AI Article Synopsis

  • The study investigates the interaction of boron-containing compounds with penicillin-binding protein (PBP) β-lactam targets, which have not been thoroughly researched before.
  • High-throughput X-ray crystallography revealed that different boron compounds can form varying types of covalent links with the PBP3 enzyme, which is significant for their inhibitory activity.
  • Findings suggest that while some modifications of benzoxaboroles inhibit PBP3 moderately, they do not exhibit antibacterial activity, highlighting the potential for developing new boron-based antibiotics that could overcome current resistance issues posed by β-lactamases.

Article Abstract

The effectiveness of β-lactam antibiotics is increasingly compromised by β-lactamases. Boron-containing inhibitors are potent serine-β-lactamase inhibitors, but the interactions of boron-based compounds with the penicillin-binding protein (PBP) β-lactam targets have not been extensively studied. We used high-throughput X-ray crystallography to explore reactions of a boron-containing fragment set with the PBP3 (PaPBP3). Multiple crystal structures reveal that boronic acids react with PBPs to give tricovalently linked complexes bonded to Ser294, Ser349, and Lys484 of PaPBP3; benzoxaboroles react with PaPBP3 via reaction with two nucleophilic serines (Ser294 and Ser349) to give dicovalently linked complexes; and vaborbactam reacts to give a monocovalently linked complex. Modifications of the benzoxaborole scaffold resulted in a moderately potent inhibition of PaPBP3, though no antibacterial activity was observed. Overall, the results further evidence the potential for the development of new classes of boron-based antibiotics, which are not compromised by β-lactamase-driven resistance.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9282634PMC
http://dx.doi.org/10.1021/acs.jmedchem.1c00717DOI Listing

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