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从抗菌肽到抗菌聚(α-氨基酸)

From Antimicrobial Peptides to Antimicrobial Poly(α-amino acid)s.

机构信息

Key Laboratory of Polymer Ecomaterials, Changchun Institute of Applied Chemistry, Chinese Academy of Sciences, Changchun, 130022, P. R. China.

University of Chinese Academy of Sciences, 19A Yuquan Road, Beijing, 100049, P. R. China.

出版信息

Adv Healthc Mater. 2018 Oct;7(20):e1800354. doi: 10.1002/adhm.201800354. Epub 2018 Jun 19.

Abstract

Conventional small-molecule antibiotics are facing a significant challenge of the rapidly developed drug resistance of pathogens. In contrast, antimicrobial peptides (AMPs), an important component for innate host defenses, are now under intensive investigation as a promising antimicrobial agent for combating drug resistant pathogens. Most AMPs can effectively kill a broad spectrum of pathogens via physical disruption of microbial cellular membranes, which is identified to be difficult to develop resistance. However, the clinical applications of AMPs are still greatly limited by several inherent impediments, such as high cost of production, potential hemolysis or toxicity, and liability to proteinase degradation. Recently, cationic poly(α-amino acid)s with structures mimicking the AMPs are found to have excellent antimicrobial activity. These polymers, termed "antimicrobial poly(α-amino acid)s (APAAs)," have some advantages over AMPs, such as easy production and modification, prolonged antimicrobial activity, low cytotoxicity, and enhanced stability to protease degradation. Here, a brief introduction of mechanisms and affecting factors of microbial killing by AMPs is first presented, followed by a systematic illustration of recent advances in design and preparation of biomimetic APAAs and a perspective in this field.

摘要

传统小分子抗生素面临着病原体耐药性迅速发展的重大挑战。相比之下,抗菌肽 (AMPs) 作为一种对抗耐药病原体的有前途的抗菌药物,作为先天宿主防御的重要组成部分,目前正在受到深入研究。大多数 AMP 可以通过物理破坏微生物细胞膜来有效杀死广谱病原体,这被认为很难产生耐药性。然而,AMP 的临床应用仍然受到几个固有障碍的极大限制,例如生产成本高、潜在的溶血或毒性以及易被蛋白酶降解。最近,结构模拟 AMP 的阳离子聚 (α-氨基酸) 被发现具有优异的抗菌活性。这些聚合物被称为“抗菌聚 (α-氨基酸) (APAAs)”,与 AMP 相比具有一些优势,例如易于生产和修饰、延长的抗菌活性、低细胞毒性和增强对蛋白酶降解的稳定性。本文首先简要介绍了 AMP 杀灭微生物的机制和影响因素,然后系统阐述了仿生 APAAs 的设计和制备方面的最新进展,并对该领域进行了展望。

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