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首页> 外文期刊>Applied and Environmental Microbiology >Synthesis of Trypsin-Resistant Variants of the Listeria-Active Bacteriocin Salivaricin P
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Synthesis of Trypsin-Resistant Variants of the Listeria-Active Bacteriocin Salivaricin P

机译:利斯特氏菌活性细菌唾液素P的抗胰蛋白酶变体的合成

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Two-component salivaricin P-like bacteriocins have demonstrated potential as antimicrobials capable of controlling infections in the gastrointestinal tract (GIT). The anti-Listeria activity of salivaricin P is optimal when the individual peptides Sln1 and Sln2 are added in succession at a 1:1 ratio. However, as degradation by digestive proteases may compromise the functionality of these peptides within the GIT, we investigated the potential to create salivaricin variants with enhanced resistance to the intestinal protease trypsin. A total of 11 variants of the salivaricin P components, in which conservative modifications at the trypsin-specific cleavage sites were explored in order to protect the peptides from trypsin degradation while maintaining their potent antimicrobial activity, were generated. Analysis of these variants revealed that eight were resistant to trypsin digestion while retaining antimicrobial activity. Combining the complementary trypsin-resistant variants Sln1-5 and Sln2-3 resulted in a MIC50 of 300 nM against Listeria monocytogenes, a 3.75-fold reduction in activity compared to the level for wild-type salivaricin P. This study demonstrates the potential of engineering bacteriocin variants which are resistant to specific protease action but which retain significant antimicrobial activity.
机译:两组分唾液霉素P样细菌素已显示出作为能够控制胃肠道(GIT)感染的抗菌剂的潜力。当单独的肽Sln1和Sln2以1:1的比例连续添加时,唾液霉素P的抗李斯特菌活性最佳。但是,由于消化蛋白酶的降解可能会损害GIT内这些肽的功能,因此我们研究了产生唾液酸蛋白变体的潜力,这些变体对肠道蛋白酶胰蛋白酶的抵抗力增强。总共产生了11种唾液霉素P变体,其中探索了胰蛋白酶特异性切割位点的保守修饰,以保护肽免受胰蛋白酶降解,同时保持其有效的抗菌活性。对这些变体的分析表明,八种对胰蛋白酶的消化具有抗性,同时保留了抗菌活性。结合互补的抗胰蛋白酶抗性变体Sln1-5和Sln2-3,针对单核细胞增生性李斯特菌的MIC50为300 nM,与野生型唾液素P的水平相比,活性降低3.75倍。这项研究证明了工程改造的潜力对特定蛋白酶作用具有抗性但仍保留显着的抗菌活性的细菌素变体。

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