Roy
☆    

India,
2020-06-12 10:44
(1406 d 13:18 ago)

Posting: # 21529
Views: 1,677
 

 Pre-Dose sample required to steady state [Regulatives / Guidelines]

Dear All,

Please Help!!!

Please find Below detail for my question,


Design: two-treatment, two-period, two-sequence, two-way crossover, multiple-dose, steady state, oral bioequivalence study.

Dosing Day: Day 1 to Day 8.

Blood Sample collection on: Day 4 to Last time Point for both period.

Wash out: 10 Days.


Question:

Pre-dose Blood sample collection for Day1, Day2 and Day3 are required?



Thanks in advance.
Helmut
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Vienna, Austria,
2020-06-12 12:17
(1406 d 11:45 ago)

@ Roy
Posting: # 21530
Views: 1,430
 

 Achievement of steady state

Hi Roy,

❝ Please Help!!!


Is your  !  key jammed?

❝ Please find Below detail for my question,


Since you posted in this category, see also this post #3. Please do your homework first.

Dosing Day: Day 1 to Day 8.

Blood Sample collection on: Day 4 to Last time Point for both period.


You mean on days 4 and 8, right?

Wash out: 10 Days.


Doesn’t make sense. If you attain (pseudo) steady state on day 4, you can immediately switch to the other treatment. EMA MR-GL (2014):

In steady-state studies, the washout period of the previous treatment can overlap with the build-up of the second treatment (direct switching), provided the build-up period is sufficiently long (at least 5 times the terminal half-life).


❝ Pre-dose Blood sample collection for Day1, Day2 and Day3 are required?


On all days.
EMA:

Whether the steady-state has been achieved is assessed by comparing at least three pre-dose concentrations for each formulation. The apparent half-life should also be taken into account.

FDA ANDA draft (2013):

We recommend that if a steady-state study is recommended, applicants carry out appropriate dosage administration and sampling to document the attainment of steady-state.


There was a consensus at two GBHI-workshops (Amsterdam, April 2018; Bethesda, December 2019) that a statistical assessment is not required. See this presentation.

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