Abstract
- A database of 62 drugs including oral bioavailability (F%) and dose was constructed
- All compounds’ reported major clearance pathways (MCP) were CYP-mediated1
- For 43 drugs with more than one reported value of F%, the average experimental CV% was 29%
- Reported F% values2 varied from 3% (fluphenazine) to 99% (diazepam, galantamine, glimepiride, indomethacin, and tamsulosin), with an average of 60%
- F% was predicted by integrating quantitative structure activity relationship (QSAR) model predictions3 and physiologically based pharmacokinetic (PBPK) simulations 4
- A 35-year-old American male physiology was use for all PBPK simulations
- All molecules were predicted to be substrates of the CYP associated with their MCP
- In 42 of the 62 molecules, the CYP isoform with highest predicted intrinsic clearance (CLint) was the same as the MCP
- Overall, 68% of the molecules were predicted within 2-fold of their reported F%
- Scaling Vmax by the CYP substrate model’s confidence estimate resulted in fewer underpredictions
13th European ISSX Meeting, June 22-25, 2015, Glasgow, Scotland
By Michael Lawless, John DiBella, Michael B. Bolger, Robert D. Clark, Eva Huehn, Marvin Waldman, Jinhua Zhang, Viera Lukacova