4.7 Article

Impact of acquired broad-spectrum β-lactamases on susceptibility to oral penems/carbapenems (tebipenem, sulopenem, and faropenem) alone or in combination with avibactam and taniborbactam β-lactamase inhibitors in Escherichia coli

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AMER SOC MICROBIOLOGY
DOI: 10.1128/aac.00547-23

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tebipenem; oral penem; faropenem; sulopenem; ceftibuten; taniborbactam; susceptibility testing; beta-lactamase; avibactam

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This study evaluated the impact of beta-lactamases on the susceptibility to oral penems/carbapenems and other carbapenem molecules. The results showed that tebipenem and sulopenem had a similar activity spectrum in Escherichia coli and exhibited lower MIC values against beta-lactamase-producing strains.
The impact of beta-lactamases on susceptibility to oral penems/carbapenems (tebipenem, sulopenem, and faropenem) and other carbapenem molecules was evaluated in Escherichia coli, alone and in combination with avibactam or taniborbactam beta-lactamase inhibitors. Tebipenem and sulopenem exhibited a similar spectrum of activity compared to the intravenous carbapenems and displayed lower MIC values than ceftibuten-avibactam against E. coli producing extended-spectrum beta-lactamases or AmpC enzymes. Combined with taniborbactam, tebipenem and sulopenem exhibited low MIC values against almost all tested recombinant E. coli, including metallo-beta-lactamase producers.

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