Approach to the prediction of the contribution of major cytochrome P450 enzymes to drug metabolism in the early drug-discovery stage

It is important to determine the cytochrome P450 (CYP) contribution of certain drugs by taking into consideration the attrition due to issues such as genetic polymorphism and inter-individual variation. In many cases in the early discovery stage, the metabolites of a new chemical have not been identified. Therefore, the present paper devised an approach in which the in vitro intrinsic clearance (CL_int) value for new chemicals was determined by measuring substrate depletion. The following prediction methods were compared to calculate CL_int using data from recombinant CYP enzymes: (1) the relative CYP content in human liver microsomes; (2) the relative activity factor (RAF) based on the V_max value; and (3) the RAF value based on the CL_int value. The most accurate prediction method was RAF based on CL_int. This method would be useful in the early drug-discovery process in cases in which the main metabolite is not identified.