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吗啡辨别性控制由μ阿片受体介导:δ阿片替代和拮抗作用的评估。

Morphine discriminative control is mediated by the mu opioid receptor: assessment of delta opioid substitution and antagonism.

作者信息

Stevenson G W, Cañadas F, Zhang X, Rice K C, Riley A L

机构信息

Psychopharmacology Laboratory, Department of Psychology, American University, Washington, DC 20016, USA.

出版信息

Pharmacol Biochem Behav. 2000 Aug;66(4):851-6. doi: 10.1016/s0091-3057(00)00280-x.

Abstract

Morphine is an effective training drug in drug discrimination procedures. In subsequent generalization tests in which other opioids are administered, mu opioid agonists selectively substitute for the training drug. Given the relative selectivity of morphine for the mu receptor, such substitution patterns suggest that the mu opioid receptor is mediating the discriminative control of this compound. The present study assessed this selective mediation by examining the ability of the delta opioid agonist SNC80 to substitute for (and the delta opioid antagonist naltrindole to antagonize) morphine stimulus effects in rats trained to discriminate morphine from its vehicle in the conditioned taste aversion baseline of drug discrimination learning. Although morphine and methadone produced dose-related substitution for morphine (10 mg/kg), there was no evidence of substitution for morphine by SNC80 at any dose tested. Further, although naloxone (3.2 mg/kg) completely blocked the discriminative effects of morphine, naltrindole (3.2-10 mg/kg) did not significantly affect the morphine stimulus. These data suggest that the discriminative control established to morphine is mediated by its activity at the mu, but not the delta, receptor.

摘要

吗啡是药物辨别程序中一种有效的训练药物。在随后给予其他阿片类药物的泛化试验中,μ阿片受体激动剂可选择性替代训练药物。鉴于吗啡对μ受体具有相对选择性,这种替代模式表明μ阿片受体介导了该化合物的辨别性控制。本研究通过检测δ阿片受体激动剂SNC80替代(以及δ阿片受体拮抗剂纳曲吲哚拮抗)吗啡刺激效应的能力,评估了这种选择性介导作用。实验用大鼠在药物辨别学习的条件性味觉厌恶基线中接受训练,以区分吗啡与其溶媒。尽管吗啡和美沙酮产生了与剂量相关的对吗啡(10毫克/千克)的替代作用,但在任何测试剂量下,均未发现SNC80对吗啡有替代作用。此外,尽管纳洛酮(3.2毫克/千克)完全阻断了吗啡的辨别效应,但纳曲吲哚(3.2 - 10毫克/千克)并未显著影响吗啡刺激。这些数据表明,对吗啡建立的辨别性控制是由其在μ受体而非δ受体上的活性介导的。

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