Dhainaut Jean-François, Laterre Pierre-François, LaRosa Steven P, Levy Howard, Garber Gary E, Heiselman Darell, Kinasewitz Gary T, Light R Bruce, Morris Peter, Schein Roland, Sollet Jean-Pierre, Bates Becky M, Utterback Barbara G, Maki Dennis
Department of Intensive Care, Cochin Hospital, Cochin Institute, Cochin Port-Royal Medical School, Paris V University, France.
Crit Care Med. 2003 Sep;31(9):2291-301. doi: 10.1097/01.CCM.0000085089.88077.AF.
In the multinational PROWESS trial, drotrecogin alfa (activated) significantly reduced mortality rate in patients with severe sepsis compared with placebo. The use of large multiple-center trials can potentially complicate interpretation of results in severe sepsis populations because of variability in medical attitudes and practices and the frequency of confounding events such as protocol violations. The objective of this study was to perform a blinded, critical, integrated review of data from the 1,690 severe sepsis patients from 164 medical centers enrolled in the PROWESS trial using a Clinical Evaluation Committee.
Blinded, critical, integrated review of data.
Participating sites.
The 1,690 severe sepsis patients from 164 medical centers enrolled in the PROWESS trial.
We performed analyses of the optimal cohort, defined as patients who had full compliance with the protocol, had evidence of an infection, and received adequate anti-infective therapy. We also performed other analyses, including significant underlying disorders, life support measures, and causes of death.
The optimal cohort of 81.4% of the intention-to-treat population [drotrecogin alfa (activated), n = 695; placebo, n = 680] had similar baseline severity of illness between the two groups, a similar pharmacodynamic effect, and a relative risk of death estimate consistent with that observed in the overall PROWESS trial (0.83, 95% confidence interval 0.69-0.99 vs. 0.806, 95% confidence interval 0.69-0.94). A beneficial effect of drotrecogin alfa (activated) similarly was observed in patients with significant underlying disorders (0.73, 95% confidence interval 0.57-0.93) who were more severely ill and had a higher percentage of patients forgoing life-sustaining therapy. In contrast with the original investigator determinations, a benefit associated with drotrecogin alfa (activated) treatment in urinary tract infection adjudicated by the Clinical Evaluation Committee was observed.
The survival benefit associated with drotrecogin alfa (activated) use was consistent with the results of the overall trial regardless of whether patients met criteria of the optimal cohort or had a significant underlying disorder.
在多中心PROWESS试验中,与安慰剂相比,活化蛋白C显著降低了严重脓毒症患者的死亡率。由于医学态度和实践的差异以及诸如违反方案等混杂事件的发生频率,大型多中心试验的结果解释可能会变得复杂。本研究的目的是使用临床评估委员会对PROWESS试验中164个医学中心的1690例严重脓毒症患者的数据进行盲法、严格、综合审查。
对数据进行盲法、严格、综合审查。
参与试验的各站点。
PROWESS试验中164个医学中心的1690例严重脓毒症患者。
我们对最佳队列进行了分析,最佳队列定义为完全符合方案、有感染证据且接受了充分抗感染治疗的患者。我们还进行了其他分析,包括严重基础疾病、生命支持措施和死亡原因。
意向性治疗人群中81.4%的最佳队列[活化蛋白C组,n = 695;安慰剂组,n = 680]两组间基线疾病严重程度相似,药效学效应相似,死亡相对风险估计与整个PROWESS试验中观察到的一致(0.83,95%置信区间0.69 - 0.99 vs. 0.806,95%置信区间0.69 - 0.94)。在患有严重基础疾病的患者中(0.73,95%置信区间0.57 - 0.93)同样观察到活化蛋白C的有益效果,这些患者病情更严重,放弃维持生命治疗的患者比例更高。与最初研究者的判定相反,临床评估委员会判定在尿路感染中活化蛋白C治疗有获益。
无论患者是否符合最佳队列标准或患有严重基础疾病,使用活化蛋白C带来的生存获益与整个试验结果一致。
