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Novel non-helical antimicrobial peptides insert into and fuse lipid model membranes.

Saheli MitraBhairavi ChandersekharYunshu LiMark CoopershlyakMargot E MahoneyBrandt EvansRachel KoenigStephen C L HallBeate KlösgenFrank HeinrichBerthony DeslouchesStephanie A Tristram-Nagle
Published in: Soft matter (2024)
This research addresses the growing menace of antibiotic resistance by exploring antimicrobial peptides (AMPs) as alternatives to conventional antibiotics. Specifically, we investigate two linear amphipathic AMPs, LE-53 (12-mer) and LE-55 (16-mer), finding that the shorter LE-53 exhibits greater bactericidal activity against both Gram-negative (G(-)) and Gram-positive (G(+)) bacteria. Remarkably, both AMPs are non-toxic to eukaryotic cells. The heightened effectiveness of LE-53 is attributed to its increased hydrophobicity (H) compared to LE-55. Circular dichroism (CD) reveals that LE-53 and LE-55 both adopt β-sheet and random coil structures in lipid model membranes (LMMs) mimicking G(-) and G(+) bacteria, so secondary structure is not the cause of the potency difference. X-ray diffuse scattering (XDS) reveals increased lipid chain order in LE-53, a potential key distinction. Additionally, XDS study uncovers a significant link between LE-53's upper hydrocarbon location in G(-) and G(+) LMMs and its efficacy. Neutron reflectometry (NR) confirms the AMP locations determined using XDS. Solution small angle X-ray scattering (SAXS) demonstrates LE-53's ability to induce vesicle fusion in bacterial LMMs without affecting eukaryotic LMMs, offering a promising strategy to combat antibiotic-resistant strains while preserving human cell integrity, whereas LE-55 has a smaller ability to induce fusion.
Keyphrases
  • gram negative
  • high resolution
  • randomized controlled trial
  • systematic review
  • endothelial cells
  • stem cells
  • magnetic resonance imaging
  • risk assessment
  • magnetic resonance
  • cell death
  • signaling pathway