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Pattern of c-Fos expression induced by tail suspension test in the mouse brain

机译:尾部悬吊试验在小鼠脑中诱导的c-Fos表达模式

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摘要

The tail suspension test (TST) has been widely used as a screening assay for antidepressant drugs. However, the neural substrates underlying the stress response and antidepressant-like effect during the TST remain largely unknown despite the prevalence of this test. In the present study, we used immunohistochemistry to examine alterations in c-Fos expression as a measure of neuronal activity in the mouse brain after acute administration of the antidepressant drugs nortriptyline or escitalopram (or saline as a control) with or without a subsequent TST session. We found that without the TST session, nortriptyline administration enhanced the density of c-Fos-immunoreactive cells in regions of the central extended amygdala, paraventricular hypothalamic nucleus, and relevant regions of the brain stem, whereas escitalopram did not change c-Fos expression in any region. Following the TST in the absence of antidepressant drugs, we observed a significant increase in c-Fos-positive cell density in a number of brain regions within the limbic telencephalon, hypothalamus, and brain stem. We detected a statistically significant interaction using an analysis of variance between the main effects of the drug and stress response in four regions: the infralimbic cortex, lateral septal nucleus (intermediate part), ventrolateral preoptic nucleus, and solitary nucleus. Following the TST, escitalopram but not nortriptyline increased c-Fos-positive cell density in the infralimbic cortex and ventrolateral preoptic nucleus, whereas nortriptyline but not escitalopram increased c-Fos expression in the solitary nucleus. Both antidepressants significantly increased c-Fos expression in the lateral septal nucleus (intermediate part). The present results indicate that neuronal activity increases in septo-hypothalamic regions and related structures, especially the lateral septal nucleus, following administration of drugs producing an antidepressant-like effect in mice subjected to the TST.
机译:尾部悬浮试验(TST)已被广泛用作抗抑郁药的筛选试验。然而,尽管该试验普遍存在,但在TST期间潜在的应激反应和抗抑郁样作用的神经基质仍然未知。在本研究中,我们使用免疫组化方法检查了抗抑郁药去甲替林或艾司西酞普兰(或以生理盐水为对照)在有或没有随后的TST疗程的情况下急性给药后c-Fos表达的变化,以此作为小鼠大脑中神经元活性的量度。我们发现,在没有TST环节的情况下,去甲替林给药可增加杏仁核中央扩展区,丘脑下丘脑旁核以及脑干相关区域c-Fos免疫反应性细胞的密度,而依西酞普兰不会改变c-Fos的表达。任何地区。在没有抗抑郁药的情况下进行TST后,我们观察到边缘端脑,下丘脑和脑干内多个大脑区域的c-Fos阳性细胞密度显着增加。我们通过分析以下四个区域中药物的主要作用与应激反应之间的方差来检测出统计学上显着的相互作用:下肢皮质,外侧中隔核(中间部分),腹侧视前核和孤立核。在TST后,依西酞普兰而不是去甲替林增加了下唇皮层和腹侧前视核中的c-Fos阳性细胞密度,而去甲替林而不是依西酞普兰却不增加了在孤核中的c-Fos表达。两种抗抑郁药均显着增加了外侧中隔核(中间部分)的c-Fos表达。本结果表明,在给予TST的小鼠中施用产生抗抑郁样作用的药物后,隔下丘脑区域和相关结构,特别是外侧中隔核的神经元活性增加。

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