4.6 Article

In Vitro Synergism of Penicillin and Ceftriaxone against Enterococcus faecalis

Journal

MICROORGANISMS
Volume 9, Issue 10, Pages -

Publisher

MDPI
DOI: 10.3390/microorganisms9102150

Keywords

E. faecalis endocarditis; synergism; OPAT; penicillin/ceftriaxone; ampicillin/ceftriaxone; checkerboard

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Funding

  1. Federal Ministry of Education and Research, Germany [01KI1501, 13N15467]

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This study suggests that benzylpenicillin/ceftriaxone is suitable for the treatment of E. faecalis infections with ceftriaxone MIC ≤ 256mg/L, but not for those with ceftriaxone MIC ≥ 512mg/L. Further investigation is needed to analyze the relationship between ceftriaxone susceptibility and penicillin/ceftriaxone synergy.
Enterococcus faecalis infective endocarditis is commonly treated with intravenous ampicillin/ceftriaxone combination therapy. Ampicillin, however, is unsuitable for outpatient parenteral antibiotic therapy (OPAT) regimens due to its instability in 24 h continuous infusors, and has been successfully replaced by benzylpenicillin used together with ceftriaxone in a few small case series. Since in vitro synergy data of penicillin/ceftriaxone against E. faecalis are still lacking, checkerboard assays were performed for 28 clinical E. faecalis isolates and one laboratory standard strain. Synergistic effects (both lowest and median FICI) were observed for penicillin/ceftriaxone in 15/29 isolates, while ampicillin/ceftriaxone exhibited synergism in 22/29 isolates. For isolates with ceftriaxone MICs & LE; 256 mg/L, the addition of free ceftriaxone trough concentrations to penicillin or ampicillin resulted in comparable synergistic effects for both combinations. In contrast, for isolates with ceftriaxone MICs & GE; 512 mg/L free ceftriaxone trough concentrations were only sufficient to exhibit synergistic effects in combination with ampicillin, but not penicillin. This study suggests that benzylpenicillin/ceftriaxone would be expected to be suitable for the OPAT treatment of enterococcal endocarditis for E. faecalis isolates with ceftriaxone MICs & LE; 256 mg/L. However, combination therapy would be expected to provide no advantage over benzylpenicillin monotherapy for isolates with ceftriaxone MICs & GE; 512 mg/L. Further investigation is required to analyse the relationship between ceftriaxone susceptibility and penicillin/ceftriaxone synergy, especially for isolates with ceftriaxone MICs of 64 to 512 mg/L.

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