Table 1.
A chart comparing the properties of 3 different chimeric mouse models is shown. The genes and type of immune deficit (adaptive and/or innate), mechanism of induction and the duration of liver injury resulting from the indicated knockout (−/−) or transgene (tg), presence of systemic toxicity, requirement for ongoing drug treatment, and selected references relating to the production of the model or use in drug metabolism are shown.
| Model |
Immune Compromise |
Liver Injury |
Systemic Toxicity |
Ongoing Drug Rx |
Selected References |
|---|---|---|---|---|---|
| uPA/SCID | Adaptive (SCID) | continuous uPA tg | Renal Bleeding | Immune Suppressive | 9–12 |
| FRG | Innate (Il2rg−/−) Adaptive (Rag2−/−) |
continuous Fah−/− | None | NTBC | 15 |
| TK-NOG | Innate Adaptive (Il2rg−/− SCID) |
time limited TK tg | None | None | 18,19,20 |