This case study shows how integrated PK/PD modeling with machine learning supported compound selection in a complex CNS program involving delayed efficacy and heterogeneous preclinical studies. Using Phoenix NLME, a unified mechanistic framework enabled objective cross compound comparisons and translational decision making. The analysis demonstrated that the most potent compound was not necessarily the optimal choice for first in human studies, leading to confident selection of the candidate with the most favorable overall pharmacological profile.
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