急性心肌梗死患者行冠状动脉介入治疗时，瑞替普酶联合阿昔单抗与单用阿昔单抗早期给药的随机对照试验。

Early administration of reteplase plus abciximab vs abciximab alone in patients with acute myocardial infarction referred for percutaneous coronary intervention: a randomized controlled trial.

作者信息

Kastrati Adnan, Mehilli Julinda, Schlotterbeck Klaus, Dotzer Franz, Dirschinger Josef, Schmitt Claus, Nekolla Stephan G, Seyfarth Melchior, Martinoff Stefan, Markwardt Christina, Clermont Günther, Gerbig Hans-Wilhelm, Leiss Johannes, Schwaiger Markus, Schömig Albert

机构信息

Deutsches Herzzentrum, Technische Universität, Munich, Germany.

出版信息

JAMA. 2004 Feb 25;291(8):947-54. doi: 10.1001/jama.291.8.947.

DOI:10.1001/jama.291.8.947

PMID:14982910

Abstract

CONTEXT

The optimal pharmacological strategy for bridging the delay between admission and performance of percutaneous coronary intervention (PCI) in patients with acute myocardial infarction (MI) is not known.

OBJECTIVE

To assess whether early administration of reteplase plus abciximab produces better results compared with abciximab alone in patients with acute MI referred for PCI.

DESIGN, SETTING, AND PATIENTS: Open-label, randomized controlled study conducted from May 3, 2001, through June 2, 2003, of 253 patients who were admitted to 13 community hospitals without catheterization facilities (n = 186) and to 5 hospitals with catheterization facilities (n = 67), with the diagnosis of an ST-segment elevation acute MI within 12 hours from onset of symptoms.

INTERVENTIONS

Patients received intravenously either the combination of a half-dose reteplase (two 5-U boluses, 30 minutes apart) with a standard dose of abciximab (0.25 mg/kg bolus, 0.125 microg/kg per minute infusion [maximum 10 microg/min for 12 hours]) or the standard dose of abciximab alone; all patients were then transferred for PCI.

MAIN OUTCOME MEASURE

Final infarct size according to a single-photon emission computed tomography study with technetium Tc 99m sestamibi performed between 5 and 10 days after randomization in 228 patients (90.1% of entire sample).

RESULTS

Of the 253 patients enrolled, 125 were assigned to reteplase plus abciximab and 128 to abciximab alone. The median (interquartile range) of the final infarct size of the left ventricle was 13.0% (3.0%-28.0%) in the reteplase plus abciximab group and 11.5% (3.0%-26.3%) in the abciximab-alone group (P =.81). The mean difference in final infarct size of left ventricle between the reteplase plus abciximab group and the abciximab group was 1.3% (95% confidence interval [CI], -3.1% to 5.7%). Within 6 months after randomization, the composite secondary end point of death, recurrent MI, or stroke occurred in 8 patients (6.4%) in the reteplase plus abciximab group and 6 patients (4.7%) in the abciximab group (relative risk, 1.4; 95% CI, 0.5-3.9; log-rank P =.56). Major bleeding complications were observed in 7 patients (5.6%) in the reteplase plus abciximab group and 2 patients (1.6%) in the abciximab group (P =.16).

CONCLUSION

Early administration of reteplase plus abciximab does not lead to a reduction of infarct size compared with abciximab alone in patients with acute MI referred for PCI.

摘要

背景

对于急性心肌梗死（MI）患者，在入院与进行经皮冠状动脉介入治疗（PCI）之间的延迟期内，最佳的药物治疗策略尚不清楚。

目的

评估在因PCI而转诊的急性MI患者中，早期给予瑞替普酶联合阿昔单抗与单独使用阿昔单抗相比，是否能产生更好的效果。

设计、地点和患者：2001年5月3日至2003年6月2日进行的一项开放标签、随机对照研究，纳入了253例患者，其中186例来自13家无导管插入设施的社区医院，67例来自5家有导管插入设施的医院，这些患者在症状发作后12小时内被诊断为ST段抬高型急性MI。

干预措施

患者静脉注射半剂量瑞替普酶（两次5单位推注，间隔30分钟）与标准剂量阿昔单抗（0.25mg/kg推注，0.125μg/kg每分钟输注[12小时内最大10μg/分钟]）的组合，或仅注射标准剂量的阿昔单抗；然后所有患者均被转至进行PCI。

主要结局指标

在随机分组后5至10天，对228例患者（占整个样本的90.1%）进行锝Tc 99m司他美比单光子发射计算机断层扫描研究，根据该研究确定最终梗死面积。

结果

在纳入的253例患者中，125例被分配至瑞替普酶联合阿昔单抗组，128例被分配至单独使用阿昔单抗组。瑞替普酶联合阿昔单抗组左心室最终梗死面积的中位数（四分位间距）为13.0%（3.0% - 28.0%），单独使用阿昔单抗组为11.5%（3.0% - 26.3%）（P = 0.81）。瑞替普酶联合阿昔单抗组与阿昔单抗组左心室最终梗死面积的平均差异为1.3%（95%置信区间[CI]为 - 3.1%至5.7%）。在随机分组后6个月内，瑞替普酶联合阿昔单抗组有8例患者（6.4%）发生死亡、复发性MI或卒中的复合次要终点事件，阿昔单抗组有6例患者（4.7%）发生（相对风险，1.4；95%CI为0.5 - 3.9；对数秩检验P = 0.56）。瑞替普酶联合阿昔单抗组有7例患者（5.6%）发生大出血并发症，阿昔单抗组有2例患者（1.6%）发生（P = 0.16）。