P-429. Infants Are Not Just Little Children: Population PK Modeling Reveals Age-Dependent Differences in Cephalexin Absorption and Clearance
Andrew Haynes, Peter Anderson, Daniel Gonzalez, Kevin Messacar

TL;DR
This study shows that infants and older children process the antibiotic cephalexin differently, affecting how well it works, and suggests age-specific dosing is needed.
Contribution
A unified population PK model reveals age-dependent differences in cephalexin absorption and clearance from infancy to adolescence.
Findings
Clearance (CL) increases with weight and postmenstrual age, significantly affecting target attainment in neonates.
Slower absorption in neonates contributes to variability in drug effectiveness, especially in infants ≤28 days old.
Model-informed dosing is recommended to account for developmental changes in cephalexin pharmacokinetics.
Abstract
Cephalexin is a widely used oral antibiotic in pediatrics, but the pharmacokinetic (PK) processes driving drug exposure—particularly absorption and clearance—change with age. These maturational shifts may influence inter-individual variability (IIV) and pharmacodynamic (PD) target attainment. We developed a combined population PK (popPK) model to characterize how age-related changes in absorption rate (Ka), lag time (Tlag), and clearance (CL) affect cephalexin exposure from early infancy to adolescence.Table 1:Combined Study Population DemographicsFigure 1:Visual Predictive CheckVisual predictive check for the final PK model showing the 5th, 50th, and 95th percentiles of observed data (solid lines) and the 90% prediction intervals for the simulated data (shaded areas). Observed data are stratified by age, with the neonatal population in orange and the older pediatric cohort in purple.…
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Taxonomy
TopicsAntibiotics Pharmacokinetics and Efficacy · Pharmaceutical studies and practices · Drug Transport and Resistance Mechanisms
