Dear NONMEM users,
Currently I am working on the simulation of a bio-equavalence trial. For
the reference compound a population PK model has been derived on basis
of data from 100 patients. Values for between-and within-patient
variability are available for all PK parameters. The simulation
comprises a randomized cross-over study with 12 patients taking the
test and reference compound. Two-hunderd trials are simulated and
summarized. During the simulations I noticed that truncation of the
simulated of PK parameters significantly influences the power of the
study to confirm bio-equivalence. For instance truncation of simulated
oral clearances of both compounds from a range of 1-300 L/hr to 5 - 30
L/hr doubled the number of positive trials (due to decreased within-
patient variability). Post-hoc estimates form the popPK study indicated
that clearance values of the reference compound are all within the
latter range of 5 to 30 L/hr. I expect that oral clearance of the test
compound will not differ more than 5% from the reference compound. In my
opinion simulation of trials with the smallest range will produce more
reliable estimates of the power to detect bio-equivalence.
I would greatly appreciate your comments on this subject.
Best regards,
Ron Mathôt
Department of Hospital Pharmacy and Clincal Pharmacology
Erasmus University Medical Center
Rotterdam
The Netherlands
Received on Tue Apr 22 2008 - 15:17:47 EDT
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