| Literature DB >> 30904754 |
Krzysztof Durka1, Agnieszka E Laudy2, Łukasz Charzewski3, Mateusz Urban1, Karolina Stępień4, Stefan Tyski5, Krystiana A Krzyśko6, Sergiusz Luliński7.
Abstract
A series of 22 benzosiloxaboroles, silicon analogues of strong antimicrobial agents - benzoxaboroles, have been synthesized and tested against β-lactamases KPC- and pAmpC-producing strains of Gram-negative rods. Comprehensive structural-property relationship studies supported by molecular modelling as well as biological studies reveal that 6-B(OH)2-substituted derivative 27 strongly inhibits the activity of cephalosporinases (chromosomally encoded AmpC and plasmid encoded CMY-2) and KPC carbapenemases. It also shows strong ability to inhibit growth of the strains producing KPC-3 when combined with meropenem. In addition, halogen-substituted (mono-, di- or tetra-) benzosiloxaboroles demonstrate high antifungal activity (MIC 1.56-6.25 mg/L) against C. tropicalis, C. guilliermondii and S. cerevisiae. The highest activity against pathogenic yeasts (C. albicans, C. krusei and C. parapsilosis - MICs 12.5 mg/L) and against Gram-positive cocci (S. aureus and E. faecalis - 6.25 mg/L and 25 mg/L respectively) was displayed by 6,7-dichloro-substituted benzosiloxaborole. The studied systems exhibit low cytotoxity toward human lung fibroblasts.Entities:
Keywords: AmpC/KPC β-lactamase inhibitory activity; Antibacterial activity; Antifungal activity; Benzosiloxaboroles; Efflux pump; Molecular docking
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Year: 2019 PMID: 30904754 DOI: 10.1016/j.ejmech.2019.03.028
Source DB: PubMed Journal: Eur J Med Chem ISSN: 0223-5234 Impact factor: 6.514