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神经胶质细胞在体外组装基于透明质酸的细胞周基质。

Glial cells assemble hyaluronan-based pericellular matrices in vitro.

作者信息

Maleski M, Hockfield S

机构信息

Section of Neurobiology, Yale University School of Medicine, New Haven, Connecticut 06520, USA.

出版信息

Glia. 1997 Jul;20(3):193-202. doi: 10.1002/(sici)1098-1136(199707)20:3<193::aid-glia3>3.0.co;2-9.

DOI:10.1002/(sici)1098-1136(199707)20:3<193::aid-glia3>3.0.co;2-9
PMID:9215728
Abstract

The extracellular matrix (ECM) of the brain contains hyaluronan and proteoglycans, as does the ECM of cartilage. Aggrecan, the major proteoglycan of cartilage, forms large aggregates with hyaluronan, which then associate with the chondrocyte cell surface through an interaction with surface hyaluronan binding proteins. In culture, chondrocytes elaborate hyaluronan-proteoglycan aggregates, which form large hydrated pericellular matrices (PCMs) that can be visualized by a particle exclusion assay (Knudson and Toole: Dev Biol 112:308, 1985). It has recently been demonstrated that embryonic glial cells can also elaborate PCMs in culture (Deyst and Toole: Dev Brain Res 28:351, 1995). We demonstrate here that different classes of glial cells elaborate different types of endogenous PCMs in culture. Less differentiated glial cells, as evidenced by their immunoreactivity for nestin, elaborate larger endogenously produced PCMs than differentiated astrocytes, as defined by immunoreactivity for GFAP. This in vitro result may be a reflection of the larger volume of extracellular space present in the embryonic than in the mature brain. We show further that glial cells can incorporate cartilage aggrecan into their PCMs, and that both endogenous and aggrecan-supplemented glial PCMs are dependent on hyaluronan. In contrast, primary neurons from newborn (P0) and P1 rat cortex neither express endogenous matrices nor can assemble exogenous hyaluronan/aggrecan aggregates into PCMs. These results suggest that immature neurons may not have the ability to assemble hyaluronan-based PCMs, and they raise the possibility that neural proteoglycans associate with neuronal surfaces through a mechanism that may not directly involve hyaluronan.

摘要

大脑的细胞外基质(ECM)含有透明质酸和蛋白聚糖,软骨的ECM也是如此。聚集蛋白聚糖是软骨的主要蛋白聚糖,它与透明质酸形成大的聚集体,然后通过与表面透明质酸结合蛋白的相互作用与软骨细胞表面结合。在培养中,软骨细胞产生透明质酸-蛋白聚糖聚集体,形成大的水合细胞周基质(PCM),可通过颗粒排除试验观察到(克努德森和图尔:《发育生物学》112:308,1985)。最近已证明,胚胎神经胶质细胞在培养中也能产生PCM(戴斯特和图尔:《发育脑研究》28:351,1995)。我们在此证明,不同类型的神经胶质细胞在培养中产生不同类型的内源性PCM。通过对巢蛋白的免疫反应性证明,分化程度较低的神经胶质细胞比通过对胶质纤维酸性蛋白(GFAP)的免疫反应性定义的分化星形胶质细胞产生更大的内源性PCM。这个体外结果可能反映了胚胎大脑中比成熟大脑中存在更大体积的细胞外空间。我们进一步表明,神经胶质细胞可以将软骨聚集蛋白聚糖纳入其PCM,并且内源性和补充了聚集蛋白聚糖的神经胶质PCM都依赖于透明质酸。相比之下,新生(P0)和P1大鼠皮质的原代神经元既不表达内源性基质,也不能将外源性透明质酸/聚集蛋白聚糖聚集体组装成PCM。这些结果表明,未成熟神经元可能没有组装基于透明质酸的PCM的能力,并且它们增加了神经蛋白聚糖通过可能不直接涉及透明质酸的机制与神经元表面结合的可能性。

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