Influence of Lipidation Pattern of the KR12 Fragment of Peptide LL-37 on Its Antibacterial and Hemolytic Activities.
Elżbieta KamyszEmilia SikorskaMarta BauerKarol SikoraDamian NeubauerPublished in: International journal of molecular sciences (2023)
Contemporary medicine has been confronted by multidrug resistance. Therefore, new antibiotics are sought to alleviate the problem. In this study, we estimated the effect of the positioning and extent of lipidation (mainly octanoic acid residue) in the KR12-NH 2 molecule on antibacterial and hemolytic activities. The effect of the conjugation of benzoic acid derivatives (C 6 H 5 -X-COOH, where X: CH 2 , CH 2 -CH 2 , CH=CH, C≡C, and CH 2 -CH 2 -CH 2 ) with the N -terminal part of KR12-NH 2 on biological activity was also studied. All analogs were tested against planktonic cells of ESKAPE bacteria and reference strains of Staphylococcus aureus . The effect of lipidation site on the helicity of the KR12-NH 2 analogs was studied using CD spectroscopy. The ability of the selected peptides to induce the aggregation of POPG liposomes was evaluated with DLS measurements. We demonstrated that both the site and extent of peptide lipidation play an essential role in the bacterial specificity of the lipopeptides. Most of the C 8 α -KR12-NH 2 ( II ) analogs that were more hydrophobic than the parent compound were also more hemolytic. A similar relationship was also found between the α-helical structure content in POPC and hemolytic activity. It is worth emphasizing that in our study, the highest selectivity against S. aureus strains with an SI value of at least 21.11 exhibited peptide XII obtained by the conjugation of the octanoic acid with the N -terminus of retro-KR12-NH 2 . All lipidated analogs with the highest net charge (+5) were the most selective toward pathogens. Therefore, the overall charge of KR12-NH 2 analogs plays pivotal role in their biological activity.
Keyphrases
- room temperature
- ionic liquid
- molecular docking
- staphylococcus aureus
- escherichia coli
- drug delivery
- induced apoptosis
- cystic fibrosis
- cell proliferation
- molecular dynamics simulations
- cell cycle arrest
- silver nanoparticles
- cell death
- multidrug resistant
- endoplasmic reticulum stress
- metal organic framework
- drug release