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Snake Venom Metalloproteinases and Their Peptide Inhibitors from Myanmar Russell’s Viper Venom

机译:来自缅甸罗素毒蛇毒液的蛇毒金属蛋白酶及其肽抑制剂

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Russell’s viper bites are potentially fatal from severe bleeding, renal failure and capillary leakage. Snake venom metalloproteinases (SVMPs) are attributed to these effects. In addition to specific antivenom therapy, endogenous inhibitors from snakes are of interest in studies of new treatment modalities for neutralization of the effect of toxins. Two major snake venom metalloproteinases (SVMPs): RVV-X and Daborhagin were purified from Myanmar Russell’s viper venom using a new purification strategy. Using the Next Generation Sequencing (NGS) approach to explore the Myanmar RV venom gland transcriptome, mRNAs of novel tripeptide SVMP inhibitors (SVMPIs) were discovered. Two novel endogenous tripeptides, pERW and pEKW were identified and isolated from the crude venom. Both purified SVMPs showed caseinolytic activity. Additionally, RVV-X displayed specific proteolytic activity towards gelatin and Daborhagin showed potent fibrinogenolytic activity. These activities were inhibited by metal chelators. Notably, the synthetic peptide inhibitors, pERW and pEKW, completely inhibit the gelatinolytic and fibrinogenolytic activities of respective SVMPs at 5 mM concentration. These complete inhibitory effects suggest that these tripeptides deserve further study for development of a therapeutic candidate for Russell’s viper envenomation.
机译:罗素的毒蛇咬伤可能会因严重出血,肾衰竭和毛细血管渗漏而致命。蛇毒金属蛋白酶(SVMP)归因于这些作用。除特定的抗蛇毒疗法外,来自蛇的内源性抑制剂在中和毒素作用的新治疗方式的研究中也很受关注。使用一种新的纯化策略,从缅甸罗素的毒蛇毒液中纯化了两种主要的蛇毒金属蛋白酶(SVMP):RVV-X和Daborhagin。使用下一代测序(NGS)方法探索缅甸RV毒液腺转录组,发现了新型三肽SVMP抑制剂(SVMPIs)的mRNA。鉴定了两种新的内源三肽,pERW和pEKW,并从粗毒液中分离出来。两种纯化的SVMP均显示酪蛋白分解活性。此外,RVV-X对明胶显示出特定的蛋白水解活性,而达博拉金(Daborhagin)显示出有效的纤维蛋白原分解活性。这些活性被金属螯合剂抑制。值得注意的是,合成肽抑制剂pERW和pEKW在5 mM的浓度下完全抑制了相应SVMP的明胶分解和纤维蛋白原分解活性。这些完全的抑制作用表明,这些三肽值得进一步研究,以开发出用于治疗罗素毒蛇毒的候选药物。

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