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CcMP-II,一种来自角蝰蛇毒的新型出血性金属蛋白酶:纯化、生化特性及氨基酸序列分析。

CcMP-II, a new hemorrhagic metalloproteinase from Cerastes cerastes snake venom: purification, biochemical characterization and amino acid sequence analysis.

作者信息

Boukhalfa-Abib Hinda, Laraba-Djebari Fatima

机构信息

USTHB, Faculty of Biological Sciences, Laboratory of Cellular and Molecular Biology, BP 32, El-Alia Bab Ezzouar, 16111 Algiers, Algeria.

USTHB, Faculty of Biological Sciences, Laboratory of Cellular and Molecular Biology, BP 32, El-Alia Bab Ezzouar, 16111 Algiers, Algeria.

出版信息

Comp Biochem Physiol C Toxicol Pharmacol. 2015 Jan;167:65-73. doi: 10.1016/j.cbpc.2014.09.004. Epub 2014 Sep 22.

DOI:10.1016/j.cbpc.2014.09.004
PMID:25251459
Abstract

Snake venom metalloproteinases (SVMPs) are the most abundant components in snake venoms. They are important in the induction of systemic alterations and local tissue damage after envenomation. CcMP-II, which is a metalloproteinase purified from Cerastes cerastes snake venom, was obtained by a combination of gel filtration, ion-exchange and affinity chromatographies. It was homogeneous on SDS-PAGE, with a molecular mass estimated to 35kDa and presents a pI of 5.6. CcMP-II has an N-terminal sequence of EDRHINLVSVADHRMXTKY, with high levels of homology with those of the members of class P-II of SVMPs, which comprises metalloproteinase and disintegrin-like domains together. This proteinase displayed a fibrinogenolytic and hemorrhagic activities. The proteolytic and hemorrhagic activities of CcMP-II were inhibited by EDTA and 1,10-phenanthroline. However, these activities were not affected by aprotinine and PMSF, suggesting that CcMP-II is a zinc-dependent hemorrhagic metalloproteinase with an α-fibrinogenase activity. The hemorrhagic metalloproteinase CcMP-II was also able to hydrolyze extracellular matrix components, such as type IV collagen and laminin. These results indicate that CcMP-II is implicated in the local and systemic bleeding, contributing thus in the toxicity of C. cerastes venom.

摘要

蛇毒金属蛋白酶(SVMPs)是蛇毒中含量最丰富的成分。它们在蛇毒中毒后引起全身改变和局部组织损伤方面起着重要作用。CcMP-II是一种从角蝰蛇蛇毒中纯化得到的金属蛋白酶,通过凝胶过滤、离子交换和亲和色谱相结合的方法获得。它在SDS-PAGE上呈均一性,估计分子量为35kDa,pI为5.6。CcMP-II的N端序列为EDRHINLVSVADHRMXTKY,与SVMPs的P-II类成员具有高度同源性,该类成员同时包含金属蛋白酶结构域和去整合素样结构域。这种蛋白酶具有纤维蛋白原溶解和出血活性。CcMP-II的蛋白水解和出血活性受到EDTA和1,10-菲啰啉的抑制。然而,这些活性不受抑肽酶和苯甲基磺酰氟的影响,这表明CcMP-II是一种具有α-纤维蛋白原酶活性的锌依赖性出血性金属蛋白酶。出血性金属蛋白酶CcMP-II还能够水解细胞外基质成分,如IV型胶原和层粘连蛋白。这些结果表明,CcMP-II与局部和全身出血有关,因此对角蝰蛇毒的毒性有贡献。

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