Literature DB >> 24675475

Phenobarbital and propiconazole toxicogenomic profiles in mice show major similarities consistent with the key role that constitutive androstane receptor (CAR) activation plays in their mode of action.

Richard A Currie1, Richard C Peffer2, Amber K Goetz3, Curtis J Omiecinski4, Jay I Goodman5.   

Abstract

Toxicogenomics (TGx) is employed frequently to investigate underlying molecular mechanisms of the compound of interest and, thus, has become an aid to mode of action determination. However, the results and interpretation of a TGx dataset are influenced by the experimental design and methods of analysis employed. This article describes an evaluation and reanalysis, by two independent laboratories, of previously published TGx mouse liver microarray data for a triazole fungicide, propiconazole (PPZ), and the anticonvulsant drug phenobarbital (PB). Propiconazole produced an increase incidence of liver tumors in male CD-1 mice only at a dose that exceeded the maximum tolerated dose (2500 ppm). Firstly, we illustrate how experimental design differences between two in vivo studies with PPZ and PB may impact the comparisons of TGx results. Secondly, we demonstrate that different researchers using different pathway analysis tools can come to different conclusions on specific mechanistic pathways, even when using the same datasets. Finally, despite these differences the results across three different analyses also show a striking degree of similarity observed for PPZ and PB treated livers when the expression data are viewed as major signaling pathways and cell processes affected. Additional studies described here show that the postulated key event of hepatocellular proliferation was observed in CD-1 mice for both PPZ and PB, and that PPZ is also a potent activator of the mouse CAR nuclear receptor. Thus, with regard to the events which are hallmarks of CAR-induced effects that are key events in the mode of action (MOA) of mouse liver carcinogenesis with PB, PPZ-induced tumors can be viewed as being promoted by a similar PB-like CAR-dependent MOA.
Copyright © 2014. Published by Elsevier Ireland Ltd.

Entities:  

Keywords:  Conazoles; Constitutive androstane receptor; Phenobarbital; Propiconazole; Toxicogenomics

Mesh:

Substances:

Year:  2014        PMID: 24675475      PMCID: PMC4089507          DOI: 10.1016/j.tox.2014.03.003

Source DB:  PubMed          Journal:  Toxicology        ISSN: 0300-483X            Impact factor:   4.221


  25 in total

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3.  Transcriptional profiles in liver from mice treated with hepatotumorigenic and nonhepatotumorigenic triazole conazole fungicides: Propiconazole, triadimefon, and myclobutanil.

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4.  Phenobarbital-responsive nuclear translocation of the receptor CAR in induction of the CYP2B gene.

Authors:  T Kawamoto; T Sueyoshi; I Zelko; R Moore; K Washburn; M Negishi
Journal:  Mol Cell Biol       Date:  1999-09       Impact factor: 4.272

5.  Xenobiotic stress induces hepatomegaly and liver tumors via the nuclear receptor constitutive androstane receptor.

Authors:  Wendong Huang; Jun Zhang; Michele Washington; Jun Liu; John M Parant; Guillermina Lozano; David D Moore
Journal:  Mol Endocrinol       Date:  2005-04-14

6.  The orphan nuclear receptor constitutive active/androstane receptor is essential for liver tumor promotion by phenobarbital in mice.

Authors:  Yukio Yamamoto; Rick Moore; Thomas L Goldsworthy; Masahiko Negishi; Robert R Maronpot
Journal:  Cancer Res       Date:  2004-10-15       Impact factor: 12.701

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8.  Mode of action in relevance of rodent liver tumors to human cancer risk.

Authors:  Michael P Holsapple; Henri C Pitot; Samuel M Cohen; Samuel H Cohen; Alan R Boobis; James E Klaunig; Timothy Pastoor; Vicki L Dellarco; Yvonne P Dragan
Journal:  Toxicol Sci       Date:  2005-10-12       Impact factor: 4.849

Review 9.  Species differences in the hepatic effects of inducers of CYP2B and CYP4A subfamily forms: relationship to rodent liver tumour formation.

Authors:  B G Lake
Journal:  Xenobiotica       Date:  2009-08       Impact factor: 1.908

Review 10.  Toxicogenomics in risk assessment: an overview of an HESI collaborative research program.

Authors:  William Pennie; Syril D Pettit; Peter G Lord
Journal:  Environ Health Perspect       Date:  2004-03       Impact factor: 9.031

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Review 4.  A predictive data-driven framework for endocrine prioritization: a triazole fungicide case study.

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5.  Hepatotoxic combination effects of three azole fungicides in a broad dose range.

Authors:  T Heise; F Schmidt; C Knebel; S Rieke; W Haider; I Geburek; L Niemann; P Marx-Stoelting
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Review 6.  The Connection of Azole Fungicides with Xeno-Sensing Nuclear Receptors, Drug Metabolism and Hepatotoxicity.

Authors:  Philip Marx-Stoelting; Constanze Knebel; Albert Braeuning
Journal:  Cells       Date:  2020-05-11       Impact factor: 6.600

Review 7.  Metabolism-Disrupting Chemicals and the Constitutive Androstane Receptor CAR.

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8.  Crosstalk between Receptor and Non-receptor Mediated Chemical Modes of Action in Rat Livers Converges through a Dysregulated Gene Expression Network at Tumor Suppressor Tp53.

Authors:  Karen M Funderburk; Scott S Auerbach; Pierre R Bushel
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Review 9.  Constitutive Androstane Receptor: A Peripheral and a Neurovascular Stress or Environmental Sensor.

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