Literature DB >> 30974156

Mechanistic identification of biofluid metabolite changes as markers of acetaminophen-induced liver toxicity in rats.

Venkat R Pannala1, Kalyan C Vinnakota2, Kristopher D Rawls3, Shanea K Estes4, Tracy P O'Brien4, Richard L Printz4, Jason A Papin3, Jaques Reifman5, Masakazu Shiota4, Jamey D Young6, Anders Wallqvist7.   

Abstract

Acetaminophen (APAP) is the most commonly used analgesic and antipyretic drug in the world. Yet, it poses a major risk of liver injury when taken in excess of the therapeutic dose. Current clinical markers do not detect the early onset of liver injury associated with excess APAP-information that is vital to reverse injury progression through available therapeutic interventions. Hence, several studies have used transcriptomics, proteomics, and metabolomics technologies, both independently and in combination, in an attempt to discover potential early markers of liver injury. However, the casual relationship between these observations and their relation to the APAP mechanism of liver toxicity are not clearly understood. Here, we used Sprague-Dawley rats orally gavaged with a single dose of 2 g/kg of APAP to collect tissue samples from the liver and kidney for transcriptomic analysis and plasma and urine samples for metabolomic analysis. We developed and used a multi-tissue, metabolism-based modeling approach to integrate these data, characterize the effect of excess APAP levels on liver metabolism, and identify a panel of plasma and urine metabolites that are associated with APAP-induced liver toxicity. Our analyses, which indicated that pathways involved in nucleotide-, lipid-, and amino acid-related metabolism in the liver were most strongly affected within 10 h following APAP treatment, identified a list of potential metabolites in these pathways that could serve as plausible markers of APAP-induced liver injury. Our approach identifies toxicant-induced changes in endogenous metabolism, is applicable to other toxicants based on transcriptomic data, and provides a mechanistic framework for interpreting metabolite alterations.
Copyright © 2019 Elsevier Inc. All rights reserved.

Entities:  

Keywords:  Acetaminophen; Blood and urine metabolites; Genome-scale model; Glutathione; Glycine limitation

Mesh:

Substances:

Year:  2019        PMID: 30974156      PMCID: PMC6599641          DOI: 10.1016/j.taap.2019.04.001

Source DB:  PubMed          Journal:  Toxicol Appl Pharmacol        ISSN: 0041-008X            Impact factor:   4.219


  82 in total

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Journal:  Toxicol Sci       Date:  2005-06-23       Impact factor: 4.849

6.  An integrated metabonomic investigation of acetaminophen toxicity in the mouse using NMR spectroscopy.

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7.  Mitochondrial permeability transition in acetaminophen-induced necrosis and apoptosis of cultured mouse hepatocytes.

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Authors:  Alexandra N Heinloth; Richard D Irwin; Gary A Boorman; Paul Nettesheim; Rickie D Fannin; Stella O Sieber; Michael L Snell; Charles J Tucker; Leping Li; Gregory S Travlos; Gordon Vansant; Pamela E Blackshear; Raymond W Tennant; Michael L Cunningham; Richard S Paules
Journal:  Toxicol Sci       Date:  2004-04-14       Impact factor: 4.849

9.  Measurement of serum acetaminophen-protein adducts in patients with acute liver failure.

Authors:  Timothy J Davern; Laura P James; Jack A Hinson; Julie Polson; Anne M Larson; Robert J Fontana; Ezmina Lalani; Santiago Munoz; A Obaid Shakil; William M Lee
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1.  Genome-Scale Model-Based Identification of Metabolite Indicators for Early Detection of Kidney Toxicity.

Authors:  Venkat R Pannala; Kalyan C Vinnakota; Shanea K Estes; Irina Trenary; Tracy P OˈBrien; Richard L Printz; Jason A Papin; Jaques Reifman; Tatsuya Oyama; Masakazu Shiota; Jamey D Young; Anders Wallqvist
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2.  Genomics and metabolomics of early-stage thioacetamide-induced liver injury: An interspecies study between guinea pig and rat.

Authors:  Patric Schyman; Richard L Printz; Venkat R Pannala; Mohamed Diwan M AbdulHameed; Shanea K Estes; Chiyo Shiota; Kelli Lynn Boyd; Masakazu Shiota; Anders Wallqvist
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4.  Predicting changes in renal metabolism after compound exposure with a genome-scale metabolic model.

Authors:  Kristopher D Rawls; Bonnie V Dougherty; Kalyan C Vinnakota; Venkat R Pannala; Anders Wallqvist; Glynis L Kolling; Jason A Papin
Journal:  Toxicol Appl Pharmacol       Date:  2020-12-31       Impact factor: 4.219

5.  Toxicant-Induced Metabolic Alterations in Lipid and Amino Acid Pathways Are Predictive of Acute Liver Toxicity in Rats.

Authors:  Venkat R Pannala; Shanea K Estes; Mohsin Rahim; Irina Trenary; Tracy P O'Brien; Chiyo Shiota; Richard L Printz; Jaques Reifman; Masakazu Shiota; Jamey D Young; Anders Wallqvist
Journal:  Int J Mol Sci       Date:  2020-11-04       Impact factor: 5.923

6.  The cardioprotective effects of the new crystal form of puerarin in isoproterenol-induced myocardial ischemia rats based on metabolomics.

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