[血清素在环唑辛引起的大鼠行为改变中的作用]。

Journal de pharmacologie Pub Date : 1986-10-01
M R Gavend, F Serre-Debeauvais, M Gavend
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引用次数: 0

摘要

Cyclazocine是一种苯佐莫孤儿衍生物,被认为是kappa和sigma阿片受体激动剂。在对大鼠的实验研究中,已知环唑辛可以增加运动活动,并产生一种奇怪的行为综合征,包括头部摇摆,向后行走,盘旋。本研究旨在探讨不同药物对5 -羟色胺能神经系统的影响,以及其对环唑嗪所致运动活动和异常行为的影响。对氯苯丙氨酸(PCPA, 400 mg/kg, 72、48、24小时)预处理对三种异常行为均有抑制作用。对氯甲基安非他明(PCMA, 15 mg/kg, 24小时)预处理可拮抗头部摇摆、向后行走并显著增强运动活动。相反,PCMA预处理(2.5 mg/kg, 15分钟)导致对环唑嗪的异常行为反应增强。l -色氨酸(50 mg/kg)、5-羟色氨酸(5-HTP, 50 mg/kg)或pargyline (50 mg/kg)抑制异常行为并降低运动活动。对5-HT1和5-HT2受体均有亲和力的5-羟色胺拮抗剂、美高林(0.25-1 mg/kg)、甲基塞吉特(1-5 mg/kg)、阿米替林(5-20 mg/kg)、dl-普萘洛尔(10-40 mg/kg)可阻断头部摇摆和向后行走;只有甲塞柳胺抑制环化。除甲塞吉特外,所有这些药物均显著增强了环唑嗪诱导的运动活性。而选择性亲和性为5-HT2受体的5-羟色胺拮抗剂酮丝氨酸(0.5 ~ 2 mg/kg)和哌烯酮(0.05 ~ 0.2 mg/kg)对大鼠异常行为和运动活性无明显影响。综上所述,这些结果表明,5 -羟色胺能介导参与了环唑嗪诱导的异常行为,5 -羟色胺对药物产生的运动活动施加抑制控制。这些作用可能与5-HT1受体有关。进一步的实验表明,这些药物能够增强环唑辛诱导的运动活性,类似地增强具有环唑辛样特性的左旋吗啡肽衍生物诱导的运动活性,但不会增强低剂量吗啡产生的多动性。这里报告的数据提供了关于混合kappa和sigma激动剂的神经中介作用的信息,并允许比较环唑辛与其他拟精神药物的作用机制。
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[The role of serotonin in the behavioral changes induced in the rat by cyclazocine].

Cyclazocine is a benzomorphan derivative, considered as a mixed kappa and and sigma opioid receptor agonist. In experimental study with rats, cyclazocine is known to increase locomotor activity and to produce a bizarre behavioral syndrome including head swaying, backward walking, circling. The present study was undertaken to investigate the effects of various drugs modifying the serotoninergic neuronal systems, upon the locomotor activity and the abnormal behaviors induced by cyclazocine. Pretreatment with p-chlorophenylalanine (PCPA, 400 mg/kg, 72, 48, 24 hr) resulted in an inhibition of the three abnormal behaviors. Pretreatment with p-chloromethylamphetamine (PCMA, 15 mg/kg, 24 hr) antagonized head swaying, backward walking and markedly enhanced locomotor activity. In the contrary, pretreatment with PCMA (2.5 mg/kg, 15 min) resulted in enhanced abnormal behavioral responses to cyclazocine. L-tryptophan (50 mg/kg), 5-hydroxytryptophan (5-HTP, 50 mg/kg), or pargyline (50 mg/kg) inhibited abnormal behaviors and decreased locomotor activity. Serotonin antagonists with affinity fir both 5-HT1 and 5-HT2 receptors, metergoline (0.25-1 mg/kg), methysergide (1-5 mg/kg), amitriptyline (5-20 mg/kg), dl-propranolol (10-40 mg/kg) blocked head swaying and backward walking; only methysergide inhibited circling. All these drugs, except methysergide, markedly enhanced the cyclazocine-induced locomotor activity. In contrast, ketanserine (0.5-2 mg/kg) and pirenperone (0.05-0.2 mg/kg), serotonin antagonists with selective affinity for 5-HT2 receptors had no effects on the abnormal behaviors and locomotor activity. Taken together, these results suggest that a serotoninergic mediation is involved in the cyclazocine-induced abnormal behaviors, and that serotonin exerts an inhibitory control on the locomotor activity produced by the drug. These effects are probably associated with 5-HT1 receptors. Further experiments have shown that the drugs having being able to potentiate cyclazocine-induced locomotor activity, similarly potentiate the locomotor activity induced by levallorphan, morphinan derivative with cyclazocine-like properties but do not enhance the hyperactivity produced by a low dose of morphine. The data reported here, provide a contribution to the informations concerning the neuromediation of the effects of mixed kappa and sigma agonists and allow to compare the mechanism of action of cyclazocine with those of other psychotomimetic drugs.

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