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硫酸乙酰肝素蛋白聚糖的功能。

The functions of the heparan sulphate proteoglycans.

作者信息

Fransson L A, Carlstedt I, Cöster L, Malmström A

出版信息

Ciba Found Symp. 1986;124:125-42. doi: 10.1002/9780470513385.ch8.

Abstract

Heparan sulphate (HS)-containing proteoglycans (HS-PGs) are present at the surface of nearly all adherent mammalian cells. The principal mode of attachment is by way of the protein core which is inserted into the plasma membrane. Other forms of HS-PG may be components of pericellular matrices, notably basement membranes. The core proteins of HS-PGs can be small (35K) as in hepatocytes, intermediate (50K) as in many mesenchymal cells, or very large (400K) as in basement membranes. A special case is the HS-PG synthesized by postconfluent fibroblasts. This proteoglycan has a core protein that closely resembles the transferrin receptor glycoprotein. It is possible that this HS-PG is a pro-form of the receptor. Low molecular weight, carbohydrate-rich HS-PG forms are probably derived from larger forms by partial degradation. The HS side-chains can contain 24 different disaccharides in an unknown number of arrangements. The biosynthetic machinery can impose considerable restrictions; for example, the extent of N-sulphation rarely exceeds 40-50%, whereas O-sulphation may range from 20% to 75% of potential sites. Nevertheless, the informational capacity of HS is formidable. By way of the HS chains, HS-PG at the surface of endothelial cells can interact specifically or selectively with a number of plasma proteins. HS-PG at the surface of matrix-producing cells is similarly in a position to interact with matrix proteins, notably collagen, fibronectin and laminin. As the cytoplasmic portion of the HS-PG core protein can bind actin, this proteoglycan can provide a connection between extracellular matrices and the cytoskeleton. A number of studies support a role for HS-PGs in the control of cell growth, and this could be one of their major functions. Whether the HS side-chains or the core protein or both are carrying out such a function remains to be determined.

摘要

含硫酸乙酰肝素(HS)的蛋白聚糖(HS-PG)存在于几乎所有贴壁哺乳动物细胞的表面。其主要附着方式是通过插入质膜的蛋白核心。HS-PG的其他形式可能是细胞周基质的成分,尤其是基底膜。HS-PG的核心蛋白可以很小(35K),如肝细胞中的;中等大小(50K),如许多间充质细胞中的;或非常大(400K),如基底膜中的。一个特殊的例子是汇合后成纤维细胞合成的HS-PG。这种蛋白聚糖的核心蛋白与转铁蛋白受体糖蛋白非常相似。这种HS-PG有可能是受体的前体形式。低分子量、富含碳水化合物的HS-PG形式可能是由较大形式部分降解而来。HS侧链可以包含24种不同的二糖,排列方式未知。生物合成机制可能会施加相当大的限制;例如,N-硫酸化程度很少超过40-50%,而O-硫酸化可能占潜在位点的20%至75%。然而,HS的信息容量是巨大的。通过HS链,内皮细胞表面的HS-PG可以与多种血浆蛋白特异性或选择性地相互作用。基质产生细胞表面的HS-PG同样能够与基质蛋白相互作用,尤其是胶原蛋白、纤连蛋白和层粘连蛋白。由于HS-PG核心蛋白的细胞质部分可以结合肌动蛋白,这种蛋白聚糖可以在细胞外基质和细胞骨架之间提供联系。许多研究支持HS-PG在控制细胞生长中发挥作用,这可能是它们的主要功能之一。HS侧链、核心蛋白还是两者都在执行这样的功能仍有待确定。

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