Prevalence of a cefazolin inoculum effect associated with blaz gene types among methicillin-susceptible staphylococcus aureus isolates from four major medical centers in chicago

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Abstract

The efficacy of cefazolin with high-inoculum methicillin-susceptible Staphylococcus aureus (MSSA) infections remains in question due to therapeutic failure inferred as being due to an inoculum effect (InE). This study investigated the local prevalence of a cefazolin InE (CInE) and its association with staphylococcal blaZ gene types among MSSA isolates in the Chicago area. Four medical centers in Chicago, IL, contributed MSSA isolates. Cefazolin MICs (C-MIC) were determined at 24 h by the broth microdilution method using a standard inoculum (SI; 5 105 CFU/ml) and a high inoculum (HI; 5 107 CFU/ml). The CInE was defined as (i) a 4-fold increase in C-MIC between SI and HI and/or (ii) a pronounced CInE, i.e., a nonsusceptible C-MIC of 16 g/ml at HI. PCR was used to amplify the blaZ gene, followed by agarose gel electrophoresis and sequencing to determine the gene type. Approximately 269 MSSA isolates were included. All but one isolate were susceptible to cefazolin at SI, and 97% remained susceptible at HI. A total of 196 isolates (73%) were blaZ positive, with the blaZ types led by gene type C (40%). CInE was seen in 45 blaZ-positive isolates (23%), with 44 (22%) presenting a 4-fold increase in C-MIC (SI to HI) and 5 (3%) a pronounced CInE. Four of the five met both definitions of CInE, two of which expressed the type A gene. The prevalence of a pronounced CInE associated with the type A blaZ gene from MSSA isolates in Chicago is low. Our predilection for cefazolin use, even early in the management of hospitalized MSSA infections, is tenable.

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Wang, S. K., Gilchrist, A., Loukitcheva, A., Plotkin, B. J., Sigar, I. M., Gross, A. E., … Scheetz, M. H. (2018). Prevalence of a cefazolin inoculum effect associated with blaz gene types among methicillin-susceptible staphylococcus aureus isolates from four major medical centers in chicago. Antimicrobial Agents and Chemotherapy, 62(8). https://doi.org/10.1128/AAC.00382-18

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