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多巴胺拮抗作用在运动序列任务中的相反效应——硫必利增加皮质兴奋性并损害运动学习。

Opposing effects of dopamine antagonism in a motor sequence task-tiapride increases cortical excitability and impairs motor learning.

作者信息

Lissek Silke, Vallana Guido S, Schlaffke Lara, Lenz Melanie, Dinse Hubert R, Tegenthoff Martin

机构信息

Department of Neurology, BG University Hospital Bergmannsheil, Ruhr-University Bochum Bochum, Germany.

Department of Neurology, BG University Hospital Bergmannsheil, Ruhr-University Bochum Bochum, Germany ; Neural Plasticity Lab, Institute for Neuroinformatics, Ruhr-University Bochum Bochum, Germany.

出版信息

Front Behav Neurosci. 2014 Jun 19;8:201. doi: 10.3389/fnbeh.2014.00201. eCollection 2014.

Abstract

The dopaminergic system is involved in learning and participates in the modulation of cortical excitability (CE). CE has been suggested as a marker of learning and use-dependent plasticity. However, results from separate studies on either motor CE or motor learning challenge this notion, suggesting opposing effects of dopaminergic modulation upon these parameters: while agonists decrease and antagonists increase CE, motor learning is enhanced by agonists and disturbed by antagonists. To examine whether this discrepancy persists when complex motor learning and motor CE are measured in the same experimental setup, we investigated the effects of dopaminergic (DA) antagonism upon both parameters and upon task-associated brain activation. Our results demonstrate that DA-antagonism has opposing effects upon motor CE and motor sequence learning. Tiapride did not alter baseline CE, but increased CE post training of a complex motor sequence while simultaneously impairing motor learning. Moreover, tiapride reduced activation in several brain regions associated with motor sequence performance, i.e., dorsolateral PFC (dlPFC), supplementary motor area (SMA), Broca's area, cingulate and caudate body. Blood-oxygenation-level-dependent (BOLD) intensity in anterior cingulate and caudate body, but not CE, correlated with performance across groups. In summary, our results do not support a concept of CE as a general marker of motor learning, since they demonstrate that a straightforward relation of increased CE and higher learning success does not apply to all instances of motor learning. At least for complex motor tasks that recruit a network of brain regions outside motor cortex, CE in primary motor cortex is probably no central determinant for learning success.

摘要

多巴胺能系统参与学习过程,并参与调节皮层兴奋性(CE)。CE被认为是学习和使用依赖性可塑性的一个标志。然而,关于运动CE或运动学习的单独研究结果对这一观点提出了挑战,表明多巴胺能调节对这些参数具有相反的作用:激动剂会降低CE,而拮抗剂会增加CE,而激动剂会增强运动学习,拮抗剂则会干扰运动学习。为了研究在同一实验设置中测量复杂运动学习和运动CE时这种差异是否仍然存在,我们研究了多巴胺能(DA)拮抗对这两个参数以及与任务相关的脑激活的影响。我们的结果表明,DA拮抗对运动CE和运动序列学习具有相反的作用。硫必利不会改变基线CE,但在复杂运动序列训练后会增加CE,同时损害运动学习。此外,硫必利减少了与运动序列表现相关的几个脑区的激活,即背外侧前额叶皮层(dlPFC)、辅助运动区(SMA)、布洛卡区、扣带回和尾状体。前扣带回和尾状体的血氧水平依赖(BOLD)强度而非CE与各组的表现相关。总之,我们的结果不支持将CE作为运动学习的一般标志这一概念,因为它们表明CE增加与更高学习成功率之间的直接关系并不适用于所有运动学习实例。至少对于需要募集运动皮层以外的脑区网络的复杂运动任务,初级运动皮层中的CE可能不是学习成功的核心决定因素。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/837f/4063238/a902cb1baf9f/fnbeh-08-00201-g0001.jpg

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