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Cyclic Peptides as Novel Therapeutic Microbicides: Engineering of Human Defensin Mimetics

机译:作为新型治疗性杀微生物剂的环肽:人防御素模拟物的工程化

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摘要

Cyclic peptides are receiving significant attention thanks to their antimicrobial activity and high serum stability, which is useful to develop and design novel antimicrobial agents. Antimicrobial peptides appear to be key components of innate defences against bacteria, viruses, and fungi. Among the others, defensins possess a strong microbicidial activity. Defensins are cationic and amphipathic peptides with six cysteine residues connected by three disulfide bonds found in plants, insects, and mammals; they are divided in three families: α-, β-, and θ-defensins. α-Defensins are contained in the primary granules of human neutrophils; β-defensins are expressed in human epithelia; and θ-defensins are pseudo-cyclic defensins not found in humans, but in primates, such as chimpanzees or gorillas. The structural diversities among the three families are reflected in a different antimicrobial action as well as in serum stability. The engineering of these peptides is an exciting opportunity to obtain more functional antimicrobial molecules highlighting their potential as therapeutic agents. The present review reports the most recent advances in the field of cyclic peptides with a specific regard to defensin analogs.
机译:环状肽由于其抗菌活性和高血清稳定性而受到了广泛的关注,这对开发和设计新型抗菌剂很有用。抗菌肽似乎是针对细菌,病毒和真菌的先天防御的关键成分。除其他外,防御素具有很强的杀菌活性。防御素是阳离子和两亲性肽,具有六个半胱氨酸残基,它们通过在植物,昆虫和哺乳动物中发现的三个二硫键相连;它们分为三个家族:α-,β-和θ-防御素。 α-防御素包含在人类嗜中性粒细胞的初级颗粒中; β-防御素在人类上皮细胞中表达; β-防御素和θ-防御素是在人类中没有发现的伪环状防御素,但在黑猩猩或大猩猩等灵长类动物中均未发现。这三个家族之间的结构多样性反映在不同的抗菌作用以及血清稳定性上。这些肽的工程改造是获得更多功能性抗菌分子的令人兴奋的机会,突出了其作为治疗剂的潜力。本文综述了环肽领域的最新进展,特别是针对防御素类似物的研究。

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