Mello N K, Negus S S
Alcohol and Drug Abuse Research Center, McLean Hospital-Harvard Medical School, Belmont, Massachusetts, USA.
J Pharmacol Exp Ther. 1998 May;285(2):444-56.
Concurrent abuse of cocaine and opioids is frequently observed clinically, and we have developed a model of "speedball" self-administration involving the simultaneous injection of cocaine and heroin combinations in rhesus monkeys (Mello et al. (1995) J Pharmacol Exp Ther 274:1325). In the present study, we evaluated the effects of buprenorphine (0.0075-0.75 mg/kg/day i.v.) and saline on speedball combinations of cocaine [0.001, 0.01 or 0.10 mg/kg/inj] and heroin [0.0001-0.032 mg/kg/inj]. We also examined the effects of buprenorphine (0.075 and 0.237 mg/kg/day i.v.) on self-administration of heroin alone (0.0001-0.01 mg/kg/inj). Drug and food (1-g banana pellets) self-administration were maintained on a second-order FR4 (VR16:S) schedule in four 1-hr sessions each day. Each buprenorphine or saline control treatment was evaluated for 10 consecutive days, and monkeys returned to base-line performance between each treatment condition. Buprenorphine (0.075-0.75 mg/kg/day) selectively reduced self-administration of speedball combinations of low-dose cocaine (0.001 mg/kg/inj) and heroin (0.001 or 0.0032 mg/kg/inj) (P < .05-.01), and buprenorphine (0.237 mg/kg/day) shifted dose-effect curves for speedball combinations of cocaine (0.001 mg/kg/inj) and heroin (0.0001-0.032 mg/kg/inj) downward (P < .05-.01) and approximately 1 log unit to the right. Buprenorphine treatment was less effective in decreasing responding maintained by speedball combinations of heroin and 0.01 and 0.10 mg/kg/inj cocaine. Buprenorphine treatment (0.075 and 0.237 mg/kg/day) also shifted the heroin dose-effect curve downward (P < .01-.001) and to the right. Both speedball and heroin self-administration were associated with dose-dependent decreases in food-maintained responding during saline control treatment. However, food-maintained responding was often higher than control levels during buprenorphine treatment (P < .05-.001), which suggests that buprenorphine antagonized the rate-decreasing effects of speedballs and of heroin. Buprenorphine's selective reduction of speedball and heroin self-administration is consistent with clinical treatment trials in opioid abusers and polydrug abusers. Thus, these primate models of speedball and heroin self-administration should be useful for preclinical evaluation of novel drug abuse treatment medications.
临床上经常观察到可卡因和阿片类药物的同时滥用情况,我们已经建立了一种“速球”自我给药模型,该模型涉及在恒河猴中同时注射可卡因和海洛因组合(Mello等人,(1995年)《药理学与实验治疗学杂志》274:1325)。在本研究中,我们评估了丁丙诺啡(静脉注射0.0075 - 0.75毫克/千克/天)和生理盐水对可卡因[0.001、0.01或0.10毫克/千克/注射]与海洛因[0.0001 - 0.032毫克/千克/注射]速球组合的影响。我们还研究了丁丙诺啡(静脉注射0.075和0.237毫克/千克/天)对单独海洛因(0.0001 - 0.01毫克/千克/注射)自我给药的影响。药物和食物(1克香蕉颗粒)自我给药维持在每天四个1小时时段的二阶FR4(VR16:S)时间表上。每种丁丙诺啡或生理盐水对照治疗连续评估10天,并且猴子在每种治疗条件之间恢复到基线表现。丁丙诺啡(0.075 - 0.75毫克/千克/天)选择性地减少了低剂量可卡因(0.001毫克/千克/注射)和海洛因(0.001或0.0032毫克/千克/注射)速球组合的自我给药(P <.05 -.01),并且丁丙诺啡(0.237毫克/千克/天)使可卡因(0.001毫克/千克/注射)和海洛因(0.0001 - 0.032毫克/千克/注射)速球组合的剂量 - 效应曲线向下移动(P <.05 -.01)并向右移动约1个对数单位。丁丙诺啡治疗在减少由海洛因与0.01和0.10毫克/千克/注射可卡因的速球组合维持的反应方面效果较差。丁丙诺啡治疗(0.075和0.237毫克/千克/天)也使海洛因剂量 - 效应曲线向下移动(P <.01 -.001)并向右移动。在生理盐水对照治疗期间,速球和海洛因自我给药均与食物维持反应的剂量依赖性降低相关。然而,在丁丙诺啡治疗期间,食物维持反应通常高于对照水平(P <.05 -.001),这表明丁丙诺啡拮抗了速球和海洛因的速率降低作用。丁丙诺啡对速球和海洛因自我给药的选择性减少与阿片类药物滥用者和多药滥用者的临床治疗试验一致。因此,这些速球和海洛因自我给药的灵长类动物模型应该有助于新型药物滥用治疗药物的临床前评估。
