认知灵活性的多巴胺能机制:一项基于PET的研究[18]。

Isabelle Miederer, Hans-Georg Buchholz, Lena Rademacher, Cindy Eckart, Dominik Kraft, Markus Piel, Christian J Fiebach, Mathias Schreckenberger
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引用次数: 0

摘要

认知灵活性是一种适当调整自己的思维和行为以适应不断变化的环境需求的能力,被概念化为执行功能的一个方面。多巴胺系统与认知灵活性有关;然而,与认知灵活性的直接联系,即神经化学方面的联系,尚未得到证实。因此,本研究的目的是研究认知灵活性是如何由腹内侧前额叶皮层(vmPFC)中的多巴胺能信号介导的。方法:在PET研究中,18名参与者采用2部分块设计测量了174±12 MBq的D2/3受体配体[18F]。虽然参与者在PET扫描的第一部分中没有在电脑屏幕上切换规则,但在第二部分注射100分钟后,他们必须灵活地在两个任务规则之间切换。多巴胺释放(γ)使用线性化简化参考区域模型进行量化,对比两个任务块(切换与无切换/基线)。结果:参数γ-图像的统计分析显示,任务转换过程中认知需求的增加引起了vmPFC中D2/3受体配体[18F]fallypride的移位(最大T值= 13.8;簇大小:528体素;家庭误差率校正P < 0.001;平均γ = 0.022±0.006 min-1)。此外,行为转换成本与vmPFC之间的相关性[18F]表明,多巴胺释放更多的参与者在任务转换中效率更高。结论:据我们所知,这是第一个显示多巴胺在任务转换范式中直接参与vmPFC的实验PET研究,证实了关于认知灵活性的神经化学基础的模型假设。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Dopaminergic Mechanisms of Cognitive Flexibility: An [18F]Fallypride PET Study.

Cognitive flexibility is the ability to appropriately adapt one's thinking and behavior to changing environmental demands and is conceptualized as an aspect of executive function. The dopamine system has been implicated in cognitive flexibility; however, a direct, that is, neurochemical, link to cognitive flexibility has not been shown yet. The aim of this study was, therefore, to investigate how cognitive flexibility is mediated by dopaminergic signaling in the ventromedial prefrontal cortex (vmPFC). Methods: Eighteen participants were measured in a PET study with 174 ± 12 MBq of the D2/3 receptor ligand [18F]fallypride in a block design with 2 parts. While participants processed 2 tasks sequentially without rule switching on a computer screen in the first part of the PET scan, they had to flexibly switch between the 2 task rules after 100 min after injection in the second part. Dopamine release (γ) was quantified using the linearized simplified reference region model contrasting the 2 task blocks (switching vs. no-switching/baseline). Results: The statistical analysis of the parametric γ-images showed that the increased cognitive demand during task switching induced a displacement of the D2/3 receptor ligand [18F]fallypride in the vmPFC (maximum T value = 13.8; cluster size: 528 voxels; familywise error rate-corrected P < 0.001; mean γ = 0.022 ± 0.006 min-1). Furthermore, a correlation between behavioral switch costs and vmPFC [18F]fallypride displacement suggested that participants showing greater dopamine release were more efficient in task switching. Conclusion: To our knowledge, this is the first experimental PET study to show direct involvement of dopamine in the vmPFC in a task-switching paradigm, confirming model assumptions about the neurochemical basis of cognitive flexibility.

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