A Boron-Dependent Antibiotic Derived from a Calcium-Dependent Antibiotic.

Angew Chem Int Ed Engl

Department of Chemistry, National Taiwan University, No. 1, Sec. 4, Roosevelt Rd., Taipei City, 10617, Taiwan.

Published: January 2024

AI Article Synopsis

  • The rise of drug-resistant bacteria poses a significant threat to healthcare, highlighting the need for new antibiotics.
  • Calcium-dependent antibiotics (CDAs) like laspartomycin C (LspC) show promise against infections, but their reliance on calcium limits their effectiveness.
  • Researchers developed a synthetic LspC analogue called B1, which uses phenylboronic acid instead of calcium, maintaining antibacterial activity against resistant strains while paving the way for innovative antibiotic design.

Article Abstract

The prevalence of drug-resistant bacterial pathogens foreshadows a healthcare crisis. Calcium-dependent antibiotics (CDAs) are promising candidates to combat infectious diseases as many of them show modes of action (MOA) orthogonal to widespread resistance mechanisms. The calcium dependence is nonetheless one of the hurdles toward realizing their full potential. Using laspartomycin C (LspC) as a model, we explored the possibility of reducing, or even eliminating, its calcium dependence. We report herein a synthetic LspC analogue (B1) whose activity no longer depends on calcium and is instead induced by phenylboronic acid (PBA). In LspC, Asp1 and Asp7 coordinate to calcium to anchor it in the active conformation; these residues are replaced by serine in B1 and condense with PBA to form a boronic ester with the same anchoring effect. Using thin-layer chromatography, MS, NMR, and complementation assays, we demonstrate that B1 inhibits bacterial growth via the same MOA as LspC, i.e., sequestering the cell wall biosynthetic intermediate undecaprenyl phosphate. B1 is as potent and effective as LspC against several Gram-positive bacteria, including methicillin-resistant Staphylococcus aureus and vancomycin-resistant Enterococcus. Our success in converting a CDA to a boron-dependent antibiotic opens a new avenue in the design and functional control of drug molecules.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10872445PMC
http://dx.doi.org/10.1002/anie.202317522DOI Listing

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