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γ-羟基丁酸(GHB)和GABA-B受体在狒狒中对GHB急性行为效应的影响。

Involvement of gamma-hydroxybutyrate (GHB) and GABA-B receptors in the acute behavioral effects of GHB in baboons.

作者信息

Goodwin Amy K, Froestl Wolfgang, Weerts Elise M

机构信息

Johns Hopkins Bayview, Behavioral Biology Research Center, 5510 Nathan Shock Dr., Suite 3000, Baltimore, MD 21224, USA.

出版信息

Psychopharmacology (Berl). 2005 Jul;180(2):342-51. doi: 10.1007/s00213-005-2165-y. Epub 2005 Mar 1.

Abstract

RATIONALE

Gamma-hydroxybutyrate (GHB) is used for the treatment of narcolepsy, but it is also a drug of abuse. The behavioral pharmacology of GHB is not well defined.

OBJECTIVES

The current study was conducted to characterize the behavioral effects of a range of GHB doses in baboons (N=4) and to evaluate whether a GABA-B receptor antagonist and a GHB receptor antagonist would block a behaviorally active dose of GHB.

METHODS

In the first experiment, GHB (32-420 mg/kg) or vehicle was administered via an intragastric catheter. Sixty min after dosing, subjects were presented with a fine-motor task and observed. Food pellets were available under a fixed-ratio schedule of reinforcement 20-h/day. In the second experiment, the GABA-B antagonist CGP36742 (10-56 mg/kg), the putative GHB antagonist NCS-382 (0.1-10 mg/kg), or vehicle were administered alone and then in combination with GHB (320 mg/kg).

RESULTS

GHB dose-dependently decreased the number of food pellets earned. Performance in the motor task was also impaired and accompanied by signs of sedation and gastrointestinal discomfort. Pretreatment with CGP36742 antagonized GHB-induced suppression of food-maintained behavior and performance on the fine-motor task. Signs of abdominal discomfort, ataxia, and muscle relaxation produced by GHB were also reduced by pretreatment with CGP36742. In contrast, pretreatment with NCS-382 sometimes restored performance in the fine-motor task and increased food-maintained behavior, but the effect was variable across doses and baboons. Some doses of NCS-382 appeared to exacerbate ataxia and gastrointestinal discomfort produced by GHB in some subjects.

CONCLUSIONS

These data indicate that while GABA-B receptors play a significant role in mediating the behavioral effects of GHB in baboon, the role of GHB receptors is less clear.

摘要

理论依据

γ-羟基丁酸(GHB)用于治疗发作性睡病,但它也是一种滥用药物。GHB的行为药理学尚未明确界定。

目的

本研究旨在描述一系列GHB剂量对狒狒(N = 4)行为的影响,并评估GABA-B受体拮抗剂和GHB受体拮抗剂是否会阻断具有行为活性剂量的GHB。

方法

在第一个实验中,通过胃内导管给予GHB(32 - 420mg/kg)或赋形剂。给药60分钟后,让受试者进行精细运动任务并观察。每天20小时按固定比率强化程序提供食物颗粒。在第二个实验中,单独给予GABA-B拮抗剂CGP36742(10 - 56mg/kg)、假定的GHB拮抗剂NCS-382(0.1 - 10mg/kg)或赋形剂,然后与GHB(320mg/kg)联合给予。

结果

GHB剂量依赖性地减少了获得的食物颗粒数量。运动任务的表现也受到损害,并伴有镇静和胃肠道不适的迹象。用CGP36742预处理可拮抗GHB诱导的对食物维持行为和精细运动任务表现的抑制。CGP36742预处理还减少了GHB引起的腹部不适、共济失调和肌肉松弛的迹象。相比之下,用NCS-382预处理有时可恢复精细运动任务的表现并增加食物维持行为,但效果因剂量和狒狒而异。某些剂量的NCS-382似乎会加重GHB在某些受试者中引起的共济失调和胃肠道不适。

结论

这些数据表明,虽然GABA-B受体在介导GHB对狒狒行为的影响中起重要作用,但GHB受体的作用尚不清楚。

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