José Pinheiro and Chyi-Hung Hsu
Johnson & Johnson PRD Novartis Pharmaceuticals
2010 Rutgers Biostatistics Day – Rutgers University – April 16, 2010
Collaboration with PhRMA Working Group on Adaptive Dose-Ranging Studies
Evaluating benefit of exposure-response modeling for dose finding - - PowerPoint PPT Presentation
Evaluating benefit of exposure-response modeling for dose finding and Jos Pinheiro Chyi-Hung Hsu Johnson & Johnson PRD Novartis Pharmaceuticals 2010 Rutgers Biostatistics Day Rutgers University April 16, 2010
Johnson & Johnson PRD Novartis Pharmaceuticals
2010 Rutgers Biostatistics Day – Rutgers University – April 16, 2010
Collaboration with PhRMA Working Group on Adaptive Dose-Ranging Studies
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Exposure-response in dose finding
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Exposure-response in dose finding
Response Dose
Selected doses
− Few doses − Pairwise comparisons “dose vs. placebo“ − Sample size based on power to detect DR Large uncertainty about the DR curve and the final dose estimate
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Exposure-response in dose finding
Preliminary investigations leading to collaborative work with ADRS WG
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Exposure-response in dose finding
, , 50 , max h ij SS AUC h EC h ij SS AUC E ij
+ + =
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Exposure-response in dose finding
ij
2 ~
⎟ ⎠ ⎞ ⎜ ⎝ ⎛ ) 2 ), ( ( ~ | ) (
y ij
ij ij
ij ij
ij
2 ~ | *
⎟ ⎟ ⎠ ⎞ ⎜ ⎜ ⎝ ⎛
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Exposure-response in dose finding
(σCL =50%)
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Exposure-response in dose finding
, , 50 max h i d h ij ED h i d E ij
+ + =
, 50 max h i d h ED h i d E i
+ + =
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Exposure-response in dose finding
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Exposure-response in dose finding
d
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Exposure-response in dose finding
− Sig-Emax ER models (4), all with E0=20 and Emax=100: − intrinsic PK variability (3): σCL = 30%, 50%, and 70% − PK measurement error var. (5): σU = 0%, 20%, 40%, 60%, and 80% − PD variability (2): σy = 10% and 20%
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Exposure-response in dose finding
− clinically relevant difference: Δ = 60 − posterior probability threshold: p = 0.7 − Estimates truncated at 101 mg (if > 100 mg)
σCL Model 30% 50% 70% 1 33 36 40 2 62 69 76 3 66 74 82 4 72 80 89
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Exposure-response in dose finding
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Exposure-response in dose finding
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Exposure-response in dose finding
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Exposure-response in dose finding
1 i k i i i
=
i
i
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Exposure-response in dose finding
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Exposure-response in dose finding
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Exposure-response in dose finding
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Exposure-response in dose finding
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Exposure-response in dose finding
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Exposure-response in dose finding
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Exposure-response in dose finding
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Exposure-response in dose finding
efficacy and safety DR profiles benefit/risk profile
(adaptive and fixed) to make recommendations on their use
promoting their use, when advantageous
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Exposure-response in dose finding
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Exposure-response in dose finding
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Exposure-response in dose finding
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Exposure-response in dose finding
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Exposure-response in dose finding
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Exposure-response in dose finding
2 / 1 2 2 U CL C
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Exposure-response in dose finding
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Exposure-response in dose finding
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Exposure-response in dose finding
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Exposure-response in dose finding