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正常人腹膜间皮细胞周围含透明质酸包被的合成与组装。

Synthesis and assembly of the hyaluronan-containing coats around normal human mesothelial cells.

作者信息

Heldin P, Pertoft H

机构信息

Department of Medical and Physiological Chemistry, University of Uppsala, Sweden.

出版信息

Exp Cell Res. 1993 Oct;208(2):422-9. doi: 10.1006/excr.1993.1264.

DOI:10.1006/excr.1993.1264
PMID:8375471
Abstract

In this study we examined the capacity of normal human mesothelial (NHM) cells and human malignant mesothelioma cells to form hyaluronan-containing pericellular matrices or "coats." The assembly of the pericellular coats was visualized by a particle exclusion assay. We found that large hyaluronan-containing coats were formed around NHM cells whereas their transformed counterparts had no or very limited coats. The coats were removed by treatment with Streptomyces hyaluronidase, which specifically degrades hyaluronan. NHM cells exhibited hyaluronan-containing pericellular matrix within 5 h after seeding. The formation of the coats was stimulated by platelet-derived growth factor and epidermal growth factor. Interestingly, the assembly of the hyaluronan-dependent pericellular matrices was inhibited by the addition of hyaluronan dodecasaccharides. The inhibitory effect on the formation of the coats was due to a destabilization of pericellular matrix and not due to an inhibitory effect of hyaluronan dodecasaccharides on hyaluronan synthesis. In contrast, hyaluronan hexasaccharides, an inhibitor of the interaction between polymeric hyaluronan and its cell surface receptors, had no effect on the size of the coat. Thus, our results are compatible with the possibility that the pericellular matrix surrounding NHM cells consists of newly synthesized hyaluronan which is extruded from the cell and independent of hyaluronan receptors on the cell surface. The coat seems to be stabilized by interactions (hyaluronan-hyaluronan or hyaluronan-protein bridges) which can be prevented by hyaluronan dodecasaccharides.

摘要

在本研究中,我们检测了正常人腹膜间皮(NHM)细胞和人恶性间皮瘤细胞形成含透明质酸的细胞周围基质或“包膜”的能力。通过颗粒排斥试验观察细胞周围包膜的组装情况。我们发现,NHM细胞周围形成了大型的含透明质酸包膜,而其转化后的对应细胞则没有或只有非常有限的包膜。用链霉菌透明质酸酶处理可去除这些包膜,该酶能特异性降解透明质酸。接种后5小时内,NHM细胞就表现出含透明质酸的细胞周围基质。血小板衍生生长因子和表皮生长因子可刺激包膜的形成。有趣的是,添加透明质酸十二糖可抑制依赖透明质酸的细胞周围基质的组装。对包膜形成的抑制作用是由于细胞周围基质的不稳定,而非透明质酸十二糖对透明质酸合成的抑制作用。相比之下,透明质酸六糖是聚合透明质酸与其细胞表面受体之间相互作用的抑制剂,对包膜大小没有影响。因此,我们的结果符合这样一种可能性,即NHM细胞周围的细胞周围基质由新合成的透明质酸组成,该透明质酸从细胞中挤出,且独立于细胞表面的透明质酸受体。包膜似乎通过相互作用(透明质酸-透明质酸或透明质酸-蛋白质桥)得以稳定,而透明质酸十二糖可阻止这种相互作用。

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