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纤溶酶溶栓:对卒中治疗的影响。

Thrombolysis with plasmin: implications for stroke treatment.

机构信息

Division of Hematology-Oncology, David Geffen School of Medicine at University of California Los Angeles, Room A3-29 Rehabilitation Building, 1000 Veteran Ave, Los Angeles, CA 90095, USA.

出版信息

Stroke. 2010 Oct;41(10 Suppl):S45-9. doi: 10.1161/STROKEAHA.110.595157.

Abstract

Plasmin is a direct-acting thrombolytic agent with a striking hemostatic safety advantage over plasminogen activators in animal models of thrombolysis and bleeding. In contradistinction to plasminogen activators, which risk bleeding at any effective thrombolytic dose, plasmin is tolerated without bleeding at several-fold higher amounts than those needed for thrombolysis. Plasmin has been safe in a current trial in patients with peripheral arterial or graft occlusion, and efforts are now directed toward therapy of stroke caused by cerebral artery occlusion. A rabbit (4 kg body weight) model of 2-hour, thrombin-induced middle cerebral artery occlusion using angiographic documentation of vascular patency and recanalization was used to perform a dose-ranging study of plasmin, delivered by catheter over a median duration of 10 minutes. Plasmin induced early recanalization in all animals (3 per group) within 10 minutes after discontinuation of 3, 2, or 1 mg of agent infusion. Control saline infusion failed to induce recanalization in 3 of 3 subjects. Plasmin rapidly induces middle cerebral artery recanalization, as determined in an angiogram-based animal model of arterial occlusion. Based on these data and other information, a phase I/IIa clinical trial of plasmin in human middle cerebral artery ischemic stroke has been initiated.

摘要

纤溶酶是一种直接作用的溶栓剂,与溶栓和出血动物模型中的纤溶酶原激活剂相比,具有显著的止血安全性优势。与有出血风险的纤溶酶原激活剂不同,纤溶酶在几倍于溶栓所需的剂量下也不会引起出血。纤溶酶在目前一项外周动脉或移植物闭塞患者的临床试验中是安全的,目前正在努力治疗由大脑动脉闭塞引起的中风。使用血管通畅性和再通的血管造影记录,在使用凝血酶诱导 2 小时的兔(4 公斤体重)大脑中动脉闭塞模型中,进行了纤溶酶剂量范围研究,通过导管在中位数 10 分钟内输注。纤溶酶在停止输注 3、2 或 1 mg 药物后 10 分钟内,所有动物(每组 3 只)均引起早期再通。在 3 名受试者中的 3 名中,生理盐水输注未能引起再通。纤溶酶在基于血管造影的动脉闭塞动物模型中迅速诱导大脑中动脉再通。基于这些数据和其他信息,已经启动了纤溶酶治疗人类大脑中动脉缺血性中风的 I/IIa 期临床试验。

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