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Antimicrobial decapeptide KSL-W attenuates Candida albicans virulence by modulating its effects on Toll-like receptor, human β-defensin, and cytokine expression by engineered human oral mucosa

机译:抗微生物蒸馏肽KSL-W通过调节其对Toll样受体,人β-防御素和细胞因子表达的影响,通过工程化的人口粘膜作用来衰减念珠菌毒症毒力

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摘要

We investigated the toxicity of synthetic antimicrobial decapeptide KSL-W on normal human gingival epithelial cell cultures, its effect on Candida albicans adhesion and growth, and the activation of epithelial cell innate immunity. Our results indicate that KSL-W had no toxic effect on cell adhesion or growth, suggesting its safe use with human cells. Pre-treating C. albicans with KSL-W attenuated the yeast’s virulence as demonstrated by its reduced adhesion and growth on engineered human oral mucosa epithelium and the subsequent decreased expression of some innate defense molecules by targeted epithelial cells. Indeed, the expression of Toll-like receptors and human β-defensins was reduced in tissues infected with KSL-W-treated Candida. Proinflammtory cytokine secretion (IL-1 β and IL-6) by the epithelial cells was also regulated by KSL-W in a manner similar to that of antifungal molecule amphotericin B. These findings therefore show that KSL-W is safe for use with human cells and is able to attenuate Candida virulence by modulating its effects on host innate immunity. This study proposes the potential application of KSL-W peptide as an alternative antifungal agent.
机译:我们研究了合成抗微生物抑制肽KSL-W对正常人牙龈上皮细胞培养物的毒性,其对念珠菌粘附和生长的影响,以及上皮细胞先天免疫的激活。我们的结果表明,KSL-W对细胞粘附或生长没有毒性影响,表明其与人体细胞的安全使用。用KSL-W预处理C. albicans减弱了酵母的毒力,如其降低的粘附和生长在工程化的人口粘膜上皮上所证明,随后通过靶向上皮细胞对一些先天性防御分子的表达减少。实际上,在用KSL-W处理的念珠菌感染的组织中减少了Toll样受体和人β-脱蜡素的表达。上皮细胞的促甲状腺细胞因子分泌(IL-1β和IL-6)也通过类似于抗真菌分子两性霉素B的方式调节。因此,这些结果表明KSL-W是安全的细胞并能够通过调节其对宿主先天免疫的影响来衰减念珠菌毒力。该研究提出了KSL-W肽作为替代抗真菌剂的潜在应用。

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