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从哥伦比亚矛头蝮蛇毒液中分离和生物学特性鉴定 Batx-I,一种弱出血和纤维蛋白原降解的 PI 金属蛋白酶。

Isolation and biological characterization of Batx-I, a weak hemorrhagic and fibrinogenolytic PI metalloproteinase from Colombian Bothrops atrox venom.

机构信息

Programa de Ofidismo/Escorpionismo, Universidad de Antioquia, Medellín 1226, Colombia.

出版信息

Toxicon. 2010 Nov;56(6):936-43. doi: 10.1016/j.toxicon.2010.06.016. Epub 2010 Jun 30.

DOI:10.1016/j.toxicon.2010.06.016
PMID:20600221
Abstract

A hemorrhagic metalloproteinase, named Batx-I, was isolated from the venom of Bothrops atrox specimens (from Southeastern Colombian region) by a combination of CM-Sephadex C25 ion-exchange and Affi-gel Blue affinity chromatographies. This enzyme accounts for about 45% of venom proteins, and it has an ESI-MS isotope-averaged molecular mass of 23296.2 Da and a blocked N-terminus. Two internal fragments sequenced by mass spectrometric analysis showed similarity to other SVMPs from Bothrops venoms. To investigate the possible participation of Batx-I in the envenomation pathophysiology, proteolytic, fibrinogenolytic, hemorrhagic, and other biological activities were evaluated. The minimal hemorrhagic dose obtained was 17 microg/20 g body weight. The enzyme showed proteolytic activity on azocasein, comparable with activity of BaP1. This activity was inhibited by EDTA and 1, 10 o-phenanthroline but not by aprotinin, pepstatin A or PMSF. Fibrinogenolytic activity was analyzed by SDS-PAGE, revealing a preference for degrading the A alpha- and B beta-chains, although partial degradation of the gamma-chain was also detected. The protein lacks coagulant and defibrinating activity. The CK levels obtained, clearly reflects a myotoxic activity induced by Batx-I. The hemorrhagic and fibrinogenolytic activities exhibited by the isolated PI-SVMP may play a role in the hemorrhagic and blood-clotting disorders observed in patients bitten by B. atrox in Colombia.

摘要

一种名为 Batx-I 的出血性金属蛋白酶,是通过 CM-Sephadex C25 离子交换和 Affi-gel Blue 亲和层析的组合,从矛头蝮属(来自哥伦比亚东南部地区)的毒液中分离出来的。这种酶约占毒液蛋白的 45%,其 ESI-MS 同位素平均分子量为 23296.2 Da,N 端封闭。通过质谱分析测序的两个内部片段显示与其他来自矛头蝮属毒液的 SVMP 具有相似性。为了研究 Batx-I 可能在蛇毒中毒理生理学中的参与,评估了其蛋白水解、纤维蛋白原水解、出血和其他生物学活性。获得的最小出血剂量为 17 μg/20 g 体重。该酶对偶氮酪蛋白具有蛋白水解活性,与 BaP1 的活性相当。这种活性被 EDTA 和 1,10 邻菲啰啉抑制,但不被抑肽酶、胃蛋白酶抑制剂 A 或 PMSF 抑制。纤维蛋白原水解活性通过 SDS-PAGE 进行分析,显示出优先降解 Aα-和 Bβ-链的趋势,尽管也检测到 γ-链的部分降解。该蛋白缺乏凝血和纤溶活性。获得的 CK 水平清楚地反映了 Batx-I 诱导的肌毒性活性。分离的 PI-SVMP 表现出的出血和纤维蛋白原水解活性可能在哥伦比亚被矛头蝮属咬伤的患者中观察到的出血和凝血障碍中发挥作用。

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