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D1 和 D2 多巴胺激动剂对非人类灵长类动物的记忆、动机、学习和反应时间的影响差异。

Differential effects of D1 and D2 dopamine agonists on memory, motivation, learning and response time in non-human primates.

机构信息

Centre for Neuroscience Studies, Queen's University, Kingston, Ontario, Canada.

Department of Surgery, Kingston General Hospital, Kingston, Ontario, Canada.

出版信息

Eur J Neurosci. 2019 Jan;49(2):199-214. doi: 10.1111/ejn.14208. Epub 2018 Nov 12.

Abstract

Dopamine (DA) plays a critical role in cognition, motivation and information processing. DA action has been shown to both improve and/or impair cognition across different receptor types, species, subjects and tasks. This complex relationship has been described as an inverted U-shaped function and may be due to the differential effects of DA receptor activation in the striatum and prefrontal cortex. We have investigated the effects of selective DA agonists on cognitive performance in healthy monkeys using a touch screen running tasks from the CAmbridge Neuropsychological Test Automated Battery (CANTAB). One of two DA agonist drugs or placebo was administered prior to each daily CANTAB session: Dihydrexidine hydrochloride (selective D1 agonist, 0.4-0.9 mg/kg), or sumanirole maleate (selective D2 agonist 0.05-0.3 mg/kg). Three CANTAB tasks were tested: (a) "self-ordered sequential search task" which tested spatial working memory, (b) "reversal learning task," which tested association learning, cognitive flexibility and attention and (c) "visually guided reaching task," which tested reaction time and accuracy. At high dosages, the D2 agonist improved spatial working memory performance, while impairing reversal learning and slowing reach response latency. No consistent cognitive effects were observed with the D1 agonist across the dosages tested. A significant decrease in trial completion rate was observed at the higher dosages of both the D1 and D2 agonists which were consistent with decreased motivation. These results are consistent with task-specific effects of a D2 agonist as well as dose specific insensitivities of a D1 agonist on cognitive and motor behaviors in a healthy monkey.

摘要

多巴胺(DA)在认知、动机和信息处理中起着关键作用。不同受体类型、物种、对象和任务的研究都表明,DA 作用既可以改善,也可以损害认知。这种复杂的关系被描述为倒 U 形函数,这可能是由于 DA 受体激活在纹状体和前额叶皮层的差异作用。我们使用剑桥神经心理学测试自动化电池(CANTAB)的触摸屏运行任务,研究了选择性 DA 激动剂对健康猴子认知表现的影响。在每天的 CANTAB 会议之前,给猴子服用两种 DA 激动剂药物之一或安慰剂:二氢麦角隐亭盐酸盐(选择性 D1 激动剂,0.4-0.9mg/kg)或琥珀酸舒马曲普坦(选择性 D2 激动剂,0.05-0.3mg/kg)。测试了三个 CANTAB 任务:(a)“自我有序序列搜索任务”,用于测试空间工作记忆;(b)“反转学习任务”,用于测试联想学习、认知灵活性和注意力;(c)“视觉引导到达任务”,用于测试反应时间和准确性。在高剂量下,D2 激动剂改善了空间工作记忆表现,而损害了反转学习并减缓了到达反应潜伏期。在测试的剂量范围内,D1 激动剂没有观察到一致的认知效应。在高剂量下,D1 和 D2 激动剂都观察到试验完成率显著下降,这与动机降低一致。这些结果与 D2 激动剂的任务特异性效应以及 D1 激动剂在健康猴子认知和运动行为上的剂量特异性不敏感性一致。

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