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阿扑吗啡和氟哌啶醇对麻醉、清醒拘束及自由活动大鼠纹状体3H-多巴胺释放的影响。

Apomorphine and haloperidol effects on striatal 3H-dopamine release in anesthetized, awake restrained and freely moving rats.

作者信息

Spampinato U, Girault J A, Danguir J, Savaki H E, Glowinski J, Besson M J

出版信息

Brain Res Bull. 1986 Feb;16(2):161-6. doi: 10.1016/0361-9230(86)90028-6.

DOI:10.1016/0361-9230(86)90028-6
PMID:3697784
Abstract

The ability of apomorphine (APO) and haloperidol (HAL) to affect the spontaneous release of newly synthesized 3H-DA in the striatum was studied in halothane anesthetized, gallamine paralyzed, awake restrained and freely moving rats. The striatum was continuously superfused through a push-pull cannula with a physiological medium enriched in 3H-tyrosine. Basal levels of 3H-DA release were different in the four experimental models: highest in halothane anesthetized rats, intermediate in awake restrained and gallamine treated rats and lowest in freely moving rats. In all experimental models IV or SC injection of APO (1 mg/kg) inhibited the release of 3H-DA (30-50%) from 15 to 90 min following its administration. In awake restrained and freely moving rats, stereotyped behaviour was observed for one hour following the APO injection. In halothane anesthetized rats the inhibitory effect of APO on 3H-DA release was prevented by pretreatment with HAL (2 mg/kg IV). Injection of HAL (2 mg/kg IV or SC) failed to enhance the release of 3H-DA in anesthetized and awake restrained rats, whilst a long-lasting increase in 3H-DA release was observed in gallamine treated and freely moving animals (55% and 120% respectively). However, catalepsy was observed in both restrained and freely moving rats. It is concluded that the modifications of 3H-DA release produced by HAL but not those produced by APO are dependent on the experimental model used, a fact possibly related to the different sites of action of these two drugs.

摘要

在氟烷麻醉、加拉明麻痹、清醒束缚和自由活动的大鼠中,研究了阿扑吗啡(APO)和氟哌啶醇(HAL)对纹状体中新合成的3H-多巴胺自发释放的影响。通过推挽式套管用富含3H-酪氨酸的生理介质连续灌流纹状体。在四种实验模型中,3H-多巴胺释放的基础水平有所不同:在氟烷麻醉的大鼠中最高,在清醒束缚和加拉明处理的大鼠中居中,在自由活动的大鼠中最低。在所有实验模型中,静脉注射或皮下注射APO(1mg/kg)在给药后15至90分钟内抑制了3H-多巴胺的释放(30-50%)。在清醒束缚和自由活动的大鼠中,注射APO后一小时观察到刻板行为。在氟烷麻醉的大鼠中,HAL(2mg/kg静脉注射)预处理可防止APO对3H-多巴胺释放的抑制作用。注射HAL(2mg/kg静脉注射或皮下注射)未能增强麻醉和清醒束缚大鼠中3H-多巴胺的释放,而在加拉明处理和自由活动的动物中观察到3H-多巴胺释放的持久增加(分别为55%和120%)。然而,在束缚和自由活动的大鼠中均观察到僵住症。得出的结论是,HAL引起的3H-多巴胺释放的改变而非APO引起的改变取决于所使用的实验模型,这一事实可能与这两种药物的不同作用部位有关。

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