微纤维的异质性:血栓反应-微纤维在内皮下层血栓形成中的作用。

F Fauvel-Lafève, B Arbeille, C de Romeuf, M Lemesle, Y J Legrand
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引用次数: 0

摘要

我们报告了对动脉内皮下微纤维的免疫金电镜分析结果,显示血栓反应蛋白(TSP)存在于40 nm直径的结构上,连接8-10 nm直径含有原纤维蛋白的微纤维。它们与VI型胶原蛋白不同,后者形成3-5纳米直径的微纤维。从人脐动脉中提取的含微原纤维的TSP不含原纤维蛋白和VI型胶原。血小板与TSP-MF的相互作用不受抗原纤维蛋白或抗VI型胶原抗体的影响。在原位,vWF与交联微原纤维结合在40nm的连接处,并观察到抗血栓反应蛋白和抗vWF抗体的双重标记。在体外,抗原纤维蛋白或抗VI型胶原抗体不抑制vWF与TSP-MF的结合。这些结果提示了微原纤维的结构和功能的异质性,并强调了TSP-MF在内皮下层血栓形成中的作用。
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Heterogeneity of microfibrils: role of thrombospondin-microfibrils in the thrombogenicity of the subendothelium.

We report the results of an immunogold electron microscopical analysis on microfibrils from the arterial subendothelium showing that thrombospondin (TSP) is present on 40 nm-diameter structures joining 8-10 nm-diameter microfibrils containing fibrillin. They differ from type VI collagen which forms 3-5 nm-diameter microfibrils. TSP containing microfibrils (TSP-MF) extracted from human umbilical arteries did not contain fibrillin or type VI collagen. Blood platelet interactions with TSP-MF were not modified by anti-fibrillin or anti-type VI collagen antibodies. In situ, vWF was bound to cross-linked microfibrils, at the level of their 40 nm junction, and a double-labeling with the anti-thrombospondin and anti-vWF antibodies was observed. In vitro, vWF binding to TSP-MF was not inhibited by anti-fibrillin or anti-type VI collagen antibodies. These results suggest a structural and functional heterogeneity of microfibrils and emphasize the role of TSP-MF in the thrombogenicity of the subendothelium.

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