Szabo Sebastian, Letsch Ronald, Ehlers Raila, Walter Thomas, Kazmaier Silke, Helber Uwe, Hoffmeister Hans Martin
Medizinische Klinik II, Städtisches Klinikum Solingen, Gotenstr 1, 42653 Solingen, Germany.
Thromb Res. 2002 Apr 15;106(2):113-9. doi: 10.1016/s0049-3848(02)00084-1.
Thrombolytic therapy in patients with acute myocardial infarction is hampered by bleeding complications and procoagulant effects favoring early reocclusion. TNK-tPA was shown in vitro to have considerable fibrin specificity. We investigated the effects of tenecteplase (TNK-tPA) and alteplase (rt-PA) on the haemostasis and fibrinolytic system.
We enrolled 30 patients with AMI into the study. Twenty patients received front-loaded rt-PA up to 100 mg; 10 patients were given TNK-tPA in a single bolus up to 50 mg. All patients received aspirin and intravenous heparin. During the first 2 days, the following parameters were repetitively determined: thrombin-antithrombin III complexes (TAT), antithrombin III (ATIII), prothrombin fragment F 1 + 2 (F 1 + 2), kallikrein-like activity (KK), activated factor XII (FXIIa), plasmin alpha 2-antiplasmin complexes (PAP), fibrinogen, D-dimers (DD), tissue-type plasminogen activator (t-PA). A total of 75 healthy persons served as control group. TAT increased significantly after rt-PA but not after TNK-tPA (3 h: 38.1 +/- 29.4 versus 10.5 +/- 4.2 microg/l; p < 0.01), indicating paradoxical thrombin activation. F 1 + 2 increased transiently after rt-PA but not after TNK-tPA. Fibrinogen was significantly lower after rt-PA versus TNK-tPA (3 h: 163 +/- 27 versus 380 +/- 54 mg/dl; p < 0.05). KK activities in the rt-PA group were significantly (p < 0.01) increased over 48 h versus TNK-tPA. PAP and D-dimers were lower over the time course of 48 h in the tenecteplase group versus rt-PA.
This study indicates that tenecteplase has higher fibrin specificity not only in vitro but also in vivo versus alteplase. TNK-tPA consecutively has no paradoxical systemic procoagulant effect due to the lower extent of activation of the kallikrein-factor XII system than alteplase.
急性心肌梗死患者的溶栓治疗受到出血并发症和促凝作用的阻碍,促凝作用有利于早期再闭塞。TNK - tPA在体外显示出相当高的纤维蛋白特异性。我们研究了替奈普酶(TNK - tPA)和阿替普酶(rt - PA)对止血和纤溶系统的影响。
我们招募了30例急性心肌梗死患者进入研究。20例患者接受高达100 mg的负荷量rt - PA;10例患者单次静脉推注高达50 mg的TNK - tPA。所有患者均接受阿司匹林和静脉肝素治疗。在最初2天内,重复测定以下参数:凝血酶 - 抗凝血酶III复合物(TAT)、抗凝血酶III(ATIII)、凝血酶原片段F1 + 2(F1 + 2)、激肽释放酶样活性(KK)、活化因子XII(FXIIa)、纤溶酶α2 - 抗纤溶酶复合物(PAP)、纤维蛋白原、D - 二聚体(DD)、组织型纤溶酶原激活剂(t - PA)。共75名健康人作为对照组。rt - PA治疗后TAT显著升高,而TNK - tPA治疗后未升高(3小时:38.1±29.4对10.5±4.2μg/l;p < 0.01),表明存在矛盾的凝血酶激活。rt - PA治疗后F1 + 2短暂升高,而TNK - tPA治疗后未升高。rt - PA治疗后纤维蛋白原显著低于TNK - tPA(3小时:163±27对380±54 mg/dl;p < 0.05)。rt - PA组的KK活性在48小时内显著高于TNK - tPA组(p < 0.01)。替奈普酶组在48小时内PAP和D - 二聚体低于rt - PA组。
本研究表明,与阿替普酶相比,替奈普酶不仅在体外而且在体内具有更高的纤维蛋白特异性。由于激肽释放酶 - 因子XII系统的激活程度低于阿替普酶,TNK - tPA连续应用无矛盾的全身促凝作用。
