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正在研发的溶栓剂。

Thrombolytic agents in development.

作者信息

Verstraete M, Lijnen H R, Collen D

机构信息

Center for Molecular and Vascular Biology, University of Leuven, Belgium.

出版信息

Drugs. 1995 Jul;50(1):29-42. doi: 10.2165/00003495-199550010-00003.

Abstract

The quest continues for thrombolytic agents with a higher thrombolytic potency, specific thrombolytic activity and/or a better fibrin selectivity. Several lines of research towards improvement of thrombolytic agents are being explored, including the construction of mutants and variants of plasminogen activators (PAs), chimaeric PAs, conjugates of PAs with monoclonal antibodies, and PAs from animal or bacterial origin. Some of these new thrombolytic agents have shown promise in animal models of venous or arterial thrombosis and in pilot clinical studies. Such molecules include numerous mutants of tissue-type PA (t-PA) with prolonged in vivo half-life and/or resistance to protease inhibitors, and chimaeric PAs consisting of different regions of t-PA and of urokinase-type PA (u-PA). Several molecular forms of the thrombolytic substance in the saliva of the vampire bat have been characterised and cloned. Vampire bat PA exhibits 85% homology to human t-PA but lacks kringle 2 and the plasmin-sensitive cleavage site. A thrombolytic enzyme of 203 amino acids is present in the venom of a southern copperhead snake. This polypeptide, termed fibrolase, is now produced by recombinant technology. Fibrolase does not activate plasminogen or protein C, but directly degrades the alpha and beta chains of fibrin and fibrinogen. Recombinant staphylokinase is not an enzyme, but it forms a 1:1 stoichiometric complex with plasminogen, which becomes active after conversion of plasminogen to plasmin. It is a potent and highly fibrin specific thrombolytic agent in animals and patients.

摘要

人们仍在寻找具有更高溶栓效力、特异性溶栓活性和/或更好纤维蛋白选择性的溶栓剂。目前正在探索多条改进溶栓剂的研究路线,包括构建纤溶酶原激活剂(PAs)的突变体和变体、嵌合型PAs、PAs与单克隆抗体的偶联物以及来自动物或细菌来源的PAs。其中一些新型溶栓剂在静脉或动脉血栓形成的动物模型以及初步临床研究中已显示出前景。这类分子包括许多体内半衰期延长和/或对蛋白酶抑制剂具有抗性的组织型PA(t-PA)突变体,以及由t-PA和尿激酶型PA(u-PA)的不同区域组成的嵌合型PAs。吸血蝙蝠唾液中的溶栓物质的几种分子形式已得到表征和克隆。吸血蝙蝠PA与人类t-PA具有85%的同源性,但缺乏kringle 2和纤溶酶敏感的切割位点。一种南方铜头蛇的毒液中存在一种由203个氨基酸组成的溶栓酶。这种多肽被称为纤维酶,现在通过重组技术生产。纤维酶不激活纤溶酶原或蛋白C,但直接降解纤维蛋白和纤维蛋白原的α链和β链。重组葡萄球菌激酶不是一种酶,但它与纤溶酶原形成1:1化学计量比的复合物,在纤溶酶原转化为纤溶酶后变得有活性。它在动物和患者中是一种强效且高度纤维蛋白特异性的溶栓剂。

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