The role of tranexamic acid in the management of postpartum haemorrhage

IF 4.7 3区 医学 Q1 ANESTHESIOLOGY
Anne-Sophie Bouthors MD,PhD (Redaction and revision of the manuscript, research investigator and coordinator) , Sixtine Gilliot PhD Student (Draft revision, research team) , Loïc Sentilhes MD,PhD (Draft revision, research coordinator) , Benjamin Hennart MD (Research team, draft revision) , Emmanuelle Jeanpierre MD (Research team, draft revision) , Catherine Deneux-Tharaux MD,PhD (Draft revision, research team coordinator) , Gilles Lebuffe MD,PhD (Research team coordinator, draft revision) , Pascal Odou PhD (Research team coordinator, draft revision)
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引用次数: 3

Abstract

In the last decades, tranexamic acid (TXA) has emerged as an essential tool in blood loss management in obstetrics. TXA prophylaxis for postpartum haemorrhage (PPH) has been studied in double-blind, placebo-controlled, randomized clinical trials (RCTs). Given the small observed preventive effect, the systematic use of TXA for vaginal and/or caesarean deliveries remains controversial. The result of a pharmacokinetic modelling suggests that relative to intravenous administration, intramuscular administration may be an equally effective alternative route for preventing PPH and may enable access to this drug in low-resource countries. Prophylaxis is currently studied in high-risk populations, such as women with prepartum anaemia or placenta previa.

TXA effectively reduces blood loss and PPH-related morbidity and mortality during active PPH, as demonstrated by high-grade evidence from large RCTs. The drug has a good safety profile: in most cases, only mild gastrointestinal or visual adverse events may be observed. TXA use does not increase the risk of serious adverse events, such as venous or arterial thromboembolism, seizures, or acute kidney injury. The TRACES in vivo analysis of biomarkers of TXA’s antifibrinolytic effect have suggested that a dose of at least 1 g is required for the treatment of PPH. The TRACES pharmacokinetic model suggests that because TXA can be lost in the haemorrhaged blood, a second dose should be administered if the PPH continues or if severe coagulopathy occurs. Future pharmacodynamic analyses will focus on the appropriateness of TXA dosing regimens with regard to the intensity of fibrinolysis in catastrophic obstetric events.

氨甲环酸在产后出血治疗中的作用
在过去的几十年里,氨甲环酸(TXA)已成为产科失血管理的重要工具。TXA预防产后出血(PPH)已经在双盲、安慰剂对照、随机临床试验(rct)中进行了研究。鉴于观察到的预防效果很小,在阴道和/或剖腹产分娩中系统使用TXA仍然存在争议。药代动力学模型的结果表明,相对于静脉给药,肌肉给药可能是预防PPH的一种同样有效的替代途径,并可能使资源匮乏的国家获得这种药物。目前正在研究高危人群的预防措施,例如患有孕前贫血或前置胎盘的妇女。大型随机对照试验的高级别证据表明,TXA可有效减少活动性PPH期间的失血和与PPH相关的发病率和死亡率。该药具有良好的安全性:在大多数情况下,可能只观察到轻微的胃肠道或视觉不良事件。使用TXA不会增加严重不良事件的风险,如静脉或动脉血栓栓塞、癫痫发作或急性肾损伤。对TXA抗纤溶作用的生物标志物的痕量体内分析表明,治疗PPH需要至少1g的剂量。TRACES药代动力学模型提示,由于TXA可在出血血液中丢失,如果PPH持续或发生严重凝血功能障碍,则应给予第二次剂量。未来的药效学分析将集中在与灾难性产科事件中纤溶强度相关的TXA给药方案的适宜性上。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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