PT  - JOURNAL ARTICLE
AU  - Colin James Henderson
AU  - Yury Kapelyukh
AU  - Nico Scheer
AU  - Anja Rode
AU  - Aileen W McLaren
AU  - Alastair Kenneth MacLeod
AU  - De Lin
AU  - Jayne Wright
AU  - Lesley Stanley
AU  - C Roland Wolf
TI  - An extensively humanised mouse model to predict pathways of drug disposition, drug/drug interactions, and to facilitate the design of clinical trials
AID  - 10.1124/dmd.119.086397
DP  - 2019 Jan 01
TA  - Drug Metabolism and Disposition
PG  - dmd.119.086397
4099  - http://dmd.aspetjournals.org/content/early/2019/03/25/dmd.119.086397.short
4100  - http://dmd.aspetjournals.org/content/early/2019/03/25/dmd.119.086397.full
AB  - Species differences in drug metabolism and disposition can confound the extrapolation of in vivo pharmacokinetic data to man, and also profoundly compromise drug efficacy studies due to differences in pharmacokinetics, in metabolites produced (which are often pharmacologically active) and in differential activation of the transcription factors CAR and PXR which regulate the expression of enzymes such as P450s and drug transporters. These differences have gained additional importance as a consequence of the use of genetically modified mouse models for drug efficacy testing and also patient-derived xenografts to predict individual patient responses to anti-cancer drugs. A number of humanised mouse models for cytochrome P450s, CAR and PXR have been reported. However, the utility of these models has been compromised as a consequence of the redundancy of P450 reactions across gene families where the remaining murine P450s can metabolise the compounds being tested. To remove this confounding factor and create a mouse model which more closely reflects human pathways of drug disposition we have substituted 33 murine P450s from the major gene families involved in drug disposition, together with Car and Pxr, for human CAR, PXR, CYP1A1, CYP1A2, CYP2C9, CYP2D6, CYP3A4 and CYP3A7. We have also created a mouse line where 34 P450s have been deleted from the mouse genome. We demonstrate using model compounds and anti-cancer drugs how these mouse lines can be applied to predict drug-drug interactions in patients and discuss their potential application in the more informed design of clinical trials and the personalised treatment of cancer.