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下丘脑泌素/食欲素系统通过作用于中脑边缘多巴胺系统调节可卡因的自我给药。

The hypocretin-orexin system regulates cocaine self-administration via actions on the mesolimbic dopamine system.

机构信息

Department of Physiology and Pharmacology, Wake Forest University Health Sciences, Winston-Salem, NC 27157, USA.

出版信息

Eur J Neurosci. 2010 Jan;31(2):336-48. doi: 10.1111/j.1460-9568.2009.07065.x. Epub 2009 Dec 23.

Abstract

Recent evidence suggests that the hypocretin-orexin system participates in the regulation of reinforcement processes. The current studies examined the extent to which hypocretin neurotransmission regulates behavioral and neurochemical responses to cocaine, and behavioral responses to food reinforcement. These studies used a combination of fixed ratio, discrete trials, progressive ratio and threshold self-administration procedures to assess whether the hypocretin 1 receptor antagonist, SB-334867, reduces cocaine self-administration in rats. Progressive ratio sucrose self-administration procedures were also used to assess the extent to which SB-334867 reduces responding to a natural reinforcer in food-restricted and food-sated rats. Additionally, these studies used microdialysis and in vivo voltammetry in rats to examine whether SB-334867 attenuates the effects of cocaine on dopamine signaling within the nucleus accumbens core. Furthermore, in vitro voltammetry was used to examine whether hypocretin knockout mice display attenuated dopamine responses to cocaine. Results indicate that when SB-334867 was administered peripherally or within the ventral tegmental area, it reduced the motivation to self-administer cocaine and attenuated cocaine-induced enhancement of dopamine signaling. SB-334867 also reduced the motivation to self-administer sucrose in food-sated but not food-restricted rats. Finally, hypocretin knockout mice displayed altered baseline dopamine signaling and reduced dopamine responses to cocaine. Combined, these studies suggest that hypocretin neurotransmission participates in reinforcement processes, likely through modulation of the mesolimbic dopamine system. Additionally, the current observations suggest that the hypocretin system may provide a target for pharmacotherapies to treat cocaine addiction.

摘要

最近的证据表明,下丘脑分泌素-食欲素系统参与了强化过程的调节。目前的研究考察了下丘脑分泌素神经传递在多大程度上调节可卡因的行为和神经化学反应,以及食物强化的行为反应。这些研究使用了固定比率、离散试验、递增比率和阈值自我给药程序的组合,以评估下丘脑分泌素 1 受体拮抗剂 SB-334867 是否减少大鼠可卡因的自我给药。递增比率蔗糖自我给药程序也用于评估 SB-334867 减少在食物限制和食物饱和的大鼠中对自然强化物的反应的程度。此外,这些研究使用微透析和大鼠体内伏安法检查 SB-334867 是否减弱可卡因对伏隔核核心内多巴胺信号的影响。此外,在体外伏安法用于检查下丘脑分泌素敲除小鼠是否显示出对可卡因的多巴胺反应减弱。结果表明,当 SB-334867 经外周或腹侧被盖区给药时,它降低了自我给予可卡因的动机,并减弱了可卡因诱导的多巴胺信号增强。SB-334867 还降低了食物饱和而非食物限制大鼠中蔗糖自我给药的动机。最后,下丘脑分泌素敲除小鼠显示出改变的基线多巴胺信号和可卡因反应减少。综上所述,下丘脑分泌素神经传递参与强化过程,可能通过调节中脑边缘多巴胺系统。此外,目前的观察结果表明,下丘脑分泌素系统可能为治疗可卡因成瘾的药物治疗提供靶点。

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