Schwartz G G, Olsson A G, Ezekowitz M D, Ganz P, Oliver M F, Waters D, Zeiher A, Chaitman B R, Leslie S, Stern T
Cardiology Section (111B), Denver VA Medical Center, 1055 Clermont St, Denver, CO 80220, USA.
JAMA. 2001 Apr 4;285(13):1711-8. doi: 10.1001/jama.285.13.1711.
Patients experience the highest rate of death and recurrent ischemic events during the early period after an acute coronary syndrome, but it is not known whether early initiation of treatment with a statin can reduce the occurrence of these early events.
To determine whether treatment with atorvastatin, 80 mg/d, initiated 24 to 96 hours after an acute coronary syndrome, reduces death and nonfatal ischemic events.
A randomized, double-blind trial conducted from May 1997 to September 1999, with follow-up through 16 weeks at 122 clinical centers in Europe, North America, South Africa, and Australasia.
A total of 3086 adults aged 18 years or older with unstable angina or non-Q-wave acute myocardial infarction.
Patients were stratified by center and randomly assigned to receive treatment with atorvastatin (80 mg/d) or matching placebo between 24 and 96 hours after hospital admission.
Primary end point event defined as death, nonfatal acute myocardial infarction, cardiac arrest with resuscitation, or recurrent symptomatic myocardial ischemia with objective evidence and requiring emergency rehospitalization.
A primary end point event occurred in 228 patients (14.8%) in the atorvastatin group and 269 patients (17.4%) in the placebo group (relative risk [RR], 0.84; 95% confidence interval [CI], 0.70-1.00; P =.048). There were no significant differences in risk of death, nonfatal myocardial infarction, or cardiac arrest between the atorvastatin group and the placebo group, although the atorvastatin group had a lower risk of symptomatic ischemia with objective evidence and requiring emergency rehospitalization (6.2% vs 8.4%; RR, 0.74; 95% CI, 0.57-0.95; P =.02). Likewise, there were no significant differences between the atorvastatin group and the placebo group in the incidence of secondary outcomes of coronary revascularization procedures, worsening heart failure, or worsening angina, although there were fewer strokes in the atorvastatin group than in the placebo group (12 vs 24 events; P =.045). In the atorvastatin group, mean low-density lipoprotein cholesterol level declined from 124 mg/dL (3.2 mmol/L) to 72 mg/dL (1.9 mmol/L). Abnormal liver transaminases (>3 times upper limit of normal) were more common in the atorvastatin group than in the placebo group (2.5% vs 0.6%; P<.001).
For patients with acute coronary syndrome, lipid-lowering therapy with atorvastatin, 80 mg/d, reduces recurrent ischemic events in the first 16 weeks, mostly recurrent symptomatic ischemia requiring rehospitalization.
急性冠脉综合征后的早期,患者死亡率和缺血事件复发率最高,但尚不清楚早期启动他汀类药物治疗是否能减少这些早期事件的发生。
确定急性冠脉综合征后24至96小时开始使用阿托伐他汀80mg/d治疗是否能降低死亡和非致死性缺血事件的发生率。
1997年5月至1999年9月进行的一项随机、双盲试验,在欧洲、北美、南非和澳大拉西亚的122个临床中心随访16周。
共3086名18岁及以上患有不稳定型心绞痛或非Q波急性心肌梗死的成年人。
患者按中心分层,在入院后24至96小时之间随机分配接受阿托伐他汀(80mg/d)治疗或匹配的安慰剂。
主要终点事件定义为死亡、非致死性急性心肌梗死、心脏骤停复苏、或有客观证据且需要紧急再次住院的复发性症状性心肌缺血。
阿托伐他汀组228名患者(14.8%)发生主要终点事件,安慰剂组269名患者(17.4%)发生主要终点事件(相对风险[RR],0.84;95%置信区间[CI],0.70 - 1.00;P = 0.048)。阿托伐他汀组和安慰剂组在死亡风险、非致死性心肌梗死或心脏骤停方面无显著差异,尽管阿托伐他汀组有客观证据且需要紧急再次住院的症状性缺血风险较低(6.2%对8.4%;RR,0.74;95%CI,0.57 - 0.95;P = 0.02)。同样,阿托伐他汀组和安慰剂组在冠状动脉血运重建术、心力衰竭恶化或心绞痛恶化等次要结局的发生率方面无显著差异,尽管阿托伐他汀组中风事件少于安慰剂组(12例对24例;P = 0.045)。在阿托伐他汀组,平均低密度脂蛋白胆固醇水平从124mg/dL(3.2mmol/L)降至72mg/dL(1.9mmol/L)。阿托伐他汀组肝转氨酶异常(>正常上限3倍)比安慰剂组更常见(2.5%对0.6%;P<0.001)。
对于急性冠脉综合征患者,每日80mg阿托伐他汀降脂治疗可在最初16周内降低缺血事件复发率,主要是需要再次住院的复发性症状性缺血。
