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消除大鼠的成瘾习惯:背内侧纹状体中的腺苷2A受体拮抗作用可挽救甲基苯丙胺诱导的目标导向行为缺陷。

Pulling habits out of rats: adenosine 2A receptor antagonism in dorsomedial striatum rescues meth-amphetamine-induced deficits in goal-directed action.

作者信息

Furlong Teri M, Supit Alva S A, Corbit Laura H, Killcross Simon, Balleine Bernard W

机构信息

Brain & Mind Research Institute, University of Sydney, Australia.

School of Psychology, University of Sydney, Australia.

出版信息

Addict Biol. 2017 Jan;22(1):172-183. doi: 10.1111/adb.12316. Epub 2015 Oct 30.

Abstract

Addiction is characterized by a persistent loss of behavioral control resulting in insensitivity to negative feedback and abnormal decision-making. Here, we investigated the influence of methamphetamine (METH)-paired contextual cues on decision-making in rats. Choice between goal-directed actions was sensitive to outcome devaluation in a saline-paired context but was impaired in the METH-paired context, a deficit that was also found when negative feedback was provided. Reductions in c-Fos-related immunoreactivity were found in dorsomedial striatum (DMS) but not dorsolateral striatum after exposure to the METH context suggesting this effect reflected a loss specifically in goal-directed control in the METH context. This reduction in c-Fos was localized to non-enkephalin-expressing neurons in the DMS, likely dopamine D1-expressing direct pathway neurons, suggesting a relative change in control by the D1-direct versus D2-indirect pathways originating in the DMS may have been induced by METH-context exposure. To test this suggestion, we infused the adenosine 2A receptor antagonist ZM241385 into the DMS prior to test to reduce activity in D2 neurons relative to D1 neurons in the hope of reducing the inhibitory output from this region of the striatum. We found that this treatment fully restored sensitivity to negative feedback in a test conducted in the METH-paired context. These results suggest that drug exposure alters decision-making by downregulation of the circuitry mediating goal-directed action, an effect that can be ameliorated by acute A receptor inhibition in this circuit.

摘要

成瘾的特征是行为控制持续丧失,导致对负面反馈不敏感和决策异常。在此,我们研究了与甲基苯丙胺(METH)配对的情境线索对大鼠决策的影响。在与生理盐水配对的情境中,目标导向行为之间的选择对结果贬值敏感,但在与METH配对的情境中受损,当提供负面反馈时也发现了这种缺陷。暴露于METH情境后,背内侧纹状体(DMS)中c-Fos相关免疫反应性降低,但背外侧纹状体中未降低,这表明这种效应反映了在METH情境中目标导向控制的特异性丧失。这种c-Fos的降低定位于DMS中不表达脑啡肽的神经元,可能是表达多巴胺D1的直接通路神经元,这表明源自DMS的D1直接与D2间接通路控制的相对变化可能是由METH情境暴露诱导的。为了验证这一观点,我们在测试前将腺苷2A受体拮抗剂ZM241385注入DMS,以降低D2神经元相对于D1神经元的活性,希望减少纹状体该区域的抑制输出。我们发现,这种处理在与METH配对的情境中进行的测试中完全恢复了对负面反馈的敏感性。这些结果表明,药物暴露通过下调介导目标导向行为的神经回路来改变决策,这种效应可通过该回路中急性A受体抑制来改善。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b2f4/4851927/5fcc8eaa0846/nihms735474f1.jpg

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