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首页> 外文期刊>Psychopharmacology >Dopamine antagonists alter response allocation but do not suppress appetite for food in rats: contrast between the effects of SKF 83566, raclopride, and fenfluramine on a concurrent choice task
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Dopamine antagonists alter response allocation but do not suppress appetite for food in rats: contrast between the effects of SKF 83566, raclopride, and fenfluramine on a concurrent choice task

机译:多巴胺拮抗剂可改变反应的分配,但不会抑制大鼠食物的食欲:SKF 83566,雷洛必利和芬氟拉明对并发选择任务的作用之间的对比

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Rationale: Dopamine is important for enabling organisms to overcome work-related response costs. One way of investigating this function has been with concurrent choice procedures using food reinforcement. In the present study, rats were given a choice between pressing a lever for preferred Bioserve pellets, or approaching and consuming a less-preferred laboratory chow that was concurrently available. In previous work with this task, dopamine antagonists and accumbens dopamine depletions decreased lever pressing but increased chow consumption. Objective: The present study assessed three drugs (two dopamine antagonists and one appetite suppressant) using the lever pressing/chow feeding task. Results: Under baseline conditions, rats pressed the lever at high rates (1,300–1,500 responses) to obtain the preferred food, and little of the laboratory chow was eaten (1–2 g). Selective D1 and D2 antagonists (SKF 83566 and raclopride) reduced fixed ratio 5 lever pressing, but substantially increased chow consumption. In contrast, the serotonergic appetite suppressant fenfluramine reduced both lever pressing and chow consumption. With the dopamine antagonists, lever pressing and chow consumption were inversely correlated across treatments, while these two measures were unrelated in the fenfluramine experiment. Conclusions: Dopamine antagonists and accumbens dopamine depletions do not simply reduce appetite. Rats with accumbens dopamine depletions, or rats treated with low doses of selective or non-selective dopamine antagonists, remain directed toward the acquisition and consumption of food. These results demonstrate that fundamental aspects of food reinforcement are left intact after treatment with low doses of dopamine antagonists.
机译:理由:多巴胺对于使生物体克服与工作有关的响应成本非常重要。研究此功能的一种方法是使用食品强化剂同时进行选择程序。在本研究中,大鼠可以选择压制首选Bioserve药丸的杠杆,还是接近并食用同时可用的不太受欢迎的实验室食物。在以前完成该任务的工作中,多巴胺拮抗剂和伏安多巴的消耗减少了杠杆的按压,但增加了食物消耗。目的:本研究使用推杆/慢食喂养法评估了三种药物(两种多巴胺拮抗剂和一种食欲抑制剂)。结果:在基线条件下,大鼠以高速率(1,300–1,500响应)按下杠杆以获得首选食物,而实验室食物却很少被食用(1-2 g)。选择性的D1和D2拮抗剂(SKF 83566和raclopride)可降低固定比率的5杆按压,但可大大增加食物消耗。相反,血清素能抑制食欲的芬氟拉明减少了杠杆的按压和食物的消耗。使用多巴胺拮抗剂时,不同治疗之间的杠杆按压和食物消耗量呈负相关,而这两种方法在芬氟拉明实验中则无关。结论:多巴胺拮抗剂和伏安定的消耗并不会简单地降低食欲。伏隔性多巴胺耗竭的大鼠,或用低剂量的选择性或非选择性多巴胺拮抗剂治疗的大鼠,仍旧针对食物的获取和食用。这些结果表明,用低剂量的多巴胺拮抗剂治疗后,食物强化的基本方面保持不变。

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