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边缘皮质纹状体系统与延迟强化。

Limbic corticostriatal systems and delayed reinforcement.

作者信息

Cardinal Rudolf N, Winstanley Catharine A, Robbins Trevor W, Everitt Barry J

机构信息

Department of Experimental Psychology, University of Cambridge, Downing Street, Cambridge CB2 3EB, UK.

出版信息

Ann N Y Acad Sci. 2004 Jun;1021:33-50. doi: 10.1196/annals.1308.004.

Abstract

Impulsive choice, one aspect of impulsivity, is characterized by an abnormally high preference for small, immediate rewards over larger delayed rewards, and can be a feature of adolescence, but also attention-deficit/hyperactivity disorder (ADHD), addiction, and other neuropsychiatric disorders. Both the serotonin and dopamine neuromodulator systems are implicated in impulsivity; manipulations of these systems affect animal models of impulsive choice, though these effects may depend on the receptor subtype and whether or not the reward is signaled. These systems project to limbic cortical and striatal structures shown to be abnormal in animal models of ADHD. Damage to the nucleus accumbens core (AcbC) causes rats to exhibit impulsive choice. These rats are also hyperactive, but are unimpaired in tests of visuospatial attention; they may therefore represent an animal model of the hyperactive-impulsive subtype of ADHD. Lesions to the anterior cingulate or medial prefrontal cortex, two afferents to the AcbC, do not induce impulsive choice, but lesions of the basolateral amygdala do, while lesions to the orbitofrontal cortex have had opposite effects in different tasks measuring impulsive choice. In theory, impulsive choice may emerge as a result of abnormal processing of the magnitude of rewards, or as a result of a deficit in the effects of delayed reinforcement. Recent evidence suggests that AcbC-lesioned rats perceive reward magnitude normally, but exhibit a selective deficit in learning instrumental responses using delayed reinforcement, suggesting that the AcbC is a reinforcement learning system that mediates the effects of delayed rewards.

摘要

冲动选择是冲动性的一个方面,其特征是异常倾向于小的即时奖励而非大的延迟奖励,它可能是青春期的一个特征,也可能是注意力缺陷多动障碍(ADHD)、成瘾及其他神经精神疾病的特征。血清素和多巴胺神经调节系统都与冲动性有关;对这些系统的操控会影响冲动选择的动物模型,不过这些影响可能取决于受体亚型以及奖励是否有信号提示。这些系统投射到在ADHD动物模型中显示异常的边缘皮质和纹状体结构。伏隔核核心(AcbC)受损会导致大鼠表现出冲动选择。这些大鼠也多动,但在视觉空间注意力测试中未受损;因此它们可能代表了ADHD多动冲动亚型的动物模型。前扣带回或内侧前额叶皮质(二者均为AcbC的传入神经)受损不会诱发冲动选择,但基底外侧杏仁核受损则会诱发,而眶额叶皮质受损在测量冲动选择的不同任务中会产生相反的效果。理论上,冲动选择可能是奖励大小异常处理的结果,或者是延迟强化效果缺陷的结果。最近的证据表明,AcbC受损的大鼠对奖励大小的感知正常,但在使用延迟强化学习工具性反应时表现出选择性缺陷,这表明AcbC是一个介导延迟奖励效果的强化学习系统。

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