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Bottom-Up Proteomic Analysis of Polypeptide Venom Components of the Giant Ant Dinoponera Quadriceps

机译:巨型蚁迪多尼亚血管曲肌肌血管基团的自下而上蛋白质组学分析

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摘要

Ant species have specialized venom systems developed to sting and inoculate a biological cocktail of organic compounds, including peptide and polypeptide toxins, for the purpose of predation and defense. The genus Dinoponera comprises predatory giant ants that inoculate venom capable of causing long-lasting local pain, involuntary shaking, lymphadenopathy, and cardiac arrhythmias, among other symptoms. To deepen our knowledge about venom composition with regard to protein toxins and their roles in the chemical−ecological relationship and human health, we performed a bottom-up proteomics analysis of the crude venom of the giant ant D. quadriceps, popularly known as the “false” tocandiras. For this purpose, we used two different analytical approaches: (i) gel-based proteomics approach, wherein the crude venom was resolved by denaturing sodium dodecyl sulfate-polyacrylamide gel electrophoresis (SDS-PAGE) and all protein bands were excised for analysis; (ii) solution-based proteomics approach, wherein the crude venom protein components were directly fragmented into tryptic peptides in solution for analysis. The proteomic data that resulted from these two methodologies were compared against a previously annotated transcriptomic database of D. quadriceps, and subsequently, a homology search was performed for all identified transcript products. The gel-based proteomics approach unequivocally identified nine toxins of high molecular mass in the venom, as for example, enzymes [hyaluronidase, phospholipase A1, dipeptidyl peptidase and glucose dehydrogenase/flavin adenine dinucleotide (FAD) quinone] and diverse venom allergens (homologous of the red fire ant Selenopsis invicta) and venom-related proteins (major royal jelly-like). Moreover, the solution-based proteomics revealed and confirmed the presence of several hydrolases, oxidoreductases, proteases, Kunitz-like polypeptides, and the less abundant inhibitor cysteine knot (ICK)-like (knottin) neurotoxins and insect defensin. Our results showed that the major components of the D. quadriceps venom are toxins that are highly likely to damage cell membranes and tissue, to cause neurotoxicity, and to induce allergic reactions, thus, expanding the knowledge about D. quadriceps venom composition and its potential biological effects on prey and victims.
机译:对于捕食和防御,蚂蚁物种具有开发的特殊毒液系统,以刺入并接种有机化合物的生物鸡尾酒,包括肽和多肽毒素。 Dinoponera属包括捕食性巨型蚂蚁,其接种能够引起持久的局部疼痛,非自愿摇晃,淋巴结病和心脏心律失常以及其他症状的毒液。要深化对毒液成分知识方面的蛋白毒素及其在化学生态关系和人类健康的作用,我们进行了巨大的D.蚂蚁股四头肌粗毒液的自下而上的蛋白质组学分析,俗称为“假“tocandiras。为此目的,我们使用了两种不同的分析方法:(i)基于凝胶的蛋白质组学方法,其中通过使十二烷基硫酸钠 - 聚丙烯酰胺凝胶电泳(SDS-PAGE)解析粗毒液,并且切除所有蛋白质条带进行分析; (ii)基于溶液的蛋白质组学方法,其中将粗毒液蛋白组分直接分割成溶液中的胰蛋白酶肽以进行分析。将由这两种方法产生的蛋白质组学数据与先前注释的D. Quaddriceps的转录组数据库进行比较,随后对所有已识别的转录产品进行了同源性搜索。基于凝胶的蛋白质组学方法明确地鉴定了毒液中的高分子质量的九种毒素,例如酶[透明质酸酶,磷脂酶A1,二肽基肽酶和葡萄糖脱氢酶/黄酮腺嘌呤二核苷酸(FAD)醌]和不同的血液过敏原(同源红火蚂蚁selenopsis Invicta)和毒液相关的蛋白质(主要的皇家果冻状)。此外,基于溶液的蛋白质组学显示并证实了几种水解酶,氧化酶,蛋白酶,Kunitz样多肽的存在,以及较少丰富的抑制剂半胱氨酸结(ICK) - 样(knottin)神经毒素和昆虫防御素。我们的研究结果表明,D. Quadriceps毒液的主要组成部分是毒素,其高可能损害细胞膜和组织,导致神经毒性,并诱导过敏反应,从而扩大D. Quadriceps毒液组成的知识及其潜力对猎物和受害者的生物效应。

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