Abstract

The mouse has become an invaluable model organism for biomedical research in the post-genome era. The decades of research to uncover linkages between the genome and phenome using mouse models has led to an accumulation of a body of knowledge on the genetic diversity and gene-environment interactions that is yet to be matched for any other mammal, including humans. Importantly, the mouse has been the stalwart of mechanistic research in toxicology, including studies of liver toxicity by ethanol. Here, the investigators are proposing to use metabolomics and mouse models in a new systems biology approach for molecular dissection and discovery of biological pathways underlying the susceptibility to ethanol-induced liver injury. The investigators will test the hypothesis that by combining a state-of-the-art in vivo model of liver toxicity and the investigators' prior knowledge of the mechanisms of ethanol-induced liver injury, novel metabolic, genomic and pathologic analyses with genetic diversity of mouse inbred strains will define a """"""""liver toxicity susceptibility state."""""""" A set of inbred strains that provides a strong link to the Mouse Phenome Project will be used in these studies.
The first aim will be to develop and test computational strategies for integration of metabolomic data with other multi-dimensional data types for studies into the mechanisms of liver injury. The optimal approaches will be applied in the second aim to a panel of fourteen inbred mouse strains to produce mouse strain-specific baseline metabolic and gene expression matrices in the target tissues.
The third aim i s to produce a mouse strain-specific multi-dimensional toxicological, metabolic and expression data set related to acute and sub-chronic liver injury due to ethanol. Results from this aim will be compared to known gene-environment interactions in these inbred strains to other liver toxicants. Finally, the investigators will perform phenotype-specific genotypic anchoring of ethanol-induced metabolic and expression changes with liver injury. The investigators will develop methods for translating the resulting information into human studies. Data collected in these studies will be deposited into publicly-available databases and mined for unique signatures indicative of common responses to ethanol, other liver toxicants and for specific genetic background dependent responses. The investigators believe that the data and computational strategies produced in this project will be useful far beyond the immediate scope of this research project since it can (i) be integrated and analyzed in conjunction with ongoing projects from the toxicogenomics consortium to identify common species-dependent and -independent responses to a variety of environmental toxins; (ii) provide valuable insights into genetically determined individual variability in response to toxicants; and (iii) identify physiologically relevant animal models for studies on specific patterns of toxicant responses observed in genetically polymorphic human individuals.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Alcohol Abuse and Alcoholism (NIAAA)
Type
Research Project (R01)
Project #
5R01AA016258-02
Application #
7125158
Study Section
Special Emphasis Panel (ZES1-JAB-C (R1))
Program Officer
Velazquez, Jose M
Project Start
2005-09-26
Project End
2010-07-31
Budget Start
2006-08-01
Budget End
2007-07-31
Support Year
2
Fiscal Year
2006
Total Cost
$510,028
Indirect Cost

  Institution

Name
University of North Carolina Chapel Hill
Department
Public Health & Prev Medicine
Type
Schools of Public Health
DUNS #
608195277
City
Chapel Hill
State
NC
Country
United States
Zip Code
27599

  Publications

Jeannot, Emmanuelle; Boorman, Gary A; Kosyk, Oksana et al. (2012) Increased incidence of aflatoxin B1-induced liver tumors in hepatitis virus C transgenic mice. Int J Cancer 130:1347-56
Tsuchiya, Masato; Ji, Cheng; Kosyk, Oksana et al. (2012) Interstrain differences in liver injury and one-carbon metabolism in alcohol-fed mice. Hepatology 56:130-9
Jeannot, Emmanuelle; Pogribny, Igor P; Beland, Frederick A et al. (2011) Chronic administration of ethanol leads to an increased incidence of hepatocellular adenoma by promoting H-ras-mutated cells. Cancer Lett 301:161-7
Gatti, Daniel M; Lu, Lu; Williams, Robert W et al. (2011) MicroRNA expression in the livers of inbred mice. Mutat Res 714:126-33
Gatti, Daniel M; Zhao, Ni; Chesler, Elissa J et al. (2010) Sex-specific gene expression in the BXD mouse liver. Physiol Genomics 42:456-68
Powell, Christine L; Bradford, Blair U; Craig, Christopher Patrick et al. (2010) Mechanism for prevention of alcohol-induced liver injury by dietary methyl donors. Toxicol Sci 115:131-9
Jeannot, Emmanuelle; Mellottee, Lucille; Bioulac-Sage, Paulette et al. (2010) Spectrum of HNF1A somatic mutations in hepatocellular adenoma differs from that in patients with MODY3 and suggests genotoxic damage. Diabetes 59:1836-44
Rusyn, Ivan; Gatti, Daniel M; Wiltshire, Timothy et al. (2010) Toxicogenetics: population-based testing of drug and chemical safety in mouse models. Pharmacogenomics 11:1127-36
Formeister, Eric J; Tsuchiya, Masato; Fujii, Hideki et al. (2010) Comparative analysis of promoter methylation and gene expression endpoints between tumorous and non-tumorous tissues from HCV-positive patients with hepatocellular carcinoma. Mutat Res 692:26-33
Pogribny, Igor P; Tryndyak, Volodymyr P; Bagnyukova, Tetyana V et al. (2009) Hepatic epigenetic phenotype predetermines individual susceptibility to hepatic steatosis in mice fed a lipogenic methyl-deficient diet. J Hepatol 51:176-86

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