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Cocaine cues drive opposing context-dependent shifts in reward processing and emotional state.

机译:可卡因提示推动了奖励过程和情绪状态中与情境相关的相反转变。

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BACKGROUND: Prominent neurobiological theories of addiction posit a central role for aberrant mesolimbic dopamine release but disagree as to whether repeated drug experience blunts or enhances this system. Although drug withdrawal diminishes dopamine release, drug sensitization augments mesolimbic function, and both processes have been linked to drug seeking. One possibility is that the dopamine system can rapidly switch from dampened to enhanced release depending on the specific drug-predictive environment. To test this, we examined dopamine release when cues signaled delayed cocaine delivery versus imminent cocaine self-administration. METHODS: Fast-scan cyclic voltammetry was used to examine real-time dopamine release while simultaneously monitoring behavioral indexes of aversion as rats experienced a sweet taste cue that predicted delayed cocaine availability and during self-administration. Furthermore, the impact of cues signaling delayed drug availability on intracranial self-stimulation, a broad measure of reward function, was assessed. RESULTS: We observed decreased mesolimbic dopamine concentrations, decreased reward sensitivity, and negative affect in response to the cocaine-predictive taste cue that signaled delayed cocaine availability. Importantly, dopamine concentration rapidly switched to elevated levels to cues signaling imminent cocaine delivery in the subsequent self-administration session. CONCLUSIONS: These findings show rapid, bivalent contextual control over brain reward processing, affect, and motivated behavior and have implications for mechanisms mediating substance abuse.
机译:背景:成瘾的重要神经生物学理论在异常中脑边缘多巴胺释放中起着核心作用,但对于重复的药物治疗是否使该系统变钝或增强这一观点,人们意见分歧。尽管停药减少了多巴胺的释放,但药物敏化增强了中脑边缘功能,并且这两个过程都与寻求药物有关。一种可能性是,根据特定的药物预测环境,多巴胺系统可以迅速从润湿释放转变为增强释放。为了测试这一点,我们检查了提示可卡因递送延迟与可卡因自我给药即将到来时的多巴胺释放。方法:快速扫描循环伏安法用于检测实时多巴胺释放,同时监测厌恶行为指标,因为大鼠经历了甜味提示,预测可卡因的可利用性以及在自我给药期间。此外,评估了信号提示药物延迟供应对颅内自我刺激的影响,颅内自我刺激是对奖励功能的广泛衡量。结果:我们观察到中脑边缘多巴胺浓度降低,奖励敏感性降低以及对可卡因预测的味觉信号的不良反应,这暗示可卡因的可用性延迟。重要的是,多巴胺的浓度迅速切换到升高的水平,以暗示在随后的自我给药过程中即将释放可卡因。结论:这些发现表明对大脑奖励过程,情感和动机行为的快速,二价语境控制,对介导滥用药物的机制有影响。

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