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The association of endothelial cell signaling, severity of illness, and organ dysfunction in sepsis

机译:脓毒症中内皮细胞信号传导,疾病严重程度和器官功能障碍的关系

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IntroductionPrevious reports suggest that endothelial activation is an important process in sepsis pathogenesis. We investigated the association between biomarkers of endothelial cell activation and sepsis severity, organ dysfunction sequential organ failure assessment (SOFA) score, and death.MethodsThis is a prospective, observational study including adult patients (age 18 years or older) presenting with clinical suspicion of infection to the emergency department (ED) of an urban, academic medical center between February 2005 and November 2008. Blood was sampled during the ED visit and biomarkers of endothelial cell activation, namely soluble fms-like tyrosine kinase-1 (sFlt-1), plasminogen activator inhibitors -1 (PAI-1), sE-selectin, soluble intercellular adhesion molecule (sICAM-1), and soluble vascular cell adhesion molecule (sVCAM-1), were assayed. The association between biomarkers and the outcomes of sepsis severity, organ dysfunction, and in-hospital mortality were analyzed.ResultsA total of 221 patients were included: sepsis without organ dysfunction was present in 32%, severe sepsis without shock in 30%, septic shock in 32%, and 6% were non-infected control ED patients. There was a relationship between all target biomarkers (sFlt-1, PAI-1, sE-selectin, sICAM-1, and sVCAM-1) and sepsis severity, P < 0.05. We found a significant inter-correlation between all biomarkers, including the strongest correlations between sFlt-1 and sE-selectin (r = 0.55, P < 0.001), and between sFlt-1 and PAI-1 (0.56, P < 0.001). Among the endothelial cell activation biomarkers, sFlt-1 had the strongest association with SOFA score (r = 0.66, P < 0.001), the highest area under the receiver operator characteristic curve for severe sepsis of 0.82, and for mortality of 0.91.ConclusionsMarkers of endothelial cell activation are associated with sepsis severity, organ dysfunction and mortality. An improved understanding of endothelial response and associated biomarkers may lead to strategies to more accurately predict outcome and develop novel endothelium-directed therapies in sepsis.
机译:简介以前的报道表明内皮细胞激活是脓毒症发病机制中的重要过程。我们调查了内皮细胞活化与脓毒症严重程度,器官功能障碍序贯器官衰竭评估(SOFA)评分和死亡之间的生物标记物之间的关系。方法这是一项前瞻性观察性研究,包括表现出临床怀疑为成人的成年患者(年龄在18岁以上)。在2005年2月至2008年11月之间感染了城市学术医疗中心的急诊科(ED)。在ED访视期间对血液进行了采样,并检测了内皮细胞活化的生物标记物,即可溶性fms样酪氨酸激酶1(sFlt-1)。分别测定了纤溶酶原激活物抑制剂-1(PAI-1),sE-选择素,可溶性细胞间粘附分子(sICAM-1)和可溶性血管细胞粘附分子(sVCAM-1)。结果共纳入221例患者,其中无器官功能障碍的败血症占32%,无休克的严重脓毒症占30%,败血性休克的生物标志物与败血症严重程度,器官功能障碍和医院内死亡率之间的相关性。 32%的非感染性对照ED患者中有6%。所有靶标生物标志物(sFlt-1,PAI-1,sE-选择素,sICAM-1和sVCAM-1)与脓毒症严重程度之间存在相关性,P <0.05。我们发现所有生物标志物之间都存在显着的相互关系,包括sFlt-1和sE-选择素之间的最强相关性(r = 0.55,P <0.001),以及sFlt-1和PAI-1之间的最强相关性(0.56,P <0.001)。在内皮细胞激活生物标志物中,sFlt-1与SOFA评分之间的关​​联最强(r = 0.66,P <0.001),在严重脓毒症的受体操作者特征曲线下面积最高,为0.82,死亡率为0.91。内皮细胞的活化与败血症的严重程度,器官功能障碍和死亡率有关。对内皮反应和相关生物标记物的更好理解可能会导致在脓毒症中更准确地预测结果并开发新的针对内皮细胞的疗法的策略。

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