Multistep optimization of a cell-penetrating peptide towards its antimicrobial activity

抗菌肽 抗菌剂 细胞穿透肽 细胞 抗生素 抗菌活性 生物化学 细胞膜 肽序列 癌细胞 多重耐药 化学 微生物学 生物 细菌细胞结构 细菌 癌症 基因 遗传学
作者
Marco Drexelius,André Reinhardt,Joshua Grabeck,Tom Cronenberg,Frank Nitsche,Pitter F. Huesgen,Berenike Maier,Ines Neundorf
出处
期刊:Biochemical Journal [Portland Press]
卷期号:478 (1): 63-78 被引量:12
标识
DOI:10.1042/bcj20200698
摘要

Multidrug resistant (MDR) bacteria have adapted to most clinical antibiotics and are a growing threat to human health. One promising type of candidates for the everlasting demand of new antibiotic compounds constitute antimicrobial peptides (AMPs). These peptides act against different types of microbes by permeabilizing pathogen cell membranes, whereas being harmless to mammalian cells. Contrarily, another class of membrane-active peptides, namely cell-penetrating peptides (CPPs), is known to translocate in eukaryotic cells without substantially affecting the cell membrane. Since CPPs and AMPs share several physicochemical characteristics, we hypothesized if we can rationally direct the activity of a CPP towards antimicrobial activity. Herein, we describe the screening of a synthetic library, based on the CPP sC18, including structure-based design to identify the active residues within a CPP sequence and to discover novel AMPs with high activity. Peptides with increased hydrophobicity were tested against various bacterial strains, and hits were further optimized leading to four generations of peptides, with the last also comprising fluorinated amino acid building blocks. Interestingly, beside strong antibacterial activities, we also detected activity in cancer cells, while non-cancerous cells remained unharmed. The results highlight our new candidates, particularly those from generation 4, as a valuable and promising source for the development of future therapeutics with antibacterial activity and beyond.
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