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从台湾眼镜蛇蛇毒中分离出的纤维蛋白原水解蛋白酶:具有激肽释放酶样和血管紧张素降解活性的丝氨酸蛋白酶。

Fibrinogenolytic proteases isolated from the snake venom of Taiwan habu: serine proteases with kallikrein-like and angiotensin-degrading activities.

作者信息

Hung C C, Chiou S H

机构信息

Institute of Biochemical Sciences, College of Science, National Taiwan University, Taipei, Taiwan.

出版信息

Biochem Biophys Res Commun. 2001 Mar 9;281(4):1012-8. doi: 10.1006/bbrc.2001.4452.

Abstract

Two venom proteases with fibrinogenolytic activity were isolated from the venom of Taiwan habu (Trimeresurus mucrosquamatus), one major crotalid snake species in Taiwan. The purified enzymes showed a strong beta-fibrinogenolytic activity, cleaving the beta-chain of fibrinogen molecules specifically. They also showed strong kallikrein-like activity in vitro, releasing bradykinin from kininogen. The purified enzymes did not coagulate human plasma, yet decreasing fibrinogen levels in plasma and prolonging bleeding without formation of fibrin clots, indicating that both proteases have specificities different from thrombin and the thrombin-like proteases of snake venom reported previously. They also exhibit amidase activity against N-benzoyl-Pro-Phe-Arg-p-nitroanilide, which is a specific synthetic substrate for kallikrein-like proteases. Their stability at high temperatures was examined and found to be more stable when compared with ancrod and thrombin. Intravenous injection of either protease was shown to lower blood pressure in experimental rats. Most noteworthy is the observation that the proteases can cleave angiotensin I and release bradykinin from plasma kininogen in vitro, which is a strong vasodilator and probably responsible for the in vivo hypotensive effect of these venom proteases.

摘要

从台湾地区主要的蝰蛇种类——台湾竹叶青蛇(Trimeresurus mucrosquamatus)的毒液中分离出了两种具有纤维蛋白原溶解活性的毒液蛋白酶。纯化后的酶表现出很强的β-纤维蛋白原溶解活性,能特异性地切割纤维蛋白原分子的β链。它们在体外还表现出很强的激肽释放酶样活性,能从激肽原中释放出缓激肽。纯化后的酶不会使人体血浆凝固,但会降低血浆中的纤维蛋白原水平并延长出血时间,且不会形成纤维蛋白凝块,这表明这两种蛋白酶具有与凝血酶以及先前报道的蛇毒类凝血酶不同的特异性。它们还对N-苯甲酰基-L-脯氨酰-L-苯丙氨酰-L-精氨酸对硝基苯胺表现出酰胺酶活性,这是一种激肽释放酶样蛋白酶的特异性合成底物。研究了它们在高温下的稳定性,发现与安克洛酶和凝血酶相比,它们更稳定。给实验大鼠静脉注射任何一种蛋白酶都会导致血压下降。最值得注意的是,这些蛋白酶在体外能切割血管紧张素I并从血浆激肽原中释放出缓激肽,缓激肽是一种强效血管舒张剂,可能是这些毒液蛋白酶在体内产生降压作用的原因。

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