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吗啡和纳洛酮对热板试验中大鼠行为的影响:一项大鼠行为药理学研究

Effects of morphine and naloxone on behaviour in the hot plate test: an ethopharmacological study in the rat.

作者信息

Espejo E F, Stinus L, Cador M, Mir D

机构信息

Departamento de Enfermería, Universidad de Sevilla, Spain.

出版信息

Psychopharmacology (Berl). 1994 Jan;113(3-4):500-10. doi: 10.1007/BF02245230.

Abstract

The objectives of this study were: i) to analyse the effects of morphine and naloxone on the rat's behaviour in the hot plate test using an ethological approach, and ii) to compare the effectiveness of repeated versus single test paradigms. Animals received either morphine (0, 3, 6 or 9 mg/kg SC) or naloxone (0, 0.01, 0.1 or 1 mg/kg SC). For repeated hot plate measures, rats were tested before and 60, 120, 180 and 240 min following morphine treatment, as well as 30, 60, 90 and 120 min after naloxone injection. For the single test schedule, rats were tested only once 60 min after morphine or 30 min after naloxone administration, or at 60, 120, 180, 240 and 300 min after 9 mg/kg morphine treatment. Behaviour was videotaped and analysed by an ethogram and ethological techniques. A cluster analysis revealed that the most frequently displayed patterns could be categorised into exploratory sniffing reactions (walk-sniff, immobile-sniff) and noxious-evoked elements, including primary (paw-licking, stamping), escape (jumping, leaning posture) and independent (hindleg-withdrawal) patterns. During repeated tests, morphine treatment induced: i) a maximum hypoalgesic effect 60 min post-injection (noxious-evoked patterns were significantly reduced), and ii) an unexpected "thermal hyperreactivity rebound effect" after 120 min (paw-licking and hindleg-withdrawal were enhanced), although changes in hindpaw-licking are more indicative of a hyperalgesic rebound effect. Most changes were quite similar during the single test schedule at 60 and 120 min after morphine injection. With regard to naloxone treatment, jumping latency was significantly decreased during the repeated test schedule, but not on single exposure to the plate. Other elements were facilitated, however, in the single test (stamping, leaning posture, hindleg-withdrawal). The results indicated that both repeated and single tests paradigms are of value for testing the effects of morphine and naloxone on rats. However, under our conditions the single test paradigm gave a better picture of the overall effects of the drug. Learning as well as habituation and sensitization may mask certain effects during repeated tests. In conclusion, an ethological analysis of the rat's behaviour in the hot plate test following administration of morphine and naloxone has been validated in this study.

摘要

本研究的目的是

i)采用行为学方法分析吗啡和纳洛酮对热板试验中大鼠行为的影响,以及ii)比较重复试验与单次试验模式的有效性。动物分别接受吗啡(0、3、6或9mg/kg皮下注射)或纳洛酮(0、0.01、0.1或1mg/kg皮下注射)。对于重复热板测量,大鼠在吗啡治疗前以及治疗后60、120、180和240分钟进行测试,以及在纳洛酮注射后30、60、90和120分钟进行测试。对于单次测试方案,大鼠在吗啡给药后60分钟或纳洛酮给药后30分钟仅测试一次,或在9mg/kg吗啡治疗后60、120、180、240和300分钟进行测试。行为通过录像并采用行为图谱和行为学技术进行分析。聚类分析表明,最常表现出的模式可分为探索性嗅闻反应(行走-嗅闻、静止-嗅闻)和有害刺激诱发的行为,包括初级行为(舔爪、跺脚)、逃避行为(跳跃、倾斜姿势)和独立行为(后肢退缩)。在重复测试中,吗啡治疗导致:i)注射后60分钟出现最大镇痛作用(有害刺激诱发的行为显著减少),以及ii)120分钟后出现意外的“热超敏反应反弹效应”(舔爪和后肢退缩增强),尽管后爪舔舐的变化更表明是痛觉过敏反弹效应。在吗啡注射后60和120分钟的单次测试方案中,大多数变化非常相似。关于纳洛酮治疗,在重复测试方案中跳跃潜伏期显著缩短,但在单次暴露于热板时未出现这种情况。然而,在单次测试中其他行为(跺脚、倾斜姿势、后肢退缩)有所增强。结果表明,重复试验和单次试验模式对于测试吗啡和纳洛酮对大鼠的影响均有价值。然而,在我们的条件下,单次测试模式能更好地反映药物的总体效果。在重复测试过程中,学习以及习惯化和敏感化可能会掩盖某些效应。总之,本研究验证了在给予吗啡和纳洛酮后对热板试验中大鼠行为进行行为学分析的有效性。

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