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培养的皮肤成纤维细胞对硫酸化蛋白聚糖的内吞作用。

Endocytosis of sulphated proteoglycans by cultured skin fibroblasts.

作者信息

Prinz R, Schwermann J, Buddecke E, von Figura K

出版信息

Biochem J. 1978 Dec 15;176(3):671-6. doi: 10.1042/bj1760671.

Abstract
  1. Human skin fibroblasts internalize homologous sulphated proteoglycans by adsorptive endocytosis. Endocytosis rate is half maximal when the concentration of the proteoglycans is 0.1 nM. At saturation, a single fibroblast may endocytose up to 8 X 10(6) proteoglycan molecules/h. 2. The kinetics of prote;glycan binding to the cell surface suggest the presence of 6 X 10(5) high-affinity binding sites per cell. The bulk of sulphated proteoglycans associates to low-affinity binding sites on the cell surface. 3. Glycosaminoglycans and other anionic macromolecules inhibit endocytosis of sulphated proteoglycans non-competitively. The lack of interaction of glycosaminoglycans with the cell-surface receptors for sulphated proteoglycans suggests that the protein core of proteoglycans is essential for binding to the cell surface. 4. The effects of trypsin, cell density, serum concentration and medium pH on endocytosis and degradation of endocytosed sulphated proteoglycans is described. 5. A comparison of the number of the high-affinity binding sites and the number of molecules endocytosed with respect to time suggests a recycling of the proteoglycan receptors between the cell surface and the endocytotic vesicles and/or the lysosomes.
摘要
  1. 人皮肤成纤维细胞通过吸附性内吞作用摄取同源硫酸化蛋白聚糖。当蛋白聚糖浓度为0.1 nM时,内吞速率达到最大值的一半。在饱和状态下,单个成纤维细胞每小时可内吞多达8×10⁶个蛋白聚糖分子。2. 蛋白聚糖与细胞表面结合的动力学表明,每个细胞存在6×10⁵个高亲和力结合位点。大部分硫酸化蛋白聚糖与细胞表面的低亲和力结合位点结合。3. 糖胺聚糖和其他阴离子大分子非竞争性地抑制硫酸化蛋白聚糖的内吞作用。糖胺聚糖与硫酸化蛋白聚糖的细胞表面受体缺乏相互作用,这表明蛋白聚糖的蛋白质核心对于与细胞表面结合至关重要。4. 描述了胰蛋白酶、细胞密度、血清浓度和培养基pH对内吞作用以及内吞的硫酸化蛋白聚糖降解的影响。5. 高亲和力结合位点数量与内吞分子数量随时间的比较表明,蛋白聚糖受体在细胞表面与内吞小泡和/或溶酶体之间循环利用。

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