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首页> 外文期刊>Scientific reports. >Conversion of Broad-Spectrum Antimicrobial Peptides into Species-Specific Antimicrobials Capable of Precisely Targeting Pathogenic Bacteria
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Conversion of Broad-Spectrum Antimicrobial Peptides into Species-Specific Antimicrobials Capable of Precisely Targeting Pathogenic Bacteria

机译:将广谱抗菌肽转化为能够精确靶向致病细菌的物种特异性抗微生物

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摘要

Currently, the majority of antibiotics in clinical use have broad activity spectra, killing pathogenic and beneficial microorganisms indiscriminately. The disruption of the ecological balance of normal flora often results in secondary infections or other antibiotic-associated complications. Therefore, targeted antimicrobial therapies capable of specifically eliminating pathogenic bacteria while retaining the protective benefits of a normal microflora would be advantageous. In this study, we successfully constructed a series of Enterococcus faecalis-targeted antimicrobial peptides from wide-spectrum antimicrobial peptide precursors. These peptides are designed based on fusion of the species-specific peptide pheromone cCF10 and modification of the active region of the antimicrobial peptide. The results showed that cCF10-C4 possessed specific antimicrobial activity against E. faecalis and was not active against other types of bacteria tested. The specificity of this hybrid peptide was shown by the absence of antimicrobial effects in the pheromone-substituted derivative. Further studies indicated that cCF10-C4 and its parent peptide C4 exert their activities by damaging cytoplasmic membrane integrity. The present study reveals the application potential of these molecules as "probiotic" antimicrobials for the control of specific bacterial infections, and it also helps to elucidate the design and construction of species-specific antimicrobials with precise targeting specificity.
机译:目前,临床用途的大多数抗生素具有广泛的活性光谱,杀死致病性和有益的微生物难以杀死。正常菌群生态平衡的破坏往往导致继发感染或其他抗生素相关的并发症。因此,靶向抗微生物疗法能够特异性地消除致病细菌,同时保留正常微氯的保护益处是有利的。在这项研究中,我们成功地构建了一系列来自宽谱抗微生物肽前体的肠球菌靶向抗微生物肽。这些肽是基于物种特异性肽信息素CCF10的融合和抗微生物肽的有源区的修饰而设计的。结果表明,CCF10-C4具有针对E.粪便的特异性抗微生物活性,并且对测试的其他类型的细菌没有活跃。通过在信息族酮取代的衍生物中没有抗微生物作用显示该杂化肽的特异性。进一步的研究表明,CCF10-C4及其亲本肽C4通过破坏细胞质膜完整性来施加活性。本研究揭示了这些分子作为控制特异性细菌感染的“益生菌”抗微生物的应用潜力,并且还有助于阐明具有精确靶向特异性的特异性抗微生物的设计和构建。

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