首页> 外文期刊>Thrombosis and Haemostasis: Journal of the International Society on Thrombosis and Haemostasis >Thrombin activatable fibrinolysis inhibitor (TAFI) affects fibrinolysis in a plasminogen activator concentration-dependent manner. Study of seven plasminogen activators in an internal clot lysis model.
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Thrombin activatable fibrinolysis inhibitor (TAFI) affects fibrinolysis in a plasminogen activator concentration-dependent manner. Study of seven plasminogen activators in an internal clot lysis model.

机译:凝血酶可激活的纤维蛋白溶解抑制剂(TAFI)以纤溶酶原激活剂浓度依赖性的方式影响纤维蛋白溶解。内部凝块溶解模型中七个纤溶酶原激活物的研究。

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摘要

TAFIa was shown to attenuate fibrinolysis. In our in vitro study, we investigated how the inhibitory effect of TAFIa depended on the type and concentration of the plasminogen activator (PA). We measured PA-mediated lysis times of plasma clots under conditions of maximal TAFI activation by thrombin-thrombo-modulin in the absence and presence of potato carboxypeptidase inhibitor. Seven different PAs were compared comprising both tPA-related (tPA, TNK-tPA, DSPA), bacterial PA-related (staphylokinase and APSAC) and urokinase-related (tcu-PA and k2tu-PA) PAs. The lysis times and the retardation factor were plotted against the PA concentration. The retardation factor plots were bell-shaped. At low PA concentrations, the retardation factor was low, probably due to the limited stability of TAFIa. At intermediate PA concentrations the retardation factor was maximal (3-6 depending on the PA), with TNK-tPA, APSAC and DSPA exhibiting the strongest effect. At high PA concentrations, the retardation factor was againlow, possibly due to inactivation of TAFIa by plasmin or to a complete conversion of glu-plasminogen into lys-plasminogen. Using individual plasmas with a reduced plasmin inhibitor activity (plasmin inhibitor Enschede) the bell-shaped curve of the retardation factor shifted towards lower tPA and DSPA concentrations, but the height did not decrease. In conclusion, TAFIa delays the lysis of plasma clots mediated by all the plasminogen activators tested. This delay is dependent on the type and concentration of the plasminogen activator, but not on the fibrin specificity of the plasminogen activator. Furthermore, plasmin inhibitor does not play a significant role in the inhibition of plasma clot lysis by TAFI.
机译:显示TAFIa减弱纤维蛋白溶解。在我们的体外研究中,我们研究了TAFIa的抑制作用如何取决于纤溶酶原激活剂(PA)的类型和浓度。我们在不存在马铃薯马铃薯羧肽酶抑制剂的情况下,在凝血酶-血栓调节蛋白最大TAFI活化条件下,测量了PA介导的血浆凝块溶解时间。比较了七个不同的PA,包括tPA相关(tPA,TNK-tPA,DSPA),细菌PA相关(葡萄激酶和APSAC)和尿激酶相关(tcu-PA和k2tu-PA)PA。将裂解时间和延迟因子对PA浓度作图。延迟因子图呈钟形。在低PA浓度下,延迟因子很低,可能是由于TAFIa的稳定性有限。在中等PA浓度下,延迟因子最大(取决于PA的3-6),其中TNK-tPA,APSAC和DSPA表现出最强的作用。在高PA浓度下,阻滞因子再次较低,这可能是由于纤溶酶使TAFIa失活或glu-纤溶酶原完全转化为lys-纤溶酶原所致。使用纤溶酶抑制剂活性降低的单个血浆(纤溶酶抑制剂Enschede),延迟因子的钟形曲线朝着较低的tPA和DSPA浓度移动,但高度并未降低。总之,TAFIa延迟了所有测试的纤溶酶原激活剂介导的血浆凝块的裂解。该延迟取决于纤溶酶原激活物的类型和浓度,而不取决于纤溶酶原激活物的纤维蛋白特异性。此外,纤溶酶抑制剂在TAFI抑制血浆凝块溶解中不发挥重要作用。

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