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急性心肌梗死早期的β受体阻滞剂治疗

Beta blockade early in acute myocardial infarction.

作者信息

Sleight P

出版信息

Am J Cardiol. 1987 Jul 15;60(2):6A-10A. doi: 10.1016/0002-9149(87)90492-9.

Abstract

Intravenous beta blockers given early in acute myocardial infarction have been shown to reduce chest pain, enzyme release and incidence of arrhythmias. Data published before the first report of the ISIS-1 group (International Studies of Infarct Survival) showed a 12% decrease in the probability of death using intravenous beta blockade but with large confidence limits. This study assessed and compared the effects of early intravenous atenolol and control treatment in the first week and first year after acute myocardial infarction in 16,027 patients. The principal endpoint was vascular death; most of the 15% decrease in mortality occurred in the first 24 to 36 hours with a significant difference at 1 week (313 vs 365 deaths in the atenolol and control groups, respectively). There was no rebound effect after stopping treatment after 7 days. Mortality at 1 year also showed a significant difference in favor of the atenolol group. Subgroup analysis found no significant difference in mortality by age, sex, initial heart rate, diabetes or entry electrocardiogram but data-derived analysis revealed a highly significant decrease in mortality if treatment began within 2 hours of the onset of pain. There was a significant 1% to 2% excess in inotrope use in the atenolol group in the first 36 hours, and first-degree heart block and bundle branch block emerged as relative contraindications to this treatment. The results suggest that early intravenous beta blockade in acute myocardial infarction is safe and effective and also cost effective in comparison with postdischarge oral beta blockade therapy.

摘要

急性心肌梗死早期静脉注射β受体阻滞剂已被证明可减轻胸痛、减少酶释放及心律失常的发生率。在ISIS-1组(心肌梗死存活国际研究)的首份报告之前发表的数据显示,静脉注射β受体阻滞剂可使死亡概率降低12%,但置信区间较大。本研究评估并比较了16027例患者在急性心肌梗死后第一周和第一年早期静脉注射阿替洛尔及对照治疗的效果。主要终点是血管性死亡;死亡率降低的15%中,大部分发生在最初的24至36小时,1周时存在显著差异(阿替洛尔组和对照组分别有313例和365例死亡)。7天后停药后无反跳效应。1年时的死亡率也显示出有利于阿替洛尔组的显著差异。亚组分析发现,按年龄、性别、初始心率、糖尿病或入院时心电图分析,死亡率无显著差异,但数据衍生分析显示,如果在疼痛发作后2小时内开始治疗,死亡率会显著降低。阿替洛尔组在最初36小时内使用正性肌力药物的比例显著高出1%至2%,一度房室传导阻滞和束支传导阻滞成为该治疗的相对禁忌证。结果表明,急性心肌梗死早期静脉注射β受体阻滞剂是安全有效的,与出院后口服β受体阻滞剂治疗相比,成本效益也更高。

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