氟哌啶醇对恒河猴可卡因自我给药及可卡因诱导的学习障碍的差异性拮抗作用。
Differential antagonism of cocaine self-administration and cocaine-induced disruptions of learning by haloperidol in rhesus monkeys.
作者信息
Winsauer Peter J, Moerschbaecher Joseph M, Roussell Alison M
机构信息
Department of Pharmacology and Experimental Theapeutics, Louisiana State University Health Sciences Center, 1901 Perdido Street, New Orleans, LA 70112-1393, USA.
出版信息
J Exp Anal Behav. 2008 Mar;89(2):225-46. doi: 10.1901/jeab.2008.89-225.
Six rhesus monkeys responding under a three-component multiple schedule were administered haloperidol to determine its effects on cocaine self-administration and on cocaine's disruptive effects on the repeated acquisition and performance of response chains. In the absence of haloperidol, 0.0032-0.032 mg/kg/infusion of cocaine increased response rate and the number of infusions in the self-administration component when compared to saline administration, whereas 0.1-0.32 mg/kg/infusion decreased response rate and the number of infusions. When compared to saline administration, the two lowest infusion doses of cocaine had little or no effect on responding in the acquisition and performance components; however, higher infusion doses of cocaine dose-dependently decreased response rate in these components. In addition, the higher doses of cocaine also increased the percentage of errors in the acquisition and performance components. Pretreatment with haloperidol (0.0032 or 0.01 mg/kg, i.m.) antagonized the effects of low doses of cocaine on the number of infusions in the self-administration component, whereas only the 0.01-mg/kg dose antagonized the effects of high doses of cocaine on the number of infusions. Neither dose of haloperidol antagonized the rate-decreasing effects of cocaine on responding in the acquisition and performance components significantly; the highest dose of haloperidol alone decreased rates of responding in each component. Antagonism of cocaine's error-increasing effects by haloperidol was only evident at one dose of cocaine (0.032 mg/kg/infusion), and was more complete in the performance components than in the acquisition components. Together, these data show the limited suitability of haloperidol for selectively antagonizing cocaine self-administration in the context of a multiple schedule involving transition behavior, and show the lack of uniform antagonism across operant behaviors.
对六只按照三分量多重程序做出反应的恒河猴施用氟哌啶醇,以确定其对可卡因自我给药的影响,以及对可卡因在反应链的重复习得和表现方面的干扰作用的影响。在没有氟哌啶醇的情况下,与施用生理盐水相比,0.0032 - 0.032毫克/千克/输注剂量的可卡因会提高自我给药部分的反应率和输注次数,而0.1 - 0.32毫克/千克/输注剂量则会降低反应率和输注次数。与施用生理盐水相比,可卡因的两个最低输注剂量对习得和表现部分的反应几乎没有影响;然而,较高的可卡因输注剂量会剂量依赖性地降低这些部分的反应率。此外,较高剂量的可卡因还会增加习得和表现部分的错误百分比。用氟哌啶醇(0.0032或0.01毫克/千克,肌肉注射)预处理可拮抗低剂量可卡因对自我给药部分输注次数的影响,而只有0.01毫克/千克的剂量能拮抗高剂量可卡因对输注次数的影响。两种剂量的氟哌啶醇均未显著拮抗可卡因对习得和表现部分反应的速率降低作用;单独使用最高剂量的氟哌啶醇会降低每个部分的反应率。氟哌啶醇对可卡因增加错误作用的拮抗作用仅在一种可卡因剂量(0.032毫克/千克/输注)下明显,且在表现部分比在习得部分更完全。总之,这些数据表明,在涉及过渡行为的多重程序背景下,氟哌啶醇对选择性拮抗可卡因自我给药的适用性有限,并且表明在操作性行为中缺乏统一的拮抗作用。
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