Iba Toshiaki, Helms Julie, Connors Jean Marie, Levy Jerrold H
Department of Emergency and Disaster Medicine, Juntendo University Graduate School of Medicine, 2-1-1 Hongo Bunkyo-Ku, Tokyo, 113-8421, Japan.
Université de Strasbourg (UNISTRA), Faculté de 1Médecine, Hôpitaux Universitaires de Strasbourg, Service de Médecine Intensive-Réanimation, Nouvel Hôpital Civil, 1, place de l'Hôpital, 67091, Strasbourg Cedex, France.
J Intensive Care. 2023 May 23;11(1):24. doi: 10.1186/s40560-023-00672-5.
The International Society on Thrombosis and Haemostasis (ISTH) released overt disseminated intravascular coagulation (DIC) diagnostic criteria in 2001. Since then, DIC has been understood as the end-stage consumptive coagulopathy and not the therapeutic target. However, DIC is not merely a decompensated coagulation disorder, but also includes early stages with systemic activation in coagulation. Thus, the ISTH has recently released sepsis-induced coagulopathy (SIC) criteria that can diagnose compensated-phase of coagulopathy with readily available biomarkers.
DIC is a laboratory-based diagnosis due to various critical conditions, although sepsis is the most common underlying disease. The pathophysiology of sepsis-associated DIC is multifactorial, and in addition to coagulation activation with suppressed fibrinolysis, multiple inflammatory responses are initiated by activated leukocytes, platelets, and vascular endothelial cells as part of thromboinflammation. Although overt DIC diagnostic criteria were established by ISTH to diagnose the advanced stage of DIC, additional criteria that can detect an earlier stage of DIC were needed for potential therapeutic considerations. Accordingly, the ISTH introduced SIC criteria in 2019 that are easy to use and require only platelet count, prothrombin time-international normalized ratio, and Sequential Organ Failure Assessment Score. SIC score can be used to evaluate disease severity and determine the timing of potential therapeutic interventions. One of the major disadvantages in treating sepsis-associated DIC is the lack of availability of specific therapeutic approaches beyond treating the underlying infection. Clinical trials to date have failed because included patients who were not coagulopathic. Nevertheless, in addition to infection control, anticoagulant therapy will be the choice for sepsis-associated DIC. Therefore, the efficacy of heparin, antithrombin, and recombinant thrombomodulin has to be proven in future clinical studies.
It is necessary to develop a novel therapeutic strategy against sepsis-associated DIC and improve the outcomes. Consequently, we recommend screening and monitoring DIC using SIC scoring system.
国际血栓与止血学会(ISTH)于2001年发布了显性弥散性血管内凝血(DIC)诊断标准。从那时起,DIC被理解为终末期消耗性凝血病,而非治疗靶点。然而,DIC不仅是一种失代偿性凝血障碍,还包括凝血系统激活的早期阶段。因此,ISTH最近发布了脓毒症诱导的凝血病(SIC)标准,该标准可通过易于获得的生物标志物诊断凝血病的代偿期。
DIC是基于实验室检查对各种危急情况做出的诊断,尽管脓毒症是最常见的基础疾病。脓毒症相关DIC的病理生理学是多因素的,除了凝血激活伴纤维蛋白溶解受抑制外,活化的白细胞、血小板和血管内皮细胞引发多种炎症反应,这是血栓炎症的一部分。尽管ISTH制定了显性DIC诊断标准以诊断DIC的晚期阶段,但出于潜在治疗考虑,仍需要能够检测DIC早期阶段的额外标准。因此,ISTH于2019年引入了SIC标准,该标准易于使用,仅需血小板计数、凝血酶原时间-国际标准化比值和序贯器官衰竭评估评分。SIC评分可用于评估疾病严重程度并确定潜在治疗干预的时机。治疗脓毒症相关DIC的主要缺点之一是除了治疗基础感染外,缺乏可用的特异性治疗方法。迄今为止的临床试验均告失败,因为纳入的患者并非凝血病患者。然而,除了控制感染外,抗凝治疗将是脓毒症相关DIC的治疗选择。因此,肝素、抗凝血酶和重组血栓调节蛋白的疗效必须在未来的临床研究中得到证实。
有必要制定针对脓毒症相关DIC的新型治疗策略并改善治疗结果。因此,我们建议使用SIC评分系统筛查和监测DIC。
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