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吗啡诱导的Fischer大鼠和Lewis大鼠位置偏爱:完全偏向程序中的习得与剂量反应

Morphine-induced place conditioning in Fischer and Lewis rats: acquisition and dose-response in a fully biased procedure.

作者信息

Davis Catherine M, Roma Peter G, Dominguez Juan M, Riley Anthony L

机构信息

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

出版信息

Pharmacol Biochem Behav. 2007 Mar;86(3):516-23. doi: 10.1016/j.pbb.2007.01.013. Epub 2007 Jan 20.

Abstract

The Fischer (F344) and Lewis (LEW) rat strains differ on a variety of behavioral assays examining the effects of morphine, with many of the differences observed during acquisition of behavioral responses. The results of these studies and others examining endogenous physiology and the biochemical effects of morphine suggest that F344 rats are more sensitive to morphine than LEW rats. However, LEW animals have shown greater conditioned place preferences (CPP) to 4 mg/kg than F344 rats. CPP is a popular assay of drug reward in which acquisition of the preference can be measured across multiple conditioning cycles, yet this aspect of CPP has not been assessed in F344 and LEW rats. As part of an ongoing effort to fully characterize the conditioned rewarding effects of abused drugs in these strains, the present study assessed the effects of 0, 1, 4 and 10 mg/kg subcutaneous (SC) morphine in adult male F344 and LEW rats (n=12/strain/dose). A fully biased place conditioning procedure was employed where morphine's effects were paired with the initially non-preferred chamber on Day 1, saline was paired with the preferred chamber on Day 2 and drug-free access to the entire apparatus was allowed on Day 3. This conditioning and testing regimen was repeated for four consecutive cycles. The F344 animals acquired CPP at 1 mg/kg only; this effect emerged after only two conditioning cycles. LEW rats never acquired a CPP at any dose tested. Peak blood morphine levels following SC injections of 1, 4 or 10 mg/kg revealed no significant strain or dose effects. These behavioral data are consistent with the hypothesis that F344 rats are more sensitive to the rewarding effects of morphine than LEW rats. Additional implications for the Fischer-Lewis model of drug abuse and the utility of CPP acquisition procedures are discussed.

摘要

费希尔(F344)和刘易斯(LEW)大鼠品系在多种检测吗啡作用的行为学试验中表现不同,许多差异在行为反应习得过程中就已观察到。这些研究以及其他检测内源性生理学和吗啡生化作用的研究结果表明,F344大鼠对吗啡的敏感性高于LEW大鼠。然而,LEW动物对4mg/kg吗啡表现出比F344大鼠更强的条件性位置偏爱(CPP)。CPP是一种常用的药物奖赏检测方法,通过多个条件化周期来测量偏爱性的获得情况,但尚未在F344和LEW大鼠中评估CPP的这一方面。作为全面描述这些品系中滥用药物条件性奖赏作用的持续努力的一部分,本研究评估了0、1、4和10mg/kg皮下(SC)注射吗啡对成年雄性F344和LEW大鼠(每组12只/品系/剂量)的影响。采用了一种完全偏向性的位置条件化程序,在第1天吗啡的作用与最初不偏爱的腔室配对,第2天生理盐水与偏爱腔室配对,第3天允许动物无药物自由进入整个装置。这个条件化和测试方案连续重复四个周期。F344动物仅在1mg/kg时获得CPP;这种效应仅在两个条件化周期后出现。LEW大鼠在任何测试剂量下均未获得CPP。皮下注射1、4或10mg/kg吗啡后的血中吗啡峰值水平未显示出显著的品系或剂量效应。这些行为学数据与F344大鼠比LEW大鼠对吗啡奖赏效应更敏感的假设一致。还讨论了费希尔 - 刘易斯药物滥用模型的其他意义以及CPP获得程序的效用。

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