Rowan Kathryn M, Welch Catherine A, North Emma, Harrison David A
Intensive Care National Audit & Research Centre, Tavistock House, Tavistock Square, London WC1H 9HR, UK.
Crit Care. 2008;12(2):R58. doi: 10.1186/cc6879. Epub 2008 Apr 22.
In March 2001, the results of the Recombinant Human Activated Protein C Worldwide Evaluation in Severe Sepsis (PROWESS) study were published, which indicated a 6.1% absolute reduction in 28-day mortality. Drotrecogin alfa (activated; DrotAA) was subsequently approved for use in patients with severe sepsis.
In December 2002, critical care units in England, Wales and Northern Ireland were invited to participate in an audit of DrotAA. Data for each infusion of DrotAA were linked to case mix and outcome data from a national audit. Use of DrotAA was described and a nonrandomized comparison of effectiveness was conducted.
1,292 infusions of DrotAA were recorded in 112 units; 61% commenced during the first 24 hours in the unit. The majority (77%) of patients had three or more organs failing; lung (42%) and abdomen (40%) were the most common primary sites of infection. Crude hospital mortality was high (45%); at 28 days, only 18% had left acute hospital and 19% were still in the unit. For 30%, the full 96-hour infusion was not completed; 24% of infusions were interrupted; 8.1% experienced one or more serious adverse events, of which 77% were serious bleeding events. Of eight relative risks estimated from individually-matched (0.75 to 0.85) and propensity-matched (0.82 to 0.90) controls, seven were consistent with the results of PROWESS. Restricting the analysis to patients receiving DrotAA during the first 24 hours resulted in larger treatment effects (relative risks 0.62 to 0.81). For all matches, similar patterns were seen across subgroups. No effect of DrotAA was seen for two organs failing or lower severity scores, compared with a significant mortality reduction for three or more organs failing or higher severity scores.
Use of DrotAA was approximately one in 16 for admissions meeting the definition for severe sepsis and with two or more organs failing. Patients receiving DrotAA were younger and more severely ill but were less likely to have serious conditions in their past medical history. Nonrandomized estimates for the effectiveness of DrotAA were consistent with the findings of PROWESS. DrotAA appeared not to be effective in patients with less severe disease.
2001年3月,重组人活化蛋白C全球严重脓毒症评估(PROWESS)研究结果发表,该研究表明28天死亡率绝对降低了6.1%。随后,重组人活化蛋白C(活性)[Drotrecogin alfa(activated);DrotAA]被批准用于严重脓毒症患者。
2002年12月,邀请英格兰、威尔士和北爱尔兰的重症监护病房参与DrotAA的一项审计。每次DrotAA输注的数据与来自一项全国审计的病例组合和结局数据相关联。描述了DrotAA的使用情况,并进行了有效性的非随机比较。
112个病房记录了1292次DrotAA输注;61%在病房的头24小时内开始。大多数(77%)患者有三个或更多器官功能衰竭;肺部(42%)和腹部(40%)是最常见的原发性感染部位。医院粗死亡率很高(45%);在28天时,只有18%的患者离开急症医院,19%的患者仍在病房。30%的患者未完成96小时的全程输注;24%的输注被中断;8.1%的患者发生了一次或多次严重不良事件,其中77%为严重出血事件。从个体匹配(0.75至0.85)和倾向匹配(0.82至0.90)对照组估计的八个相对风险中,有七个与PROWESS的结果一致。将分析限制在头24小时内接受DrotAA的患者中,治疗效果更大(相对风险为0.62至0.81)。对于所有匹配情况,各亚组均观察到相似模式。与三个或更多器官功能衰竭或更高严重程度评分患者的死亡率显著降低相比,两个器官功能衰竭或较低严重程度评分患者未观察到DrotAA的效果。
对于符合严重脓毒症定义且有两个或更多器官功能衰竭的入院患者,DrotAA的使用比例约为十六分之一。接受DrotAA治疗的患者更年轻且病情更严重,但既往病史中严重疾病的可能性较小。DrotAA有效性的非随机估计与PROWESS的结果一致。DrotAA在病情较轻的患者中似乎无效。
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