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Engineering Selectively Targeting Antimicrobial Peptides
Annual Review of Biomedical Engineering ( IF 9.7 ) Pub Date : 2021-07-13 , DOI: 10.1146/annurev-bioeng-010220-095711
Ming Lei 1 , Arul Jayaraman 2, 3 , James A Van Deventer 1, 4 , Kyongbum Lee 1
Affiliation  

The rise of antibiotic-resistant strains of bacterial pathogens has necessitated the development of new therapeutics. Antimicrobial peptides (AMPs) are a class of compounds with potentially attractive therapeutic properties, including the ability to target specific groups of bacteria. In nature, AMPs exhibit remarkable structural and functional diversity, which may be further enhanced through genetic engineering, high-throughput screening, and chemical modification strategies. In this review, we discuss the molecular mechanisms underlying AMP selectivity and highlight recent computational and experimental efforts to design selectively targeting AMPs. While there has been an extensive effort to find broadly active and highly potent AMPs, it remains challenging to design targeting peptides to discriminate between different bacteria on the basis of physicochemical properties. We also review approaches for measuring AMP activity, point out the challenges faced in assaying for selectivity, and discuss the potential for increasing AMP diversity through chemical modifications.

中文翻译:


工程选择性靶向抗菌肽

细菌病原体的抗生素抗性菌株的兴起使得开发新的治疗方法成为必要。抗菌肽 (AMP) 是一类具有潜在吸引力的治疗特性的化合物,包括靶向特定细菌群的能力。在自然界中,AMPs 表现出显着的结构和功能多样性,可以通过基因工程、高通量筛选和化学修饰策略进一步增强。在这篇综述中,我们讨论了 AMP 选择性的分子机制,并重点介绍了最近设计选择性靶向 AMP 的计算和实验工作。虽然已经做出了广泛的努力来寻找广泛活跃和高效的 AMP,设计靶向肽以根据物理化学特性区分不同的细菌仍然具有挑战性。我们还回顾了测量 AMP 活性的方法,指出了在检测选择性方面面临的挑战,并讨论了通过化学修饰增加 AMP 多样性的潜力。

更新日期:2021-07-14
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