroscience Research Group, Department of Clinical Psychology and Psychobiology, University of Barcelona, Barcelona, Spain.

出版信息

PLoS One. 2017 Feb 21;12(2):e0172362. doi: 10.1371/journal.pone.0172362. eCollection 2017.

Abstract

Attention capture by potentially relevant environmental stimuli is critical for human survival, yet it varies considerably among individuals. A large series of studies has suggested that attention capture may depend on the cognitive balance between maintenance and manipulation of mental representations and the flexible switch between goal-directed representations and potentially relevant stimuli outside the focus of attention; a balance that seems modulated by a prefrontostriatal dopamine pathway. Here, we examined inter-individual differences in the cognitive control of attention through studying the effects of two single nucleotide polymorphisms regulating dopamine at the prefrontal cortex and the striatum (i.e., COMTMet108/158Val and ANKK1/DRD2TaqIA) on stimulus-driven attention capture. Healthy adult participants (N = 40) were assigned to different groups according to the combination of the polymorphisms COMTMet108/158Val and ANKK1/DRD2TaqIA, and were instructed to perform on a well-established distraction protocol. Performance in individuals with a balance between prefrontal dopamine display and striatal receptor density was slowed down by the occurrence of unexpected distracting events, while those with a rather unbalanced dopamine activity were able maintain task performance with no time delay, yet at the expense of a slightly lower accuracy. This advantage, associated to their distinct genetic profiles, was paralleled by an electrophysiological mechanism of phase-resetting of gamma neural oscillation to the novel, distracting events. Taken together, the current results suggest that the epistatic interaction between COMTVal108/158Met and ANKK1/DRD2 TaqIa genetic polymorphisms lies at the basis of stimulus-driven attention capture.

摘要

被潜在相关环境刺激捕获注意力对人类生存至关重要,但个体之间差异很大。大量研究表明,注意力捕获可能取决于心理表征的维持与操纵之间的认知平衡,以及目标导向表征与注意力焦点之外潜在相关刺激之间的灵活切换;这种平衡似乎由前额叶纹状体多巴胺通路调节。在此,我们通过研究调节前额叶皮质和纹状体多巴胺的两个单核苷酸多态性(即COMTMet108/158Val和ANKK1/DRD2TaqIA)对刺激驱动的注意力捕获的影响,来考察注意力认知控制中的个体差异。健康成年参与者(N = 40)根据COMTMet108/158Val和ANKK1/DRD2TaqIA多态性的组合被分配到不同组,并被要求执行一个成熟的分心任务协议。前额叶多巴胺表现与纹状体受体密度之间平衡的个体,其表现会因意外分心事件的出现而减慢,而多巴胺活动相当不平衡的个体能够在没有时间延迟的情况下维持任务表现,但代价是准确性略低。这种与他们独特基因特征相关的优势,伴随着伽马神经振荡对新奇分心事件进行相位重置的电生理机制。综上所述,当前结果表明COMTVal108/158Met和ANKK1/DRD2 TaqIa基因多态性之间的上位相互作用是刺激驱动的注意力捕获的基础。

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