Sarullo F M, Pasquale P D, D'Alfonso G, Amerigo L, Cannizzaro S, Castello A
Division of Cardiology, Buccheri La Ferla-Fatebenefratelli Hospital, Palermo, Italy.
Ital Heart J. 2001 Aug;2(8):605-11.
The goal of therapy in acute myocardial infarction (AMI) is the complete and timely restoration of coronary blood flow. Platelets have a pivotal role in the pathophysiology of AMI. The study was aimed at evaluating the safety and efficacy of the combination of 50 mg alteplase plus tirofiban vs 100 mg alteplase in AMI patients.
One hundred twenty patients (83 males, 37 females; mean age 54.3 +/- 8 years) were hospitalized for suspected AMI within 6 hours of the onset of symptoms. All patients presented pain and persistent ST-segment elevation, were suitable candidates for thrombolysis (1st episode) and were randomized (double blind) into two groups. Group A (n = 60,42 males, 18 females) received 50 mg alteplase (15 mg as bolus, followed by an infusion of 35 mg over 60 min) in combination with tirofiban (0.4 mcg/kg/min for 30 min followed by an infusion of 0.1 mcg/kg/min for 3 days). Group B (n = 60, 41 males, 19 females) received 100 mg of accelerated-dose alteplase alone. Reperfusion criteria were defined as follows: > 50% reduction in the ST-segment elevation; resolution of chest pain; double marker of creatine kinase (CK) and CK-MB activity 2 hours after the start of thrombolysis; reperfusion arrhythmias within the first 120 min of thrombolysis. The blood pressure, heart rate and ECG were continuously monitored. The mortality, re-AMI, recurrent angina, major and minor bleeding, and emergency bypass surgery or coronary angioplasty were checked.
The groups were similar with regard to clinical data, risk factors, time elapsed from the onset of symptoms to thrombolytic therapy and AMI localization. Forty-seven patients (78.3%) from group A showed reperfusion (15-60 min) vs 25 patients (41.7%) from group B (43-105 min after the end of full-thrombolysis, p = 0.01). Group A patients showed an earlier CK peak and lower CK and CK-MB peaks than those in the control group (p = 0.0001, p = 0.011, p = 0.005, respectively). Nine patients (7.5%) died: 6 (10%) in group B and 3 (5%) in group A (p = NS). A non-fatal re-AMI occurred in 8 patients from group A and in 4 patients from group B (p = NS). Recurrent angina occurred in 27 patients (45%) from group A and in 11 (18.3%) from group B (p = 0.037). Twenty-three of these patients underwent urgent coronary angioplasty (17 from group A and 6 from group B) and 3 from group A and 1 from group B underwent urgent coronary artery bypass grafting (p = NS). The frequency of minor bleeding was higher in group A than in group B (56.7 vs 25%, p = 0.033). No major bleeding was observed in the study groups. At the predischarge echocardiogram, the ejection fraction was higher in group A than in group B (50 +/- 9 vs 44 +/- 7%, p = 0.001).
Our data suggest that the combination of glycoprotein IIb/IIIa inhibitors plus alteplase is feasible in AMI patients and that the increased risk of bleeding is an acceptable risk considering the advantage in terms of the reduction in the extent of an AMI. In addition, this combination can allow one to gain time when it is necessary to perform mechanical revascularization in patients admitted to a hospital without an interventional cardiology laboratory or in those who have to be referred to another hospital for urgent coronary artery bypass grafting.
急性心肌梗死(AMI)治疗的目标是完全且及时地恢复冠状动脉血流。血小板在AMI的病理生理过程中起关键作用。本研究旨在评估50mg阿替普酶联合替罗非班与100mg阿替普酶用于AMI患者的安全性和有效性。
120例患者(83例男性,37例女性;平均年龄54.3±8岁)在症状发作6小时内因疑似AMI入院。所有患者均有胸痛且ST段持续抬高,均适合进行溶栓治疗(首次发作),并被随机(双盲)分为两组。A组(n = 60,42例男性,18例女性)接受50mg阿替普酶(15mg静脉推注,随后在60分钟内输注35mg)联合替罗非班(0.4μg/kg/min持续30分钟,随后0.1μg/kg/min输注3天)。B组(n = 60,41例男性,19例女性)仅接受100mg加速剂量的阿替普酶。再灌注标准定义如下:ST段抬高降低>50%;胸痛缓解;溶栓开始2小时后肌酸激酶(CK)和CK-MB活性出现双峰;溶栓开始后120分钟内出现再灌注心律失常。持续监测血压、心率和心电图。检查死亡率、再发AMI、复发性心绞痛、严重和轻微出血以及急诊搭桥手术或冠状动脉成形术。
两组在临床数据、危险因素、从症状发作到溶栓治疗的时间以及AMI部位方面相似。A组47例患者(78.3%)出现再灌注(15 - 60分钟),而B组25例患者(41.7%)出现再灌注(溶栓结束后43 - 105分钟,p = 0.01)。A组患者的CK峰值出现更早,CK和CK-MB峰值低于对照组(分别为p = 0.0001、p = 0.011、p = 0.005)。9例患者(7.5%)死亡:B组6例(10%),A组3例(5%)(p = 无统计学意义)。A组8例患者和B组4例患者发生非致命性再发AMI(p = 无统计学意义)。A组27例患者(45%)出现复发性心绞痛,B组11例患者(18.3%)出现复发性心绞痛(p = 0.037)。其中23例患者接受了紧急冠状动脉成形术(A组17例,B组6例),A组3例和B组1例接受了紧急冠状动脉搭桥术(p = 无统计学意义)。A组轻微出血的发生率高于B组(56.7%对25%,p = 0.033)。研究组未观察到严重出血。出院前超声心动图检查显示,A组射血分数高于B组(50±9%对44±7%,p = 0.001)。
我们的数据表明,糖蛋白IIb/IIIa抑制剂联合阿替普酶用于AMI患者是可行的,考虑到在减少AMI范围方面的优势,出血风险增加是可接受的。此外,对于入住没有介入心脏病学实验室的医院的患者或必须转诊至其他医院进行紧急冠状动脉搭桥术的患者,这种联合用药在需要进行机械性血运重建时可节省时间。
