首页> 外文期刊>Pharmacology, Biochemistry and Behavior >Nalorphine's ability to substitute for morphine in a drug discrimination procedure is a function of training dose.
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Nalorphine's ability to substitute for morphine in a drug discrimination procedure is a function of training dose.

机译:纳洛啡在药物鉴别程序中替代吗啡的能力是训练剂量的函数。

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摘要

Rats trained to discriminate the mu agonists fentanyl or morphine from their respective vehicles generalize to the partial mu agonist nalorphine incompletely and inconsistently. Any number of factors may influence the generalization patterns obtained, one of which being the specific dose of the full opioid agonist used during training, a factor reported to influence generalization with other partial opioid agonists. To assess if training dose influences stimulus generalization to nalorphine and to support its role in the aforementioned variability across studies, in the present experiments rats were trained to discriminate either a low (5.6 mg/kg) or a high (10 mg/kg) dose of morphine from distilled water within the taste aversion baseline of drug discrimination learning. Subjects were then given a range of doses of morphine, nalorphine, methadone, or naloxone to assess the degree of substitution (if any) of these compounds for the training dose of morphine. For all subjects, morphine fully substituted for itself, and the opioid antagonist naloxone failed to substitute for the morphine cue. Rats generalized the morphine cue to nalorphine in subjects trained at the lower dose but not in subjects trained at the higher dose. Rats generalized the morphine cue to methadone in the latter group (the high dose group), indicating that the failure to generalize to nalorphine in this group was not a general inability of an opioid agonist to substitute for morphine. Naloxone blocked morphine stimulus control in all subjects and nalorphine control in the low-dose group for which nalorphine substituted for morphine, suggesting that morphine control (and the nalorphine substitution) was based on opioid activity. These results indicate that the substitution patterns of nalorphine in morphine-trained subjects are a function in part of the dose of morphine used in training and support the position that nalorphine is a partial opioid agonist with intermediate efficacy.
机译:受过训练以将mu激动剂芬太尼或吗啡与其各自媒介物区分开的大鼠,会不完全和不一致地泛化为部分mu激动剂纳洛啡。任何数量的因素都可能影响获得的泛化模式,其中之一是训练期间使用的全剂量阿片类激动剂的具体剂量,据报道该因素会影响其他部分阿片类激动剂的泛化。为了评估训练剂量是否会影响对纳洛啡的一般性刺激并支持其在上述研究中的上述变异性中的作用,在本实验中,对大鼠进行了训练以区分低剂量(5.6 mg / kg)或高剂量(10 mg / kg)歧视学习中在味觉厌恶基线内蒸馏水中吗啡的含量然后给受试者一定剂量范围的吗啡,纳洛啡,美沙酮或纳洛酮,以评估这些化合物对吗啡训练剂量的取代度(如果有的话)。对于所有受试者,吗啡完全替代了自身,而阿片类药物拮抗剂纳洛酮未能替代吗啡提示。大鼠在低剂量训练的受试者中将吗啡提示推广至纳洛啡,但在高剂量训练的受试者中未将其归纳为吗啡。大鼠在后一组(高剂量组)中将吗啡提示推广至美沙酮,这表明在该组中未能推广至纳洛啡并不是阿片类激动剂一般无法替代吗啡。纳洛酮阻断了所有受试者的吗啡刺激控制,而低剂量组的纳洛啡控制被纳洛啡替代了吗啡,这表明吗啡控制(和纳洛啡替代)是基于阿片类药物的活性。这些结果表明,吗啡训练对象中纳洛啡的取代模式是用于训练的部分吗啡剂量的函数,并支持纳洛啡是具有中等功效的部分阿片类激动剂。

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