Faculty, Staff and Student Publications

Language

English

Publication Date

12-31-2023

Journal

International Journal of Biological Macromolecules

DOI

10.1016/j.ijbiomac.2023.126398

PMID

37634788

Abstract

The conserved process of cell division in bacteria has been a long-standing target for antimicrobials, although there are few examples of potent broad-spectrum compounds that inhibit this process. Most currently available compounds acting on division are directed towards the FtsZ protein, a self-assembling GTPase that is a central element of the division machinery in most bacteria. Benzodioxane-benzamides are promising candidates, but poorly explored in Gram-negatives. We have tested a number of these compounds on E. coli FtsZ and found that many of them significantly stabilized the polymers against disassembly and reduced the GTPase activity. Reconstitution in crowded cell-like conditions showed that FtsZ bundles were also susceptible to these compounds, including some compounds that were inactive on protofilaments in dilute conditions. They efficiently killed E. coli cells defective in the AcrAB efflux pump. The activity of the compounds on cell growth and division generally showed a good correlation with their effect in vitro, and our experiments are consistent with FtsZ being the target in vivo. Our results uncover the detrimental effects of benzodioxane-benzamides on permeable E. coli cells via its central division protein, implying that lead compounds may be found within this class for the development of antibiotics against Gram-negative bacteria.

Keywords

Escherichia coli, Bacterial Proteins, Benzamides, Cytoskeletal Proteins, Bacteria, GTP Phosphohydrolases, 1, 4-Benzodioxane-benzamides, Antimicrobial resistance, Bacterial division, FtsZ assembly, Gram-negative bacteria, In vitro and in vivo

Published Open-Access

yes

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