Ceftaroline-fosamil efficacy against methicillin-resistant staphylococcus aureus in a rabbit prosthetic joint infection model

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Abstract

Ceftaroline (CPT), the active metabolite of the prodrug ceftaroline-fosamil (CPT-F), demonstrates in vitro bactericidal activity against methicillin-resistant Staphylococcus aureus (MRSA) and is effective in rabbit models of difficult-to-treat MRSA endocarditis and acute osteomyelitis. However, its in vivo efficacy in a prosthetic joint infection (PJI) model is unknown. Using a MRSAinfected knee PJI model in rabbits, the efficacies of CPT-F or vancomycin (VAN) alone and combined with rifampin (RIF) were compared. After each partial knee replacement with a silicone implant that fit into the tibial intramedullary canal was performed, 5×107 MRSA CFU (MICs of 0.38, 0.006, and 1 mg/liter for CPT, RIF, and VAN, respectively) was injected into the knee. Infected animals were randomly assigned to receive no treatment (controls) or CPT-F (60 mg/kg of body weight intramuscularly [i.m.]), VAN (60 mg/kg i.m.), CPT-F plus RIF (10 mg/kg i.m.), or VAN plus RIF starting 7 days postinoculation and lasting for 7 days. Surviving bacteria in crushed tibias were counted 3 days after ending treatment. Although the in vivo mean log10 CFU/g of CPT-treated (3.0±0.9, n=12) and VAN-treated (3.5±1.1, n=12) crushed bones was significantly lower than those of controls (5.6±1.1, n=14) (P<0.001), neither treatment fully sterilized the bones (3/12 were sterile with each treatment). The mean log10 CFU/g values for the antibiotics in combination with RIF were 1.9±0.5 (12/14 were sterile) for CPT-F and 1.9±0.5 (12/14 were sterile) for VAN. In this MRSA PJI model, the efficacies of CPT-F and VAN did not differ; thus, CPT appears to be a promising antimicrobial agent for the treatment of MRSA PJIs.

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Gatin, L., Saleh-Mghir, A., Tasse, J., Ghout, I., Laurent, F., & Crémieux, A. C. (2014). Ceftaroline-fosamil efficacy against methicillin-resistant staphylococcus aureus in a rabbit prosthetic joint infection model. Antimicrobial Agents and Chemotherapy, 58(11), 6496–6500. https://doi.org/10.1128/AAC.03600-14

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