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从矛头蝮蛇血浆中提取的磷脂酶A2肌毒素抑制剂的生化特性及药理性质

Biochemical characterization and pharmacological properties of a phospholipase A2 myotoxin inhibitor from the plasma of the snake Bothrops asper.

作者信息

Lizano S, Lomonte B, Fox J W, Gutiérrez J M

机构信息

Instituto Clodomiro Picado, Facultad de Microbiología, Universidad de Costa Rica, San José, Costa Rica.

出版信息

Biochem J. 1997 Sep 15;326 ( Pt 3)(Pt 3):853-9. doi: 10.1042/bj3260853.

Abstract

A protein that neutralizes the biological activities of basic phospholipase A2 (PLA2) myotoxin isoforms from the venom of the snake Bothrops asper was isolated from its blood by affinity chromatography with Sepharose-immobilized myotoxins. Biochemical characterization of this B. asper myotoxin inhibitor protein (BaMIP) indicated a subunit molecular mass of 23-25 kDa, an isoelectric point of 4, and glycosylation. Gel-filtration studies revealed a molecular mass of 120 kDa, suggesting that BaMIP possesses an oligomeric structure composed of five 23-25 kDa subunits. Functional studies indicated that BaMIP inhibits the PLA2 activity of B. asper basic myotoxins I and III, as well as the myotoxicity and edema-forming activity in vivo and cytolytic activity in vitro towards cultured endothelial cells, of all four myotoxin isoforms (I-IV) tested. Sequence analysis of the first 63 amino acid residues from the N-terminus of BaMIP indicated more than 65% sequence similarity to the PLA2 inhibitors isolated from the blood of the crotalid snakes Trimeresurus flavoviridis and Agkistrodon blomhoffii siniticus. These inhibitors also share sequences similar to the carbohydrate-recognition domains of human and rabbit cellular PLA2 receptors, suggesting a common domain evolution among snake plasma PLA2 inhibitors and mammalian PLA2 receptors. Despite this similarity, this is the first description of a natural anti-myotoxic factor from snake blood.

摘要

通过用固定在琼脂糖上的肌毒素进行亲和层析,从蛇(矛头蝮)的血液中分离出一种能中和来自其毒液的碱性磷脂酶A2(PLA2)肌毒素亚型生物活性的蛋白质。对这种矛头蝮肌毒素抑制蛋白(BaMIP)的生化特性分析表明,其亚基分子量为23 - 25 kDa,等电点为4,且存在糖基化。凝胶过滤研究显示其分子量为120 kDa,这表明BaMIP具有由五个23 - 25 kDa亚基组成的寡聚结构。功能研究表明,BaMIP能抑制矛头蝮碱性肌毒素I和III的PLA2活性,以及所有四种测试的肌毒素亚型(I - IV)在体内的肌毒性和形成水肿的活性,以及在体外对培养的内皮细胞的细胞溶解活性。对BaMIP N端前63个氨基酸残基的序列分析表明,它与从竹叶青蛇和日本蝮蛇血液中分离出的PLA2抑制剂有超过65%的序列相似性。这些抑制剂还与人和兔细胞PLA2受体的碳水化合物识别结构域有相似序列,这表明蛇血浆PLA2抑制剂和哺乳动物PLA2受体之间存在共同的结构域进化。尽管有这种相似性,但这是首次对来自蛇血的天然抗肌毒素因子进行描述。

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