Daunorubicin and Its Active Metabolite Pharmacokinetic Profiles in Acute Myeloid Leukaemia Patients: A Pharmacokinetic Ancillary Study of the BIG-1 Trial
Guillaume Drevin,
Marie Briet,
Caroline Bazzoli,
Emmanuel Gyan,
Aline Schmidt,
Hervé Dombret,
Corentin Orvain,
Aurelien Giltat,
Christian Recher,
Norbert Ifrah,
Philippe Guardiola,
Mathilde Hunault-Berger,
Chadi Abbara
Affiliations
Guillaume Drevin
Service de Pharmacologie-Toxicologie et Pharmacovigilance, Centre Hospitalo-Universitaire d’Angers, F-49100 Angers, France
Marie Briet
Service de Pharmacologie-Toxicologie et Pharmacovigilance, Centre Hospitalo-Universitaire d’Angers, F-49100 Angers, France
Caroline Bazzoli
Grenoble INP, TIMC-IMAG, Université Grenoble Alpes, CNRS, F-38000 Grenoble, France
Emmanuel Gyan
Service d’Hématologie et Thérapie Cellulaire, Equipe LNOx, ERL CNRS 7001, Centre Hospitalier Universitaire, Université de Tours, F-37000 Tours, France
Aline Schmidt
UFR Santé, Université Angers, F-49100 Angers, France
Hervé Dombret
Blood Disease Department, University Hospital Saint Louis AP-HP, F-75010 Paris, France
Corentin Orvain
Fédération Hospitalo-Universitaire GOAL, F-49033 Angers, France
Aurelien Giltat
Fédération Hospitalo-Universitaire GOAL, F-49033 Angers, France
Christian Recher
Insitut Universitaire du Cancer de Toulouse Oncolpole, Unversité Toulouse III Paul Sabatier, F-31000 Toulouse, France
Norbert Ifrah
UFR Santé, Université Angers, F-49100 Angers, France
Philippe Guardiola
UFR Santé, Université Angers, F-49100 Angers, France
Mathilde Hunault-Berger
UFR Santé, Université Angers, F-49100 Angers, France
Chadi Abbara
Service de Pharmacologie-Toxicologie et Pharmacovigilance, Centre Hospitalo-Universitaire d’Angers, F-49100 Angers, France
Daunorubicin pharmacokinetics (PK) are characterised by an important inter-individual variability, which raises questions about the optimal dose regimen in patients with acute myeloid leukaemia. The aim of the study is to assess the joint daunorubicin/daunorubicinol PK profile and to define an optimal population PK study design. Fourteen patients were enrolled in the PK ancillary study of the BIG-1 trial and 6–8 samples were taken up to 24 h after administration of the first dose of daunorubicin (90 mg/m2/day). Daunorubicin and daunorubicinol quantifications were assessed using a validated liquid chromatography technique coupled with a fluorescence detector method. Data were analysed using a non-compartmental approach and non-linear mixed effects modelling. Optimal sampling strategy was proposed using the R function PFIM. The median daunorubicin and daunorubicinol AUC0-tlast were 577 ng/mL·hr (Range: 375–1167) and 2200 ng/mL·hr (range: 933–4683), respectively. The median metabolic ratio was 0.32 (range: 0.1–0.44). Daunorubicin PK was best described by a three-compartment parent, two-compartment metabolite model, with a double first-order transformation of daunorubicin to metabolite. Body surface area and plasma creatinine had a significant impact on the daunorubicin and daunorubicinol PK. A practical optimal population design has been derived from this model with five sampling times per subject (0.5, 0.75, 2, 9, 24 h) and this can be used for a future population PK study.
