Hi Everybody,
I am planning a multiple dose generic study vs. PR product which could be taken once or twice daily. The new EMA MR guidance does not specificaly deal with this sort of case.
I have a few questions:
- Is there a preference from a regulatory point of view whether to design the study as BID or QD? I had seen some generic PARs for this product having QD dosing, however, they are older than 2010…
- If there is no regulatory preference, what would be better from study design and PK perspective?
- I believe QD would be better ethically
- I was thinking that QD dosing would better allow to show BE in case profiles of test and reference are somewhat different. Is my assumption correct?
- On the other hand, is it possible that ISCV of Cτ following QD would be more variable than Cτ following BID, as concentration is lower?
- Are there other points I should take into consideration upon deciding?
Thanks in advance for your response,
Kind regards,
Nisha
Edit: Category changed.
[Helmut]
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Ing. Helmut Schütz