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Tranexamic acid and trauma-induced coagulopathy

机译:氨甲环酸与创伤性凝血病

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摘要

Tranexamic acid (TXA) is a synthetic derivative of the amino acid lysine that inhibits fibrinolysis by blocking the interaction of plasminogen with the lysine residues of fibrin. Historically, TXA is commonly used for reduction of blood loss in perioperative situations, while recently it has attracted attention for clinical use in the trauma field. In 2010, the Clinical Randomization of an Antifibrinolytic in Significant Hemorrhage 2 (CRASH-2) trial demonstrated that intravenous administration of TXA improved mortality significantly in trauma patients with significant bleeding. After the launch of its sensational results, the main stream treatment protocol in trauma changed worldwide to include TXA administration.In this review, first we summarize the recent evidence or recommendations in the related guidelines concerning TXA. Also, we next tried to explore in detail not only the benefits but also the harm introduced by TXA in trauma patients, because the main adverse event results for TXA, such as vascular occlusive events in the CRASH-2 trial, are still being discussed in several papers. Thus, we briefly summarized the evidence for the safety of TXA administration by a systematic review method using observational studies. Consequently, the pooled relative risk for venous thromboembolisms was 1.61 (95% CI, 0.86–3.01), indicating a non-significant increase in the venous thromboembolism risk of TXA therapy.Regarding the basic mechanism, TXA potentially possesses the risk of venous thromboembolisms, so it should be used cautiously and selectively. Further investigation is needed to delineate the optimal targeted trauma patients to earn the maximum survival benefits with minimized risk of thrombotic complications.
机译:氨甲环酸(TXA)是氨基酸赖氨酸的合成衍生物,可通过阻止纤溶酶原与纤维蛋白赖氨酸残基的相互作用来抑制纤维蛋白溶解。从历史上看,TXA通常用于减少围手术期出血量,而近来它已引起了创伤领域临床应用的关注。 2010年,一项针对严重出血的抗纤维蛋白溶解药物2(CRASH-2)的临床随机试验证明,静脉内给予TXA可以显着改善出血严重的创伤患者的死亡率。在其轰动性结果发布后,创伤方面的主流治疗方案在全球范围内发生了变化,包括TXA管理。在本综述中,我们首先总结了有关TXA的相关指南中的最新证据或建议。此外,我们接下来尝试详细探讨TXA对创伤患者的益处和伤害,因为TXA的主要不良事件结果(例如CRASH-2试验中的血管闭塞事件)仍在讨论中。几篇论文。因此,我们通过使用观察性研究的系统评价方法,简要总结了TXA管理安全性的证据。因此,合并的静脉血栓栓塞相对风险为1.61(95%CI,0.86–3.01),表明TXA治疗的静脉血栓栓塞风险没有显着增加。就基本机制而言,TXA可能具有静脉血栓栓塞的风险,因此应谨慎选择使用。需要进一步的研究来确定最佳的靶向创伤患者,以在降低血栓形成并发症风险的情况下获得最大的生存收益。

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