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在固定连续数给药方案下对大鼠进行阿片类激动剂和拮抗剂效果的评估。

Evaluation of the effects of opioid agonists and antagonists under a fixed-consecutive-number schedule in rats.

作者信息

Picker M, Heise J W, Dykstra L A

出版信息

Pharmacol Biochem Behav. 1987 May;27(1):73-80. doi: 10.1016/0091-3057(87)90479-5.

DOI:10.1016/0091-3057(87)90479-5
PMID:3615550
Abstract

The effects of several opioid agonists and the opioid antagonist naloxone were examined in rats responding under a fixed-consecutive-number (FCN) schedule. Under this schedule, a reinforced response run consisted of responding eight or more times on one response lever, and then responding once on a second response lever. In one component of this schedule, an external discriminative stimulus signalled the completion of the response requirement on the first lever, whereas no stimulus change was programmed in the other. Morphine, l-methadone, U50488, ketocyclazocine, phencyclidine, and (+/-)N-allylnormetazocine decreased the percent of reinforced response runs (accuracy) under the FCN schedule without the external discriminative stimulus, but had no effect under the FCN schedule with the external discriminative stimulus. Naloxone and bremazocine, in contrast, had no effect on the accuracy of the discrimination under either FCN schedule. With the exception of bremazocine and U50488, which increased rates of responding at low doses, all drugs produced comparable decreases in rates of responding under both FCN schedules. During tests of antagonism, a 0.1 mg/kg dose of naloxone reversed completely the accuracy-decreasing effects produced by U50488 and morphine. The rate-decreasing effects of morphine and U50488 were reversed completely by a 0.01 and 1.0 mg/kg dose of naloxone, respectively. These results suggest that the addition of an external discriminative stimulus can modulate the disruptive effects of opioids, and that mu, sigma and some kappa agonists produce similar effects when evaluated under the FCN schedules.

摘要

在按照固定连续次数(FCN)程序作出反应的大鼠中,研究了几种阿片类激动剂和阿片类拮抗剂纳洛酮的作用。按照该程序,一次强化反应过程包括在一个反应杆上进行八次或更多次反应,然后在第二个反应杆上进行一次反应。在该程序的一个部分中,一种外部辨别性刺激表明第一个反应杆上的反应要求已完成,而在另一个部分中则未设定刺激变化。吗啡、左旋美沙酮、U50488、酮环唑辛、苯环己哌啶和(±)N-烯丙基去甲左啡诺在没有外部辨别性刺激的FCN程序下降低了强化反应过程的百分比(准确性),但在有外部辨别性刺激的FCN程序下没有影响。相比之下,纳洛酮和布瑞马唑辛在两种FCN程序下对辨别准确性均无影响。除了布瑞马唑辛和U50488在低剂量时增加反应速率外,所有药物在两种FCN程序下均使反应速率产生了类似程度的降低。在拮抗试验中,0.1mg/kg剂量的纳洛酮完全逆转了U50488和吗啡产生的准确性降低作用。吗啡和U50488的反应速率降低作用分别被0.01mg/kg和1.0mg/kg剂量的纳洛酮完全逆转。这些结果表明,添加外部辨别性刺激可以调节阿片类药物的干扰作用,并且在FCN程序下评估时,μ、σ和一些κ激动剂产生类似的作用。

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Evaluation of the effects of opioid agonists and antagonists under a fixed-consecutive-number schedule in rats.在固定连续数给药方案下对大鼠进行阿片类激动剂和拮抗剂效果的评估。
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