Author: Verscheijden, Laurens F. M.; van der Zanden, Tjitske M.; van Bussel, Lianne P. M.; de Hoopâ€Sommen, Marika; Russel, Frans G. M.; Johnson, Trevor N.; de Wildt, Saskia N.
Title: Chloroquine Dosing Recommendations for Pediatric COVIDâ€19 Supported by Modeling and Simulation Cord-id: 5n55yl2s Document date: 2020_5_21
ID: 5n55yl2s
Snippet: As chloroquine (CHQ) is part of the Dutch Centre for Infectious Disease Control coronavirus disease 2019 (COVIDâ€19) experimental treatment guideline, pediatric dosing guidelines are needed. Recent pediatric data suggest that existing World Health Organization (WHO) dosing guidelines for children with malaria are suboptimal. The aim of our study was to establish bestâ€evidence to inform pediatric CHQ doses for children infected with COVIDâ€19. A previously developed physiologicallyâ€based ph
Document: As chloroquine (CHQ) is part of the Dutch Centre for Infectious Disease Control coronavirus disease 2019 (COVIDâ€19) experimental treatment guideline, pediatric dosing guidelines are needed. Recent pediatric data suggest that existing World Health Organization (WHO) dosing guidelines for children with malaria are suboptimal. The aim of our study was to establish bestâ€evidence to inform pediatric CHQ doses for children infected with COVIDâ€19. A previously developed physiologicallyâ€based pharmacokinetic (PBPK) model for CHQ was used to simulate exposure in adults and children and verified against published pharmacokinetic data. The COVIDâ€19 recommended adult dosage regimen of 44 mg/kg total was tested in adults and children to evaluate the extent of variation in exposure. Based on differences in area under the concentrationâ€time curve from zero to 70 hours (AUC(0–70h)) the optimal CHQ dose was determined in children of different ages compared with adults. Revised doses were reâ€introduced into the model to verify that overall CHQ exposure in each age band was within 5% of the predicted adult value. Simulations showed differences in drug exposure in children of different ages and adults when the same bodyâ€weight based dose is given. As such, we propose the following total cumulative doses: 35 mg/kg (CHQ base) for children 0–1 month, 47 mg/kg for 1–6 months, 55 mg/kg for 6 months–12 years, and 44 mg/kg for adolescents and adults, not to exceed 3,300 mg in any patient. Our study supports ageâ€adjusted CHQ dosing in children with COVIDâ€19 in order to avoid suboptimal or toxic doses. The knowledgeâ€driven, modelâ€informed dose selection paradigm can serve as a scienceâ€based alternative to recommend pediatric dosing when pediatric clinical trial data is absent.
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