替奈普酶辅助与直接经皮冠状动脉介入治疗ST段抬高型急性心肌梗死患者（ASSENT-4 PCI）：随机试验

Primary versus tenecteplase-facilitated percutaneous coronary intervention in patients with ST-segment elevation acute myocardial infarction (ASSENT-4 PCI): randomised trial.

出版信息

Lancet. 2006 Feb 18;367(9510):569-78. doi: 10.1016/S0140-6736(06)68147-6.

Abstract

BACKGROUND

Primary percutaneous coronary intervention (PCI) is more effective than fibrinolytic therapy for ST-segment elevation acute myocardial infarction (STEMI), but time to intervention can be considerable. Our aim was to investigate whether the administration of full-dose tenecteplase before a delayed PCI could mitigate the negative effect of this delay.

METHODS

We did a randomised study in which we assigned patients with STEMI of less than 6 h duration (scheduled to undergo primary PCI with an anticipated delay of 1-3 h) to standard PCI (n=838) or PCI preceded by administration of full-dose tenecteplase (n=829). All patients received aspirin and a bolus, without an infusion, of unfractionated heparin. Our primary endpoint was death or congestive heart failure or shock within 90 days. Analyses were by intention to treat. This study is registered with , number NCT00168792.

FINDINGS

We planned to enroll 4000 patients, but early cessation of enrollment was recommended by the data and safety monitoring board because of a higher in-hospital mortality in the facilitated than in the standard PCI group (6% [43 of 664] vs 3% [22 of 656], p=0.0105). Of those enrolled, six were lost to follow-up in the facilitated PCI group and seven in the other group. Median time from randomisation to first balloon inflation was similar in both groups. The median time from bolus tenecteplase to first balloon inflation was 104 min. We noted the primary endpoint in 19% (151 of 810) of patients assigned facilitated PCI versus 13% (110 of 819) of those randomised to primary PCI (relative risk 1.39, 95% CI 1.11-1.74; p=0.0045). During hospital stay, significantly more strokes (1.8% [15 of 829] vs 0, p<0.0001), but not major non-cerebral bleeding complications (6% [46 of 829] vs 4% [37 of 838], p=0.3118), were reported in patients assigned facilitated rather than standard PCI. We also noted more ischaemic cardiac complications, such as reinfarction (6% [49 of 805] vs 4% [30 of 820], p=0.0279) or repeat target vessel revascularisation (7% [53 of 805] vs 3% [28 of 818], p=0.0041) within 90 days in this study group.

INTERPRETATION

A strategy of full-dose tenecteplase with antithrombotic co-therapy, as used in this study and preceding PCI by 1-3 h, was associated with more major adverse events than PCI alone in STEMI and cannot be recommended.

摘要

背景

对于ST段抬高型急性心肌梗死（STEMI），直接经皮冠状动脉介入治疗（PCI）比溶栓治疗更有效，但介入治疗的时间可能较长。我们的目的是研究在延迟PCI之前给予全剂量替奈普酶是否可以减轻这种延迟的负面影响。

方法

我们进行了一项随机研究，将发病时间小于6小时（计划接受直接PCI且预期延迟1 - 3小时）的STEMI患者随机分为标准PCI组（n = 838）或在PCI前给予全剂量替奈普酶组（n = 829）。所有患者均接受阿司匹林和一剂未进行静脉滴注的普通肝素。我们的主要终点是90天内的死亡、充血性心力衰竭或休克。分析采用意向性分析。本研究已在注册，注册号为NCT00168792。

研究结果

我们计划招募4000名患者，但数据与安全监测委员会建议提前终止入组，因为与标准PCI组相比，易化PCI组的院内死亡率更高（6% [664例中的43例] 对3% [656例中的22例]，p = 0.0105）。在已入组的患者中，易化PCI组有6例失访，另一组有7例失访。两组从随机分组到首次球囊扩张的中位时间相似。从推注替奈普酶到首次球囊扩张的中位时间为104分钟。在接受易化PCI的患者中，19%（810例中的151例）出现了主要终点事件，而在接受直接PCI的患者中这一比例为13%（819例中的110例）（相对风险1.39，95%可信区间1.11 - 1.74；p = 0.0045）。在住院期间，接受易化PCI而非标准PCI的患者报告的卒中显著更多（1.8% [829例中的15例] 对0，p < 0.0001），但主要非脑出血并发症无显著差异（6% [829例中的46例] 对4% [838例中的37例]，p = 0.3118）。在本研究组中，我们还注意到90天内缺血性心脏并发症更多，如再梗死（6% [805例中的49例] 对4% [820例中的30例]，p = 0.0279）或再次进行靶血管血运重建（7% [805例中的53例] 对3% [818例中的28例]，p = 0.0041）。