Novel short antibacterial and antifungal peptides with low cytotoxicity: Efficacy and action mechanisms

抗真菌 细胞毒性 微生物学 生物 生物化学 抗菌活性 动作(物理) 抗菌肽 药理学 细菌 化学 体外 物理 量子力学 遗传学
作者
Xiaobao Qi,Chuncai Zhou,Peng Li,Weixin Xu,Ye Cao,Hua Ling,Wei Ning Chen,Chang Ming Li,Rong Xu,Mouad Lamrani,Yuguang Mu,Susanna Su Jan Leong,Matthew Wook Chang,Mary B. Chan‐Park
出处
期刊:Biochemical and Biophysical Research Communications [Elsevier]
卷期号:398 (3): 594-600 被引量:73
标识
DOI:10.1016/j.bbrc.2010.06.131
摘要

Short antimicrobial peptides with nine and eleven residues were developed against several clinically important bacterial and fungal pathogens (specifically Escherichia coli, Pseudomonas aeruginosa, Staphylococcus aureus, Candida albicans, and Fusarium solani). Twelve analogues of previously reported peptides BP76 (KKLFKKILKFL) and Pac-525 (KWRRWVRWI) were designed, synthesized, and tested for their antimicrobial activities. Two of our eleven amino acid peptides, P11-5 (GKLFKKILKIL) and P11-6 (KKLIKKILKIL), have very low MICs of 3.1-12.5microg ml(-1) against all five pathogens. The MICs of these two peptides against S. aureus, C. albicans and F. solani are four to ten times lower than the corresponding MICs of the reference peptide BP76. P9-4 (KWRRWIRWL), our newly designed nine-amino acid analogue, also has particularly low MICs of 3.1-6.2microg ml(-1) against four of the tested pathogens; these MICs are two to eight times lower than those reported for Pac-525 (6.2-50microg ml(-1)).These new peptides (P11-5, P11-6 and P9-4) also exhibit improved stability in the presence of salts, and have low cytotoxicity as shown by the hemolysis and MTT assays. From the results of field-emission scanning electron microscopy, membrane depolarization and dye-leakage assays, we propose that these peptides exert their action by disrupting membrane lipids. Molecular dynamics simulation studies confirm that P11-6 peptide maintains relatively stable helical structure and exerts more perturbation action on the order of acyl tail of lipid bilayer.
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