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Abstract
1. A structural model of CYP3A4 is reported on the basis of a novel amino acid sequence alignment between the CYP3 family and CYP102, a bacterial P450 of known crystal structure.
2. Construction of the CYP3A4 model from CYP102 is facilitated by the relatively high sequence homology between the two proteins (52% homology; 27% identity) with many conservative amino acid changes, yielding a structure of low internal energy.
3. A considerable number of specific substrates, and some specific inhibitors, are shown to occupy the putative CYP3A4 active site via interactions with the same amino acid residues in almost all cases investigated.
4. The CYP3A4 model rationalizes the known positions of metabolism for many substrates of this major human P450 such that the route of metabolism in novel development compounds can be predicted.