Pharmacokinetic study of single doses of oral fludarabine phosphate in patients with "low-grade" non-Hodgkin's lymphoma and B-cell chronic lymphocytic leukemia

Authors
Foran, JM Oscier, D Orchard, J Johnson, SA Tighe, M Cullen, MH de Takats, PG Kraus, C Klein, M Lister, TA
Citation
Jm. Foran et al., Pharmacokinetic study of single doses of oral fludarabine phosphate in patients with "low-grade" non-Hodgkin's lymphoma and B-cell chronic lymphocytic leukemia, J CL ONCOL, 17(5), 1999, pp. 1574-1579
Citations number
24
Categorie Soggetti
Oncology,"Onconogenesis & Cancer Research
Journal title
JOURNAL OF CLINICAL ONCOLOGY
ISSN journal
0732183X → ACNP
Volume
17
Issue
5
Year of publication
1999
Pages
1574 - 1579
Database
ISI
SICI code
0732-183X(199905)17:5<1574:PSOSDO>2.0.ZU;2-B
Abstract
Purpose: Fludarabine phosphate (F-AMP), a purine analog, requires daily int ravenous administration. A pharmacokinetic study of an oral formulation (10 mg immediate-release tablet) was undertaken in patients with "low-grade" n on-Hodgkin's lymphoma and B-cell chronic lymphocytic leukemia. Patients and Methods Oral F-AMP was incorporated into the "conventional" tr eatment schedule. Single oral trial doses of 50, 70, and 90 mg of F-AMP wer e given on the first day of three cycles of treatment; a comparative 50-mg intravenous trial dose was given on the first day of the fourth cycle, Intr avenous F-AMP (25 mg/m(2)) war given on days 2 to 5 at 4-week intervals. Ph armacokinetic samples taken after each trial dose were analyzed for plasma 2-fluoro-arabinofuranosyladenine (2F-ara-A) concentration (its main metabol ite); area under the curve 0 to 24 hours (AUC(0-24h)) and maximum concentra tion (C-max) were calculated. Eighteen patients received all three oral tri al doses, and bioavailability was determined in 15 patients who completed f our courses of therapy. Results: Oral administration of F-AMP resulted in a dose-dependent increase in C-max and AUC(0-24h) of 2F-ara-A and achieved an AUC(0-24h) similar to intravenous administration, although at a lower C-max. The linear increase in mean AUC(0-24h) by factors of 1.36 +/- 0.22 (mean +/- SD) and 1.72 +/- 0 .31 corresponded well with the increase in oral dose from 50 to 70 mg (fact or of 1.4) and 90 mg (factor of 1.8), respectively. Bioavailability (approx imately 55%, with low intraindividual variation) and time to C-max were dos e independent. Conclusion: Oral doses of F-AMP can achieve an AUC(0-24h) of 2F-ara-A simil ar to intravenous administration, with dose-independent bioavailability, Th e tablet will greatly enhance the use of F-AMP in a palliative setting. J C lin Oncol 17:1574-1579. (C) 1999 by American Society of Clinical Oncology.