Bioequivalence and Bioavailability Forum • half-life in multiple-dosed steady-state BE/BA study?

half-life in multiple-dosed steady-state BE/BA study? [NCA / SHAM]

posted by yjlee168 – Kaohsiung, Taiwan, 2009-07-14 16:16 (5393 d 00:15 ago) – Posting: # 3954
Views: 16,387

Dear All,

I just like to know if it is reasonable to estimate lambda_z when doing data analysis of a multiple-dosed steady-state (SS) BE/BA study. It is because we just collect the plasma/blood sample within one dosing interval (Tau) at steady-state in a multiple-dosed BE/BA study. It looks like there is no such terminal phase at all in multiple-dosed BE/BA study. If it is not reasonable, is there any way to estimate the elimination rate constant (k_el), half-life, V_ss or the accumulation index? In WinNonlin v5.x, lambda_z still needs to be estimated first for further calculations of other NCA parameters. Thanks in advanced.

—
All the best,
-- Yung-jin Lee
bear v2.9.1:- created by Hsin-ya Lee & Yung-jin Lee
Kaohsiung, Taiwan https://www.pkpd168.com/bear
Download link (updated) -> here

Complete thread:

half-life in multiple-dosed steady-state BE/BA study?yjlee168 2009-07-14 14:16
- half-life in steady state; WinNonlin Helmut 2009-07-15 15:09
  - no lambda(z), no NCA? yjlee168 2009-07-16 11:53
    - NCA without lambda(z) Helmut 2009-07-16 14:06
      - No rule is the rule - lambda(z) of MD BE yjlee168 2009-07-16 22:17
  - Distinguish accumulation oksanachlebko 2018-01-05 00:10