纤溶酶体外诱导内皮细胞损伤。

K Okajima, H Abe, B R Binder
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摘要

我们研究了纤溶酶对内皮细胞完整性和功能的影响,以阐明在溶栓治疗中可能诱导出血或再血栓形成的机制。与培养的人脐静脉内皮细胞(HUVECs)孵育10分钟后,纤溶酶增加了内皮细胞对血清白蛋白的通透性。纤溶酶在培养30分钟后破坏细胞膜,培养3小时后使细胞脱离基质,最终诱导细胞裂解。纤溶酶原或纤溶酶经抑酶蛋白和α 2-纤溶酶抑制剂预处理后,未观察到对huvec的这种损伤作用,提示纤溶酶的催化功能在诱导这种损伤中起重要作用。血浆纤溶酶与HUVECs孵育1h后,HUVECs的硫35标记的糖胺聚糖(35S-GAGs)降低,蛋白C活化量测定HUVECs的凝血调节素(TM)活性降低。经抑酶蛋白和α 2-纤溶酶抑制剂预处理的纤溶酶孵育后,35S-GAGs和HUVECs的TM活性均未降低。这些发现表明,内皮细胞的非血栓形成特性可被纤溶酶的蛋白水解作用破坏。综上所述,我们的研究结果表明,纤溶酶损害内皮屏障功能、内皮细胞完整性和非血栓性。纤溶酶对内皮细胞的这些破坏作用可能与在接受大剂量溶栓治疗的血栓患者中观察到的出血或再血栓形成的病理生理学有关。
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Endothelial cell injury induced by plasmin in vitro.

We investigated the effect of plasmin on the integrity and function of endothelial cells to elucidate the mechanism by which bleeding or rethrombosis may be induced in thrombolytic therapy. When incubated with cultured human umbilical vein endothelial cells (HUVECs), plasmin increased the endothelial permeability to serum albumin 10 minutes after the incubation. Plasmin damaged the cell membranes 30 minutes after the incubation, detached the cells from the matrix 3 hours after the incubation, and finally induced cell lysis. Such damaging effects on HUVECs were not observed with plasminogen or plasmin pretreated with aprotinin and alpha 2-plasmin inhibitor, suggesting that the catalytic function of plasmin plays an important role in inducing this damage. Sulfur 35-labeled glycosaminoglycans (35S-GAGs) of HUVECs were decreased 1 hour after the incubation of plasmin with HUVECs, and the thrombomodulin (TM) activity of HUVECs measured by protein C activation capacity was decreased 6 hours after the incubation. Neither 35S-GAGs nor the TM activity of HUVECs was decreased after the incubation of plasmin pretreated with aprotinin and alpha 2-plasmin inhibitor. These findings suggest that the nonthrombogenic properties of endothelial cells can be damaged by the proteolytic action of plasmin. Our findings, taken together, suggest that plasmin damages the endothelial barrier function, endothelial cell integrity, and nonthrombogenic properties. These damaging effects of plasmin on endothelial cells may be related to the pathophysiology of bleeding or rethrombosis observed in patients undergoing high-dose thrombolytic therapy for thrombosis.

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