TY - JOUR T1 - Predictions of Hepatic Disposition Properties Using a Mechanistically Realistic, Physiologically Based Model JF - Drug Metabolism and Disposition JO - Drug Metab Dispos SP - 759 LP - 768 DO - 10.1124/dmd.107.019067 VL - 36 IS - 4 AU - Li Yan AU - Shahab Sheihk-Bahaei AU - Sunwoo Park AU - Glen E. P. Ropella AU - C. Anthony Hunt Y1 - 2008/04/01 UR - http://dmd.aspetjournals.org/content/36/4/759.abstract N2 - Quantitative mappings were established between drug physicochemical properties (PCPs) and parameter values of a physiologically based, mechanistically realistic, in silico liver (ISL). The ISL plugs together autonomous software objects that represent hepatic components at different scales and levels of detail. Microarchitectural features are represented separately from the mechanisms that influence drug metabolism. The same ISL has been validated against liver perfusion data for sucrose and four cationic drugs: antipyrine, atenolol, labetalol, and diltiazem. Parameters sensitive to drug-specific PCPs were tuned so that ISL outflow profiles from a single ISL matched in situ perfused rat liver outflow profiles of all five compounds. Quantitative relationships were then established between the four sets of drug PCPs and the corresponding four sets of PCP-sensitive, ISL parameter values; those relationships were used to predict PCP-sensitive, ISL parameter values for prazosin and propranolol given only their PCPs. Relationships were established using three different methods: 1) a simple linear correlation method, 2) the fuzzy c-means algorithm, and 3) a simple artificial neural network. Each relationship was used separately to predict ISL parameter values for prazosin and propranolol, given their PCPs. Those values were applied in the ISL used earlier to predict the hepatic disposition details for each drug. Although we had only sparse data available, all predicted disposition profiles were judged reasonable (within a factor of 2 of referent profile data). The order of precision, based on a similarity measure, was 3 > 2 > 1. ER -