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Activity of antimicrobial peptide mimetics in the oral cavity: I. Activity against biofilms of Candida albicans.

机译:抗菌肽模拟物在口腔中的活性:I.针对白色念珠菌生物膜的活性。

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摘要

Naturally occurring antimicrobial peptides hold promise as therapeutic agents against oral pathogens such as Candida albicans but numerous difficulties have slowed their development. Synthetic, non-peptidic analogs that mimic the properties of these peptides have many advantages and exhibit potent, selective antimicrobial activity. Several series of mimetics (with molecular weight < 1000) were developed and screened against oral Candida strains as a proof-of-principle for their antifungal properties. One phenylalkyne and several arylamide compounds with reduced mammalian cytotoxicities were found to be active against C. albicans. These compounds demonstrated rapid fungicidal activity in liquid culture even in the presence of saliva, and demonstrated synergy with standard antifungal agents. When assayed against biofilms grown on denture acrylic, the compounds exhibited potent fungicidal activity as measured by metabolic and fluorescent viability assays. Repeated passages in sub-minimum inhibitory concentration levels did not lead to resistant Candida, in contrast to fluconazole. Our results demonstrate the proof-of principle for the use of these compounds as anti-Candida agents, and their further testing is warranted as novel anti-Candida therapies.
机译:天然存在的抗菌肽有望作为针对口腔病原体(例如白色念珠菌)的治疗剂,但是许多困难减缓了它们的发展。模仿这些肽的性质的合成的非肽类似物具有许多优点,并表现出有效的,选择性的抗菌活性。开发了数个模拟物系列(分子量<1000),并针对口服念珠菌菌株进行了筛选,以作为其抗真菌特性的原理证明。发现一种具有降低的哺乳动物细胞毒性的苯基炔烃和几种芳基酰胺化合物对白色念珠菌具有活性。这些化合物甚至在唾液存在下,在液体培养中也显示出快速的杀真菌活性,并证明了与标准抗真菌剂的协同作用。当针对在义齿丙烯酸板上生长的生物膜进行测定时,这些化合物表现出有效的杀真菌活性,如通过代谢和荧光活力测定所测量的。与氟康唑相反,次最低抑菌浓度水平的反复传代并未导致耐药念珠菌。我们的结果证明了将这些化合物用作抗念珠菌药物的原理证明,并且有必要对它们进行进一步的测试,作为新颖的抗念珠菌疗法。

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