Vet BE Guideline [Power / Sample Size]

posted by mittyri – Russia, 2024-02-05 17:49 (252 d 17:24 ago) – Posting: # 23857
Views: 2,420

Hi Helmut and BEQool!

❝ ❝ France and Ireland - however, it was for veterinary product

❝ This might explain it. The last time I read the vet-GL it was crap (politely speaking).


That's interesting how CHMP EMA Guidelines invade CVMP Guidelines. I am trying to catch the logic:

For substances with highly variable disposition where it is difficult to show bioequivalence due to high intra-individual variability, different alternative designs have been suggested in the literature (e.g. replicate study design). A replicate cross-over study design using 3 periods (partial replication where only the reference product is replicated in all animals) or 4 periods (full replication, where each subject receives the test and reference products twice) can be carried out.
So CVMP people have some concerns about other designs we don't know yet.:-D

Kind regards,
Mittyri

Complete thread:

UA Flag
Activity
 Admin contact
23,258 posts in 4,886 threads, 1,671 registered users;
75 visitors (0 registered, 75 guests [including 10 identified bots]).
Forum time: 12:13 CEST (Europe/Vienna)

Tortured data will confess to anything.    Fredric Menger

The Bioequivalence and Bioavailability Forum is hosted by
BEBAC Ing. Helmut Schütz
HTML5