Litcius/Paper detail

Peptidoglycan biosynthesis is driven by lipid transfer along enzyme-substrate affinity gradients

Abraham O. Oluwole, Robin A. Corey, Chelsea M. Brown, Víctor M. Hernández‐Rocamora, Phillip J. Stansfeld, Waldemar Vollmer, Jani Reddy Bolla, Carol V. Robinson

2022Nature Communications33 citationsDOIOpen Access PDF

Abstract

Abstract Maintenance of bacterial cell shape and resistance to osmotic stress by the peptidoglycan (PG) renders PG biosynthetic enzymes and precursors attractive targets for combating bacterial infections. Here, by applying native mass spectrometry, we elucidate the effects of lipid substrates on the PG membrane enzymes MraY, MurG, and MurJ. We show that dimerization of MraY is coupled with binding of the carrier lipid substrate undecaprenyl phosphate (C 55 -P). Further, we demonstrate the use of native MS for biosynthetic reaction monitoring and find that the passage of substrates and products is controlled by the relative binding affinities of the different membrane enzymes. Overall, we provide a molecular view of how PG membrane enzymes convey lipid precursors through favourable binding events and highlight possible opportunities for intervention.

Topics & Concepts

Lipid IIPeptidoglycanEnzymeBiochemistryBiosynthesisSubstrate (aquarium)ChemistryBacterial cell structureOsmotic shockGlycolipidMembraneLipid ABacteriaBiologyGeneGeneticsEcologyBacterial Genetics and BiotechnologyBacteriophages and microbial interactionsGenomics and Phylogenetic Studies