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下丘脑食欲素(下丘脑泌素)神经元表达囊泡谷氨酸转运体VGLUT1或VGLUT2。

Hypothalamic orexin (hypocretin) neurons express vesicular glutamate transporters VGLUT1 or VGLUT2.

作者信息

Rosin Diane L, Weston Matthew C, Sevigny Charles P, Stornetta Ruth L, Guyenet Patrice G

机构信息

Department of Pharmacology, University of Virginia, Charlottesville, Virginia 22908, USA.

出版信息

J Comp Neurol. 2003 Oct 27;465(4):593-603. doi: 10.1002/cne.10860.

Abstract

Initially recognized for their importance in control of appetite, orexins (also called hypocretins) are neuropeptides that are also involved in regulating sleep, arousal, and cardiovascular function. Loss of orexin appears to be the primary cause of narcolepsy. Cells expressing the orexins are restricted to a discrete region of the hypothalamus, but their terminal projections are widely distributed throughout the brain. With the diversity of function and broad distribution of orexin terminals, it is not known whether the orexin cells constitute a homogeneous population. Because orexins produce neuroexcitatory effects, we hypothesized that orexin-containing neurons are glutamatergic. In the present study we used digoxigenin-labeled cRNA probes for the vesicular glutamate transporters, VGLUT1 and VGLUT2, for in situ hybridization studies in combination with immunohistochemical detection of orexin cell bodies in the hypothalamus. In general, cells in the hypothalamus expressed low levels of the vesicular glutamate transporters relative to other areas of the forebrain, such as the cortex and thalamus. Light labeling for VGLUT2 mRNA was detected in about 50% of the orexin-immunoreactive neurons, and a much smaller percentage (approximately 13%) of orexin-immunoreactive cells was found to express VGLUT1. Despite the fact that intense labeling for GAD67 mRNA was found in a large number of cells throughout the hypothalamus, none of the orexin-immunoreactive cells was found to be GABAergic. These findings, showing that many of the orexin neurons are glutamatergic, are consistent with the neuroexcitatory effects of orexin but suggest that another neurochemical phenotype may define the remaining subset of orexin neurons.

摘要

食欲素(也称为下丘脑泌素)最初因其在控制食欲方面的重要性而被认识,它们是神经肽,也参与调节睡眠、觉醒和心血管功能。食欲素的丧失似乎是发作性睡病的主要原因。表达食欲素的细胞局限于下丘脑的一个离散区域,但其终末投射广泛分布于整个大脑。鉴于食欲素功能的多样性和其终末的广泛分布,目前尚不清楚食欲素细胞是否构成一个同质群体。由于食欲素产生神经兴奋作用,我们推测含食欲素的神经元是谷氨酸能的。在本研究中,我们使用地高辛标记的cRNA探针检测囊泡谷氨酸转运体VGLUT1和VGLUT2,结合下丘脑食欲素细胞体的免疫组织化学检测进行原位杂交研究。一般来说,下丘脑的细胞相对于前脑的其他区域,如皮层和丘脑,表达的囊泡谷氨酸转运体水平较低。在约50%的食欲素免疫反应性神经元中检测到VGLUT2 mRNA的轻度标记,而发现表达VGLUT1的食欲素免疫反应性细胞的比例要小得多(约13%)。尽管在下丘脑的大量细胞中发现了GAD67 mRNA的强烈标记,但未发现任何食欲素免疫反应性细胞是γ-氨基丁酸能的。这些结果表明许多食欲素神经元是谷氨酸能的,这与食欲素的神经兴奋作用一致,但提示另一种神经化学表型可能定义了食欲素神经元的其余子集。

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