Differential effects of dopamine agonists on locomotion in intact and reserpine-treated mice.

M R Zarrindast, A Eliassi
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引用次数: 17

Abstract

1. Apomorphine and bromocriptine induced a dose-dependent locomotion in mice. The responses of both drugs were decreased by SCH 23390 or sulpiride pretreatment. 2. Locomotor activity induced by apomorphine was increased and that of bromocriptine was decreased by reserpine. 3. SKF 38393 or quinpirole also induced locomotion. The response of SKF 38393 was decreased by reserpine. 4. Combination of SKF 38393 with bromocriptine induced a significant locomotor activity different from that of SKF 38393 or bromocriptine in reserpinized animals. 5. Combination of quinpirole with bromocriptine even decreased the response of bromocriptine in intact animals. 6. In conclusion, bromocriptine needs intact dopaminergic neurons and activation of D-1 receptor for expression of locomotion. High doses of quinpirole may induce locomotor activity possibly through D-1/D-2 receptor activation and quinpirole may potentiate the effect of bromocriptine on autoreceptor for inducing sedation.

多巴胺激动剂对完整小鼠和利血平小鼠运动的不同影响。
1. 阿波啡和溴隐亭诱导小鼠剂量依赖性运动。经SCH 23390或舒必利预处理后,两种药物的疗效均下降。2. 阿波啡引起的运动活性增加,利血平引起的溴隐亭运动活性降低。3.SKF 38393或喹匹罗也能引起运动。利血平降低SKF 38393的疗效。4. 在利血平化动物中,SKF 38393与溴隐亭联合使用可诱导明显不同于SKF 38393或溴隐亭的运动活性。5. 喹匹罗与溴隐亭联用甚至降低了完好动物对溴隐亭的反应。6. 综上所述,溴隐亭的运动表达需要完整的多巴胺能神经元和D-1受体的激活。高剂量喹匹罗可能通过激活D-1/D-2受体诱导大鼠的运动活动,而喹匹罗可能增强溴隐亭对自身受体的诱导镇静作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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