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血管紧张素原在胎鼠和新生鼠脑中的免疫细胞化学定位

Immunocytochemical localization of angiotensinogen in the fetal and neonatal rat brain.

作者信息

Mungall B A, Shinkel T A, Sernia C

机构信息

Department of Physiology and Pharmacology, University of Queensland, Australia.

出版信息

Neuroscience. 1995 Jul;67(2):505-24. doi: 10.1016/0306-4522(95)00044-j.

Abstract

The aim of this study was to define the temporal appearance and regional distribution of angiotensinogen in the fetal and neonatal rat brain. This was done by immunocytochemical localization of angiotensinogen in brains from embryonic day 16 to postnatal day 12. Immunostaining was first observed on embryonic day 18, and persisted to postnatal day 2, in the choroid plexus and ependymal cells lining the third ventricle. This initial expression of angiotensinogen at embryonic day 18 was followed at postnatal day 20 by a rapid progression of angiotensinogen staining appearing in astrocytes in the paraventricular nucleus, medial preoptic area, ventromedial and arcuate hypothalamic nuclei; these areas showed the highest astrocyte staining intensity in the brain. This was followed sequentially by staining in areas of the thalamus, midbrain, forebrain and brainstem. In general, neuroglial staining was higher in regions proximal to the cerebral ventricles and cerebral aqueduct. Neuronal angiotensinogen was observed at day postnatal day 0 and later. The most consistent immunopositive areas were in the forebrain and thalamus; in particular, the hippocampus, anterior and posterior cingulate cortex, basal and lateral amygdala, the caudate-putamen, globus pallidus, lateral septum, medial habenular nuclei and lateral thalamic nuclei. Most of the immunopositive cells in the hypothalamus and brainstem were astrocytes, while those in the cortex were almost exclusively neurons. Staining in thalamic regions was both neuronal and neuroglial. From the intensity of staining and cell density, it was determined that a rapid increase in angiotensinogen occurs between embryonic day 20 and postnatal day 0, followed by further, smaller increases postnatally. In conclusion, this study has shown that angiotensinogen, the protein from which angiotensin II is generated, is present in the rat fetal brain. The timing of its appearance supports the establishment of a renin-angiotensin system by late gestation. Its predominance in fetal hypothalamic nuclei and in thalamic, cerebellar and cortical neurons suggests major roles in prenatal fluid and electrolyte balance, in sensorimotor development and in brain maturation.

摘要

本研究的目的是确定血管紧张素原在胎鼠和新生鼠脑中的出现时间及区域分布。通过对胚胎第16天至出生后第12天大鼠脑内血管紧张素原进行免疫细胞化学定位来实现这一目的。免疫染色最早在胚胎第18天观察到,并持续至出生后第2天,出现在脉络丛和第三脑室衬里的室管膜细胞中。胚胎第18天血管紧张素原的这种初始表达,在出生后第20天,紧接着在室旁核、视前内侧区、腹内侧和弓状下丘脑核的星形胶质细胞中出现血管紧张素原染色的快速进展;这些区域在脑中显示出最高的星形胶质细胞染色强度。随后依次在丘脑、中脑、前脑和脑干区域出现染色。一般来说,脑室和脑导水管近端区域的神经胶质染色较高。在出生后第0天及之后观察到神经元血管紧张素原。最一致的免疫阳性区域在前脑和丘脑;特别是海马、前扣带回和后扣带回皮质、基底和外侧杏仁核、尾状核 - 壳核、苍白球、外侧隔、内侧缰核和外侧丘脑核。下丘脑和脑干中的大多数免疫阳性细胞是星形胶质细胞,而皮质中的几乎全是神经元。丘脑区域的染色既有神经元的也有神经胶质的。从染色强度和细胞密度来看,确定血管紧张素原在胚胎第20天至出生后第0天之间迅速增加,随后在出生后进一步有较小幅度的增加。总之,本研究表明,血管紧张素原(血管紧张素II由此产生的蛋白质)存在于大鼠胎脑中。其出现时间支持在妊娠晚期建立肾素 - 血管紧张素系统。它在胎儿下丘脑核以及丘脑、小脑和皮质神经元中的优势表明,它在产前液体和电解质平衡、感觉运动发育以及脑成熟中起主要作用。

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