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急性心肌梗死患者立即溶栓治疗与延迟直接血管成形术的死亡率获益比较。

Comparison of mortality benefit of immediate thrombolytic therapy versus delayed primary angioplasty for acute myocardial infarction.

作者信息

Kent David M, Ruthazer Robin, Griffith John L, Beshansky Joni R, Grines Cindy L, Aversano Thomas, Concannon Thomas W, Zalenski Robert J, Selker Harry P

机构信息

Center for Cardiovascular Health Services Research, Institute for Clinical Research and Health Policy Studies, Tufts-New England Medical Center, Tufts University School of Medicine, Boston, MA, USA.

出版信息

Am J Cardiol. 2007 May 15;99(10):1384-8. doi: 10.1016/j.amjcard.2006.12.068. Epub 2007 Mar 26.

Abstract

Primary percutaneous coronary intervention (PPCI) yields superior mortality outcomes compared with thrombolysis in ST-elevation acute myocardial infarction (STEMI) but takes longer to administer. Previous meta-regressions have estimated that a procedure-related delay of 60 minutes would nullify the benefits of PPCI on mortality. Using a combined database from randomized clinical trials and registries (n = 2,781) and an independently developed model of mortality risk in STEMI, we developed logistic regression models predicting 30-day mortality for PPCI and thrombolysis by examining the influence of baseline risk on the treatment effect of PPCI and on the hazard of treatment delay. We used these models to solve mathematically for "time interval to mortality equivalence," defined as the PPCI-related delay that would nullify its expected mortality benefit over thrombolysis, and to explore the influence of baseline risk on this value. As baseline risk increases, the relative benefit of PPCI compared with thrombolytic therapy significantly increases (p = 0.002); patients with STEMI at relatively low risk of mortality accrue little or no incremental mortality benefit from PPCI, but high-risk patients benefit greatly. However, as baseline risk increases, the hazard associated with longer treatment-related delay also increases (p = 0.007). These 2 effects are compensatory and yield a roughly uniform time interval to mortality equivalence of approximately 100 minutes in patients who have at least a moderate degree of mortality risk (> approximately 4%). In conclusion, the mortality benefits of PPCI and the hazard of PPCI-related delay depend on baseline risk. Previous meta-regressions appear to have underestimated the PPCI-related delay that would nullify the incremental benefits of PPCI.

摘要

在ST段抬高型急性心肌梗死(STEMI)患者中,与溶栓治疗相比,直接经皮冠状动脉介入治疗(PPCI)能带来更好的死亡率结局,但实施时间更长。以往的Meta回归分析估计,与手术相关的60分钟延迟会抵消PPCI在死亡率方面的益处。我们使用来自随机临床试验和登记处的合并数据库(n = 2781)以及自主开发的STEMI死亡风险模型,通过研究基线风险对PPCI治疗效果和治疗延迟风险的影响,建立了逻辑回归模型来预测PPCI和溶栓治疗的30天死亡率。我们使用这些模型通过数学方法求解“死亡率等效时间间隔”,即会抵消PPCI相对于溶栓治疗预期死亡率益处的与PPCI相关的延迟,并探讨基线风险对该值的影响。随着基线风险增加,PPCI相对于溶栓治疗的相对益处显著增加(p = 0.002);死亡率相对较低的STEMI患者从PPCI中获得的额外死亡率益处很少或没有,但高危患者获益巨大。然而,随着基线风险增加,与更长治疗相关延迟相关的风险也增加(p = 0.007)。这两种效应相互补偿,在至少有中度死亡风险(>约4%)的患者中产生大致统一的死亡率等效时间间隔,约为100分钟。总之,PPCI的死亡率益处和与PPCI相关延迟的风险取决于基线风险。以往的Meta回归分析似乎低估了会抵消PPCI额外益处的与PPCI相关的延迟。

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