Brain substrates for reinforcement and drug self-administration

Roy A. Wise, Michael A. Bozarth
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引用次数: 109

Abstract

  • 1.

    1. Animals will work for stimulation of some parts of their own brains; this suggests that the brain has specialized circuitry for mediation of reward.

  • 2.

    2. Current evidence identifies two links in such circuitry: a myelinated, descending, medial forebrain bundle link and an ascending, dopaminergic, medial forebrain bundle link. The myelinated link makes probable synaptic contact with the dopaminergic cells of the ventral tegmental area and substantia nigra. These dopaminergic cells may receive other myelinated and reward-relevant afferents as well, particularly from the brainstem.

  • 3.

    3. Psychomotor stimulants facilitate intracranial self-stimulation by acting at terminals of the dopaminergic link, particularly in nucleus accumbens. Opiates facilitate self-stimulation by acting at the dopamine cell bodies in the ventral tegmentum. Facilitation of self-stimulation by other drugs of abuse has not been localized to a site of action.

  • 4.

    4. Psychomotor stimulants have rewarding actions of their own in nucleus accumbens. Opiates have rewarding actions at the dopaminergic cell body region of the ventral tegmentum. The sites of rewarding action have not been determined for other drugs of abuse.

  • 5.

    5. The substrate mediating rewarding actions of opiates and psychomotor stimulants also mediates the rewarding action of more natural rewards like food and water. The fact that some drugs of abuse can come to dominate behavior in relation to more natural rewards may stem from the more direct central actions of drugs on the reward substrate. The fact that the rewarding effects of food, water, opiates, and psychomotor stimulants feel subjectively dissimilar may simply reflect the fact that while a common rewarding action is shared by these agents, many other effects which are subjectively experienced differ between agents and obscure awareness of a common dimension of all positive rewards.

强化和自我给药的脑底物
1.1. 动物会努力刺激自己大脑的某些部分;这表明大脑有专门的回路来调解奖励。目前的证据确定了这种电路中的两个环节:有髓鞘的、下行的、内侧前脑束的联系和上升的、多巴胺能的、内侧前脑束的联系。髓鞘连接可能与腹侧被盖区和黑质的多巴胺能细胞进行突触接触。这些多巴胺能细胞也可以接受其他髓鞘和奖励相关的传入,特别是来自脑干的传入。精神运动兴奋剂通过作用于多巴胺能连接的末端,特别是伏隔核,促进颅内自我刺激。阿片类药物通过作用于腹侧被盖的多巴胺细胞体促进自我刺激。其他滥用药物对自我刺激的促进作用尚未局限于作用部位。精神运动兴奋剂在伏隔核中有其自身的奖励作用。阿片类药物在腹侧被盖的多巴胺能细胞体区域有奖励作用。其他滥用药物的奖赏作用位点尚未确定。介导阿片类药物和精神运动兴奋剂的奖励作用的底物也介导更自然的奖励作用,如食物和水。一些滥用药物可以支配与更自然的奖励相关的行为,这一事实可能源于药物对奖励基质的更直接的中心作用。食物、水、鸦片和精神运动兴奋剂的奖励效果在主观上是不同的,这一事实可能只是反映了这样一个事实:虽然这些主体共享一个共同的奖励行为,但在主观上体验到的许多其他效果在主体之间是不同的,并且模糊了所有积极奖励的共同维度。
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