Literature DB >> 23308384

Screening for drug-induced hepatotoxicity in primary mouse hepatocytes using acetaminophen, amiodarone, and cyclosporin a as model compounds: an omics-guided approach.

Anke Van Summeren1, Johan Renes, Daneida Lizarraga, Freek G Bouwman, Jean-Paul Noben, Joost H M van Delft, Jos C S Kleinjans, Edwin C M Mariman.   

Abstract

Drug-induced hepatotoxicity is a leading cause of attrition for candidate pharmaceuticals in development. New preclinical screening methods are crucial to predict drug toxicity prior to human studies. Of all in vitro hepatotoxicity models, primary human hepatocytes are considered as 'the gold standard.' However, their use is hindered by limited availability and inter-individual variation. These barriers may be overcome by using primary mouse hepatocytes. We used differential in gel electrophoresis (DIGE) to study large-scale protein expression of primary mouse hepatocytes. These hepatocytes were exposed to three well-defined hepatotoxicants: acetaminophen, amiodarone, and cyclosporin A. Each hepatotoxicant induces a different hepatotoxic phenotype. Based on the DIGE results, the mRNA expression levels of deregulated proteins from cyclosporin A-treated cells were also analyzed. We were able to distinguish cyclosporin A from controls, as well as acetaminophen and amiodarone-treated samples. Cyclosporin A induced endoplasmic reticulum (ER) stress and altered the ER-Golgi transport. Moreover, liver carboxylesterase and bile salt sulfotransferase were differentially expressed. These proteins were associated with a protective adaptive response against cyclosporin A-induced cholestasis. The results of this study are comparable with effects in HepG2 cells. Therefore, we suggest both models can be used to analyze the cholestatic properties of cyclosporin A. Furthermore, this study showed a conserved response between primary mouse hepatocytes and HepG2 cells. These findings collectively lend support for use of omics strategies in preclinical toxicology, and might inform future efforts to better link preclinical and clinical research in rational drug development.

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Year:  2013        PMID: 23308384      PMCID: PMC3567623          DOI: 10.1089/omi.2012.0079

Source DB:  PubMed          Journal:  OMICS        ISSN: 1536-2310


  47 in total

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2.  Influence of culture time on the expression of drug-metabolizing enzymes in primary human hepatocytes and hepatoma cell line HepG2.

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Journal:  Proc Natl Acad Sci U S A       Date:  2001-02-27       Impact factor: 11.205

Review 4.  Paracetamol (acetaminophen)-induced toxicity: molecular and biochemical mechanisms, analogues and protective approaches.

Authors:  J G Bessems; N P Vermeulen
Journal:  Crit Rev Toxicol       Date:  2001-01       Impact factor: 5.635

Review 5.  Bile salt transporters: molecular characterization, function, and regulation.

Authors:  Michael Trauner; James L Boyer
Journal:  Physiol Rev       Date:  2003-04       Impact factor: 37.312

6.  Cholestasis and regulation of genes related to drug metabolism and biliary transport in rat liver following treatment with cyclosporine A and sirolimus (Rapamycin).

Authors:  S Bramow; P Ott; F Thomsen Nielsen; K Bangert; N Tygstrup; K Dalhoff
Journal:  Pharmacol Toxicol       Date:  2001-09

7.  Cyclosporin-induced dyslipoproteinemia is associated with selective activation of SREBP-2.

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Review 8.  Drug-related hepatotoxicity and acute liver failure.

Authors:  Karen F Murray; Nedim Hadzic; Stefan Wirth; Mikelle Bassett; Deirdre Kelly
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9.  Gene expression in two hepatic cell lines, cultured primary hepatocytes, and liver slices compared to the in vivo liver gene expression in rats: possible implications for toxicogenomics use of in vitro systems.

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Review 10.  Comparing protein abundance and mRNA expression levels on a genomic scale.

Authors:  Dov Greenbaum; Christopher Colangelo; Kenneth Williams; Mark Gerstein
Journal:  Genome Biol       Date:  2003-08-29       Impact factor: 13.583

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3.  Extending the limits of quantitative proteome profiling with data-independent acquisition and application to acetaminophen-treated three-dimensional liver microtissues.

Authors:  Roland Bruderer; Oliver M Bernhardt; Tejas Gandhi; Saša M Miladinović; Lin-Yang Cheng; Simon Messner; Tobias Ehrenberger; Vito Zanotelli; Yulia Butscheid; Claudia Escher; Olga Vitek; Oliver Rinner; Lukas Reiter
Journal:  Mol Cell Proteomics       Date:  2015-02-27       Impact factor: 5.911

4.  Increased liver-specific proteins in circulating extracellular vesicles as potential biomarkers for drug- and alcohol-induced liver injury.

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Journal:  PLoS One       Date:  2017-02-22       Impact factor: 3.240

5.  The human hepatocyte TXG-MAPr: gene co-expression network modules to support mechanism-based risk assessment.

Authors:  Giulia Callegaro; Steven J Kunnen; Panuwat Trairatphisan; Solène Grosdidier; Marije Niemeijer; Wouter den Hollander; Emre Guney; Janet Piñero Gonzalez; Laura Furlong; Yue W Webster; Julio Saez-Rodriguez; Jeffrey J Sutherland; Jennifer Mollon; James L Stevens; Bob van de Water
Journal:  Arch Toxicol       Date:  2021-10-09       Impact factor: 5.153

Review 6.  Role of endoplasmic reticulum stress in drug-induced toxicity.

Authors:  Fabienne Foufelle; Bernard Fromenty
Journal:  Pharmacol Res Perspect       Date:  2016-02-04
  6 in total

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