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Early drotrecogin alpha (activated) administration in severe sepsis is associated with lower mortality: a retrospective analysis of the Canadian ENHANCE cohort

机译:严重败血症早期使用drotrecoginα(活化)给药可降低死亡率:加拿大ENHANCE队列的回顾性分析

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IntroductionEarly multimodal treatment of severe sepsis, including the use of drotrecogin alfa (activated) (DrotAA) when indicated, is considered essential for optimum outcome. However, predicting which infected patients will progress to severe sepsis and the need for aggressive intervention continues to be problematic. We therefore wished to explore whether there were any potential early markers that might predict improved survival in response to early use of DrotAA in patients with severe sepsis. In particular, in the dynamic setting of severe sepsis, we postulated that changes in markers reflecting evolving rather than baseline clinical status might guide therapy.MethodsData on a cohort of 305 Canadian patients from the open label ENHANCE trial of DrotAA in severe sepsis was retrospectively analyzed to search for potential clinical predictors of outcome in severe sepsis. Patients received a 96-hour infusion of DrotAA and were followed for 28 days. The association between time to treatment and mortality within subgroups defined by dynamic changes in various potential markers was explored.ResultsMortality at 28 days was 22.6% and the variables of age, time to treatment, and early changes in serum creatinine and platelet count were identified by logistic regression as independent predictors of mortality. Across all age ranges, 28-day mortality was lower when DrotAA was administered within 24 hours of first sepsis-induced organ dysfunction compared to administration after 24 hours for both subgroups of patients defined by changes in platelet count and creatinine within the first day.ConclusionsThese findings suggest that when indicated, treatment with DrotAA should be initiated as soon as possible, regardless of age.Trial RegistrationPrevious trial registration number: NCT00568893
机译:前言严重脓毒症的早期多式联运治疗,包括在需要时使用drotrecogin alfa(活化)(DrotAA),被认为是最佳治疗效果的关键。然而,预测哪些感染患者将发展为严重败血症,以及是否需要积极干预仍然存在问题。因此,我们希望探讨在严重脓毒症患者中,是否有任何潜在的早期标志物可预测因早期使用DrotAA而改善的生存率。特别是在严重脓毒症的动态背景下,我们假设反映进化而不是基线临床状况的标志物变化可能指导治疗。方法回顾性分析来自DrotAA的开放标签ENHANCE试验中305名加拿大患者在严重脓毒症中的数据寻找潜在的严重败血症临床预后指标。患者接受DrotAA的96小时输注,并随访28天。结果探讨了28天的死亡率为22.6%,通过年龄,治疗时间以及血清肌酐和血小板计数的早期变化确定了变量在亚组中的治疗时间与死亡率之间的关系。 Logistic回归是死亡率的独立预测因子。在所有年龄段,两个亚组患者在首次败血症引起的器官功能障碍的24小时内给予DrotAA的28天死亡率要低于第一天血小板计数和肌酐变化所定义的两个亚组的24天后死亡率。研究结果表明,在指示时,无论年龄大小,都应尽快开始DrotAA治疗。试验注册先前的试验注册号:NCT00568893

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