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跨链相互作用、中央弯曲和序列模式作为简化 β-发夹抗菌两亲分子的生物调节剂。

Cross-Strand Interaction, Central Bending, and Sequence Pattern Act as Biomodulators of Simplified β-Hairpin Antimicrobial Amphiphiles.

机构信息

Institute of Animal Nutrition, Northeast Agricultural University, Harbin, 150030, P. R. China.

出版信息

Small. 2021 Feb;17(7):e2003899. doi: 10.1002/smll.202003899. Epub 2020 Dec 23.

Abstract

Novel antimicrobial peptides (AMPs) have revolutionarily evolved into formidable candidates for antibiotic substitute materials against pathogenic infections. However, cost, lability, disorderly sequences, systemic toxicology, and biological profiles have plagued the perennial search. Here, a progressive β-hairpin solution with the simplest formulation is implanted into an AMP-based therapeutic strategy to systematically reveal the complex balance between function and toxicity of structural moieties, including cationicity, hydrophobicity, cross-strand interactions, center bending, and sequence pattern. Comprehensive implementation of structural identification, ten microorganisms, eleven in vitro barriers, four mammalian cells, and a diversified membrane operation setup led to the emergence of β-hairpin prototypes from a 24-member library. Lead amphiphiles, WKF-PG and WRF-NG, can tackle bacterial infection through direct antimicrobial efficacy and potential inflammation-limiting capabilities, such as an Escherichia coli challenge in a mouse peritonitis-sepsis model, without observed toxicity after systemic administration. Their optimal states with dissimilar modulators and the unavailable drug resistance related to membrane lytic mechanisms, also provide an usher for renewed innovation among β-sheet peptide-based antimicrobial biomaterials.

摘要

新型抗菌肽 (AMPs) 已革命性地演变为对抗致病感染的抗生素替代材料的有力候选物。然而,成本、不稳定性、无序序列、全身毒理学和生物学特征一直困扰着人们的长期研究。在这里,一种具有最简单配方的渐进式 β-发夹解决方案被植入到基于 AMP 的治疗策略中,以系统地揭示结构部分(包括正电性、疏水性、跨链相互作用、中心弯曲和序列模式)的功能和毒性之间的复杂平衡。综合实施结构鉴定、十种微生物、十一种体外屏障、四种哺乳动物细胞和多样化的膜操作设置,从一个由 24 个成员组成的文库中产生了β-发夹原型。先导两亲分子 WKF-PG 和 WRF-NG 可以通过直接的抗菌功效和潜在的炎症限制能力来解决细菌感染问题,例如在大肠杆菌引起的小鼠腹膜炎-败血症模型中,在全身给药后没有观察到毒性。它们与膜溶解机制相关的最佳状态和不可用的耐药性以及不同的调节剂为基于 β-折叠肽的抗菌生物材料的创新提供了新的契机。

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