MRP3 is an ABC transporter localized in the basolateral membrane of epithelial cells such as hepatocytes and enterocytes. In this study, the role of Mrp3 in drug disposition was investigated. Because Mrp3 preferentially transports glucuronide conjugates, we investigated the in vivo disposition of acetaminophen (APAP) and its metabolites. Mrp3 ؉/؉ and Mrp3 ؊/؊ knockout mice received APAP (150 mg/kg), and bile was collected. Basolateral and canalicular excretion of APAP was also assessed in the isolated perfused liver. In separate studies, mice received 400 mg APAP/kg for assessment of hepatotoxicity. No differences were found in the biliary excretion of APAP, APAP-sulfate, and APAPglutathione between Mrp3 ؉/؉ and Mrp3 ؊/؊ mice. However, 20-fold higher accumulation of APAPglucuronide (APAP-GLUC) was found in the liver of Mrp3 ؊/؊ mice. Concomitantly, plasma APAP-GLUC content in Mrp3 ؊/؊ mice was less than 10% of that in Mrp3 ؉/؉ mice. In addition, APAP-GLUC excretion in bile of Mrp3 ؊/؊ mice was tenfold higher than in Mrp3 ؉/؉ mice. In the isolated perfused liver, we also found a strong decrease of APAP-GLUC secretion into the perfusate of Mrp3 ؊/؊ livers. Plasma alanine aminotransferase (ALT), aspartate aminotransferase (AST), and histopathology showed that Mrp3 ؊/؊ mice are more resistant to APAP hepatotoxicity than Mrp3 ؉/؉ mice, which is most likely a result of the faster repletion of hepatic GSH. Substrates exported from hepatocytes by MRP1-3 include conjugates of glutathione, glucuronide, and sulfate as well as organic amphiphilic anions. MRP3, which is expressed in liver and gastrointestinal tract, 2,3 prefers glucuronide over glutathione conjugates. 4,5 Mice lacking Mrp3 were recently developed; these mice are viable, fertile, and have no apparent phenotype. 2 Because of the potential role of Mrp3 in basolateral secretion of glucuronidated drugs, the disposition of acetaminophen (APAP) in Mrp3 Ϫ/Ϫ mice was investigated.Acetaminophen is a popular analgesic and antipyretic that can produce acute liver failure with excessive dosing. 6,7 This drug is metabolized in the liver by conjugation with glucuronic acid and sulfate, while a reactive metabolite generated by CYP450 is detoxified by conjugation Abbreviations: MRP, multidrug resistance protein; APAP, acetaminophen; GSH,
