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将苯二氮䓬确立为口服强化剂:恒河猴对咪达唑仑和地西泮的自我给药

Establishing benzodiazepines as oral reinforcers: midazolam and diazepam self-administration in rhesus monkeys.

作者信息

Stewart R B, Lemaire G A, Roache J D, Meisch R A

机构信息

Department of Psychiatry and Behavioral Sciences, University of Texas, Houston Health Science Center, Houston.

出版信息

J Pharmacol Exp Ther. 1994 Oct;271(1):200-11.

PMID:7965716
Abstract

Oral benzodiazepine self-administration was examined in four adult male rhesus monkeys with histories of ethanol- and pentobarbital-reinforced behavior. Drug solutions and vehicle were concurrently available for 3-hr each day under fixed-ratio (FR) reinforcement schedules. Initially, the monkeys rejected a midazolam solution (0.1 mg/ml) after direct substitution of the drug for an 8% ethanol solution. However, midazolam self-administration was subsequently established by using a fading procedure in which increasing amounts of drug (0.0125-0.2 mg/ml) were gradually added to an 8% ethanol solution, followed by gradual reduction of the ethanol concentration to zero. Midazolam was an effective reinforcer for three of four monkeys tested, i.e., responding that was maintained by the drug solution exceeded that maintained by the drug vehicle. The fourth monkey also self-administered midazolam but drug-maintained responding was not consistently greater than vehicle-maintained responding. The responding maintained by the drug was an inverted-U-shaped or bitonic function of midazolam concentration. The midazolam intake (in milligrams per kilogram) increased as a function of increases in the drug concentration. At the higher concentrations, marked sedative intoxication was observed. There was an inverse relationship between FR size (varied from FR 8 to FR 32) and the amount of drug self-administered. The three monkeys in which midazolam functioned as a reinforcer were then tested with diazepam (0.2 mg/ml), which maintained drug self-administration behavior on direct substitution for 0.2-mg/ml midazolam. Diazepam-maintained responding usually exceeded water responding as the diazepam concentration was increased to 0.8 mg/ml. These data demonstrate robust reinforcing effects of both "short-" and "long-acting" benzodiazepines delivered by the oral route.

摘要

在四只具有乙醇和戊巴比妥强化行为史的成年雄性恒河猴中研究了口服苯二氮䓬类药物的自我给药情况。在固定比率(FR)强化程序下,每天同时提供药物溶液和溶剂3小时。最初,在用咪达唑仑溶液(0.1毫克/毫升)直接替代8%乙醇溶液后,猴子拒绝了该溶液。然而,随后通过一种递减程序建立了咪达唑仑的自我给药,即在8%乙醇溶液中逐渐加入越来越多的药物(0.0125 - 0.2毫克/毫升),然后将乙醇浓度逐渐降至零。对于四只接受测试的猴子中的三只,咪达唑仑是一种有效的强化剂,即由药物溶液维持的反应超过了由溶剂维持的反应。第四只猴子也自我给药咪达唑仑,但药物维持的反应并不始终大于溶剂维持的反应。由药物维持的反应是咪达唑仑浓度的倒U形或双峰函数。咪达唑仑摄入量(每千克毫克数)随药物浓度增加而增加。在较高浓度下,观察到明显的镇静性中毒。FR大小(从FR 8变化到FR 32)与自我给药的药物量之间存在反比关系。然后用0.2毫克/毫升的地西泮对三只将咪达唑仑用作强化剂的猴子进行测试,直接替代0.2毫克/毫升咪达唑仑时,地西泮维持了药物自我给药行为。随着地西泮浓度增加到0.8毫克/毫升,地西泮维持的反应通常超过水维持的反应。这些数据表明口服途径给药的“短效”和“长效”苯二氮䓬类药物均具有强大的强化作用。

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