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This research examines cefazolin target attainment in MSSA isolates with and without the inoculum effect.

January 14, 2026Open Access

Comparative Analysis of Cefazolin Target Attainment in Methicillin-Susceptible Staphylococcus aureus (MSSA) Isolates With and Without the Cefazolin Inoculum Effect (CzIE)

Key Points

This research examines cefazolin target attainment in MSSA isolates with and without the inoculum effect.
Single-center, retrospective review of adults with MSSA bacteremia.
Included patients received cefazolin and had steady-state serum cefazolin concentrations.
CzIE defined as increased MIC at high inoculum compared to standard inoculum.
CzIE isolates had lower cefazolin pharmacodynamic target attainment at high inoculum.
17.6% of isolates exhibited CzIE with significant differences in MIC levels.
Therapeutic drug monitoring may help in optimizing cefazolin dosing.

Abstract

Abstract Background Clinical failures with cefazolin have been linked to the CzIE where increased bacterial inoculum leads to elevated cefazolin minimum inhibitory concentrations (MICs) against MSSA. The role of therapeutic drug monitoring (TDM) in optimizing cefazolin dosing in the context of the CzIE remains unclear. This study aimed to determine the prevalence of the CzIE and compare cefazolin pharmacokinetic/pharmacodynamic (PK/PD) target attainment in MSSA isolates with and without the CzIE. Methods A single-center, retrospective review included adults (≥18 years) with MSSA bacteremia admitted between Jun 2021–Dec 2023 who received cefazolin and had steady-state serum cefazolin concentrations. CzIE was defined as a cefazolin MIC ≥16 µg/mL at high inoculum (10⁷ CFU/mL) and ≤8 µg/mL at standard inoculum (10⁵ CFU/mL). Total cefazolin concentrations were adjusted for 80% protein binding. PK/PD targets were 100%fT≥MIC and 100%fT≥4×MIC (100% free drug time above MIC or 4x MIC, respectively). Results Among 51 patients included in the analysis, median age was 61 years (IQR, 39.5–70.5). Common bacteremia sources included endocarditis (n=11, 21.6%), musculoskeletal (n=11, 21.6%), and pneumonia (n=9, 17.6%). Nine isolates (17.6%) exhibited the CzIE and 32 (62.7%) were blaZ-positive. Median cefazolin trough was 5.9 µg/mL (IQR, 3.2–11.6) in CzIE infected vs. 4.2 µg/mL (IQR, 2.5–10.4) in patients infected with a non-CzIE isolate. In CzIE isolates, modal MICs were 1 µg/mL at standard inoculum and 16 µg/mL at high inoculum; in non-CzIE, both were 0.5 µg/mL. In the CzIE group at standard inoculum, 100% (n=9) achieved 100%fT≥MIC and 66.7% (n=6) achieved 100%fT≥4×MIC; at high inoculum, 11.1% (n=1) achieved 100%fT≥MIC and none achieved 100%fT≥4×MIC. In the non-CzIE group at standard inoculum, 88.1% (n=37) achieved 100%fT≥MIC and 73.8% (n=31) achieved 100%fT≥4×MIC; at high inoculum 88.1% (n=37) achieved 100%fT≥MIC and 61.9% (n=26) achieved 100%fT≥4×MIC. Conclusion Cefazolin PK/PD target attainment was markedly reduced in patients with CzIE isolates at high inoculum. These findings underscore the potential utility of TDM in detecting suboptimal cefazolin exposure and the need to consider alternative dosing strategies in this setting. Disclosures Cesar A. Arias, MD/PhD, UptoDate: Royalties

Comparative Analysis of Cefazolin Target Attainment in Methicillin-Susceptible Staphylococcus aureus (MSSA) Isolates With and Without the Cefazolin Inoculum Effect (CzIE)

Key Points

Abstract

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