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A Reversible Aptamer Improves Outcome and Safety in Murine Models of Stroke and Hemorrhage

机译:可逆的适体改善了中风和出血的小鼠模型的结果和安全性。

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摘要

Treatment of acute ischemic stroke with intravenous tissue-type plasminogen activator is underutilized partly due to the risk of life-threatening hemorrhage. In response to the clinical need for safer stroke therapy, we explored using an aptamer-based therapeutic strategy to promote cerebral reperfusion in a murine model of ischemic stroke. Aptamers are nucleic acid ligands that bind to their targets with high affinity and specificity, and can be rapidly reversed with an antidote. Here we show that a Factor IXa aptamer administered intravenously after 60 minutes of cerebral ischemia and reperfusion improved neurological function and was associated with reduced thrombin generation and decreased inflammation. Moreover, when the aptamer was administered in the setting of intracranial hemorrhage, treatment with its specific antidote reduced hematoma volume and improved survival. The ability to rapidly reverse a pharmacologic agent that improves neurological function after ischemic stroke should intracranial hemorrhage arise indicates that aptamer–antidote pairs may represent a novel, safer approach to treatment of stroke.
机译:静脉内使用组织型纤溶酶原激活剂治疗急性缺血性中风的方法未得到充分利用,部分原因是存在危及生命的出血风险。为了响应对更安全的中风治疗的临床需求,我们探索了使用基于适体的治疗策略来促进缺血性中风的鼠模型中的脑再灌注。适体是以高亲和力和特异性结合其靶标的核酸配体,并且可以用解毒剂迅速逆转。在这里,我们显示脑缺血和再灌注60分钟后静脉给药的IXa因子适体改善了神经功能,并与凝血酶生成减少和炎症减少有关。此外,当在颅内出血的情况下施用适体时,用其特定解毒剂进行治疗可减少血肿量并提高生存率。如果发生颅内出血,在缺血性中风后迅速逆转改善神经功能的药物的能力表明,适体-解毒剂对可能代表一种新颖,更安全的中风治疗方法。

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