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多巴胺受体介导的机制参与灵长类动物纹状体神经元习得性活动的表达。

Dopamine receptor-mediated mechanisms involved in the expression of learned activity of primate striatal neurons.

作者信息

Watanabe K, Kimura M

机构信息

Faculty of Health and Sport Sciences, Osaka University, Toyonaka, Osaka 560.

出版信息

J Neurophysiol. 1998 May;79(5):2568-80. doi: 10.1152/jn.1998.79.5.2568.

Abstract

To understand the mechanisms by which basal ganglia neurons express acquired activities during and after behavioral learning, selective dopamine (DA) receptor antagonists were applied while recording the activity of striatal neurons in monkeys performing behavioral tasks. In experiment 1, a monkey was trained to associate a click sound with a drop of reward water. DA receptor antagonists were administered by micropressure using a stainless steel injection cannula (300 microm ID) through which a Teflon-coated tungsten wire for recording neuronal activity had been threaded. Responses to sound by tonically active neurons (TANs), a class of neurons in the primate striatum, were recorded through a tungsten wire electrode during the application of either D1- or D2-class DA receptor antagonists (total volume <1 microl, at a rate of 1 microl/5-10 min). Application of the D2-class antagonist, (-)-sulpiride (20 micrograms/microl, 58 mM, pH 6.8), abolished the responses of four of five TANs examined. In another five TANs, neither the D2-class antagonist nor the D1-class antagonists, SCH23390 (10 micrograms/microl, 31 mM, pH 5.7) or cis-flupenthixol (30 micrograms/microl, 59 mM, pH 6.6) significantly suppressed responses. In experiment 2, four- or five-barreled glass microelectrodes were inserted into the striatum. The central barrel was used for extracellular recording of activity of TANs. Each DA receptor antagonist was iontophoretically applied through one of the surrounding barrels. SCH23390 (10 mM, pH 4.5) and (-)-sulpiride (10 mM, pH 4.5) were used. The effects of iontophoresis of both D1- and D2-class antagonists were examined in 40 TANs. Of 40 TANs from which recordings were made, responses were suppressed exclusively by the D2-class antagonist in 19 TANs, exclusively by the D1-class antagonist in 3 TANs, and by both D1- and D2-class antagonists in 7 TANs. When 0.9% NaCl, saline, was applied by pressure (<1 microl) or by iontophoresis (<30 nA) as a control, neither the background discharge rates nor the responses of TANs were significantly influenced. Background discharge rate of TANs was also not affected by D1- or D2-class antagonists applied by either micropressure injection or iontophoresis. It was concluded that the nigrostriatal DA system enables TANs to express learned activity primarily through D2-class and partly through D1-class receptor-mediated mechanisms in the striatum.

摘要

为了解基底神经节神经元在行为学习期间及之后表达习得性活动的机制,在记录猴子执行行为任务时纹状体神经元活动的同时,应用了选择性多巴胺(DA)受体拮抗剂。在实验1中,训练一只猴子将点击声与一滴奖励水联系起来。使用不锈钢注射套管(内径300微米)通过微压给药DA受体拮抗剂,一根涂有聚四氟乙烯的钨丝穿过该套管用于记录神经元活动。在应用D1类或D2类DA受体拮抗剂(总体积<1微升,以1微升/5 - 10分钟的速率)期间,通过钨丝电极记录灵长类纹状体中一类神经元——紧张性活动神经元(TANs)对声音的反应。应用D2类拮抗剂(-)-舒必利(20微克/微升,58毫摩尔,pH 6.8)使所检测的5个TANs中的4个的反应消失。在另外5个TANs中,D2类拮抗剂以及D1类拮抗剂SCH23390(10微克/微升,31毫摩尔,pH 5.7)或顺式氟奋乃静(30微克/微升,59毫摩尔,pH 6.6)均未显著抑制反应。在实验2中,将四管或五管玻璃微电极插入纹状体。中央管用于细胞外记录TANs的活动。每种DA受体拮抗剂通过周围的一个管进行离子电渗法给药。使用了SCH23390(10毫摩尔,pH 4.5)和(-)-舒必利(10毫摩尔,pH 4.5)。在40个TANs中检测了D1类和D2类拮抗剂离子电渗法的效果。在进行记录的40个TANs中,19个TANs的反应仅被D2类拮抗剂抑制,3个TANs的反应仅被D1类拮抗剂抑制,7个TANs的反应被D1类和D2类拮抗剂均抑制。当通过压力(<1微升)或离子电渗法(<30纳安)应用0.9%氯化钠溶液(生理盐水)作为对照时,TANs的背景放电率和反应均未受到显著影响。通过微压注射或离子电渗法应用D1类或D2类拮抗剂也未影响TANs的背景放电率。得出的结论是,黑质纹状体DA系统使TANs能够主要通过D2类且部分通过D1类受体介导的机制在纹状体中表达习得性活动。

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