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Drug Metabolism Reviews Volume 36, 2004 - Issue 3-4
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Research Article

Acetaminophen‐Induced Hepatotoxicity: Role of Metabolic Activation, Reactive Oxygen/Nitrogen Species, and Mitochondrial Permeability Transition

Jack A. Hinson Department of Pharmacology and Toxicology, University of Arkansas for Medical Sciences, Slot 638, Little Rock, Arkansas, 72205, USA
,
Angela B. Reid Department of Pharmacology and Toxicology, University of Arkansas for Medical Sciences, Slot 638, Little Rock, Arkansas, 72205, USA
,
Sandra S. McCullough Department of Pharmacology and Toxicology, University of Arkansas for Medical Sciences, Slot 638, Little Rock, Arkansas, 72205, USA; Department of Pediatrics, College of Medicine, University of Arkansas for Medical Sciences, Little Rock, Arkansas, 72205, USA
&
Laura P. James Department of Pharmacology and Toxicology, University of Arkansas for Medical Sciences, Slot 638, Little Rock, Arkansas, 72205, USA; Department of Pediatrics, College of Medicine, University of Arkansas for Medical Sciences, Little Rock, Arkansas, 72205, USA
Pages 805-822 | Published online: 25 Oct 2004
 
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Abstract

Large doses of the analgesic acetaminophen cause centrilobular hepatic necrosis in man and in experimental animals. It has been previously shown that acetaminophen is metabolically activated by CYP enzymes to N‐acetyl‐p‐benzoquinone imine. This species is normally detoxified by GSH, but following a toxic dose GSH is depleted and the metabolite covalently binds to a number of different proteins. Covalent binding occurs only to the cells developing necrosis. Recently we showed that these cells also contain nitrated tyrosine residues. Nitrotyrosine is mediated by peroxynitrite, a reactive nitrogen species formed by rapid reaction between nitric oxide and superoxide and is normally detoxified by GSH. Thus, acetaminophen toxicity occurs with increased oxygen/nitrogen stress. This manuscript will review current data on acetaminophen covalent binding, increased oxygen/nitrogen stress, and mitochondrial permeability transition, a toxic mechanism that is both mediated by and leads to increased oxygen/nitrogen stress.

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