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Design and synthesis of unprecedented cyclic γ-AApeptides for antimicrobial development

机译:设计和合成史无前例的用于抗菌开发的环状γ-AA肽

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摘要

Antimicrobial drug resistance is one of the greatest threats facing mankind. Antimicrobial peptides (AMPs) can potentially circumvent drug resistance, probably through a bacterial membrane-disruption mechanism. However, they suffer from low in vivo stability, potential immunogenicity, and difficulty in optimization. The development of antimicrobial peptidomimetics is therefore an emerging research area as they avoid the potential disadvantages of AMPs. Cyclic peptidomimetics are of significant interest since constraints induced by cyclization are expected to further improve their antimicrobial activity. Nonetheless, the report of cyclic oligomeric peptidomimetics for antimicrobial development is rare. Herein, for the first time, we report the design and synthesis of cyclic γ-AApeptides via an on-resin cyclization. These cyclic γ-AApeptides are potent and broad-spectrum active against fungus and multidrug resistant Gram-positive and Gram-negative bacterial pathogens. Our results demonstrate the potential of cyclic γ-AApeptides as a new class of antibiotics to circumvent drug resistance by mimicking the bactericidal mechanism of AMPs. Meanwhile, the facile synthesis of cyclic γ-AApeptides may further expand the applications of γ-AApeptides in biomedical sciences.
机译:抗菌药物耐药性是人类面临的最大威胁之一。抗菌肽(AMP)可能会通过细菌膜破坏机制来规避耐药性。然而,它们遭受体内稳定性低,潜在的免疫原性和优化困难的困扰。因此,抗菌肽模拟物的开发是新兴的研究领域,因为它们避免了AMPs的潜在缺点。环肽模拟物是令人关注的,因为预期由环化引起的限制将进一步改善其抗菌活性。然而,环状低聚拟肽用于抗菌药物开发的报道很少。在此,我们首次通过树脂上的环化方法报道了环状γ-AA肽的设计与合成。这些环状γ-AA肽对真菌和多重耐药性革兰氏阳性和革兰氏阴性细菌病原体均有效且具有广谱活性。我们的结果证明了环状γ-AA肽作为新型抗生素通过模仿AMPs的杀菌机制来规避耐药性的潜力。同时,环状γ-AA肽的简便合成可以进一步扩大γ-AA肽在生物医学领域的应用。

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