Department of Neurology, Erasmus MC University Medical Center, Rotterdam, the Netherlands.
Department of Radiology and Nuclear Medicine, Erasmus MC University Medical Center, Rotterdam, the Netherlands.
Trials. 2022 Aug 9;23(1):641. doi: 10.1186/s13063-022-06596-z.
The effectiveness of alteplase for ischemic stroke treatment is limited, partly due to the occurrence of intracranial and extracranial hemorrhage. Mutant pro-urokinase (m-proUK) does not deplete fibrinogen and lyses fibrin only after induction with alteplase. Therefore, this treatment has the potential to be safer and more efficacious than treatment with alteplase alone. The aim of this study is to assess the safety and efficacy of thrombolytic treatment consisting of a small bolus alteplase followed by m-proUK compared with standard thrombolytic treatment with alteplase in patients presenting with ischemic stroke.
DUMAS is a multicenter, phase II trial with a prospective randomized open-label blinded end-point (PROBE) design, and an adaptive design for dose optimization. Patients with ischemic stroke, who meet the criteria for treatment with intravenous (IV) alteplase can be included. Patients eligible for endovascular thrombectomy are excluded. Patients are randomly assigned (1:1) to receive a bolus of IV alteplase (5mg) followed by a continuous IV infusion of m-proUK (40 mg/h during 60 min) or usual care with alteplase (0.9 mg/kg). Depending on the results of interim analyses, the dose of m-proUK may be revised to a lower dose (30 mg/h during 60 min) or a higher dose (50 mg/h during 60 min). We aim to include 200 patients with a final diagnosis of ischemic stroke. The primary outcome is any post-intervention intracranial hemorrhage (ICH) on neuroimaging at 24 h according to the Heidelberg Bleeding Classification, analyzed with binary logistic regression. Efficacy outcomes include stroke severity measured with the National Institutes of Health Stroke Scale (NIHSS) at 24 h and 5-7 days, score on the modified Rankin scale (mRS) assessed at 30 days, change (pre-treatment vs. post-treatment) in abnormal perfusion volume, and blood biomarkers of thrombolysis at 24 h. Secondary safety endpoints include symptomatic intracranial hemorrhage, death, and major extracranial hemorrhage. This trial will use a deferred consent procedure.
When dual thrombolytic therapy with a small bolus alteplase and m-proUK shows the anticipated effect on the outcome, this will lead to a 13% absolute reduction in the occurrence of ICH in patients with ischemic stroke.
NL7409 (November 26, 2018)/NCT04256473 (February 5, 2020).
阿替普酶治疗缺血性脑卒中的效果有限,部分原因是颅内和颅外出血的发生。突变型组织型纤溶酶原激活物(m-proUK)不会耗尽纤维蛋白原,仅在阿替普酶诱导后才溶解纤维蛋白。因此,这种治疗方法比单独使用阿替普酶更安全、更有效。本研究旨在评估小剂量阿替普酶溶栓治疗联合 m-proUK 与标准阿替普酶溶栓治疗在缺血性脑卒中患者中的安全性和疗效。
DUMAS 是一项多中心、二期、前瞻性随机开放标签设盲终点(PROBE)设计的临床试验,设计具有适应性,用于剂量优化。符合静脉(IV)阿替普酶治疗标准的缺血性脑卒中患者可纳入研究。适合血管内血栓切除术的患者除外。患者随机分为(1:1)接受 IV 阿替普酶(5mg)推注,然后连续 IV 输注 m-proUK(60 分钟内 40mg/h)或标准阿替普酶治疗。根据中期分析结果,m-proUK 的剂量可能会修订为低剂量(60 分钟内 30mg/h)或高剂量(60 分钟内 50mg/h)。我们计划纳入 200 例最终诊断为缺血性脑卒中的患者。主要结局是 24 小时神经影像学检查根据海德堡出血分类的任何介入后颅内出血(ICH),采用二项逻辑回归分析。疗效结局包括 24 小时和 5-7 天的 NIH 卒中量表(NIHSS)评分、30 天改良 Rankin 量表(mRS)评分、异常灌注体积的变化(治疗前与治疗后)以及 24 小时的溶栓血生物标志物。次要安全性终点包括症状性颅内出血、死亡和主要颅外出血。该试验将采用延迟同意程序。
当小剂量阿替普酶联合 m-proUK 的双重溶栓治疗对结局产生预期效果时,这将导致缺血性脑卒中患者 ICH 的发生率降低 13%。
NL7409(2018 年 11 月 26 日)/NCT04256473(2020 年 2 月 5 日)。
