The first-in-patient study for olokizumab (OKZ) employed model-based, optimal design and adaptive execution to define the concentration-C-reactive protein (CRP) suppression response. Modeling and exploratory statistics activities involved: Reverse engineering of first-in-class (tocilizumab) pharmacokinetic/pharmacodynamic (PK/PD) models, adaptation of models to OKZ with a priori knowledge and preclinical data translation, application of multidimensional Desirability Index for optimal study design, sample size reestimation based on new information, optimization of second study part via Bayesian analysis of interim data, and interim and final analysis for PK/PD objective attainment. Design work defined a dose window (0.1-3 mg/kg) for CRP suppression exploration and suggested 72 patients in five single-dose levels would suffice. During execution, new information resulted in reestimating the study size to half. Halting the first part and conducting interim analysis for second part optimization followed. Second interim and final analyses confirmed attainment of study objective, illustrating efficiency and optimality of the study. © 2014 ASCPT All rights reserved 2163-8306/14.
CITATION STYLE
Kretsos, K., Jullion, A., Zamacona, M., Harari, O., Shaw, S., Boulanger, B., & Oliver, R. (2014). Model-based optimal design and execution of the first-inpatient trial of the anti-il-6, olokizumab. CPT: Pharmacometrics and Systems Pharmacology, 3(6). https://doi.org/10.1038/psp.2014.17
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