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来自巴西游走蛛毒液的一种类虾红素金属蛋白酶毒素的鉴定、克隆、表达及功能特性分析

Identification, cloning, expression and functional characterization of an astacin-like metalloprotease toxin from Loxosceles intermedia (brown spider) venom.

作者信息

da Silveira Rafael B, Wille Ana C M, Chaim Olga M, Appel Marcia H, Silva Dilza T, Franco Célia R C, Toma Leny, Mangili Oldemir C, Gremski Waldemiro, Dietrich Carl P, Nader Helena B, Veiga Silvio S

机构信息

Department of Biochemistry, Federal University of São Paulo, Rua 3 de maio, 100 5 andar, São Paulo, Brazil.

出版信息

Biochem J. 2007 Sep 1;406(2):355-63. doi: 10.1042/BJ20070363.

Abstract

Injuries caused by brown spiders (Loxosceles genus) are associated with dermonecrotic lesions with gravitational spreading and systemic manifestations. The venom has a complex composition containing many different toxins, of which metalloproteases have been described in many different species of this genus. These toxins may degrade extracellular matrix constituents acting as a spreading factor. By using a cDNA library from an Loxosceles intermedia venom gland, we cloned and expressed a 900 bp cDNA, which encoded a signal peptide and a propeptide, which corresponded to a 30 kDa metalloprotease, now named LALP (Loxosceles astacin-like protease). Recombinant LALP was refolded and used to produce a polyclonal antiserum, which showed cross-reactivity with a 29 kDa native venom protein. CD analysis provided evidence that the recombinant LALP toxin was folded correctly, was still in a native conformation and had not aggregated. LALP addition to endothelial cell cultures resulted in de-adhesion of the cells, and also in the degradation of fibronectin and fibrinogen (this could be inhibited by the presence of the bivalent chelator 1,10-phenanthroline) and of gelatin in vitro. Sequence comparison (nucleotide and deduced amino acid), phylogenetic analysis and analysis of the functional recombinant toxin revealed that LALP is related in both structure and function to the astacin family of metalloproteases. This suggests that an astacin-like toxin is present in a animal venom secretion and indicates that recombinant LALP will be a useful tool for future structural and functional studies on venom and the astacin family.

摘要

棕色蜘蛛(洛氏蛛属)造成的损伤与具有重力扩散和全身表现的皮肤坏死性病变有关。其毒液成分复杂,含有许多不同毒素,其中金属蛋白酶已在该属的许多不同物种中被描述。这些毒素可能降解细胞外基质成分,起到扩散因子的作用。通过使用中间洛氏蛛毒液腺的cDNA文库,我们克隆并表达了一个900 bp的cDNA,它编码一个信号肽和一个前肽,对应于一种30 kDa的金属蛋白酶,现命名为LALP(洛氏蛛类虾红素样蛋白酶)。重组LALP被复性并用于制备多克隆抗血清,该抗血清与一种29 kDa的天然毒液蛋白显示出交叉反应性。圆二色性分析提供了证据,表明重组LALP毒素折叠正确,仍处于天然构象且未聚集。将LALP添加到内皮细胞培养物中导致细胞脱黏附,并且在体外还导致纤连蛋白、纤维蛋白原(这可被二价螯合剂1,10 - 菲咯啉的存在所抑制)和明胶的降解。序列比较(核苷酸和推导的氨基酸)、系统发育分析以及对功能性重组毒素的分析表明,LALP在结构和功能上与金属蛋白酶的虾红素家族相关。这表明一种类虾红素毒素存在于动物毒液分泌中,并表明重组LALP将成为未来对毒液和虾红素家族进行结构和功能研究的有用工具。

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