首页> 外文期刊>The Journal of Pharmacology and Experimental Therapeutics: Official Publication of the American Society for Pharmacology and Experimental Therapeutics >Differential Effects of D1- and D2-Like Compounds on Cocaine Self-Administration in Lewis and Fischer 344 Inbred Rats
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Differential Effects of D1- and D2-Like Compounds on Cocaine Self-Administration in Lewis and Fischer 344 Inbred Rats

机译:D1和D2类化合物对Lewis和Fischer 344自交大鼠可卡因自我给药的差异作用

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Genetic factors influence behavioral responses to cocaine as seen in comparisons of Lewis and Fischer 344 inbred rats. Lewis rats have lower D2-like receptor and Gi_(#alpha#) levels in nucleus accumbens, an important area in behavioral responses to cocaine. This study assessed the effects of manipulating D2-and D1 levels pharmacologically in these strains. Experiment 1 investigated how the D2-like antagonist eticlopride (0.01-0.1mg/kg), the D1-like antagonist SCH 23390 (0.005-0.05mg/kg), the D2/D3 agonist quinpirole (0.001-0.1 mg/kg), and the partial D1 agonist SKF 38393 (0.1-10 mg/kg) affected responding for food under a fixed ratio 15 schedule. Quinpirole disrupted rates more readily in Lewis versus Fischer 344 rats. In experiment 2, the effects of these agents on cocaine discrimination (10 mg/kg) were examined. Quinpirole substituted and SCH 23390-attenuated cocaine discrimination in both strains. Doses of the drugs that dit not disrupt responding in these experiments were tested in cocaine self-administration in experiment 3. Cocaine self-administration (0.25-1.0 mg/kg) was increased by eticlopride (0.03 mg/kg) in Lewis rats but had no effect in Fischer 344 rats, whereas SCH 23390 (0.01 mg/kg) led ot greater increased cocaine self-administration in Fischer 344 versus Lewis rats. The dopamine agonists had differential effects on cocaine self-administration in the strains. Cocaine self-administration was decreased in Lewis rats and increased in Fischer 344 rats by SKF 38393 (1 mg/kg). These data show that manipulating D1- and D2-like receptor availability has strain-selective effects on the reinforcing, but not discriminative stimulus, effects of cocaine that are predicted by inherent differences in nucleus accumbens receptor populations.
机译:遗传因素影响对可卡因的行为反应,如Lewis和Fischer 344近交大鼠的比较所见。 Lewis大鼠在伏伏核中具有较低的D2样受体和Gi _(#alpha#)水平,这是对可卡因的行为反应中的重要区域。这项研究评估了在药理学上操纵这些菌株中D2和D1水平的作用。实验1研究了D2类拮抗剂依替普利(0.01-0.1mg / kg),D1类拮抗剂SCH 23390(0.005-0.05mg / kg),D2 / D3激动剂喹吡罗(0.001-0.1 mg / kg)如何进行研究, D1激动剂SKF 38393(0.1-10 mg / kg)会以固定比例15的时间表影响食物响应。与Fischer 344大鼠相比,喹吡罗更易破坏速率。在实验2中,检查了这些药物对可卡因鉴别的影响(10 mg / kg)。两种菌株均用喹吡罗取代和SCH 23390减弱了可卡因鉴别。在实验3中通过可卡因自我给药测试了在这些实验中不会破坏反应的药物剂量。艾替洛必利(0.03 mg / kg)使可卡因的自我给药(0.25-1.0 mg / kg)在Lewis大鼠中增加,但在Fischer 344大鼠中没有可卡因的作用,而SCH 23390(0.01 mg / kg)导致在Fischer 344大鼠中可卡因的自给药量比Lewis大鼠更大。多巴胺激动剂对菌株中的可卡因自我给药具有不同的作用。通过SKF 38393(1 mg / kg),可卡因自我给药在Lewis大鼠中减少,在Fischer 344大鼠中增加。这些数据表明,操纵D1和D2样受体的可用性对增强可卡因具有应变选择性作用,但对歧视性刺激没有应变作用,而可卡因的作用是由伏伏核受体群体固有差异预测的。

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