Khara Jasmeet Singh, Obuobi Sybil, Wang Ying, Hamilton Melissa Shea, Robertson Brian D, Newton Sandra M, Yang Yi Yan, Langford Paul R, Ee Pui Lai Rachel
Department of Pharmacy, National University of Singapore, 18 Science Drive 4, Singapore 117543, Singapore; Section of Paediatrics, Department of Medicine, St Mary's Campus, Imperial College London, London W2 1PG, United Kingdom; MRC Centre for Molecular Bacteriology and Infection, Department of Medicine, Imperial College London, London SW7 2AZ, United Kingdom.
Department of Pharmacy, National University of Singapore, 18 Science Drive 4, Singapore 117543, Singapore.
Acta Biomater. 2017 Jul 15;57:103-114. doi: 10.1016/j.actbio.2017.04.032. Epub 2017 Apr 29.
The escalating threat of antimicrobial resistance has increased pressure to develop novel therapeutic strategies to tackle drug-resistant infections. Antimicrobial peptides have emerged as a promising class of therapeutics for various systemic and topical clinical applications. In this study, the de novo design of α-helical peptides with idealized facial amphiphilicities, based on an understanding of the pertinent features of protein secondary structures, is presented. Synthetic amphiphiles composed of the backbone sequence (XYYX), where X and X are hydrophobic residues (Leu or Ile or Trp), Y and Y are cationic residues (Lys), and n is the number repeat units (2 or 2.5 or 3), demonstrated potent broad-spectrum antimicrobial activities against clinical isolates of drug-susceptible and multi-drug resistant bacteria. Live-cell imaging revealed that the most selective peptide, (LKKL), promoted rapid permeabilization of bacterial membranes. Importantly, (LKKL) not only suppressed biofilm growth, but effectively disrupted mature biofilms after only 2h of treatment. The peptides (LKKL) and (WKKW) suppressed the production of LPS-induced pro-inflammatory mediators to levels of unstimulated controls at low micromolar concentrations. Thus, the rational design strategies proposed herein can be implemented to develop potent, selective and multifunctional α-helical peptides to eradicate drug-resistant biofilm-associated infections.
Antimicrobial peptides (AMPs) are increasingly explored as therapeutics for drug-resistant and biofilm-related infections to help expand the size and quality of the current antibiotic pipeline in the face of mounting antimicrobial resistance. Here, synthetic peptides rationally designed based upon principles governing the folding of natural α-helical AMPs, comprising the backbone sequence (XYYX), and which assemble into α-helical structures with idealized facial amphiphilicity, is presented. These multifunctional peptide amphiphiles demonstrate high bacterial selectivity, promote the disruption of pre-formed drug-resistant biofilms, and effectively neutralize endotoxins at low micromolar concentrations. Overall, the design strategies presented here could provide a useful tool for developing therapeutic peptides with broad-ranging clinical applications from the treatment and prevention of drug-resistant biofilms to the neutralization of bacterial endotoxins.
抗菌药物耐药性威胁的不断升级,增加了开发新型治疗策略以应对耐药性感染的压力。抗菌肽已成为一类有前景的治疗药物,可用于各种全身和局部临床应用。在本研究中,基于对蛋白质二级结构相关特征的理解,提出了具有理想表面两亲性的α-螺旋肽的从头设计。由主链序列(XYYX)组成的合成两亲物,其中X和X为疏水残基(亮氨酸或异亮氨酸或色氨酸),Y和Y为阳离子残基(赖氨酸),n为重复单元数(2或2.5或3),对药物敏感和多重耐药细菌的临床分离株表现出强大的广谱抗菌活性。活细胞成像显示,最具选择性的肽(LKKL)能促进细菌膜的快速通透化。重要的是,(LKKL)不仅抑制生物膜生长,而且在仅处理2小时后就能有效破坏成熟生物膜。肽(LKKL)和(WKKW)在低微摩尔浓度下就能将脂多糖诱导的促炎介质的产生抑制到未刺激对照的水平。因此,本文提出的合理设计策略可用于开发强效、选择性和多功能的α-螺旋肽,以根除与耐药生物膜相关的感染。
抗菌肽(AMPs)作为耐药和生物膜相关感染的治疗药物正受到越来越多的探索,以帮助在抗菌药物耐药性不断增加的情况下扩大当前抗生素产品线的规模和质量。在此,展示了基于天然α-螺旋抗菌肽折叠原理合理设计的合成肽,其主链序列为(XYYX),并组装成具有理想表面两亲性的α-螺旋结构。这些多功能肽两亲物表现出高细菌选择性,促进对预先形成的耐药生物膜的破坏,并在低微摩尔浓度下有效中和内毒素。总体而言,本文提出的设计策略可为开发具有广泛临床应用的治疗性肽提供有用工具,从治疗和预防耐药生物膜到中和细菌内毒素。
Zotero 插件