Publication | Closed Access
Modulation of Acetaminophen-Induced Hepatotoxicity by the Xenobiotic Receptor CAR
313
Citations
22
References
2002
Year
Xenobiotic Receptor CarHealth SciencesBiochemistryPharmacological StudyMedicineLiver PhysiologyCar ActivityToxicologyPharmacotherapyCar Null MiceHepatotoxicityPharmacologyDrug-induced Liver InjuryToxicological MechanismDrug DiscoveryDrug Resistance
We have identified the xenobiotic receptor CAR (constitutive androstane receptor) as a key regulator of acetaminophen metabolism and hepatotoxicity. Known CAR activators as well as high doses of acetaminophen induced expression of three acetaminophen-metabolizing enzymes in wild-type but not in CAR null mice, and the CAR null mice were resistant to acetaminophen toxicity. Inhibition of CAR activity by administration of the inverse agonist ligand androstanol 1 hour after acetaminophen treatment blocked hepatotoxicity in wild type but not in CAR null mice. These results suggest an innovative therapeutic approach for treating the adverse effects of acetaminophen and potentially other hepatotoxic agents.
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