Article date: June 2011
By: Saik Urien, Ghislaine Firtion, Suzanne T. Anderson, Deborah Hirt, Caroline Solas, Gilles Peytavin, Albert Faye, Isabelle Thuret, Marthe Leprevost, Carole Giraud, Hermione Lyall, Saye Khoo, Stéphane Blanche, Jean‐Marc Tréluyer, in Volume 71, Issue 6, pages 956-960
WHAT IS ALREADY KNOWN ABOUT THIS SUBJECT
• Lopinavir/ritonavir pharmacokinetics have been fully investigated in adults and children.
WHAT THIS STUDY ADDS
• Lopinavir/ritonavir population pharmacokinetics in 96 neonates and infants from birth to less than 2 years (1.16 to 10.4 kg) showed that CL/F and V/F were dependent on body weight on an allometric basis and post‐menstrual age.
AIMS Because of immature hepatic metabolism, lopinavir could present specific pharmacokinetics in the first weeks of life. We aimed at determining the optimal dosing regimen in neonates and infants weighing 1 to 10.5 kg.
METHODS Lopinavir/ritonavir (LPV/r) pharmacokinetics were studied in 96 infants using a population approach.
RESULTS A one‐compartment model described LPV/r pharmacokinetics. Normalized to a 70 kg adult using allometry, clearance (CL/F) and distribution volume (V/F) estimates were 5.87 l h−1 70 kg−1 and 91.7 l 70 kg−1. The relative bioavailabilty, F, increased with post‐menstrual age (PMA) and reached 50% of the adult value at 39.7 weeks.
CONCLUSIONS Size and PMA explained some CL/F and V/F variability in neonates/infants. Based upon trough concentration limitations, suggested LPV/r dosing regimens were 40 mg 12 h−1, 80 mg 12 h−1 and 120 mg 12 h−1 in the 1–2 kg, 2–6 kg and 6–10 kg group, respectively.
DOI: 10.1111/j.1365-2125.2011.03926.x
View this article