Clinical Epidemiology Program, Ottawa Hospital Research Institute, Ottawa, ON, Canada.
BMJ. 2012 Sep 11;345:e5798. doi: 10.1136/bmj.e5798.
To estimate the relative risks of death, myocardial infarction, stroke, and renal failure or dysfunction between antifibrinolytics and no treatment following the suspension of aprotinin from the market in 2008 for safety reasons and its recent reintroduction in Europe and Canada.
Systematic review and network meta-analysis.
A Cochrane review of antifibrinolytic treatments was chosen as the starting point for this systematic review. Medline, Embase, and the Cochrane register of trials were searched with no date restrictions for observational evidence.
Propensity matched or adjusted observational studies with two or more of the interventions of interest (aprotinin, tranexamic acid, epsilon-aminocaproic acid, and no treatment) that were carried out in patients undergoing cardiac surgery.
Network meta-analysis was used to compare treatments, and odds ratios with 95% credible intervals were estimated. Meta-analyses were carried out for randomised controlled trials alone and for randomised controlled trials with observational studies.
106 randomised controlled trials and 11 observational studies (43,270 patients) were included. Based on the results from analysis of randomised controlled trials, tranexamic acid was associated on average with a reduced risk of death compared with aprotinin (odds ratio 0.64, 95% credible interval 0.41 to 0.99). When observational data were incorporated, comparisons showed an increased risk of mortality with aprotinin on average relative to tranexamic acid (odds ratio 0.71, 95% credible interval 0.50 to 0.98) and epsilon-aminocaproic acid (0.60, 0.43 to 0.87), and an increased risk of renal failure or dysfunction on average relative to all comparators: odds ratio 0.66 (95% credible interval 0.45 to 0.88) compared with no treatment, 0.66 (0.48 to 0.91) versus tranexamic acid, and 0.65 (0.45 to 0.88) versus epsilon-aminocaproic acid.
Although meta-analyses of randomised controlled trials were largely inconclusive, inclusion of observational data suggest concerns remain about the safety of aprotinin. Tranexamic and epsilon-aminocaproic acid are effective alternatives that may be safer for patients.
评估因安全性原因于 2008 年停用抑肽酶,随后在欧洲和加拿大重新引入该药后,抑肽酶与不治疗相比,在死亡、心肌梗死、卒中和肾衰竭或功能障碍方面的相对风险。
系统评价和网络荟萃分析。
选择 Cochrane 对纤维蛋白溶解抑制剂治疗的综述作为本系统评价的起点。无日期限制地检索 Medline、Embase 和 Cochrane 试验登记处的观察性证据。
对接受心脏手术的患者进行了两项或多项干预(抑肽酶、氨甲环酸、ε-氨基己酸和不治疗)的倾向匹配或调整的观察性研究。
使用网络荟萃分析比较治疗方法,并估计比值比及其 95%可信区间。对随机对照试验单独进行荟萃分析,并对随机对照试验和观察性研究进行荟萃分析。
纳入 106 项随机对照试验和 11 项观察性研究(43270 例患者)。基于对随机对照试验分析的结果,氨甲环酸与抑肽酶相比,平均死亡风险降低(比值比 0.64,95%可信区间 0.41 至 0.99)。当纳入观察性数据时,比较表明,与氨甲环酸相比,抑肽酶平均风险增加(比值比 0.71,95%可信区间 0.50 至 0.98)和 ε-氨基己酸(0.60,0.43 至 0.87)),与所有对照相比,平均风险增加肾功能衰竭或功能障碍:与不治疗相比,比值比为 0.66(95%可信区间 0.45 至 0.88),与氨甲环酸相比为 0.66(0.48 至 0.91),与 ε-氨基己酸相比为 0.65(0.45 至 0.88)。
尽管对随机对照试验的荟萃分析基本没有定论,但纳入观察性数据表明,人们仍然对抑肽酶的安全性表示担忧。氨甲环酸和 ε-氨基己酸是有效的替代品,对患者可能更安全。
Zotero 插件
