Pharmacokinetics of fexofenadine: Evaluation of a microdose and assessment of absolute oral bioavailability
2010; Elsevier BV; Volume: 40; Issue: 2 Linguagem: Inglês
10.1016/j.ejps.2010.03.009
ISSN1879-0720
AutoresGraham Lappin, Yoko Shishikura, Roeline Jochemsen, Richard Weaver, Charlotte Gesson, Brian Houston, B. Oosterhuis, Ole J. Bjerrum, Malcolm Rowland, Colin Garner,
Tópico(s)Antibiotics Pharmacokinetics and Efficacy
ResumoA human pharmacokinetic study was performed to assess the ability of a microdose to predict the pharmacokinetics of a therapeutic dose of fexofenadine and to determine its absolute oral bioavailability. Fexofenadine was chosen to represent an unmetabolized transporter substrate (P-gP and OATP). Fexofenadine was administered to 6 healthy male volunteers in a three way cross-over design. A microdose (100 μg) of 14C-drug was administered orally (period 1) and intravenously by 30 min infusion (period 2). In period 3 an intravenous tracer dose (100 μg) of 14C-drug was administered simultaneously with an oral unlabelled therapeutic dose (120 mg). Plasma was collected from all 3 periods and analysed for both total 14C content and parent drug by accelerator mass spectrometry (AMS). For period 3, plasma samples were also analysed using HPLC-fluorescence to determine total drug concentration. Urine was collected and analysed for total 14C. Good concordance between the microdose and therapeutic dose pharmacokinetics was observed. Microdose: CL 13 L/h, CLR 4.1 L/h, Vss 54 L, t1/2 16 h; therapeutic dose: CL 16 L/h, CLR 6.2 L/h, Vss 64 L, t1/2 12 h. The absolute oral bioavailability of fexofenadine was 0.35 (microdose 0.41, therapeutic dose 0.30). Despite a 1200-fold difference in dose of fexofenadine, the microdose predicted well the pharmacokinetic parameters following a therapeutic dose for this transporter dependent compound.
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