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首页> 外文期刊>Acute Medicine & Surgery >Anticoagulant therapy for septic coagulopathy and disseminated intravascular coagulation: where do KyberSept and SCARLET leave us?
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Anticoagulant therapy for septic coagulopathy and disseminated intravascular coagulation: where do KyberSept and SCARLET leave us?

机译:抗凝血治疗用于脓肠病凝血病,散发血管内凝血:Kyberept和Scarlet的血管内凝血呢?

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摘要

The use of antithrombin and thrombomodulin to restore impaired anticoagulant pathways in septic coagulopathy has been shown to significantly increase the resolution rate of disseminated intravascular coagulation. In KyberSept and SCARLET, two large, international, randomized controlled trials in patients with sepsis, these anticoagulants have not shown significantly reduced mortality. The aim of this assessment was to compare the heterogeneity in responses to treatment in the two trials according to different patient phenotypes. Results of the KyberSept and SCARLET trials reported in original and post‐hoc publications were analyzed and directly compared for treatment effects in various patient subgroups. In both KyberSept and SCARLET, the septic coagulopathy phenotype that benefited most from endogenous anticoagulant supplementation showed markers of excessive activation of coagulation. Interaction between concomitant thromboprophylactic heparin and the endogenous anticoagulants abrogated the efficacy of both antithrombin and thrombomodulin. In both trials, higher disease severity was associated with better treatment outcome. In conclusion, in two landmark studies of endogenous anticoagulants in patients with sepsis, similar findings of beneficial effects in the coagulopathy phenotype and interactions with heparin comedication and disease severity support the potential roles that thrombomodulin and antithrombin might play in treating septic coagulopathy and disseminated intravascular coagulation. Further prospective validation is warranted. Future trial designs to definitively establish the therapeutic relevance of antithrombin and thrombomodulin in septic coagulopathy should focus on involvement of patients characterized by coagulopathy and disease severity as well as interactions between endogenous anticoagulants and exogenous heparin. Intriguing similarities in the results of two large randomized controlled landmark trials with endogenous anticoagulants in septic coagulopathy are identified from post‐hoc subgroup and meta‐analyses. Findings of shared patient phenotypes could inform trial design of future studies to definitively confirm treatment benefit of antithrombin and thrombomodulin in this indication.
机译:使用抗凝血酶和血栓调节蛋白,恢复受损的感染性凝血功能障碍的抗凝血途径已经显示出显著增加弥散性血管内凝血的解决率。在KyberSept朱红色,两个大的,国际的,随机对照败血症患者的试验中,这些抗凝血剂还没有表现出显著降低死亡率。这一评估的目的是根据不同的患者的表型在两个试验中反应的异质性比较处理。在KyberSept和SCARLET试验的结果报告原件及事后的出版物进行了分析,并直接用于各种患者亚组的治疗效果进行比较。在这两个KyberSept和SCARLET,那受益最大内源性抗凝血剂补充化粪池凝血异常表型表现出凝血过度活化的标志物。伴随thromboprophylactic肝素和内源性抗凝血剂之间的相互作用废除既抗凝血酶和凝血调节蛋白的功效。在这两项试验中,较高的疾病严重程度与更好的治疗效果有关。总之,内源性抗凝血剂的败血症患者的两个具有里程碑意义的研究,在凝血功能异常表型有利影响和相互作用类似的发现与肝素comedication和疾病的严重程度支持的潜在作用是血栓和抗凝血酶可能在治疗感染性凝血功能障碍发挥和弥散性血管内凝血。进一步的前瞻性验证是必要的。未来的试验设计,以明确确立的治疗相关性抗凝血酶和血栓调节蛋白在感染性凝血功能障碍应注重对患者的特点是凝血功能障碍和疾病的严重程度,以及内源性抗凝血剂和外源性肝素之间的互动参与。在两个大的随机对照试验的地标与脓毒症凝血病的内源性抗凝血剂的结果令人感兴趣的相似性从事后亚组和荟萃分析鉴定。共享病人的表型的发现可以在此指示告知未来研究的试验设计抗凝血酶的明确确认的治疗效益和血栓。

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