首页> 外文期刊>Behavioural Brain Research: An International Journal >Dopaminergic modulation of the orbitofrontal cortex affects attention, motivation and impulsive responding in rats performing the five-choice serial reaction time task.
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Dopaminergic modulation of the orbitofrontal cortex affects attention, motivation and impulsive responding in rats performing the five-choice serial reaction time task.

机译:在执行五选择序列反应时间任务的大鼠中,眶额皮质的多巴胺能调节影响注意力,动机和冲动反应。

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Understanding the neurobiological factors underlying individual differences in impulsivity may provide valuable insight into vulnerability to impulse control disorders. Recent data implicate both the orbitofrontal cortex (OFC) and the dopaminergic system in psychiatric disorders associated with high levels of impulsivity, including substance abuse, mania and obsessive-compulsive disorder. However, the consequences of modulating dopaminergic activity within the OFC on impulsive behaviour are largely unknown. The effects of direct intra-OFC infusions of agonists and antagonists at the dopamine D(1) and D(2) receptors were therefore assessed in rats performing the five-choice serial reaction time test (5CSRT) of attention and motor impulsivity. Intra-OFC administration of SCH23390, a D(1) receptor antagonist, decreased impulsive responding in highly impulsive (HI) rats, but did not affect behaviour in less impulsive (LI) animals. Furthermore, the D(2) agonist quinpirole caused significant deficits in task performance, impairing accuracy, increasing omissions and decreasing the number of trials completed, which resembled the effects of systemic administration. In contrast, the D(1) agonist SKF 81297 had little effect on behaviour. Neither agonist increased impulsivity. These data provide partial support for the suggestion that high levels of impulsivity are associated with increased dopamine levels within the OFC, but further indicate that simulating dopamine's actions selectively at the D(1) or D(2) receptor cannot reproduce a highly impulsive phenotype. Dopaminergic activity within the OFC may therefore modulate impulsivity indirectly, perhaps in conjunction with other neurotransmitter systems. Furthermore, D(2)-mediated neurotransmission within the OFC could make a more fundamental contribution to cognitive behaviour.
机译:了解冲动个体差异背后的神经生物学因素,可能会为冲动控制障碍的脆弱性提供有价值的见解。最近的数据表明,与高冲动性有关的精神疾病包括眶额皮质(OFC)和多巴胺能系统,包括药物滥用,躁狂症和强迫症。然而,在OFC内调节多巴胺能活性对冲动行为的后果在很大程度上是未知的。因此,在进行注意力和运动冲动的五选择系列反应时间测试(5CSRT)的大鼠中评估了直接激动剂和拮抗剂对多巴胺D(1)和D(2)受体的OFC内直接输注的影响。 SCH23390(一种D(1)受体拮抗剂)的OFC内给药可降低高冲动(HI)大鼠的冲动反应,但不影响冲动较小(LI)的动物的行为。此外,D(2)激动剂喹吡罗引起任务表现严重不足,准确性降低,遗漏增加和完成的试验次数减少,这类似于全身给药的效果。相反,D(1)激动剂SKF 81297对行为的影响很小。两种激动剂均未增加冲动性。这些数据为高冲动与OFC中多巴胺水平升高相关的建议提供了部分支持,但进一步表明模拟D(1)或D(2)受体选择性模拟多巴胺的行为不能重现高度冲动的表型。因此,OFC内的多巴胺能活动可能间接地与其他神经递质系统一起调节冲动。此外,OFC中D(2)介导的神经传递可以对认知行为做出更根本的贡献。

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