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Dopamine's Actions in Primate Prefrontal Cortex: Challenges for Treating Cognitive Disorders

机译:多巴胺在灵长类动物前额叶皮层中的作用:应对认知障碍的挑战。

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The prefrontal cortex (PFC) elaborates and differentiates in primates, and there is a corresponding elaboration in cortical dopamine (DA). DA cells that fire to both aversive and rewarding stimuli likely project to the dorsolateral PFC (dlPFC), signaling a salient event. Since 1979, we have known that DA has an essential influence on dlPFC working memory functions. DA has differing effects via D1 (D1R) versus D2 receptor (D2R) families. D1R are concentrated on dendritic spines, and D1/5R stimulation produces an inverted U-shaped dose response on visuospatial working memory performance and Delay cell firing, the neurons that generate representations of visual space. Optimal levels of D1R stimulation gate out "noise," whereas higher levels, e.g., during stress, suppress Delay cell firing. These effects likely involve hyperpolarization-activated cyclic nucleotide-gated channel opening, activation of GABA interneurons, and reduced glutamate release. Dysregulation of D1R has been related to cognitive deficits in schizophrenia, and there is a need for new, lower-affinity D1R agonists that may better mimic endogenous DA to enhance mental representations and improve cognition. In contrast to D1R, D2R are primarily localized on layer V pyramidal cell dendrites, and D2/3R stimulation speeds and magnifies the firing of Response cells, including Response Feedback cells. Altered firing of Feedback neurons may relate to positive symptoms in schizophrenia. Emerging research suggests that DA may have similar effects in the ventrolateral PFC and frontal eye fields. Research on the orbital PFC in monkeys is just beginning and could be a key area for future discoveries.
机译:前额叶皮层(PFC)在灵长类动物中细化和分化,而皮质多巴胺(DA)也有相应的作用。对厌恶和奖励刺激均有效的DA细胞可能投射到背外侧PFC(dlPFC),这标志着一个突出事件。自1979年以来,我们就知道DA对dlPFC工作记忆功能具有至关重要的影响。 DA通过D1(D1R)与D2受体(D2R)家族具有不同的作用。 D1R集中在树突棘上,D1 / 5R刺激在视觉空间工作记忆表现和延迟细胞放电(产生视觉空间表示的神经元)上产生倒U型剂量反应。最佳水平的D1R刺激可以消除“噪音”,而较高的水平(例如在压力期间)可以抑制“延迟细胞发射”。这些作用可能涉及超极化激活的环状核苷酸门控通道的开放,GABA interneurons的激活和谷氨酸释放的减少。 D1R的失调与精神分裂症的认知缺陷有关,因此需要一种新的,较低亲和力的D1R激动剂,以更好地模仿内源性DA来增强心理表现并改善认知能力。与D1R不同,D2R主要位于V层锥体细胞树突上,D2 / 3R刺激速度加快并放大了包括反应反馈细胞在内的反应细胞的放电。反馈神经元放电的改变可能与精神分裂症的阳性症状有关。新兴研究表明,DA在腹外侧PFC和额眼视野中可能具有类似的作用。对猴子中的轨道PFC的研究才刚刚开始,可能成为未来发现的关键领域。

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