Nature Communications (Oct 2022)

Antibiotic polymyxin arranges lipopolysaccharide into crystalline structures to solidify the bacterial membrane

  • Selen Manioglu,
  • Seyed Majed Modaresi,
  • Noah Ritzmann,
  • Johannes Thoma,
  • Sarah A. Overall,
  • Alexander Harms,
  • Gregory Upert,
  • Anatol Luther,
  • Alexander B. Barnes,
  • Daniel Obrecht,
  • Daniel J. Müller,
  • Sebastian Hiller

DOI
https://doi.org/10.1038/s41467-022-33838-0
Journal volume & issue
Vol. 13, no. 1
pp. 1 – 12

Abstract

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Abstract Polymyxins are last-resort antibiotics with potent activity against multi-drug resistant pathogens. They interact with lipopolysaccharide (LPS) in bacterial membranes, but mechanistic details at the molecular level remain unclear. Here, we characterize the interaction of polymyxins with native, LPS-containing outer membrane patches of Escherichia coli by high-resolution atomic force microscopy imaging, along with structural and biochemical assays. We find that polymyxins arrange LPS into hexagonal assemblies to form crystalline structures. Formation of the crystalline structures is correlated with the antibiotic activity, and absent in polymyxin-resistant strains. Crystal lattice parameters alter with variations of the LPS and polymyxin molecules. Quantitative measurements show that the crystalline structures decrease membrane thickness and increase membrane area as well as stiffness. Together, these findings suggest the formation of rigid LPS–polymyxin crystals and subsequent membrane disruption as the mechanism of polymyxin action and provide a benchmark for optimization and de novo design of LPS-targeting antimicrobials.