PK/PD modeling to characterize placebo and treatment effect of omalizumab for chronic spontaneous urticaria

Author:

Oh Elise1,Wada Russ2,Le Kha1,Zheng Yanan1,Jin Jin1,Poon Victor1,Wong Kit3,Owen Ryan1,Yoshida Kenta1ORCID

Affiliation:

1. Department of Clinical Pharmacology Genentech, Inc. South San Francisco California USA

2. Quantitative Solutions Inc. Menlo Park California USA

3. OMNI Biomarker Development Genentech, Inc. South San Francisco California USA

Abstract

AbstractThe pharmacokinetic (PK) characteristics of omalizumab and its pharmacodynamic (PD) effect in patients has yet to be fully characterized in chronic spontaneous urticaria, which could elucidate its pathogenesis and treatment response. This study has two objectives; (1) characterize the population PK of omalizumab and its PD effect on IgE, and (2) develop a drug effect model of omalizumab in urticaria (via change in weekly itch severity score). The target‐mediated population of PK/PD model incorporating omalizumab‐IgE binding and turnover adequately described PK and PD of omalizumab. The effect compartment model and linear drug effect and additive placebo response adequately described placebo and treatment effects of omalizumab. Several baseline covariates were identified for PK/PD and drug effect models. The developed model has the potential to aid in understanding variability in PK/PD as well as response to omalizumab treatment.

Publisher

Wiley

Subject

Pharmacology (medical),Modeling and Simulation

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