Abstract

There is a wealth of information implicating cumulative cellular injury inflicted by reactive oxygen species and heavy metal toxicity in neuronal damage and neurodegenerative diseases. Cells have evolved various endogenous antioxidant defenses to afford protection from oxidative injury or to reduce oxidative stress. Selenium is an essential contributor to these defenses, as it is required for the activity of a family of antioxidant enzymes that protect cells against the damaging products of normal oxygen metabolism. Selenium has also long been known to function as an antidote to toxicity of heavy metals. Selenoprotein P has recently been shown to function as a selenium delivery protein to brain, providing a source of this essential trace element for synthesis of other selenoproteins when selenium is deficient in the diet. Targeted disruption of the selenoprotein P gene results in neurological dysfunction. The overall goals of this study are to investigate the selenium delivery function of selenoprotein P in cells of neuronal origin, and to identify the crucial target selenoproteins which function in protection from oxidant and heavy metal induced damage, and which presumably explain the neurological effects of selenoprotein P gene disruption. These goals will be addressed through the following specific aims: ? 1. Investigate the means by which selenoprotein P serves as a Se donor to cells in culture, including interactions at the cell membrane and within the cell. ? 2. Investigate the expression levels and subcellular localization of specific selenoproteins, and whether localization or expression levels or patterns change in response to oxidative damage. Investigate the expression of specific selenoproteins in tissue sections from different brain regions in mice, and the changes in the expression levels or localization in response to GSH depletion or ischemia/reperfusion injury. ? 3. Identify the specific selenoproteins in neuronal cells responsible for protection from oxidative damage, resulting from either reactive oxygen species production or accumulation, or heavy metal induced damage. ? 4. Investigate expression of selenoproteins in brain sections obtained at autopsy from a cohort of Japanese men diagnosed with Alzheimer's or Parkinson's disease, vascular dementia, other neurological damage or with no evidence of neurodegenerative disease. ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
5R01NS040302-08
Application #
7113808
Study Section
Special Emphasis Panel (ZRG1-REB (02))
Program Officer
Sutherland, Margaret L
Project Start
2000-07-01
Project End
2008-05-31
Budget Start
2006-06-01
Budget End
2007-05-31
Support Year
8
Fiscal Year
2006
Total Cost
$478,204
Indirect Cost

  Institution

Name
University of Hawaii
Department
Anatomy/Cell Biology
Type
Schools of Medicine
DUNS #
965088057
City
Honolulu
State
HI
Country
United States
Zip Code
96822

  Publications

Dewing, Andrea S T; Rueli, Rachel H; Robles, Michael J et al. (2012) Expression and regulation of mouse selenoprotein P transcript variants differing in non-coding RNA. RNA Biol 9:1361-9
Bellinger, Frederick P; Raman, Arjun V; Rueli, Rachel H et al. (2012) Changes in selenoprotein P in substantia nigra and putamen in Parkinson's disease. J Parkinsons Dis 2:115-26
Raman, A V; Pitts, M W; Seyedali, A et al. (2012) Absence of selenoprotein P but not selenocysteine lyase results in severe neurological dysfunction. Genes Brain Behav 11:601-13
Pitts, M W; Raman, A V; Hashimoto, A C et al. (2012) Deletion of selenoprotein P results in impaired function of parvalbumin interneurons and alterations in fear learning and sensorimotor gating. Neuroscience 208:58-68
Takemoto, Andrea S; Berry, Marla J; Bellinger, Frederick P (2010) Role of selenoprotein P in Alzheimer's disease. Ethn Dis 20:S1-92-5
Stoytcheva, Zoia R; Vladimirov, Vladimir; Douet, Vanessa et al. (2010) Metal transcription factor-1 regulation via MREs in the transcribed regions of selenoprotein H and other metal-responsive genes. Biochim Biophys Acta 1800:416-24
Stoytcheva, Zoia R; Berry, Marla J (2009) Transcriptional regulation of mammalian selenoprotein expression. Biochim Biophys Acta 1790:1429-40
Bellinger, Frederick P; Raman, Arjun V; Reeves, Mariclair A et al. (2009) Regulation and function of selenoproteins in human disease. Biochem J 422:11-22
Bellinger, Frederick P; He, Qing-Ping; Bellinger, Miyoko T et al. (2008) Association of selenoprotein p with Alzheimer's pathology in human cortex. J Alzheimers Dis 15:465-72
Morozova, Nadya; Khrapko, Konstantin; Panee, Jun et al. (2007) Glutathione depletion in hippocampal cells increases levels of H and L ferritin and glutathione S-transferase mRNAs. Genes Cells 12:561-7

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