| Literature DB >> 32155326 |
Xiaoyan Ju1,2, Jun Chen3, Mengxue Zhou3, Meng Zhu1, Zhuang Li1, Sijia Gao1, Jinzhao Ou1, Dandan Xu1, Man Wu1, Shidong Jiang1, Yi Hu3, Ye Tian1, Zhongwei Niu1,4.
Abstract
Pseudomonas aeruginosa (P. aeruginosa) biofilms are associated with a wide range of infections, from chronic tissue diseases to implanted medical devices. In a biofilm, the extracellular polymeric substance (EPS) causes an inhibited penetration of antibacterial agents, leading to a 100-1000 times tolerance of the bacteria. In view of the water-filled channels in biofilms and the highly negative charge of EPS, we design a chitosan-polyethylene glycol-peptide conjugate (CS-PEG-LK13) in this study. The CS-PEG-LK13 prefers a neutrally charged assembly at a size of ∼100 nm in aqueous environment, while undergoes disassembly to expose the α-helical peptide at the bacterial cell membrane. This behavior provides CS-PEG-LK13 superiorities in both penetrating the biofilms and inactivating the bacteria. At a concentration of 8 times the minimum inhibitory concentration, CS-PEG-LK13 has a much higher antibacterial efficiency (72.70%) than LK13 peptide (15.24%) and tobramycin (33.57%) in an in vitro P. aeruginosa biofilm. Moreover, CS-PEG-LK13 behaves comparable capability of combating an implanted P. aeruginosa biofilm to highly excess tobramycin. This work has implications for the design of new antibacterial agents in biofilm combating.Entities:
Keywords: Pseudomonas aeruginosa; antimicrobial peptides; biofilm; chitosan; self-assembly
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Year: 2020 PMID: 32155326 DOI: 10.1021/acsami.0c02034
Source DB: PubMed Journal: ACS Appl Mater Interfaces ISSN: 1944-8244 Impact factor: 9.229