Adams J U, Holtzman S G
Department of Pharmacology, Emory University School of Medicine, Atlanta, GA 30322.
Eur J Pharmacol. 1991 Jan 25;193(1):67-73. doi: 10.1016/0014-2999(91)90201-z.
Rats were trained to lever-press on a multiple-trial, fixed-interval, 3-min schedule of food-reinforcement; each trial consisted of a 10-min time-out and a 9.5-min response period. Naltrexone, injected s.c. prior to each trial, reduced response rates in a dose-related fashion, with an ED50 of 21 mg/kg. Four-hour pretreatment with i.c.v. morphine (3.0-30 micrograms) produced leftward shifts of the naltrexone dose-effect curve of up to 3 orders of magnitude. The selective mu agonist, [D-Ala2,NMePhe4,Gly-ol5]enkephalin (DAGO; 0.1-0.3 microgram i.c.v.), sensitized animals to the rate-decreasing effects of naltrexone by more than 2 orders of magnitude. Pretreatment with the selective kappa agonist, dynorphin A-(1-17) (30 micrograms i.c.v.) or the selective delta agonist, [D-Pen2, D-Pen5]enkephalin (DPDPE; 30-100 micrograms i.c.v.) induced moderate sensitization with leftward shifts of 1.0-1.5 log units. Thus, the naltrexone-sensitizing effect of acute opioid pretreatment is centrally mediated, consistent with the hypothesis that the phenomenon is related to the initiation of opioid physical dependence. Further, the effect appears to be mediated predominantly by mu-opioid receptors, because mu agonists consistently produced the largest sensitization to naltrexone.
大鼠接受训练,在多次试验、固定间隔、3分钟食物强化的时间表上进行杠杆按压;每次试验包括10分钟的超时和9.5分钟的反应期。在每次试验前皮下注射纳曲酮,以剂量相关的方式降低反应率,ED50为21mg/kg。脑室内注射吗啡(3.0 - 30微克)进行4小时预处理,使纳曲酮剂量效应曲线向左移动高达3个数量级。选择性μ激动剂[D - Ala2,NMePhe4,Gly - ol5]脑啡肽(DAGO;0.1 - 0.3微克脑室内注射)使动物对纳曲酮的速率降低效应敏感化超过2个数量级。用选择性κ激动剂强啡肽A -(1 - 17)(30微克脑室内注射)或选择性δ激动剂[D - Pen2,D - Pen5]脑啡肽(DPDPE;30 - 100微克脑室内注射)预处理诱导中度敏感化,剂量效应曲线向左移动1.0 - 1.5个对数单位。因此,急性阿片类药物预处理的纳曲酮敏感化效应是由中枢介导的,这与该现象与阿片类药物身体依赖的起始有关的假设一致。此外,这种效应似乎主要由μ阿片受体介导,因为μ激动剂始终对纳曲酮产生最大的敏感化作用。
