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伏隔核核心的部分失活可降低大鼠的延迟折扣,而不影响其对延迟或大小的敏感性。

Partial inactivation of nucleus accumbens core decreases delay discounting in rats without affecting sensitivity to delay or magnitude.

作者信息

Moschak Travis M, Mitchell Suzanne H

机构信息

Oregon Health & Science University, USA.

Oregon Health & Science University, USA.

出版信息

Behav Brain Res. 2014 Jul 15;268:159-68. doi: 10.1016/j.bbr.2014.03.044. Epub 2014 Apr 2.

Abstract

Increased preference for smaller, sooner rewards (delay discounting) is associated with several behavioral disorders, including ADHD and substance use disorders. However, delay discounting is a complex cognitive process and the relationship is unclear between the pathophysiology of the disorders and the component processes underlying delay discounting, including sensitivity to reinforcer delay and sensitivity to reinforcer magnitude. To investigate these processes, male Long Evans rats were trained in one of three tasks measuring sensitivity to delay, sensitivity to magnitude, or both (typical delay discounting task). After learning the task, animals were implanted with bilateral cannulae into either the nucleus accumbens core (AcbC) or the lateral orbitofrontal cortex (lOFC), both of which have been implicated in delay discounting. Upon recovering from the surgery, a baclofen/muscimol cocktail was infused to temporarily inactivate each of these two regions and task performance was assessed. Unlike previous studies showing that lesions of the AcbC increased delay discounting, partial inactivation of the AcbC decreased delay discounting, although it had no effects on the tasks independently assessing either sensitivity to delay or magnitude. The effects of AcbC inactivation were larger in animals that had low levels of delay discounting at baseline. Inactivation of the lOFC had no effects on behavior in any task. These findings suggest that the AcbC may act to promote impulsive choice in individuals with low impulsivity. Furthermore, the data suggest that the AcbC is able to modulate delay and magnitude sensitivity together, but not either of the two in isolation.

摘要

对更小、更早的奖励(延迟折扣)的偏好增加与多种行为障碍有关,包括注意力缺陷多动障碍(ADHD)和物质使用障碍。然而,延迟折扣是一个复杂的认知过程,这些障碍的病理生理学与延迟折扣背后的组成过程(包括对强化物延迟的敏感性和对强化物大小的敏感性)之间的关系尚不清楚。为了研究这些过程,雄性朗·埃文斯大鼠接受了三项任务中的一项训练,这三项任务分别测量对延迟的敏感性、对大小的敏感性或两者(典型的延迟折扣任务)。在学会任务后,动物被双侧插管植入伏隔核核心(AcbC)或外侧眶额叶皮层(lOFC),这两个区域都与延迟折扣有关。手术后恢复时,注入巴氯芬/蝇蕈醇混合剂以暂时使这两个区域失活,并评估任务表现。与之前显示AcbC损伤会增加延迟折扣的研究不同,AcbC的部分失活降低了延迟折扣,尽管它对独立评估对延迟或大小敏感性的任务没有影响。在基线时延迟折扣水平较低的动物中,AcbC失活的影响更大。lOFC的失活对任何任务中的行为都没有影响。这些发现表明,AcbC可能在低冲动性个体中起到促进冲动选择的作用。此外,数据表明,AcbC能够同时调节延迟和大小敏感性,但不能单独调节两者中的任何一个。

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