AI Article Synopsis

  • UyCT peptides are antimicrobial peptides from Australian scorpion venom that show effectiveness against various bacteria, including multi-drug resistant strains.
  • Their interaction with membranes was analyzed using techniques like dye release and isothermal titration calorimetry, revealing a mechanism that disrupts bacterial membranes while minimizing damage to red blood cells.
  • The findings suggest that UyCT peptides could be developed into treatments for resistant bacterial infections, particularly targeting pathogens such as Acinetobacter baumannii, with potential for improving their delivery and safety profiles.

Article Abstract

UyCT peptides are antimicrobial peptides isolated from the venom of the Australian scorpion. The activity of the UyCT peptides against Gram positive and Gram negative bacteria and red blood cells was determined. The membrane interactions of these peptides were evaluated by dye release (DR) of the fluorophore calcein from liposomes and isothermal titration calorimetry (ITC); and their secondary structure was determined by circular dichroism (CD). Three different lipid systems were used to mimic red blood cells, Escherichia coli and Staphylococcus aureus membranes. UyCT peptides exhibited broad spectrum antimicrobial activity with low MIC for S. aureus and multi-drug resistant Gram negative strains. Peptide combinations showed some synergy enhancing their potency but not hemolytic activity. The UyCT peptides adopted a helical structure in lipid environments and DR results confirmed that the mechanism of action is by disrupting the membrane. ITC data indicated that UyCT peptides preferred prokaryotic rather than eukaryotic membranes. The overall results suggest that UyCT peptides could be pharmaceutical leads for the treatment of Gram negative multiresistant bacterial infections, especially against Acinetobacter baumanni, and candidates for peptidomimetics to enhance their potency and minimize hemolysis. This article is part of a Special Issue entitled: Interfacially Active Peptides and Proteins. Guest Editors: William C. Wimley and Kalina Hristova.

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Source
http://dx.doi.org/10.1016/j.bbamem.2013.10.022DOI Listing

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