Abstract

? ? Nonalcoholic steatohepatitis (NASH) associated with obesity and type II diabetes is emerging as one of the most common etiologies of chronic liver disease. Recent evidence supports a """"""""two-hit"""""""" hypothesis for NASH with the """"""""first-hit"""""""" involving the accumulation of fat in hepatocytes as a consequence of insulin resistance followed by the """"""""second-hit"""""""", which entails mitochondrial dysfunction and oxidative and nitrosative stress. Thus, the mitochondrion is postulated to play a central role in the development of NASH with disrupted energy metabolism and excess oxidant production contributing to pathology. The mechanism by which oxidative stress leads to mitochondrial damage is likely to involve the post-translational modification of mitochondrial proteins. Oxidative modifications to mitochondrial proteins will impair mitochondrial bioenergetics and lead to further increases in oxidants, which are proposed to play a key role in the progression from simple fatty liver to NASH. The molecular pathways and targets that underlie these changes to mitochondria in NASH are unknown and the focus of this application. One factor that has hindered progress in elucidating the molecular mechanisms of NASH and development of targeted therapeutics is the lack of appropriate experimental animal models. Preliminary data indicate that feeding a high-fat diet to mice reproduces the key histopathologic features of NASH with mitochondrial dysfunction. Based on these observations it is hypothesized that the inability to adapt to the metabolic alterations associated with obesity results in the overproduction of mitochondrial oxidants, which leads to post-translational modification of proteins, impaired mitochondrial function, and NASH.
The first aim of this exploratory project is to characterize and quantify the development of NASH and mitochondrial damage in response to a high-fat diet in mice. The use of this model will facilitate future studies with transgenic and/or knockout mouse models to investigate mechanisms of protection from metabolic stress in liver mitochondria.
The second aim i s to characterize post-translational modifications to the hepatic mitochondria proteome in response to NASH. Completion of these studies using novel proteomic approaches will enable the identification of the molecular defects in metabolic pathways and/or proteins in NASH that can be targeted by mitochondria-specific therapeutic strategies for treatment and prevention. Public health relevance (lay description) - Studies report an increasing prevalence of obesity in the world. Obesity is associated with serious health problems including heart disease and diabetes and is recognized as the most common risk factor for development of chronic non alcohol-related liver diseases. The studies in this application are important as they will identify the underlying factors responsible for obesity-related liver diseases, which will lead to the discovery of new treatments. ? ? ? ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Exploratory/Developmental Grants (R21)
Project #
1R21DK073775-01
Application #
7029306
Study Section
Special Emphasis Panel (ZDK1-GRB-N (O1))
Program Officer
Doo, Edward
Project Start
2006-03-10
Project End
2008-02-29
Budget Start
2006-03-10
Budget End
2007-02-28
Support Year
1
Fiscal Year
2006
Total Cost
$218,250
Indirect Cost

  Institution

Name
University of Alabama Birmingham
Department
Public Health & Prev Medicine
Type
Schools of Public Health
DUNS #
063690705
City
Birmingham
State
AL
Country
United States
Zip Code
35294

  Publications

Mitchell, Tanecia; Chacko, Balu; Ballinger, Scott W et al. (2013) Convergent mechanisms for dysregulation of mitochondrial quality control in metabolic disease: implications for mitochondrial therapeutics. Biochem Soc Trans 41:127-33
Feldstein, Ariel E; Bailey, Shannon M (2011) Emerging role of redox dysregulation in alcoholic and nonalcoholic fatty liver disease. Antioxid Redox Signal 15:421-4
Eccleston, Heather B; Andringa, Kelly K; Betancourt, Angela M et al. (2011) Chronic exposure to a high-fat diet induces hepatic steatosis, impairs nitric oxide bioavailability, and modifies the mitochondrial proteome in mice. Antioxid Redox Signal 15:447-59
Andringa, Kelly K; King, Adrienne L; Eccleston, Heather B et al. (2010) Analysis of the liver mitochondrial proteome in response to ethanol and S-adenosylmethionine treatments: novel molecular targets of disease and hepatoprotection. Am J Physiol Gastrointest Liver Physiol 298:G732-45
Andringa, Kelly K; Bailey, Shannon M (2010) Detection of protein thiols in mitochondrial oxidative phosphorylation complexes and associated proteins. Methods Enzymol 474:83-108
King, Adrienne L; Bailey, Shannon M (2010) Assessment of mitochondrial dysfunction arising from treatment with hepatotoxicants. Curr Protoc Toxicol Chapter 14:Unit14.8
Hill, Bradford G; Dranka, Brian P; Bailey, Shannon M et al. (2010) What part of NO don't you understand? Some answers to the cardinal questions in nitric oxide biology. J Biol Chem 285:19699-704
Andringa, Kelly; King, Adrienne; Bailey, Shannon (2009) Blue native-gel electrophoresis proteomics. Methods Mol Biol 519:241-58
Mantena, Sudheer K; Vaughn, Denty Paul; Andringa, Kelly K et al. (2009) High fat diet induces dysregulation of hepatic oxygen gradients and mitochondrial function in vivo. Biochem J 417:183-93
Andringa, Kelly K; Bajt, Mary Lynn; Jaeschke, Hartmut et al. (2008) Mitochondrial protein thiol modifications in acetaminophen hepatotoxicity: effect on HMG-CoA synthase. Toxicol Lett 177:188-97

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