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尼古丁的长期治疗增强了调节大鼠纹状体多巴胺释放的多巴胺自身受体的敏感性。

[Chronic treatment with nicotine enhances the sensitivity of dopamine autoreceptors that modulate dopamine release from the rat striatum].

作者信息

Takaki T

机构信息

Institute of Brain Diseases, Kurume University School of Medicine, Japan.

出版信息

Nihon Shinkei Seishin Yakurigaku Zasshi. 1995 Aug;15(4):335-44.

PMID:7584728
Abstract

This study was undertaken to investigate the effect of chronic nicotine treatment on electrically evoked dopamine (DA) release from striatal slices and locomotor activity in rats under the influence of DA autoreceptor agonists and antagonist. Nicotine was supplied chronically by Alzet osmotic minipump for two weeks. B-HT920 and quinpirole decreased and (-)-sulpiride increased the evoked DA release from striatal slices. The B-HT920 and quinpirole-induced decrease and the (-)-sulpiride-induced increase in evoked DA release were enhanced by chronic treatment with nicotine. Nicotine itself has little effect on the evoked DA release. B-HT920 and quinpirole decreased and (-)-sulpiride, methamphetamine and apomorphine increased the locomotor activity in the rat. The B-HT920 and quinpirole-induced decrease and the (-)-sulpiride-induced increase in locomotor activity were enhanced by chronic treatment with nicotine. On the other hand, the methamphetamine and apomorphine-induced increase in locomotor activity were unaltered by chronic treatment with nicotine. Chronic nicotine treatment itself has no effect on locomotor activity. These data indicate that chronic treatment with nicotine caused a supersensitivity in presynaptic DA autoreceptors that modulate DA release from DA terminals in the rat striatum, and no change in the function of postsynaptic DA receptors.

摘要

本研究旨在探讨慢性尼古丁处理对大鼠纹状体切片中电诱发多巴胺(DA)释放以及在DA自身受体激动剂和拮抗剂影响下大鼠运动活性的作用。尼古丁通过Alzet渗透微型泵持续给药两周。B-HT920和喹吡罗降低,而(-)-舒必利增加纹状体切片中诱发的DA释放。尼古丁慢性处理增强了B-HT920和喹吡罗引起的诱发DA释放的降低以及(-)-舒必利引起的诱发DA释放的增加。尼古丁本身对诱发的DA释放影响很小。B-HT920和喹吡罗降低,而(-)-舒必利、甲基苯丙胺和阿扑吗啡增加大鼠的运动活性。尼古丁慢性处理增强了B-HT920和喹吡罗引起的运动活性降低以及(-)-舒必利引起的运动活性增加。另一方面,尼古丁慢性处理未改变甲基苯丙胺和阿扑吗啡引起的运动活性增加。尼古丁慢性处理本身对运动活性无影响。这些数据表明,尼古丁慢性处理导致大鼠纹状体中调节DA终末DA释放的突触前DA自身受体超敏,且对突触后DA受体功能无影响。

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