Safety evaluation of a recombinant plasmin derivative lacking kringles 2-5 and rt-PA in a rat model of transient ischemic stroke.

R Christian Crumrine, Victor J Marder, G McLeod Taylor, Joseph C LaManna, Constantinos P Tsipis, Valery Novokhatny, Philip Scuderi, Stephen R Petteway, Vikram Arora
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引用次数: 8

Abstract

Background: Tissue type plasminogen activator is the only approved thrombolytic agent for the treatment of ischemic stroke. However, it carries the disadvantage of a 10-fold increase in symptomatic and asymptomatic intracranial hemorrhage. A safer thrombolytic agent may improve patient prognosis and increase patient participation in thrombolytic treatment. A novel direct-acting thrombolytic agent, Δ(K2-K5) plasmin, promising an improved safety profile was examined for safety in the snare ligature model of stroke in the rat.

Methods: Male spontaneously hypertensive rats were subjected to 6 hours middle cerebral artery occlusion followed by 18 hours reflow. Beginning 1 minute before reflow, they were dosed with saline, vehicle, Δ(K2-K5) plasmin (0.15, 0.5, 1.5, and 5 mg/kg) or recombinant tissue-type plasminogen activator (10 and 30 mg/kg) by local intra-arterial infusion lasting 10 to 60 minutes. The rats were assessed for bleeding score, infarct volume, modified Bederson score and general behavioral score. In a parallel study, temporal progression of infarct volume was determined. In an in vitro study, whole blood clots from humans, canines and rats were exposed to Δ(K2-K5). Clot lysis was monitored by absorbance at 280 nm.

Results: The main focus of this study was intracranial hemorrhage safety. Δ(K2-K5) plasmin treatment at the highest dose caused no more intracranial hemorrhage than the lowest dose of recombinant tissue type plasminogen activator, but showed at least a 5-fold superior safety margin. Secondary results include: temporal infarct volume progression shows that the greatest expansion of infarct volume occurs within 2-3 hours of middle cerebral artery occlusion in the spontaneously hypertensive rat. A spike in infarct volume was observed at 6 hours ischemia with reflow. Δ(K2-K5) plasmin tended to reduce infarct volume and improve behavior compared to controls. In vitro data suggests that Δ(K2-K5) plasmin is equally effective at lysing clots from humans, canines and rats.

Conclusions: The superior intracranial hemorrhage safety profile of the direct-acting thrombolytic Δ(K2-K5) plasmin compared with recombinant tissue type plasminogen activator makes this agent a good candidate for clinical evaluation in the treatment of acute ischemic stroke.

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缺乏kringles 2-5和rt-PA的重组纤溶蛋白衍生物在大鼠短暂性缺血性脑卒中模型中的安全性评价。
背景:组织型纤溶酶原激活剂是唯一被批准用于缺血性脑卒中治疗的溶栓药物。然而,它的缺点是有症状和无症状的颅内出血增加10倍。一种更安全的溶栓药物可以改善患者预后,增加患者对溶栓治疗的参与。一种新型的直接作用溶栓剂Δ(K2-K5)纤溶酶在大鼠脑卒中陷阱结扎模型中的安全性得到了提高。方法:雄性自发性高血压大鼠大脑中动脉闭塞6 h,再灌注18 h。从再流前1分钟开始,通过局部动脉内输注生理盐水、载药、Δ(K2-K5)纤溶酶(0.15、0.5、1.5和5mg /kg)或重组组织型纤溶酶原激活剂(10和30mg /kg),持续10至60分钟。对大鼠进行出血评分、梗死体积、改良Bederson评分和一般行为评分。在一项平行研究中,确定了梗死体积的时间进展。在一项体外研究中,将人、犬和大鼠的全血凝块暴露于Δ(K2-K5)。用280 nm吸光度监测凝块溶解。结果:本研究的重点是颅内出血的安全性。Δ(K2-K5)最高剂量的纤溶酶治疗并不比最低剂量的重组组织型纤溶酶原激活剂引起更多的颅内出血,但显示出至少5倍的安全范围。继发结果包括:颞叶梗死体积进展显示,自发性高血压大鼠大脑中动脉闭塞后2-3小时内梗死体积扩张最大。缺血6小时伴血流时,梗死体积出现尖峰。与对照组相比,Δ(K2-K5)纤溶酶倾向于减少梗死面积和改善行为。体外数据表明Δ(K2-K5)纤溶蛋白对人、犬和大鼠的凝块同样有效。结论:与重组组织型纤溶酶原激活剂相比,直接溶栓Δ(K2-K5)型纤溶酶原激活剂具有更好的颅内出血安全性,是临床评价急性缺血性脑卒中治疗的良好候选药物。
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