氨氯地平可减轻冠心病患者的短暂性心肌缺血：欧洲昼夜抗缺血计划（CAPE试验）。

Amlodipine reduces transient myocardial ischemia in patients with coronary artery disease: double-blind Circadian Anti-Ischemia Program in Europe (CAPE Trial).

作者信息

Deanfield J E, Detry J M, Lichtlen P R, Magnani B, Sellier P, Thaulow E

机构信息

Cardiothoracic Unit, Hospital for Sick Children, London, England, United Kingdom.

出版信息

J Am Coll Cardiol. 1994 Nov 15;24(6):1460-7. doi: 10.1016/0735-1097(94)90140-6.

DOI:10.1016/0735-1097(94)90140-6

PMID:7930276

Abstract

OBJECTIVES

This study was carried out to determine the effect of the once-daily calcium channel blocking agent amlodipine (half-life 35 to 50 h) on the circadian pattern of myocardial ischemia in patients with chronic stable angina.

BACKGROUND

Myocardial ischemia during normal daily life, both symptomatic and asymptomatic, has been associated with increased risk of cardiovascular morbidity and mortality, and the circadian pattern parallels that for myocardial infarction and sudden death.

METHODS

The Circadian Anti-Ischemia Program in Europe (CAPE) was a large, 10-week international (63 sites), double-blind, parallel study. After a 2-week, single-blind placebo phase, during which stable doses of antianginal treatment were maintained (beta-adrenergic blocking agents in 65% of patients), patients with chronic stable angina with at least three attacks of angina per week, with at least four ischemic episodes or > or = 20 min of ST segment depression in 48 h of Holter monitoring, were randomized to receive treatment with either 5 mg/day of amlodipine or placebo (2:1 randomization). The dose was increased to 10 mg/day after 4 weeks. During week 7 of treatment, 48-h ambulatory ECG monitoring was repeated.

RESULTS

Three hundred fifteen of 1,160 patients screened were eligible, and 250 had complete evaluable data. Compared with placebo, amlodipine significantly reduced both the frequency of ST segment depression episodes (60% for amlodipine vs. 44% for placebo, p = 0.025) and total integrated ST ischemic area (62% mm-min vs. 50% mm-min, p = 0.042). Amlodipine reduced ischemia over the 24 h with the intrinsic circadian pattern maintained. In addition, diary data showed a significant reduction in angina (70% for amlodipine vs. 44% for placebo, p = 0.0001) and in nitroglycerin consumption (67% vs. 22%, respectively, p = 0.0006). Amlodipine and placebo demonstrated similar safety profiles (adverse events 17.3% for amlodipine and 13.3% for placebo; discontinuation rates due to adverse events were 2% vs. 4.4%, respectively).

CONCLUSIONS

Once-daily amlodipine, when added to background treatment, significantly reduced both symptomatic and asymptomatic ischemic events over 24 h in patients with chronic stable angina.

摘要

目的

本研究旨在确定每日一次的钙通道阻滞剂氨氯地平（半衰期35至50小时）对慢性稳定性心绞痛患者心肌缺血昼夜模式的影响。

背景

日常生活中的心肌缺血，无论有无症状，都与心血管疾病发病率和死亡率的增加相关，其昼夜模式与心肌梗死和猝死相似。

方法

欧洲昼夜抗缺血项目（CAPE）是一项为期10周的大型国际（63个地点）双盲平行研究。在为期2周的单盲安慰剂阶段，维持稳定剂量的抗心绞痛治疗（65%的患者使用β-肾上腺素能阻滞剂）后，每周至少发作三次心绞痛、动态心电图监测48小时内至少有四次缺血发作或ST段压低≥20分钟的慢性稳定性心绞痛患者，被随机分为接受5毫克/天氨氯地平或安慰剂治疗（2:1随机分组）。4周后剂量增加至10毫克/天。在治疗第7周时，重复进行48小时动态心电图监测。

结果

1160名筛查患者中有315名符合条件，250名有完整的可评估数据。与安慰剂相比，氨氯地平显著降低了ST段压低发作频率（氨氯地平组为60%，安慰剂组为44%，p = 0.025）和总ST段缺血积分面积（62%毫米-分钟对50%毫米-分钟，p = 0.042）。氨氯地平在24小时内减少了缺血，同时维持了内在的昼夜模式。此外，日记数据显示心绞痛显著减少（氨氯地平组为70%，安慰剂组为44%，p = 0.0001），硝酸甘油消耗量也显著减少（分别为67%和22%，p = 0.0006）。氨氯地平和安慰剂的安全性相似（氨氯地平组不良事件发生率为17.3%，安慰剂组为13.3%；因不良事件停药率分别为2%和4.4%）。