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腹侧苍白球中的食欲素热点增强了对甜味的享乐性“喜好”。

An orexin hotspot in ventral pallidum amplifies hedonic 'liking' for sweetness.

机构信息

Department of Psychology, University of Michigan, Ann Arbor, MI 48109-1043, USA.

出版信息

Neuropsychopharmacology. 2013 Aug;38(9):1655-64. doi: 10.1038/npp.2013.62. Epub 2013 Mar 5.

Abstract

Orexin (hypocretin) is implicated in stimulating appetite as well as arousal, and in both food reward and drug reward. The ventral pallidum (VP) receives orexin projections from lateral hypothalamus neurons (LH), and orexin terminals are especially dense in the posterior half of VP, which is also the location of an opioid hedonic hotspot. The VP hotspot is a roughly cubic-millimeter site where mu opioid stimulation can amplify the hedonic impact of sweetness, expressed as an increase in 'liking' reactions to sucrose taste. The anatomical overlap in posterior VP between opioid hotspot and orexin inputs raises the possibility that the hedonic hotspot might allow orexin to amplify 'liking' too. We examined whether microinjections of orexin-A into the VP hotspot enhance the hedonic impact of sucrose, as assessed via affective taste reactivity measures of 'liking' reactions, and additionally compared effects at nearby sites in adjacent LH and extended amygdala. Taste reactivity results indicated that orexin stimulation specifically in the VP hotspot nearly doubled the magnitude of positive 'liking' reactions elicited by the taste of sucrose. Mapping results for localization of function, aided by Fos plume measures of the local spread of orexin impact, suggested that hedonic enhancement was generated by essentially the same cubic-millimeter of posterior VP previously identified as the opioid hotspot. By contrast, microinjection sites in the anterior half of VP, or in LH or extended amygdala, generally failed to produce any hedonic enhancement. We conclude that an orexin hedonic hotspot exists in posterior VP, with similar boundaries to the opioid hotspot. An orexin hedonic hotspot may permit regulatory hypothalamic circuitry to make foods more 'liked' during hunger by acting through VP. Dysfunction in a VP orexin hotspot in addiction or mood disorders might also contribute to some types of affective psychopathology.

摘要

食欲素(下丘脑泌素)参与刺激食欲和觉醒,以及食物奖励和药物奖励。腹侧苍白球(VP)接收来自外侧下丘脑神经元(LH)的食欲素投射,食欲素末梢在 VP 的后半部分特别密集,这也是阿片类物质快感热点的位置。VP 热点是一个大约立方毫米的位点,在这个位点,μ 阿片类刺激可以放大甜味的快感影响,表现为对蔗糖味觉的“喜欢”反应增加。在 VP 后区,阿片类物质热点和食欲素输入之间的解剖重叠,使得快感热点可能允许食欲素放大“喜欢”的可能性增加。我们检查了将食欲素-A 微注射到 VP 热点是否会增强蔗糖的快感影响,通过评估“喜欢”反应的情感味觉反应测量来评估,此外还比较了在相邻 LH 和扩展杏仁核中的附近部位的影响。味觉反应结果表明,食欲素刺激 VP 热点特异性地使蔗糖味觉引起的正“喜欢”反应的幅度增加了近一倍。功能定位的映射结果,借助食欲素影响的局部扩散的 Fos 羽流测量,表明快感增强是由以前确定为阿片类物质热点的 VP 后区的基本上相同的立方毫米产生的。相比之下,VP 前区、LH 或扩展杏仁核中的微注射部位通常不会产生任何快感增强。我们得出结论,VP 中的一个食欲素快感热点存在,与阿片类物质热点具有相似的边界。食欲素快感热点可能允许调节性下丘脑回路通过 VP 使食物在饥饿时更“喜欢”,在成瘾或情绪障碍中 VP 中的食欲素热点功能障碍也可能导致某些类型的情感精神病理学。

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