Literature DB >> 19246624

Altered disposition of acetaminophen in Nrf2-null and Keap1-knockdown mice.

Scott A Reisman1, Iván L Csanaky, Lauren M Aleksunes, Curtis D Klaassen.   

Abstract

Acetaminophen (AA) is a widely used antipyretic drug that causes hepatotoxicity at high doses. Nuclear factor erythroid 2-related factor 2 (Nrf2) is a transcription factor that mitigates electrophilic stress from AA by inducing genes, such as NAD(P)H:quinone oxidoreductase 1 (Nqo1), multidrug resistance-associated proteins (Mrps), and glutathione (GSH) synthesis enzymes. To determine whether Nrf2 activation alters the biotransformation and excretion of AA, male wild-type, Nrf2-null, and Keap1 (Kelch-like ECH-associated protein 1)-knockdown (Keap1-kd) mice (which have increased activation of Nrf2) were administered a single subtoxic dose of AA (50 mg/kg, iv), after which, AA and its metabolites (AA-glucuronide [AA-GLUC]; AA-sulfate [AA-SULF]; AA-glutathione [AA-GSH]) were quantified in plasma, bile, and liver. AA-GLUC concentrations were reduced in plasma and elevated in livers of Nrf2-null mice due to decreased glucuronidation activity and lower expression of the basolateral efflux transporter Mrp3. In contrast, Keap1-kd mice had higher plasma and lower hepatic AA-GLUC concentrations, due to higher Mrp3 expression. Lower glucuronidation activity of Nrf2-null mice increased the proportion of AA available for sulfation, resulting in elevated AA-SULF concentrations in plasma, bile, and liver. Decreased AA-sulfation activity in Keap1-kd mice resulted in lower AA-SULF concentrations. AA-GSH conjugates were increased in Nrf2-null mice and tended to be lower in Keap1-kd mice. Furthermore, Nqo1, an enzyme capable of detoxifying the reactive intermediate of AA metabolism, N-acetyl-p-benzoquinone imine (NAPQI), had 85% lower activity in Nrf2-null mice and 415% higher activity in Keap1-kd mice relative to wild-type. In conclusion, lack of Nrf2 results in decreased AA glucuronidation, leading to increased AA available for NAPQI formation and decreased efflux of AA-GLUC via Mrp3; however, activation of Nrf2, as in Keap1-kd mice, results in decreased sulfotransferase activity, decreased AA-SULF formation, and enhanced elimination of AA-GLUC due to increased expression of Mrp3.

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Year:  2009        PMID: 19246624      PMCID: PMC2675638          DOI: 10.1093/toxsci/kfp047

Source DB:  PubMed          Journal:  Toxicol Sci        ISSN: 1096-0929            Impact factor:   4.849


  39 in total

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Review 2.  Xenobiotic transporters: ascribing function from gene knockout and mutation studies.

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3.  Role of NAD(P)H:quinone oxidoreductase 1 in clofibrate-mediated hepatoprotection from acetaminophen.

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Journal:  Toxicology       Date:  2006-11-19       Impact factor: 4.221

4.  Evaluation of the role of multidrug resistance-associated protein (Mrp) 3 and Mrp4 in hepatic basolateral excretion of sulfate and glucuronide metabolites of acetaminophen, 4-methylumbelliferone, and harmol in Abcc3-/- and Abcc4-/- mice.

Authors:  Maciej J Zamek-Gliszczynski; Ken-ichi Nezasa; Xianbin Tian; Arlene S Bridges; Kun Lee; Martin G Belinsky; Gary D Kruh; Kim L R Brouwer
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5.  Altered hepatobiliary disposition of acetaminophen glucuronide in isolated perfused livers from multidrug resistance-associated protein 2-deficient TR(-) rats.

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Authors:  Lauren M Aleksunes; Michael Goedken; José E Manautou
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7.  Ursodeoxycholic acid stimulates Nrf2-mediated hepatocellular transport, detoxification, and antioxidative stress systems in mice.

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Journal:  Am J Physiol Gastrointest Liver Physiol       Date:  2008-08-07       Impact factor: 4.052

8.  Oxidative and electrophilic stress induces multidrug resistance-associated protein transporters via the nuclear factor-E2-related factor-2 transcriptional pathway.

Authors:  Jonathan M Maher; Matthew Z Dieter; Lauren M Aleksunes; Angela L Slitt; Grace Guo; Yuji Tanaka; George L Scheffer; Jefferson Y Chan; Jose E Manautou; Ying Chen; Timothy P Dalton; Masayuki Yamamoto; Curtis D Klaassen
Journal:  Hepatology       Date:  2007-11       Impact factor: 17.425

Review 9.  Emerging role of Nrf2 in protecting against hepatic and gastrointestinal disease.

Authors:  Lauren M Aleksunes; José E Manautou
Journal:  Toxicol Pathol       Date:  2007-06       Impact factor: 1.902

10.  Increased Nrf2 activation in livers from Keap1-knockdown mice increases expression of cytoprotective genes that detoxify electrophiles more than those that detoxify reactive oxygen species.

Authors:  Scott A Reisman; Ronnie L Yeager; Masayuki Yamamoto; Curtis D Klaassen
Journal:  Toxicol Sci       Date:  2009-01-06       Impact factor: 4.849

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  42 in total

1.  M1 muscarinic receptors modify oxidative stress response to acetaminophen-induced acute liver injury.

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Journal:  Free Radic Biol Med       Date:  2014-10-31       Impact factor: 7.376

2.  Regulation of hepatic phase II metabolism in pregnant mice.

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3.  Activator protein-1 regulation of murine aldehyde dehydrogenase 1a1.

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Journal:  Mol Pharmacol       Date:  2012-06-26       Impact factor: 4.436

4.  Acetaminophen-induced hepatotoxicity in mice occurs with inhibition of activity and nitration of mitochondrial manganese superoxide dismutase.

Authors:  Rakhee Agarwal; Lee Ann MacMillan-Crow; Tonya M Rafferty; Hamida Saba; Dean W Roberts; E Kim Fifer; Laura P James; Jack A Hinson
Journal:  J Pharmacol Exp Ther       Date:  2010-12-30       Impact factor: 4.030

Review 5.  Updated perspectives on the cytosolic sulfotransferases (SULTs) and SULT-mediated sulfation.

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Review 6.  Stress-activated cap'n'collar transcription factors in aging and human disease.

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Review 7.  Role of nrf2 in oxidative stress and toxicity.

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8.  Gene expression profiling in male B6C3F1 mouse livers exposed to kava identifies--changes in drug metabolizing genes and potential mechanisms linked to kava toxicity.

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Journal:  Food Chem Toxicol       Date:  2009-12-03       Impact factor: 6.023

Review 9.  Molecular basis of electrophilic and oxidative defense: promises and perils of Nrf2.

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Journal:  Pharmacol Rev       Date:  2012-09-10       Impact factor: 25.468

Review 10.  Altered Expression of Transporters, its Potential Mechanisms and Influences in the Liver of Rodent Models Associated with Diabetes Mellitus and Obesity.

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