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重新审视内侧基底下丘脑的屏障

A second look at the barriers of the medial basal hypothalamus.

作者信息

Peruzzo B, Pastor F E, Blázquez J L, Schöbitz K, Peláez B, Amat P, Rodríguez E M

机构信息

Departamento de Anatomía e Histología Humanas, Facultad de Medicina, Universidad de Salamanca, Spain.

出版信息

Exp Brain Res. 2000 May;132(1):10-26. doi: 10.1007/s002219900289.

Abstract

The cell bodies of hypothalamic secretory neurons are localized in areas protected by the blood-brain barrier (BBB), whereas their axon terminals are localized in the median eminence, which lacks a BBB. This implies a complex barrier system, allowing neurons of the central nervous system to secrete into the blood stream without making the BBB leaky. In the present study, three experimental protocols were applied to clarify certain relevant aspects of the barriers operating in the medial basal hypothalamus of the rat. We established that the milieu of the arcuate nucleus is exposed to both the ventricular and the subarachnoidal cerebrospinal fluid (CSF). The median eminence milieu, the perivascular space of the portal vessels, and the subarachnoid space appear to be in open communication; also, beta2-tanycytes establish an efficient barrier between the median eminence milieu and the ventricular CSF. Similarly, beta1-tanycytes establish a lateral barrier, separating the intercellular space of the median eminence from that of the arcuate nucleus. We also found that the glucose transporter I (GLUT I), a BBB marker, is localized throughout the whole plasma membrane of beta1-tanycytes, but is missing from beta2-tanycytes. Expression of GLUT I by tanycytes progressively develops during the first postnatal weeks; while the degree of damage of the arcuate nucleus by administration of monosodium glutamate, at different postnatal intervals, parallels that of the GLUT I immunoreactivity of beta1-tanycytes. An explanation is offered for the selective destruction of the arcuate neurons by the parenteral administration of monosodium glutamate to infant rats.

摘要

下丘脑分泌神经元的细胞体位于血脑屏障(BBB)保护的区域,而它们的轴突终末位于缺乏血脑屏障的正中隆起。这意味着存在一个复杂的屏障系统,使中枢神经系统的神经元能够分泌到血流中而不破坏血脑屏障的完整性。在本研究中,应用了三种实验方案来阐明大鼠内侧基底下丘脑屏障的某些相关方面。我们确定,弓状核的微环境暴露于脑室和蛛网膜下腔脑脊液(CSF)。正中隆起微环境、门静脉血管的血管周围间隙和蛛网膜下腔似乎是相通的;此外,β2-伸展细胞在正中隆起微环境与脑室脑脊液之间建立了有效的屏障。同样,β1-伸展细胞建立了一个侧向屏障,将正中隆起的细胞间隙与弓状核的细胞间隙分隔开。我们还发现,血脑屏障标志物葡萄糖转运体I(GLUT I)定位于β1-伸展细胞的整个质膜,但在β2-伸展细胞中缺失。伸展细胞中GLUT I的表达在出生后的头几周逐渐发展;而在不同出生后时间段通过给予谷氨酸单钠对弓状核造成的损伤程度与β1-伸展细胞的GLUT I免疫反应性程度平行。本文对给幼鼠经肠外给予谷氨酸单钠导致弓状神经元选择性破坏的现象提供了一种解释。

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