首页> 外文期刊>The journal of trauma and acute care surgery >Tranexamic acid corrects fibrinolysis in the presence of acidemia in a swine model of severe ischemic reperfusion
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Tranexamic acid corrects fibrinolysis in the presence of acidemia in a swine model of severe ischemic reperfusion

机译:在严重缺血再灌注的猪模型中,氨甲环酸可在存在酸血症的情况下纠正纤维蛋白溶解

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BACKGROUND: Tranexamic acid (TXA) is an antifibrinolytic with anti-inflammatory properties associated with improved outcomes when administered to trauma patients at risk for bleeding; however, its efficacy is unknown in acidemia. We evaluated the efficacy of TXA on hyperfibrinolysis using an established porcine traumatic hemorrhage ischemic shock model. METHODS: Ten Yorkshire swine underwent a controlled hemorrhage followed by supraceliac aortic cross-clamping. During standard resuscitation, control animals received recombinant tissue plasminogen activator (rtPA) after cross-clamp removal, and experimental animals received rtPA followed by TXA. Rotational thromboelastometry analysis was performed at baseline, 5 minutes and 15 minutes after rtPA dosing, and 4 hours after cross-clamp removal. RESULTS: Control and experimental animals had similar hemodynamics and routine laboratory values at baseline and throughout resuscitation. At the time of TXA administration, average pH was 7.2. Clot formation time was prolonged from baseline and all resuscitation time points in both groups, with no difference at any time point. Maximum clot firmness decreased from baseline at all resuscitation time points in both groups. Maximum lysis increased from baseline (9% control vs. 9% TXA) after tissue plasminogen activator administration in both groups (100% control vs. 99% TXA). In experimental animals, maximum lysis returned to baseline 10 minutes after TXA administration (92% vs. 9%, p < 0.001). CONCLUSION: TXA rapidly and fully reverses hyperfibrinolysis despite severe acidemia in a porcine trauma model. TXA is a promising adjunct to trauma resuscitation that is easily administered in austere or prehospital settings.
机译:背景:氨甲环酸(TXA)是一种抗纤维蛋白溶解剂,具有抗炎特性,当用于有出血风险的创伤患者时,其转归改善。然而,在酸血症中其疗效尚不清楚。我们使用已建立的猪创伤性出血缺血性休克模型评估了TXA对高纤蛋白溶解的疗效。方法:对十只约克郡猪进行了控制性出血,随后进行race上主动脉交叉钳夹术。在标准复苏过程中,对照动物在交叉钳移除后接受重组组织纤溶酶原激活剂(rtPA),实验动物接受rtPA,然后接受TXA。在基线,rtPA给药后5分钟和15分钟以及交叉钳移除后4小时进行了旋转血栓弹力测定法分析。结果:对照组和实验动物在基线和整个复苏过程中具有相似的血液动力学和常规实验室值。在TXA给药时,平均pH为7.2。两组的血凝块形成时间均从基线和所有复苏时间点延长,任何时间点均无差异。两组中所有复苏时间点的最大血凝块硬度均低于基线。两组均施用组织纤溶酶原激活剂后,最大裂解量较基线增加(9%对照vs. 9%TXA)(100%对照vs. 99%TXA)。在实验动物中,TXA给药后10分钟,最大裂解恢复到基线(92%对9%,p <0.001)。结论:尽管在猪的创伤模型中发生了严重的酸血症,TXA仍能迅速并完全逆转高纤维蛋白溶解。 TXA是创伤性复苏的有希望的辅助手段,可以在严峻或院前环境中轻松实施。

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