Risk of Potentially Neurotoxic Exposure in Infants Under High-Dose Cefepime Treatment—A Pharmacometric Simulation Study

Risk of Potentially Neurotoxic Exposure in Infants Under High-Dose Cefepime Treatment—A Pharmacometric Simulation Study

<b>Background:</b> Optimal dosing of cefepime in infants 1–2 months remains undefined. <b>Objectives</b>: We aimed to quantify the risk of potentially neurotoxic exposure with high-dose cefepime (50 mg/kg/8 h) in infants 1–2 months of age, as compared to adjacent age groups (...

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Bibliographic Details
Main Authors: Verena Gotta, Chantal Csajka, Antonia Glauser, Christoph Berger, Marc Pfister, Paolo Paioni
Format: Article
Language:English
Published: MDPI AG 2025-04-01
Series:Pharmaceutics
Subjects:
cefepime
neurotoxicity
infants
neonates
children
pharmacokinetics
Online Access:https://www.mdpi.com/1999-4923/17/5/544
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Summary:<b>Background:</b> Optimal dosing of cefepime in infants 1–2 months remains undefined. <b>Objectives</b>: We aimed to quantify the risk of potentially neurotoxic exposure with high-dose cefepime (50 mg/kg/8 h) in infants 1–2 months of age, as compared to adjacent age groups (neonates, infants 2–12 months) and lower dose treatment (50 mg/kg/12 h). <b>Methods</b>: Pharmacometric simulations were performed using two published population pharmacokinetic models combined with demographic data, including serum creatinine, for neonates and infants ≤ 12 months. Adult-derived safety thresholds for potential neurotoxicity were defined as steady-state trough concentration (C<sub>trough</sub>) > 20 or > 35 mg/L, respectively. The corresponding probability of target attainment (PTA) was calculated as free concentration, 50% of the time during the dosing interval above the minimal inhibitory concentration (MIC) breakpoint of 8 mg/L (<i>Pseudomonas</i> spp.) (50% fT>MIC<sub>8mg/L</sub>). <b>Results</b>: The predicted risk of C<sub>trough</sub> > 20 (>35) mg/L under high-dose cefepime was 40–54% (12–22%) in infants 1–2 months while providing high PTA (100%). It was predicted to be 1.3–1.7 fold higher in neonates (model 1), and reduced 1.8–2.4 fold in infants 2–12 months (model 1), or to be similar (model 2), respectively. Both models predicted approximately 2–4 fold reduced risk using lower dose treatments while maintaining high PTA (≥97%). <b>Conclusions</b>: The risk of potential neurotoxic concentrations in infants > 1 month treated with cefepime 50 mg/kg/8 h is high if defined by adult safety thresholds. Lower dose cefepime in infants 1–2 months could be a safe option without compromising PTA, if defined as 50% fT>MIC<sub>8mg/L</sub>. Achievement of 100% fT>MIC<sub>8mg/L</sub> may require prolonged infusion time even under high-dose treatment. Future research is required to evaluate potentially age-dependent safety thresholds.
ISSN:1999-4923

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