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Hi Helmut,
I don't think the proposed scheme is good enough for modelling such difficult things. There are no Ctau's planned. Moreover, I would mix the A and B for that purpose.
And sorry for a broken link, I cannot carve in my mind that tags for years
❝ ❝ B) Capture day 1 PK from time 0 to end of dosing interval, repeat dosing for x # of days (base on dosing interval) to hit SS. On last day of dosing capture time 0 - x (x = whatever hrs needed to fully capture the elimination phase + half-life).
❝
❝ To characterize the PK of a new drug by PK modeling you would always go with this approach and sample as long as possible. Funky things may happen in nonlinear PK (auto-induction / -inhibition, capacity-limited elimination, …)
I don't think the proposed scheme is good enough for modelling such difficult things. There are no Ctau's planned. Moreover, I would mix the A and B for that purpose.
And sorry for a broken link, I cannot carve in my mind that tags for years
—
Kind regards,
Mittyri
Kind regards,
Mittyri
Complete thread:
- Study which captures SD and SS PK Profiles jag009 2020-02-03 20:15
![[Mix]](https://static.bebac.at/img/mix.png "open in Mix view")
- A vs B mittyri 2020-02-03 21:05
- A vs B jag009 2020-02-03 21:29
- ANDA or NDA? Helmut 2020-02-04 00:57
- Modellingmittyri 2020-02-04 09:02
- Modelling Helmut 2020-02-04 12:17
- Modelling: SD+SS mittyri 2020-02-04 12:38
- Modelling Helmut 2020-02-04 12:17
- Modellingmittyri 2020-02-04 09:02
- A vs B mittyri 2020-02-03 21:05
Ing. Helmut Schütz