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D-二聚体校正后的凝血酶和纤溶酶生成是脓毒症患者死亡率的一个强有力的预测因子。

D-dimer corrected for thrombin and plasmin generation is a strong predictor of mortality in patients with sepsis.

机构信息

Department of Biomedical Sciences and Human Oncology, "Aldo Moro" University, Bari, Italy.

Department of Anaesthesia and Critical Care, AOU "S. Luigi Gonzaga", Department of Oncology, University of Turin, Turin, Italy.

出版信息

Blood Transfus. 2020 Jul;18(4):304-311. doi: 10.2450/2019.0175-19. Epub 2019 Nov 19.

Abstract

BACKGROUND

D-dimer (DD) is the most used fibrin-related marker and has been proposed, either alone or in combination with other variables, as prognostic factor in patients with sepsis. However, DD generation depends on both coagulation and fibrinolysis, meaning that it may give false negative results in conditions associated with marked fibrinolytic inhibition such as sepsis. In this study, we tested whether correction of DD for thrombin and plasmin generation could improve its prognostic significance in septic patients.

MATERIAL AND METHODS

We performed a nested study in 269 septic patients from the ALBIOS trial. DD, prothrombin fragment 1+2 (F1+2) and plasmin-antiplasmin complex (PAP) were assayed at day 1. Corrected DD (DD) was calculated by the formula DD×PAP/F1+2, such that the lower the DD the greater the imbalance in favour of fibrin formation over fibrin lysis, and vice-versa. Primary outcome was 90-day mortality.

RESULTS

DD showed a J-shaped relationship with mortality, which was highest in the first DD tertile (low fibrinolysis), intermediate in the 3 (high fibrinolysis), and lowest in the 2 (balanced fibrinolysis), suggesting an increased risk whenever the coagulation-fibrinolysis balance is tilted (p<0.0001). Neither DD, nor PAP or F1+2 showed a comparable association with mortality. DD was an independent prognostic factor in multivariable Cox models and significantly improved risk stratification (cNRI≥0.28). Finally, by combining DD and SOFA tertiles, we developed a score with high discriminatory power.

DISCUSSION

DD is a good marker of the in vivo coagulation-fibrinolysis balance and displays a prognostic value in sepsis much higher than DD.

摘要

背景

D-二聚体(DD)是最常用的纤维蛋白相关标志物,它被单独或与其他变量联合应用于脓毒症患者的预后预测。然而,DD 的生成依赖于凝血和纤溶两个系统,这意味着在存在明显纤维蛋白溶解抑制的情况下,如脓毒症,它可能会给出假阴性结果。在这项研究中,我们检测了校正 DD 对凝血酶和纤溶酶生成的影响,以改善其在脓毒症患者中的预后意义。

材料和方法

我们对 ALBIOS 试验中的 269 例脓毒症患者进行了嵌套研究。在第 1 天检测了 DD、凝血酶原片段 1+2(F1+2)和纤溶酶-抗纤溶酶复合物(PAP)。通过公式 DD×PAP/F1+2 计算校正 DD(DD),从而得出 DD 值越低,纤维蛋白形成相对于纤维蛋白溶解的失衡越大,反之亦然。主要结局是 90 天死亡率。

结果

DD 与死亡率呈 J 型关系,死亡率在第 1 个 DD 三分位数(低纤溶)最高,在第 3 个(高纤溶)中等,在第 2 个(平衡纤溶)最低,这表明当凝血-纤溶平衡发生倾斜时,风险增加(p<0.0001)。DD、PAP 或 F1+2 均与死亡率无类似关联。在多变量 Cox 模型中,DD 是一个独立的预后因素,且显著改善了风险分层(cNRI≥0.28)。最后,通过将 DD 和 SOFA 三分位数结合起来,我们开发了一个具有高判别能力的评分。

讨论

DD 是体内凝血-纤溶平衡的良好标志物,在脓毒症中的预后价值高于 DD。

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