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Proteomic characterization of the hyaluronidase (e.c. 3.2.1.35) from the venom of the social wasp polybia paulista

机译:透明质酸酶的蛋白质组学表征(例如,3.2.1.35)来自社会性黄蜂多发性保罗鲍利斯塔毒液

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Polybia paulista wasp venom possesses three major allergens: phospholipase A1, hyaluronidase and antigen-5. To the best of our knowledge, no hyaluronidase from the venom of Neotropical social wasps was structurally characterized up to this moment, mainly due to its reduced amount in the venom of the tropical wasp species (about 0.5% of crude venom). Four different glycoproteic forms of this enzyme were detected in the venom of the wasp Polybia paulista. In the present investigation, an innovative experimental approach was developed combining 2-D SDS-PAGE with in-gel protein digestion by different proteolytic enzymes, followed by mass spectrometry analysis under collision-induced dissociation CID) conditions for the complete assignment of the protein sequencing. Thus, the most abundant form of this enzyme in P. paulista venom, the hyaluronidase-III, was sequenced, revealing that the first 47 amino acid residues from the N-terminal region, common to other Hymenoptera venom hyaluronidases, are missing. The molecular modeling revealed that hyaluronidase-III has a single polypeptide chain, folded into a tertiary structure, presenting a central (β/α)5 core with alternation of β-strands and α-helices; the tertiary structure stabilized by a single disulfide bridge between the residues Cys189 and Cys201. The structural pattern reported for P. paulista venom hyaluronidase-III is compatible with the classification of the enzyme as member of the family 56 of glycosidase hydrolases. Moreover, its structural characterization will encourage the use of this protein as a model for future development of component-resolved diagnosis'.
机译:bia虫黄蜂毒液具有三种主要的过敏原:磷脂酶A1,透明质酸酶和抗原5。据我们所知,到目前为止,尚没有新热带社会黄蜂毒液中的透明质酸酶的结构特征,这主要是由于其在热带黄蜂物种毒液中的含量减少了(约占粗毒液的0.5%)。在黄蜂Polybia paulista的毒液中检测到该酶的四种不同糖蛋白形式。在本研究中,开发了一种创新的实验方法,该方法将2-D SDS-PAGE与通过不同蛋白水解酶进行的凝胶内蛋白质消化相结合,然后在碰撞诱导的解离CID)条件下进行质谱分析,以完成蛋白质序列的完全分配。因此,测序了该酶在P. paulista毒液中最丰富的形式,透明质酸酶-III,揭示了与其他膜翅目毒液透明质酸酶相同的,来自N-末端区域的前47个氨基酸残基缺失。分子模型表明,透明质酸酶III具有一条折叠成三级结构的多肽链,呈中心(β/α)5核,且β链和α螺旋交替排列。三级结构由残基Cys189和Cys201之间的单个二硫键稳定。报导的保罗·波利斯塔毒液透明质酸酶-III的结构模式与该酶作为糖苷酶水解酶家族56的成员的分类兼容。而且,它的结构特征将鼓励使用这种蛋白质作为将来进行组分分辨诊断的模型。

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