去氨普酶治疗急性缺血性卒中试验(DIAS):一项基于MRI的9小时窗急性卒中静脉溶栓Ⅱ期试验,使用静脉注射去氨普酶。
The Desmoteplase in Acute Ischemic Stroke Trial (DIAS): a phase II MRI-based 9-hour window acute stroke thrombolysis trial with intravenous desmoteplase.
作者信息
Hacke Werner, Albers Greg, Al-Rawi Yasir, Bogousslavsky Julien, Davalos Antonio, Eliasziw Michael, Fischer Michael, Furlan Anthony, Kaste Markku, Lees Kennedy R, Soehngen Mariola, Warach Steven
机构信息
Department of Neurology, University of Heidelberg, Im Neuenheimer Feld 400, 69120 Heidelberg, Germany.
出版信息
Stroke. 2005 Jan;36(1):66-73. doi: 10.1161/01.STR.0000149938.08731.2c. Epub 2004 Nov 29.
BACKGROUND AND PURPOSE
Most acute ischemic stroke patients arrive after the 3-hour time window for recombinant tissue plasminogen activator (rtPA) administration. The Desmoteplase In Acute Ischemic Stroke trial (DIAS) was a dose-finding randomized trial designed to evaluate the safety and efficacy of intravenous desmoteplase, a highly fibrin-specific and nonneurotoxic thrombolytic agent, administered within 3 to 9 hours of ischemic stroke onset in patients with perfusion/diffusion mismatch on MRI.
METHODS
DIAS was a placebo-controlled, double-blind, randomized, dose-finding phase II trial. Patients with National Institute of Health Stroke Scale (NIHSS) scores of 4 to 20 and MRI evidence of perfusion/diffusion mismatch were eligible. Of 104 patients, the first 47 (referred to as Part 1) were randomized to fixed doses of desmoteplase (25 mg, 37.5 mg, or 50 mg) or placebo. Because of an excessive rate of symptomatic intracranial hemorrhage (sICH), lower weight-adjusted doses escalating through 62.5 microg/kg, 90 microg/kg, and 125 microg/kg were subsequently investigated in 57 patients (referred to as Part 2). The safety endpoint was the rate of sICH. Efficacy endpoints were the rate of reperfusion on MRI after 4 to 8 hours and clinical outcome as assessed by NIHSS, modified Rankin scale, and Barthel Index at 90 days.
RESULTS
Part 1 was terminated prematurely because of high rates of sICH with desmoteplase (26.7%). In Part 2, the sICH rate was 2.2%. No sICH occurred with placebo in either part. Reperfusion rates up to 71.4% (P=0.0012) were observed with desmoteplase (125 microg/kg) compared with 19.2% with placebo. Favorable 90-day clinical outcome was found in 22.2% of placebo-treated patients and between 13.3% (62.5 microg/kg; P=0.757) and 60.0% (125 microg/kg; P=0.0090) of desmoteplase-treated patients. Early reperfusion correlated favorably with clinical outcome (P=0.0028). Favorable outcome occurred in 52.5% of patients experiencing reperfusion versus 24.6% of patients without reperfusion.
CONCLUSIONS
Intravenous desmoteplase administered 3 to 9 hours after acute ischemic stroke in patients selected with perfusion/diffusion mismatch is associated with a higher rate of reperfusion and better clinical outcome compared with placebo. The sICH rate with desmoteplase was low, using doses up to 125 microg/kg.
背景与目的
大多数急性缺血性脑卒中患者在重组组织型纤溶酶原激活剂(rtPA)给药的3小时时间窗之后才到达医院。急性缺血性脑卒中去氨普酶试验(DIAS)是一项剂量探索性随机试验,旨在评估静脉注射去氨普酶的安全性和有效性。去氨普酶是一种高度纤维蛋白特异性且无神经毒性的溶栓药物,在缺血性脑卒中发病3至9小时内,对MRI显示灌注/扩散不匹配的患者给药。
方法
DIAS是一项安慰剂对照、双盲、随机、剂量探索性II期试验。符合条件的患者为美国国立卫生研究院卒中量表(NIHSS)评分4至20分且MRI有灌注/扩散不匹配证据者。在104例患者中,前47例(称为第1部分)被随机分配至去氨普酶固定剂量组(25mg、37.5mg或50mg)或安慰剂组。由于症状性颅内出血(sICH)发生率过高,随后在57例患者(称为第2部分)中研究了通过62.5μg/kg、90μg/kg和125μg/kg递增的较低体重调整剂量。安全性终点是sICH发生率。疗效终点是4至8小时后MRI的再灌注率以及90天时通过NIHSS、改良Rankin量表和Barthel指数评估的临床结局。
结果
第1部分因去氨普酶组sICH发生率高(26.7%)而提前终止。在第2部分中,sICH发生率为2.2%。两部分中安慰剂组均未发生sICH。与安慰剂组的19.2%相比,去氨普酶(125μg/kg)组观察到的再灌注率高达71.4%(P = 0.0012)。安慰剂治疗患者中有22.2%在90天时临床结局良好,去氨普酶治疗患者中这一比例在13.3%(62.5μg/kg;P = 0.757)至60.0%(125μg/kg;P = 0.0090)之间。早期再灌注与临床结局呈良好相关性(P = 0.0028)。再灌注患者中有52.5%临床结局良好,未再灌注患者中这一比例为24.6%。
结论
对于经选择有灌注/扩散不匹配的急性缺血性脑卒中患者,在发病3至9小时后静脉注射去氨普酶与安慰剂相比,再灌注率更高,临床结局更好。使用高达125μg/kg的剂量时,去氨普酶的sICH发生率较低。
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