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帕吉林诱发吗啡依赖小鼠的戒断样综合征

Precipitation of abstinence-like syndrome in morphine-dependent mice by pargyline.

作者信息

Way E L, Iwamoto E T, Khanna S, Ho I K, Shen F, Loh H H

出版信息

J Pharmacol Exp Ther. 1976 Nov;199(2):400-7.

PMID:10429
Abstract

In mice rendered morphine-dependent by pellet implantation for 3 days, the administration of pargyline 6 hours after pellet removal intensified narcotic abstinence behavior, particularly the narcotic withdrawal jumping response. Pargyline, 75 mg/kg i.p., caused a 6- to 9-fold increase in the incidence of jumping in mice withdrawing from morphine 6 hours after removal of the pellet, whereas this effect was not observed: 1) 1 hour after the injection of pargyline or 2) in animals still implanted with the morphine pellet. The median effective dose (ED50) of pargyline required to elicit withdrawal jumping in mice implanted with morphine decreased with increasing physical dependence. The ED50 for 72 hours was about one-sixth that after 24 hours of implantation. Additionally, pargyline potentiated naloxone-precipitated withdrawal jumping as evidenced by a reduction of the naloxone ED50 by approximately one-half. Administration of other monoamine oxidase inhibitors such as pheniprazine, iproiazid or tranylcypromine failed to alter the indicence of jumping in dependent mice undergoind abrupt morphine with drawal. Further, dopamine receptor stimulation by amphetamine, pheniprazine or amantadine antagonized the pargyline-induced jumping response. These data suggest that the increased incidence of withdrawal jumping observed after pargyline in morphine-dependent mice is not related to monoamine oxidase inhibition but rather to a possible pargyline-induced decrease in dopaminergic activity.

摘要

通过植入药丸使小鼠吗啡依赖3天后,在取出药丸6小时后给予帕吉林会加剧戒断行为,尤其是戒断跳跃反应。腹腔注射75mg/kg的帕吉林,会使取出药丸6小时后正在戒除吗啡的小鼠的跳跃发生率增加6至9倍,而在以下情况未观察到这种效应:1)注射帕吉林1小时后;2)仍植入吗啡药丸的动物。在植入吗啡的小鼠中引发戒断跳跃所需的帕吉林的半数有效剂量(ED50)随着身体依赖性的增加而降低。72小时的ED50约为植入24小时后的六分之一。此外,帕吉林增强了纳洛酮诱发的戒断跳跃,纳洛酮的ED50降低了约一半就证明了这一点。给予其他单胺氧化酶抑制剂,如苯乙肼、异烟肼或反苯环丙胺,未能改变依赖小鼠突然戒除吗啡时的跳跃发生率。此外,苯丙胺、苯乙肼或金刚烷对多巴胺受体的刺激拮抗了帕吉林诱导的跳跃反应。这些数据表明,吗啡依赖小鼠在帕吉林给药后观察到的戒断跳跃发生率增加与单胺氧化酶抑制无关,而是可能与帕吉林诱导的多巴胺能活性降低有关。

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