From the Department of Cerebrovascular Medicine (M.K., M. Inoue, S. Yoshimura, M.F.-D., K. Miwa, K. Minematsu, K. Toyoda).
Center for Advancing Clinical and Translational Sciences (H.Y.), National Cerebral and Cardiovascular Center, Suita.
Stroke. 2020 May;51(5):1530-1538. doi: 10.1161/STROKEAHA.119.028127. Epub 2020 Apr 6.
Background and Purpose- We assessed whether lower-dose alteplase at 0.6 mg/kg is efficacious and safe for acute fluid-attenuated inversion recovery-negative stroke with unknown time of onset. Methods- This was an investigator-initiated, multicenter, randomized, open-label, blinded-end point trial. Patients met the standard indication criteria for intravenous thrombolysis other than a time last-known-well >4.5 hours (eg, wake-up stroke). Patients were randomly assigned (1:1) to receive alteplase at 0.6 mg/kg or standard medical treatment if magnetic resonance imaging showed acute ischemic lesion on diffusion-weighted imaging and no marked corresponding hyperintensity on fluid-attenuated inversion recovery. The primary outcome was a favorable outcome (90-day modified Rankin Scale score of 0-1). Results- Following the early stop and positive results of the WAKE-UP trial (Efficacy and Safety of MRI-Based Thrombolysis in Wake-Up Stroke), this trial was prematurely terminated with 131 of the anticipated 300 patients (55 women; mean age, 74.4±12.2 years). Favorable outcome was comparable between the alteplase group (32/68, 47.1%) and the control group (28/58, 48.3%; relative risk [RR], 0.97 [95% CI, 0.68-1.41]; =0.892). Symptomatic intracranial hemorrhage within 22 to 36 hours occurred in 1/71 and 0/60 (RR, infinity [95% CI, 0.06 to infinity]; >0.999), respectively. Death at 90 days occurred in 2/71 and 2/60 (RR, 0.85 [95% CI, 0.06-12.58]; >0.999), respectively. Conclusions- No difference in favorable outcome was seen between alteplase and control groups among patients with ischemic stroke with unknown time of onset. The safety of alteplase at 0.6 mg/kg was comparable to that of standard treatment. Early study termination precludes any definitive conclusions. Registration- URL: https://www.clinicaltrials.gov; Unique identifier: NCT02002325.
背景与目的-我们评估了对于起病时间不明的急性液体衰减反转恢复(FLAIR)阴性卒中,使用 0.6mg/kg 低剂量阿替普酶是否有效且安全。方法-这是一项由研究者发起的、多中心、随机、开放标签、盲终点试验。患者除了最后一次已知时间(last-known-well,LKW)>4.5 小时外,符合静脉溶栓的标准适应证标准(例如,觉醒型卒中)。如果磁共振成像(MRI)显示扩散加权成像(DWI)上有急性缺血性病变且 FLAIR 上无明显相应高信号,则患者被随机(1:1)分配接受阿替普酶 0.6mg/kg 或标准治疗。主要结局为 90 天改良 Rankin 量表(mRS)评分 0-1 分的良好结局。结果-在 WAKE-UP 试验(MRI 指导的溶栓治疗在觉醒型卒中的疗效和安全性)提前终止并得出阳性结果后,本试验也提前终止,原计划入组 300 例患者,仅纳入了 131 例(55 例女性;平均年龄 74.4±12.2 岁)。阿替普酶组(32/68,47.1%)和对照组(28/58,48.3%)的良好结局无差异(相对风险 [RR],0.97[95%置信区间,0.68-1.41];=0.892)。22 至 36 小时内症状性颅内出血分别发生于 1/71 例和 0/60 例(RR,无穷大[95%置信区间,0.06 至无穷大];>0.999)。90 天死亡分别发生于 2/71 例和 2/60 例(RR,0.85[95%置信区间,0.06-12.58];>0.999)。结论-对于起病时间不明的缺血性卒中患者,阿替普酶组与对照组的良好结局无差异。阿替普酶 0.6mg/kg 的安全性与标准治疗相当。早期研究终止使得无法得出任何明确结论。注册-网址:www.clinicaltrials.gov;唯一标识符:NCT02002325。
