AI Article Synopsis

  • - The study explores how tweaking the structure of antimicrobial peptides (AMPs) by disrupting their amphipathicity can improve their selectivity and efficacy against bacteria.
  • - The lead peptide, RI-18, showed strong antibacterial properties without causing harm to human cells, effectively targeting both free-floating and biofilm-associated bacteria.
  • - By tuning the characteristics of AMPs like RI-18, researchers aim to develop more effective treatments that combat bacterial infections without causing resistance.

Article Abstract

The advancement of antimicrobial peptides (AMPs) as therapeutic agents is hindered by their poor selectivity. Recent evidence indicates that controlled disruption of the amphipathicity of α-helical AMPs may increase the selectivity. This study investigated the role of imperfect amphipathicity in optimizing AMPs with varied sequences to enhance their activity and selectivity. Among these, the lead peptide RI-18, characterized by an imperfectly amphipathic α-helical structure, demonstrated potent and broad-spectrum antibacterial activity without inducing hemolytic or cytotoxic effects. RI-18 effectively eliminated planktonic and biofilm-associated bacteria as well as persister cells and exhibited high bacterial plasma membrane affinity, inducing rapid membrane permeabilization and rupture. Notably, RI-18 significantly reduced bacterial loads without promoting bacterial resistance, highlighting its therapeutic potential. Overall, this study identified RI-18 as a promising antimicrobial candidate. The rational strategy of tuning imperfect amphipathicity to enhance the AMP activity and selectivity may facilitate the design and development of AMPs.

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Source
http://dx.doi.org/10.1021/acs.jmedchem.4c01855DOI Listing

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