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Polymer Multilayers Loaded with Antifungal β-Peptides Kill Planktonic Candida albicans and Reduce Formation of Fungal Biofilms on the Surfaces of Flexible Catheter Tubes

机译:载有抗真菌β肽的聚合物多层膜可杀死浮游性念珠菌白色念珠菌并减少在柔性导管表面上真菌生物膜的形成。

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摘要

Candida albicans is the most common fungal pathogen responsible for hospital-acquired infections. Most C albicans infections are associated with the implantation of medical devices that act as points of entry for the pathogen and as substrates for the growth of fungal biofilms that are notoriously difficult to eliminate by systemic administration of conventional antifungal agents. In this study, we report a fill-and-purge approach to the layer-by-layer fabrication of biocompatible, nanoscale ‘polyelectrolyte multilayers’ (PEMs) on the luminal surfaces of flexible catheters, and an investigation of this platform for the localized, intraluminal release of a cationic β-peptide-based antifungal agent. We demonstrate that polyethylene catheter tubes with luminal surfaces coated with multilayers ~700 nm thick fabricated from poly-L-glutamic acid (PGA) and poly-L-lysine (PLL) can be loaded, post-fabrication, by infusion with β-peptide, and that this approach promotes extended intraluminal release of this agent (over ~4 months) when incubated in physiological media. The β-peptide remained potent against intraluminal inoculation of the catheters with C albicans and substantially reduced the formation of C albicans biofilms on the inner surfaces of film-coated catheters. Finally, we report that these β-peptide-loaded coatings exhibit antifungal activity under conditions that simulate intermittent catheter use and microbial challenge for at least three weeks. We conclude that β-peptide-loaded PEMs offer a novel and promising approach to kill C albicans and prevent fungal biofilm formation on surfaces, with the potential to substantially reduce the incidence of device-associated infections in indwelling catheters. β-Peptides comprise a promising new class of antifungal agents that could help address problems associated with the use of conventional antifungal agents. The versatility of the layer-by-layer approach used here thus suggests additional opportunities to exploit these new agents in other biomedical and personal care applications in which fungal infections are endemic.
机译:白色念珠菌是导致医院获得性感染的最常见真菌病原体。大多数白色念珠菌感染与植入医疗器械有关,这些医疗器械是病原体的进入点,并且是真菌生物膜生长的基质,而众所周知,这些真菌生物膜很难通过全身施用常规抗真菌剂来消除。在这项研究中,我们报告了一种在柔性导管腔表面上逐层制造生物相容性纳米级“聚电解质多层”(PEM)的填充和吹扫方法,并对该平台的局部化,阳离子β-肽类抗真菌剂的腔内释放。我们证明,可通过加载β肽,在制造后加载带有聚L-谷氨酸(PGA)和聚L-赖氨酸(PLL)制成的多层表面约700 nm厚的聚乙烯表面的聚乙烯导管。 ,并且这种方法可在生理介质中孵育时促进该药的腔内释放(约4个月以上)。 β-肽仍然有效抵抗用白念珠菌对管腔内接种,并且大大减少了在薄膜包衣的导管的内表面上白念珠菌生物膜的形成。最后,我们报道了在模拟间歇性使用导管和微生物攻击至少三周的条件下,这些装有β肽的涂层具有抗真菌活性。我们得出的结论是,装载β肽的PEM提供了一种新颖而有前途的方法,可以杀死白色念珠菌并防止在表面形成真菌生物膜,并有可能大大减少留置导管中与设备相关的感染的发生率。 β-肽包含一类有希望的新型抗真菌剂,可以帮助解决与使用常规抗真菌剂相关的问题。因此,此处使用的逐层方法的多功能性为在真菌感染为流行的其他生物医学和个人护理应用中开发这些新试剂提供了更多机会。

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