University of Hertfordshire

In silico structural evaluation of short cationic antimicrobial peptides

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Original languageEnglish
Article number72
JournalPharmaceutics
Journal publication date21 Jun 2018
Volume10
Issue3
DOIs
StatePublished - 21 Jun 2018

Abstract

Cationic peptides with antimicrobial properties are ubiquitous in nature and have been studied for many years in an attempt to design novel antibiotics. However, very few molecules are used in the clinic so far, due sometimes to their complexity but mostly the unfavorable pharmacokinetic profile associated with peptides. The aim of this work is to investigate them in order to identify common structural features which could be useful for the design of small peptides or peptido-mimetics with improved drug-like properties and activity against Gram negative bacteria. Two sets of cationic peptides (AMPs) with known antimicrobial activity have been investigated. The first reference set comprised molecules with experimentally known conformations available in the protein databank (PDB), and the second one was composed of short peptides active against Gram negative bacteria but with no significant structural information available. The predicted structures of the peptides from the first set were in excellent agreement with those experimentally observed, which allowed analysis of the structural features of the second group using computationally derived conformations. The peptide conformations, either experimentally available or predicted, were clustered in an “all vs. all” fashion and the most populated clusters were then analyzed. It was confirmed that these peptides tend to assume an amphipathic conformation regardless of the environment. It was also observed that positively charged amino acids can often be found next to aromatic ones. Finally, a protocol was evaluated for the investigation of the behavior of short cationic peptides in the presence of a membrane-like environment such as dodecylphosphocholine (DPC) micelles. The results presented herein introduce a promising approach to inform the design of novel short peptides with a potential antimicrobial activity.

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