GABAA/α1受体激动剂和拮抗剂：对小鼠酒精自我给药后物种典型和增强的攻击行为的影响。

GABAA/alpha1 receptor agonists and antagonists: effects on species-typical and heightened aggressive behavior after alcohol self-administration in mice.

作者信息

de Almeida Rosa M M, Rowlett James K, Cook James M, Yin Wenyuan, Miczek Klaus A

机构信息

Department of Psychology, Tufts University, Bacon Hall, 530 Boston Avenue, Medford, MA 02155, USA.

出版信息

Psychopharmacology (Berl). 2004 Mar;172(3):255-63. doi: 10.1007/s00213-003-1661-1. Epub 2003 Nov 25.

DOI:10.1007/s00213-003-1661-1

PMID:14647970

Abstract

RATIONALE

The positive modulation of gamma-aminobutyric acid type-A (GABAA) receptors is a putative mechanism via which alcohol escalates aggressive behavior. Broad-spectrum benzodiazepine antagonists block alcohol-heightened aggression in rats and monkeys. However, the degree to which GABAA subunit composition plays a role in heightened aggressive behavior induced by self-administration of a moderate alcohol dose remains unresolved.

OBJECTIVE

Beta-carboline-3-carboxylate-t-butyl ester (beta-CCt) and zolpidem act preferentially at GABAA receptors containing the alpha1 subunit as antagonist and agonist, respectively, and serve as useful tools to evaluate the role of GABAA receptor subtypes in self-administered alcohol on aggression.

METHODS

Male resident mice, housed in breeding pairs, were conditioned to nose-poke in a removable panel in their home cage, with each fifth poke being reinforced by the delivery of 0.05 ml of 6% ethanol (EtOH). After consuming EtOH, the resident mice were given the antagonists beta-CCt and flumazenil or agonists zolpidem and triazolam, and then confronted an intruder male in their home cage for a 5-min period.

RESULTS

Following self-administration of EtOH (1.0 g/kg, 1.7 g/kg), 14 of 37 resident mice displayed unusually large increases in the frequency of attack bites and sideways threats. Flumazenil or beta-CCt decreased alcohol-heightened and non-heightened aggression in a dose-dependent manner. Administration of 3 mg/kg beta-CCt lowered the aggression-heightening effects of 1 g/kg and 1.7 g/kg EtOH, but did not antagonize the sedative effects of 3.0 g/kg EtOH. Triazolam and zolpidem decreased alcohol-heightened and non-heightened aggressive behavior, and these antiaggressive effects were accompanied by reduced motor activity, indicating sedation.

CONCLUSIONS

Benzodiazepine antagonists, particularly those acting preferentially at GABAA/alpha1 subunit-containing receptors, decrease alcohol-heightened and species-typical aggressive behavior, but are ineffective in attenuating the sedative effects of alcohol.

摘要

理论依据

γ-氨基丁酸A型（GABAA）受体的正向调节是酒精加剧攻击行为的一种推测机制。广谱苯二氮䓬拮抗剂可阻断大鼠和猴子中酒精引发的攻击行为增强。然而，GABAA亚基组成在中等剂量酒精自我给药诱导的攻击行为增强中所起作用的程度仍未明确。

目的

β-咔啉-3-羧酸叔丁酯（β-CCt）和唑吡坦分别作为拮抗剂和激动剂，优先作用于含有α1亚基的GABAA受体，是评估GABAA受体亚型在酒精自我给药对攻击行为影响中作用的有用工具。

方法

将成对饲养的雄性常驻小鼠训练至在其饲养笼中的可移动面板上戳鼻，每第五次戳鼻会给予0.05毫升6%乙醇（EtOH）作为强化。在摄入EtOH后，给常驻小鼠注射拮抗剂β-CCt和氟马西尼或激动剂唑吡坦和三唑仑，然后在其饲养笼中与一只入侵雄性小鼠对峙5分钟。

结果

在自我给药EtOH（1.0克/千克，1.7克/千克）后，37只常驻小鼠中有14只的攻击咬伤频率和侧向威胁频率出现异常大幅增加。氟马西尼或β-CCt以剂量依赖方式降低酒精增强和未增强的攻击行为。给予3毫克/千克的β-CCt可降低1克/千克和1.7克/千克EtOH的攻击增强作用，但不拮抗3.0克/千克EtOH的镇静作用。三唑仑和唑吡坦降低酒精增强和未增强的攻击行为，且这些抗攻击作用伴随着运动活动减少，表明有镇静作用。

结论

苯二氮䓬拮抗剂，尤其是那些优先作用于含GABAA/α1亚基受体的拮抗剂，可降低酒精增强和物种典型的攻击行为，但在减轻酒精的镇静作用方面无效。

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GABAA/α1受体激动剂和拮抗剂：对小鼠酒精自我给药后物种典型和增强的攻击行为的影响。

GABAA/alpha1 receptor agonists and antagonists: effects on species-typical and heightened aggressive behavior after alcohol self-administration in mice.

作者信息

机构信息

出版信息

RATIONALE

OBJECTIVE

METHODS

RESULTS

CONCLUSIONS

理论依据

目的

方法

结果

结论

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