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急性吗啡诱导大鼠脑内c-fos信使核糖核酸的模式

Pattern of c-fos mRNA induction in rat brain by acute morphine.

作者信息

Gutstein H B, Thome J L, Fine J L, Watson S J, Akil H

机构信息

Mental Health Research Institute, University of Michigan, Ann Arbor 48109-0720, USA.

出版信息

Can J Physiol Pharmacol. 1998 Mar;76(3):294-303.

PMID:9673793
Abstract

Initially, opioid signaling had been thought to be mainly inhibitory in nature. However, it has been shown that opioids can activate specific signaling pathways and induce immediate early gene (IEG) transcription in brain. IEGs can then regulate the transcription of other genes, leading to changes in neuronal function in response to extracellular stimuli. This study was designed to identify brain regions that demonstrate specific induction of the IEG c-fos, a component of the AP-1 transcription factor, in response to acute morphine, and to contrast this induction with the stressful effects of the injection itself. Rats received either 10 mg/kg morphine or an equivalent volume of saline injected subcutaneously. Animals were then sacrificed 15, 30, or 60 min after injection. Specific induction of c-fos mRNA by morphine was seen in dorsomedial caudate-putamen, paraventricular nucleus of the thalamus, central and intralaminar thalamic nuclei, dorsal central grey, superior colliculus, lateral parabrachial nucleus, inferior olivary complex, and caudal nucleus tractus solitarius. These findings represent the first complete anatomical mapping of c-fos induction in rat brain, and show that acute morphine administration alters gene expression in several areas related to known functional properties of opioids. However, regions showing c-fos induction are not all classically associated with opioid receptors and opioid-mediated effects. These findings are considered in the context of the effects of opioids on neural circuitry as well as direct, receptor-mediated effects of morphine on neural cells.

摘要

最初,人们认为阿片类信号本质上主要是抑制性的。然而,已有研究表明,阿片类物质可激活特定的信号通路并诱导大脑中即刻早期基因(IEG)的转录。然后,IEG可调节其他基因的转录,从而导致神经元功能因细胞外刺激而发生变化。本研究旨在确定在急性给予吗啡后,大脑中哪些区域会出现AP-1转录因子的组成部分——IEG c-fos的特异性诱导,并将这种诱导与注射本身的应激效应进行对比。大鼠皮下注射10mg/kg吗啡或等量的生理盐水。然后在注射后15、30或60分钟处死动物。吗啡可在背内侧尾状核-壳核、丘脑室旁核、丘脑中央核和板内核、背侧中央灰质、上丘、外侧臂旁核、下橄榄复合体以及延髓尾侧孤束核中诱导c-fos mRNA的特异性表达。这些发现代表了大鼠脑中c-fos诱导的首次完整解剖图谱,并表明急性给予吗啡会改变与阿片类物质已知功能特性相关的几个区域的基因表达。然而,显示c-fos诱导的区域并非都与阿片受体和阿片介导的效应有经典关联。这些发现是在阿片类物质对神经回路的影响以及吗啡对神经细胞的直接、受体介导的效应的背景下进行考虑的。

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