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Interoceptive conditioning with nicotine using extinction and re-extinction to assess stimulus similarity with bupropion

机译:使用灭绝和再灭绝评估烟碱对烟碱的刺激相似性

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摘要

Bupropion is an atypical antidepressant that increases long-term quit rates of tobacco smokers. A better understanding of the relation between nicotine and this first-line medication may provide insight into improving treatment. For all experiments, rats first had nicotine (0.4 mg base/kg) and saline session intermixed; intermittent access to sucrose only occurred on nicotine session. Nicotine in this protocol comes to differentially control “anticipatory” dipper entries. To more closely examine the overlap in the interoceptive stimulus effects of nicotine and bupropion, we assessed whether subsequent prolonged and repeated non-reinforced (extinction) sessions with the bupropion stimulus could weaken responding to nicotine (i.e., transfer of extinction). We also examined whether retraining the discrimination after initial extinction and then conducting extinction again (i.e., re-extinction) with bupropion would affect responding. We found that bupropion (20 and 30 mg/kg) fully substituted for the nicotine stimulus in repeated 20-min extinction sessions. The extent of substitution in extinction did not necessarily predict performance in the transfer test (e.g., nicotine responding unchanged after extinction with 20 mg/kg bupropion). Generalization of extinction back to nicotine was not seen with 20 mg/kg bupropion even after increasing the number of extinction session from 6 to 24. Finally, there was evidence that learning in the initial extinction phase was retained in the re-extinction phase for nicotine and bupropion. These findings indicate that learning involving the nicotine stimuli are complex and that assessment approach for stimulus similarity changes conclusions regarding substitution by bupropion. Further research will be needed to identify whether such differences may be related to different facets of nicotine dependence and/or its treatment.
机译:安非他酮是一种非典型抗抑郁药,可增加吸烟者的长期戒烟率。更好地了解尼古丁和这种一线药物之间的关系可以为改善治疗提供见识。对于所有实验,首先将大鼠的尼古丁(0.4 mg碱/ kg)和生理盐水混合。蔗糖间歇性访问仅发生在尼古丁时段。该协议中的尼古丁可差分控制“预期”的北斗星进入。为了更仔细地检查尼古丁和安非他酮在感受性刺激作用中的重叠,我们评估了随后使用安非他酮刺激进行的延长和反复的非强化(消光)疗程是否会减弱对尼古丁的反应(即消光转移)。我们还研究了在最初灭绝后重新训练辨别力,然后再用安非他酮灭绝(即再次灭绝)是否会影响响应。我们发现安非他酮(20和30 mg / kg)在重复20分钟的灭绝过程中完全替代了尼古丁刺激。灭绝中的取代程度不一定能预测转移试验的效果(例如,尼古丁在灭绝后用20 mg / kg安非他酮响应未变)。即使将灭绝次数从6次增加到24次,安非他酮20 mg / kg安非他酮后仍未见灭绝回到尼古丁的现象。最后,有证据表明尼古丁的灭绝阶段仍保留了最初灭绝阶段的学习。和安非他酮。这些发现表明,涉及尼古丁刺激的学习是复杂的,并且刺激相似性的评估方法改变了有关用安非他酮替代的结论。需要进一步的研究来确定这种差异是否可能与尼古丁依赖和/或其治疗的不同方面有关。

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