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神经胶质细胞的形态学研究。VI. 小胶质细胞的出生后发育

Morphological studies on neuroglia. VI. Postnatal development of microglial cells.

作者信息

Murabe Y, Sano Y

出版信息

Cell Tissue Res. 1982;225(3):469-85. doi: 10.1007/BF00214798.

Abstract

The postnatal development of microglial cells was investigated in the neonatal rat brain by use of light- and electron microscopy, including enzyme-histochemical techniques. Microglial cells were selectively stained by demonstration of their nucleoside diphosphatase (NDPase) activity and classified into three types: 1) In the early postnatal period "primitive microglial cells" showing scantily ramified processes were found in the cerebral cortex, the hippocampal formation, and the hypothalamus. During the course of the first postnatal week the processes of this cell type developed gradually and the cells were transformed into typical ramified microglial cells, called "resting microglial cells". 2) "Amoeboid microglial cells "showing typical features of macrophages were characteristic of the cerebral white matter. 3) "Round microglial cells" possessing a round soma and few pseudopodia but no characteristic processes occurred in large numbers in the subventricular zone of the lateral ventricle and as single elements in the vicinity of blood vessels. Histochemically, thiamine pyrophosphatase (TPPase) was demonstrated only in the fully developed, ramified microglial cells ("resting microglial cells"), which could be readily observed in the central nervous tissue from the age of 14 day. "Round and amoeboid microglial cells" did not show TPPase activity and disappeared after 14 days of postnatal life. By use of electron microscopy, in neonatal rats NDPase activity was apparent in the plasma membrane of the three types of microglial cells ("primitive, round, and amoeboid" types). They showed basically similar submicroscopic characteristics, i.e., well-developed Golgi apparatus, long strands of rough-surfaced endoplasmic reticulum, single dense bodies and vacuoles, and numerous ribosomes. "Amoeboid microglial cells" were characterized by their well-developed cytoplasmic vacuoles and phagocytic inclusion bodies. The present study strongly suggests a mesodermal origin for these microglial elements.

摘要

利用光学显微镜和电子显微镜,包括酶组织化学技术,对新生大鼠脑内小胶质细胞的出生后发育进行了研究。通过显示其核苷二磷酸酶(NDPase)活性对小胶质细胞进行选择性染色,并将其分为三种类型:1)在出生后早期,在大脑皮质、海马结构和下丘脑发现了具有稀疏分支突起的“原始小胶质细胞”。在出生后的第一周内,这种细胞类型的突起逐渐发育,细胞转变为典型的分支状小胶质细胞,称为“静止小胶质细胞”。2)表现出巨噬细胞典型特征的“阿米巴样小胶质细胞”是脑白质的特征。3)具有圆形胞体和少量伪足但无特征性突起的“圆形小胶质细胞”大量出现在侧脑室室管膜下区,并作为单个细胞出现在血管附近。组织化学上,仅在完全发育的分支状小胶质细胞(“静止小胶质细胞”)中显示硫胺素焦磷酸酶(TPPase)活性,从14日龄起在中枢神经组织中很容易观察到这种细胞。“圆形和阿米巴样小胶质细胞”未显示TPPase活性,并在出生后14天消失。通过电子显微镜观察,在新生大鼠中,三种类型的小胶质细胞(“原始、圆形和阿米巴样”类型)的质膜中均有明显的NDPase活性。它们表现出基本相似的亚微观特征,即发达的高尔基体、长链糙面内质网、单个致密体和液泡以及大量核糖体。“阿米巴样小胶质细胞”的特征是其发达的细胞质液泡和吞噬包涵体。本研究强烈提示这些小胶质细胞成分起源于中胚层。

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