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在大鼠进行安非他命自我给药以及复吸期间,前额叶皮层和伏隔核中多巴胺和谷氨酸释放的失调。

Dysregulation of dopamine and glutamate release in the prefrontal cortex and nucleus accumbens following methamphetamine self-administration and during reinstatement in rats.

机构信息

Department of Neurosciences, Medical University of South Carolina Charleston, Charleston, SC, USA.

1] Department of Neurosciences, Medical University of South Carolina Charleston, Charleston, SC, USA [2] Faculty of Medicine, University of Tabuk, Tabuk, Saudi Arabia.

出版信息

Neuropsychopharmacology. 2014 Mar;39(4):811-22. doi: 10.1038/npp.2013.231. Epub 2013 Sep 2.

Abstract

Methamphetamine (meth) addicts often exhibit enduring cognitive and neural deficits that likely contribute to persistent drug seeking and the high rates of relapse. These deficits may be related to changes in the prefrontal cortex (PFC) and its glutamatergic projections to the nucleus accumbens (NAc). Here, we performed in vivo microdialysis in the PFC and NAc in rats following either meth self-administration or yoked-saline control histories to assess baseline glutamate (GLU) levels, or reinstatement-evoked GLU and dopamine (DA) efflux in both regions simultaneously under cue-induced, meth-primed, or combined cues+meth reinstatement conditions. Our results show that meth self-administration (1) reduced basal GLU levels in both the dmPFC and NAc, (2) concurrently increased dmPFC and NAc GLU efflux during reinstatement, and (3) increased DA efflux in the dmPFC, but not in the NAc, under all reinstatement conditions when compared with yoked-saline controls. These data demonstrate for the first time that a history of psychostimulant self-administration alters GLU homeostasis not only in the NAc, but also in the dmPFC, its primary GLU projection source. Furthermore, combined cues+meth-primed reinstatement conditions produced the most pronounced increases in mPFC and NAc extracellular GLU, suggesting that the cue and meth prime conditions are additive in promoting reinstatement. Finally, increased efflux of DA in the dmPFC, but not in the NAc, across reinstatement conditions suggests that DA release in the dmPFC may be an important mediator of drug seeking initiated by multiple relapse triggers.

摘要

甲基苯丙胺(冰毒)成瘾者经常表现出持久的认知和神经缺陷,这可能导致持续的觅药行为和高复发率。这些缺陷可能与前额叶皮层(PFC)及其谷氨酸能投射到伏隔核(NAc)的变化有关。在这里,我们在接受过冰毒自我给药或配对盐水控制历史的大鼠的 PFC 和 NAc 中进行了体内微透析,以评估基线谷氨酸(GLU)水平,或在线索诱导、冰毒引发或联合线索+冰毒引发的条件下,同时评估两个区域的再摄取引发的 GLU 和多巴胺(DA)外排。我们的结果表明,冰毒自我给药(1)降低了 dmPFC 和 NAc 中基础 GLU 水平,(2)同时在再摄取期间增加了 dmPFC 和 NAc GLU 外排,(3)与配对盐水对照相比,在所有再摄取条件下增加了 dmPFC 中的 DA 外排,但在 NAc 中没有。这些数据首次表明,兴奋剂自我给药的历史不仅改变了 NAc 中的 GLU 动态平衡,而且改变了其主要 GLU 投射源 dmPFC 中的 GLU 动态平衡。此外,联合线索+冰毒引发的再摄取条件产生了最显著的 dmPFC 和 NAc 细胞外 GLU 增加,表明线索和冰毒引发条件在促进再摄取方面是相加的。最后,dmPFC 中的 DA 外排增加,但 NAc 中没有,这表明 dmPFC 中的 DA 释放可能是多种复发性触发因素引发觅药行为的重要介质。

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