首页> 外文期刊>Neuropharmacology >Upregulation of the dorsal raphe nucleus-prefrontal cortex serotonin system by chronic treatment with escitalopram in hyposerotonergic Wistar-Kyoto rats.
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Upregulation of the dorsal raphe nucleus-prefrontal cortex serotonin system by chronic treatment with escitalopram in hyposerotonergic Wistar-Kyoto rats.

机译:用慢性致胰岛蛋白核苷酸慢性处理慢性治疗慢性治疗慢性治疗慢性治疗慢性卟啉血酮大鼠的慢性治疗。

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摘要

Wistar-Kyoto (WKY) rats are sensitive to chronic stressors and exhibit depression-like behavior. Dorsal raphe nucleus (DRN) serotonin (5-HT) neurons projecting to the prefrontal cortex (PFC) comprise the important neurocircuitry underlying the pathophysiology of depression. To evaluate the DRN-PFC 5-HT system in WKY rats, we examined the effects of escitalopram (ESCIT) on the extracellular 5-HT level in comparison with Wistar rats using dual-probe microdialysis. The basal levels of 5-HT in the DRN, but not in the PFC, in WKY rats was reduced as low as 30% of Wistar rats. Responses of 5-HT in the DRN and PFC to ESCIT administered systemically and locally were attenuated in WKY rats. Feedback inhibition of DRN 5-HT release induced by ESCIT into the PFC was also attenuated in WKY rats. Chronic ESCIT induced upregulation of the DRN-PFC 5-HT system in WKY rats, with increases in basal 5-HT in the DRN, responsiveness to ESCIT in the DRN and PFC, and feedback inhibition, whereas downregulation of these effects was induced in Wistar rats. Thus, the WKY rat is an animal model of depression with low activity of the DRN-PFC 5HT system. The finding that chronic ESCIT upregulates the 5-HT system in hyposerotonergic WKY rats may contribute to improved understanding of mechanisms of action of antidepressants, especially in depression with 5-HT deficiency.
机译:Wistar-kyoto(WKY)大鼠对慢性压力源敏感,表现出抑郁症状的行为。突出前额叶皮质(PFC)的二甲状腺核(DRN)血清素(5-HT)神经元包括抑郁症病理生理学潜在的重要神经皮序。为了评估WKY大鼠的DRN-PFC 5-HT系统,我们研究了使用双探针微透过的Wistar大鼠的Escitalopram(ESCIT)对细胞外5-HT水平的影响。在WKY大鼠中,DRN中的5-HT的基础水平为5-HT,低至Wistar大鼠的30%低至30%。在WKY大鼠中,DRN和PFC中5-HT在DRN和PFC中的反应衰减。反馈抑制通过escit诱导的REC进入PFC的DRN 5-HT释放在WKY大鼠中也衰减。慢性转述诱导WKY大鼠DrN-PFC 5-HT系统的上调,DRN中的基础5-HT增加,在DRN和PFC中的反应性和反馈抑制,而在Wistar诱导这些效应的下调老鼠。因此,WKY大鼠是DRN-PFC 5HT系统低活性的抑郁症的动物模型。慢性转向上调慢性致盲肠病大鼠5-HT系统的发现可能有助于改善对抗抑郁药的作用机制的理解,特别是在5-HT缺乏的抑郁症中。

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