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伐尼克兰或氟伏沙明降低对乙醇而非食物反应的相对效力取决于同时获得的食物的有无。

Relative potency of varenicline or fluvoxamine to reduce responding for ethanol versus food depends on the presence or absence of concurrently earned food.

作者信息

Ginsburg Brett C, Lamb Richard J

出版信息

Alcohol Clin Exp Res. 2014 Mar;38(3):860-70. doi: 10.1111/acer.12285.

Abstract

BACKGROUND

Varenicline, a nicotinic partial agonist, selectively reduces ethanol (EtOH)- versus sucrose-maintained behavior when tested in separate groups, yet like the indirect agonist fluvoxamine, this selectively inverts when EtOH and food are concurrently available.

METHODS

Here, we extend these findings by examining varenicline and fluvoxamine effects under a multiple concurrent schedule where food and EtOH are concurrently available in different components: Component 1 where the food fixed-ratio was 25 and Component 2 where the food fixed-ratio was 75. The EtOH fixed-ratio was always 5. Food-maintained responding predominated in Component 1, while EtOH-maintained responding predominated in Component 2. In a second experiment, varenicline effects were assessed under a multiple schedule where food, then EtOH, then again food were available in separate 5-minute components with fixed-ratios of 5 for each reinforcement.

RESULTS

In the multiple concurrent schedule, varenicline was more potent at reducing food- versus EtOH-maintained responding in both components and reduced EtOH-maintained responding more potently during Component 1 (when food was almost never earned) than in Component 2 (where food was often earned). Fluvoxamine was similarly potent at reducing food- and EtOH-maintained responding. Under the multiple schedule, varenicline, like fluvoxamine, more potently decreases EtOH- versus food maintained responding when only food or EtOH is available in separate components.

CONCLUSIONS

These results demonstrate that selective effects on drug- versus alternative-maintained behavior depend on the schedule arrangement, and assays in which EtOH or an alternative is the only programmed reinforcement may overestimate the selectivity of treatments to decrease EtOH self-administration. Thus selective effects obtained under one assay may not generalize to another. Better understanding the behavioral mechanisms responsible for these results may help to guide pharmaco-therapeutic development for substance use disorders.

摘要

背景

伐尼克兰是一种烟碱型部分激动剂,在对不同组进行测试时,能选择性地降低乙醇(EtOH)维持的行为与蔗糖维持的行为,但与间接激动剂氟伏沙明一样,当乙醇和食物同时可得时,这种选择性会发生反转。

方法

在此,我们通过在多重并发程序下研究伐尼克兰和氟伏沙明的作用来扩展这些发现,在该程序中,食物和乙醇在不同成分中同时可得:成分1中食物固定比率为25,成分2中食物固定比率为75。乙醇固定比率始终为5。在成分1中,食物维持的反应占主导,而在成分2中,乙醇维持的反应占主导。在第二个实验中,在多重程序下评估伐尼克兰的作用,在该程序中,食物、然后乙醇、然后再次食物在单独的5分钟成分中可得,每次强化的固定比率均为5。

结果

在多重并发程序中,伐尼克兰在降低两个成分中食物维持的反应与乙醇维持的反应方面更有效,并且在成分1(食物几乎从未获得)期间比在成分2(食物经常获得)期间更有效地降低乙醇维持的反应。氟伏沙明在降低食物和乙醇维持的反应方面同样有效。在多重程序下,与氟伏沙明一样,当单独成分中只有食物或乙醇可得时,伐尼克兰更有效地降低乙醇维持的反应与食物维持的反应。

结论

这些结果表明,对药物维持的行为与替代物维持的行为的选择性作用取决于程序安排,但乙醇或替代物是唯一程序化强化物的试验可能会高估治疗减少乙醇自我给药的选择性。因此,在一种试验中获得的选择性作用可能无法推广到另一种试验。更好地理解导致这些结果的行为机制可能有助于指导物质使用障碍的药物治疗开发。

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