AI Article Synopsis

  • The spread of antibiotic-resistant pathogens is a significant issue, especially since β-lactam antibiotics are crucial in treating infections.
  • Researchers have developed phenylboronic acid derivatives that effectively inhibit certain antibiotic-degrading enzymes (KPC-2, GES-5, and AmpC).
  • The study confirmed these compounds can protect β-lactams from being broken down, showing potential for restoring effectiveness of antibiotics like meropenem without causing cytotoxicity.

Article Abstract

Worldwide dissemination of pathogens resistant to almost all available antibiotics represent a real problem preventing efficient treatment of infectious diseases. Among antimicrobial used in therapy, β-lactam antibiotics represent 40% thus playing a crucial role in the management of infections treatment. We report a small series of phenylboronic acids derivatives (BAs) active against class A carbapenemases KPC-2 and GES-5, and class C cephalosporinases AmpC. The inhibitory profile of our BAs against class A and C was investigated by means of molecular docking, enzyme kinetics and X-ray crystallography. We were interested in the mechanism of recognition among class A and class C to direct the design of broad serine β-Lactamases (SBLs) inhibitors. Molecular modeling calculations vs GES-5 and crystallographic studies vs AmpC reasoned, respectively, the ortho derivative and the meta derivative binding affinity. The ability of our BAs to protect β-lactams from BLs hydrolysis was determined in biological assays conducted against clinical strains: Fractional inhibitory concentration index (FICI) tests confirmed their ability to be synergic with β-lactams thus restoring susceptibility to meropenem. Considering the obtained results and the lack of cytotoxicity, our derivatives represent validated probe for the design of SBLs inhibitors.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6963673PMC
http://dx.doi.org/10.3390/antibiotics8040171DOI Listing

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