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急性治疗剂量或奖赏剂量的苯丙胺对巴甫洛夫式自动塑造及腹侧纹状体多巴胺信号传导习得的影响。

Effects of an acute therapeutic or rewarding dose of amphetamine on acquisition of Pavlovian autoshaping and ventral striatal dopamine signaling.

作者信息

Schuweiler D R, Athens J M, Thompson J M, Vazhayil S T, Garris P A

机构信息

School of Biological Sciences, Illinois State University, Campus Box 4120 Normal, IL 61790-4120, USA.

School of Biological Sciences, Illinois State University, Campus Box 4120 Normal, IL 61790-4120, USA.

出版信息

Behav Brain Res. 2018 Jan 15;336:191-203. doi: 10.1016/j.bbr.2017.09.003. Epub 2017 Sep 5.

Abstract

Rewarding doses of amphetamine increase the amplitude, duration, and frequency of dopamine transients in the ventral striatum. Debate continues at the behavioral level about which component of reward, learning or incentive salience, is signaled by these dopamine transients and thus altered in addiction. The learning hypothesis proposes that rewarding drugs result in pathological overlearning of drug-predictive cues, while the incentive sensitization hypothesis suggests that rewarding drugs result in sensitized attribution of incentive salience to drug-predictive cues. Therapeutic doses of amphetamine, such as those used to treat attention-deficit hyperactivity disorder, are hypothesized to enhance the ventral striatal dopamine transients that are critical for reward-related learning and to enhance Pavlovian learning. However, the effects of therapeutic doses of amphetamine on Pavlovian learning are poorly understood, and the effects on dopamine transients are completely unknown. We determined the effects of an acute pre-training therapeutic or rewarding amphetamine injection on the acquisition of Pavlovian autoshaping in the intact rat. We also determined the effects of these doses on electrically evoked transient-like dopamine signals using fast-scan cyclic voltammetry in the anesthetized rat. The rewarding dose enhanced the amplitude and duration of DA signals, caused acute task disengagement, impaired learning for several days, and triggered incentive sensitization. The therapeutic dose produced smaller enhancements in DA signals but did not have similar behavioral effects. These results underscore the necessity of more studies using therapeutic doses, and suggest a hybrid learning/incentive sensitization model may be required to explain the development of addiction.

摘要

给予奖赏剂量的苯丙胺会增加腹侧纹状体中多巴胺瞬变的幅度、持续时间和频率。在行为层面,关于这些多巴胺瞬变所传递的奖赏成分(学习或动机显著性)以及因此在成瘾过程中发生改变的成分,争论仍在继续。学习假说提出,奖赏性药物会导致对药物预测线索的病理性过度学习,而动机敏感化假说则表明,奖赏性药物会导致对药物预测线索的动机显著性的敏感化归因。据推测,治疗剂量的苯丙胺,如用于治疗注意力缺陷多动障碍的剂量,可增强对奖赏相关学习至关重要的腹侧纹状体多巴胺瞬变,并增强经典条件反射学习。然而,治疗剂量的苯丙胺对经典条件反射学习的影响了解甚少,对多巴胺瞬变的影响则完全未知。我们确定了急性预训练治疗性或奖赏性苯丙胺注射对完整大鼠经典条件反射自动形成习得的影响。我们还使用快速扫描循环伏安法在麻醉大鼠中确定了这些剂量对电诱发的类似瞬变多巴胺信号的影响。奖赏剂量增强了多巴胺信号的幅度和持续时间,导致急性任务脱离,在数天内损害学习,并引发动机敏感化。治疗剂量对多巴胺信号的增强作用较小,但没有类似的行为影响。这些结果强调了使用治疗剂量进行更多研究的必要性,并表明可能需要一种混合的学习/动机敏感化模型来解释成瘾的发展。

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