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血小板反应蛋白可抑制血小板与玻璃及蛋白覆盖基质的黏附。

Thrombospondin inhibits adhesion of platelets to glass and protein-covered substrata.

作者信息

Lahav J

机构信息

Department of Polymer Research, Weizmann Institute of Science, Rehovot, Israel.

出版信息

Blood. 1988 Apr;71(4):1096-9.

PMID:3355889
Abstract

Glass and protein-covered surfaces when treated with the platelet-secreted glycoprotein thrombospondin lose their capacity to bind unstimulated platelets. In comparison to the number that bind to fibronectin-covered glass surfaces, less than 3% bind to thrombospondin-covered glass surfaces. When the fibronectin-covered surface is incubated with thrombospondin, it loses 87% of its binding capacity for platelets. The inhibitory effect of thrombospondin on platelet binding increases with increasing amounts of the adsorbed protein and reaches maximal values at 65% saturation of the adsorption of thrombospondin to the surface. Platelet spreading on the surface is also completely inhibited by thrombospondin. These data suggest that thrombospondin is nonthrombogenic and can modulate platelet adhesion to the subendothelium.

摘要

用血小板分泌的糖蛋白血小板反应蛋白处理玻璃和覆盖有蛋白质的表面时,它们失去了结合未受刺激血小板的能力。与结合纤连蛋白覆盖的玻璃表面的血小板数量相比,结合血小板反应蛋白覆盖的玻璃表面的血小板不到3%。当纤连蛋白覆盖的表面与血小板反应蛋白一起孵育时,它对血小板的结合能力丧失了87%。血小板反应蛋白对血小板结合的抑制作用随着吸附蛋白量的增加而增强,并在血小板反应蛋白吸附到表面达到65%饱和度时达到最大值。血小板在表面的铺展也被血小板反应蛋白完全抑制。这些数据表明血小板反应蛋白是非血栓形成性的,并且可以调节血小板与内皮下层的粘附。

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