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短暂暴露于捕食者气味及由此产生的焦虑会增强CD-1小鼠的中脑皮质边缘系统活动和脑啡肽表达。

Brief exposure to predator odor and resultant anxiety enhances mesocorticolimbic activity and enkephalin expression in CD-1 mice.

作者信息

Hebb Andrea L O, Zacharko Robert M, Gauthier Michelle, Trudel France, Laforest Sylvie, Drolet Guy

机构信息

Institute of Neuroscience, Carleton University, Ottawa, Ontario, Canada.

出版信息

Eur J Neurosci. 2004 Nov;20(9):2415-29. doi: 10.1111/j.1460-9568.2004.03704.x.

Abstract

The present study assessed alterations in mesolimbic enkephalin (ENK) mRNA levels after predator [2,5-dihydro-2,4,5-trimethylethiazoline (TMT)] and non-predator (butyric acid) odor encounter and/or light-dark (LD) testing in CD-1 mice immediately, 24, 48 and 168 h after the initial odor encounter and/or LD testing. The nucleus accumbens, ventral tegmental area, basolateral (BLA), central (CEA) and medial amygdaloid nuclei, prelimbic and infralimbic cortex were assessed for fos-related antigen (FRA) and/or ENK mRNA as well as neuronal activation of ENK neurons (FRA/ENK). Mice exposed to TMT displayed enhanced freezing and spent less time in the light of the immediate LD test relative to saline- or butyric acid-treated mice. Among mice exposed to TMT, LD anxiety-like behavior was associated with increased FRA in the prelimbic cortex and accumbal shell and decreased ENK-positive neurons in the accumbal core. Mice displaying high TMT-induced LD anxiety exhibited increased ENK-positive neurons in the BLA, CEA and medial amygdaloid nuclei relative to mice that displayed low anxiety-like behavior in the LD test after TMT exposure. In the BLA and CEA, 'high-anxiety' mice also displayed increased FRA/ENK after TMT exposure and LD testing. In contrast to neural cell counts, the level of ENK transcript was decreased in the BLA and CEA of 'high-anxiety' mice after TMT exposure and LD testing. These data suggest that increased FRA may regulate stressor-responsive genes and mediate long-term behavioral changes. Indeed, increased ENK availability in mesolimbic sites may promote behavioral responses that detract from the aversiveness of the stressor experience.

摘要

本研究评估了在CD-1小鼠初次接触捕食者[2,5-二氢-2,4,5-三甲基噻唑啉(TMT)]和非捕食者(丁酸)气味以及/或者明暗(LD)测试后,立即、24小时、48小时和168小时时中脑边缘脑啡肽(ENK)mRNA水平的变化。对伏隔核、腹侧被盖区、基底外侧(BLA)、中央(CEA)和内侧杏仁核、前边缘皮层和边缘下皮层进行了fos相关抗原(FRA)和/或ENK mRNA以及ENK神经元的神经元激活(FRA/ENK)评估。与盐水或丁酸处理的小鼠相比,接触TMT的小鼠在即时LD测试中表现出增强的僵立反应,且在明处停留的时间更少。在接触TMT的小鼠中,LD焦虑样行为与前边缘皮层和伏隔核壳中的FRA增加以及伏隔核核心中ENK阳性神经元减少有关。与在TMT暴露后的LD测试中表现出低焦虑样行为的小鼠相比,表现出高TMT诱导的LD焦虑的小鼠在BLA、CEA和内侧杏仁核中ENK阳性神经元增加。在BLA和CEA中,“高焦虑”小鼠在TMT暴露和LD测试后也表现出FRA/ENK增加。与神经细胞计数相反,“高焦虑”小鼠在TMT暴露和LD测试后,BLA和CEA中的ENK转录水平降低。这些数据表明,FRA增加可能调节应激源反应基因并介导长期行为变化。事实上,中脑边缘部位ENK可用性增加可能促进行为反应,从而减轻应激源体验的厌恶感。

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