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血小板反应蛋白与内皮细胞的相互作用:受体介导的结合与降解

Interactions of thrombospondin with endothelial cells: receptor-mediated binding and degradation.

作者信息

Murphy-Ullrich J E, Mosher D F

机构信息

Department of Medicine, University of Wisconsin, Madison 53706.

出版信息

J Cell Biol. 1987 Oct;105(4):1603-11. doi: 10.1083/jcb.105.4.1603.

Abstract

We studied binding and degradation of labeled platelet thrombospondin (TSP) by normal and variant bovine aorta endothelial (BAE) cells. [125I]-labeled TSP bound to cells at 37 degrees C in a specific, saturable, and time-dependent fashion. Incubation of cell monolayers with fluoresceinated TSP resulted in punctate cellular staining, but no staining of the extracellular matrix. Heparin, fucoidan, chondroitin sulfate, platelet factor 4, beta-thromboglobulin, unlabeled TSP, and serum derived from whole blood all competed for binding of [125I]TSP. [125I]TSP was degraded to TCA-soluble radioactivity, which appeared in the medium after a 60-90-min lag. Degradation was inhibited to the same extent as binding by increasing concentrations of heparin, fucoidan, platelet factor 4, or whole blood serum. Normal BAE cells bound and degraded less [125I]TSP than variant BAE cells. The dissociation constants (Kds) for binding and the constants for degradation (Kms) for degradation by the two cell strains, however, were similar (30-50 nM). The inhibitory effects of heparin and platelet factor 4 were lost when the two inhibitors were present in a 1:1 (wt/wt) ratio. Treatment of suspended cells with trypsin or heparitinase caused less binding of TSP. These results indicate that there is a specific receptor for TSP on endothelial cells which mediates binding and degradation. This receptor may be a heparan sulfate proteoglycan.

摘要

我们研究了正常和变异牛主动脉内皮(BAE)细胞对标记血小板凝血酶敏感蛋白(TSP)的结合和降解情况。[125I]标记的TSP在37℃下以特异性、可饱和且时间依赖性的方式与细胞结合。用荧光素标记的TSP孵育细胞单层导致细胞出现点状染色,但细胞外基质无染色。肝素、岩藻依聚糖、硫酸软骨素、血小板因子4、β-血小板球蛋白、未标记的TSP以及全血来源的血清均竞争[125I]TSP的结合。[125I]TSP降解为三氯乙酸可溶性放射性物质,在延迟60 - 90分钟后出现在培养基中。随着肝素、岩藻依聚糖、血小板因子4或全血血清浓度的增加,降解受到的抑制程度与结合受到的抑制程度相同。正常BAE细胞比变异BAE细胞结合和降解的[125I]TSP更少。然而,两种细胞株结合的解离常数(Kds)和降解的常数(Kms)相似(30 - 50 nM)。当两种抑制剂以1:1(重量/重量)比例存在时,肝素和血小板因子4的抑制作用消失。用胰蛋白酶或乙酰肝素酶处理悬浮细胞导致TSP的结合减少。这些结果表明内皮细胞上存在TSP的特异性受体,其介导结合和降解。该受体可能是硫酸乙酰肝素蛋白聚糖。

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