Abstract

This project is designed to increase our knowledge of the inflammatory response that follows toxic insults to the brain, especially the role of N0. It is hypothesized that inducible N0 synthase (N0S II) in astrocytes provides a tonic source of N0 tat contributes to neuronal degeneration. Towards that end, the principal investigator will characterize the induction of N0S II (No production, N0S II mRNA, protein and activity) in cultured astrocytes and the V1 cell line. This project will make extensive use of the chemical synthetic core to evaluation the ability of newly synthesized inhibitors of N0S II to selectively inhibit astrocyte versus macrophage N0S II. Such inhibitors would provide the ability to manipulate the production of N0 in the brain following injury. The principal investigator will also evaluate the contribution of astrocyte-derived N0 to neuronal injury and death. The effects of lead on N0S II will also be evaluated. N0 generating agents will be evaluated for alterations in the survival and growth of PC12 cells and cerebral cortical neurons in culture after acute and chronic exposures, and for their concentration and time dependent effects. Astrocytes and macrophages will also be compared for their N0S II induction by N0 generating agents. The principal investigator will also evaluate the ability of newly-synthesized N0S II and N0 trapping agents and lead to alter the toxicity of astrocytes and macrophages in culture.
The third aim i s to evaluate the role of N) in an in vivo model of inflammation following neuronal injury. Preliminary data indicate an increase in N)S I and N)S Ii following a discrete stab wound to the cerebral cortex and striatum. The investigator proposes to evaluate changes in the levels of all N0S isoforms following injury using Western and Northern blots as well as immunocytochemistry, followed by the evaluation of the effects of N0S II antagonists on the gliotic response or neuronal cell death following injury.
The fourth aim continues to be the evaluation of inflammatory responses in transgenic mice that have knocked out IFN receptor expression. Preliminary data indicated that these mice have reduced levels of iN0S following trauma as compared to wild type activity. The inflammatory response in IFN receptor knockouts will also be assessed in mice with normal astrocyte grafts. Overall, these studies seek to increase knowledge of the role of N0 in neural degeneration, and to identify strategies by which the toxic effects of N0 can be limited.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Environmental Health Sciences (NIEHS)
Type
Research Program Projects (P01)
Project #
1P01ES006897-01A3
Application #
6239674
Study Section
Project Start
1997-09-15
Project End
1998-08-31
Budget Start
1996-10-01
Budget End
1997-09-30
Support Year
1
Fiscal Year
1997
Total Cost
Indirect Cost

  Institution

Name
University of Medicine & Dentistry of NJ
Department
Type
DUNS #
622146454
City
Piscataway
State
NJ
Country
United States
Zip Code
08854

  Publications

Jan, Yi-Hua; Richardson, Jason R; Baker, Angela A et al. (2016) Novel approaches to mitigating parathion toxicity: targeting cytochrome P450-mediated metabolism with menadione. Ann N Y Acad Sci 1378:80-86
Kazanecki, Christian C; Kowalski, Aaron J; Ding, Tony et al. (2007) Characterization of anti-osteopontin monoclonal antibodies: Binding sensitivity to post-translational modifications. J Cell Biochem 102:925-35
Kazanecki, Christian C; Uzwiak, Dana J; Denhardt, David T (2007) Control of osteopontin signaling and function by post-translational phosphorylation and protein folding. J Cell Biochem 102:912-24
Gray, Joshua P; Heck, Diane E; Mishin, Vladimir et al. (2007) Paraquat increases cyanide-insensitive respiration in murine lung epithelial cells by activating an NAD(P)H:paraquat oxidoreductase: identification of the enzyme as thioredoxin reductase. J Biol Chem 282:7939-49
Ishijima, Muneaki; Ezura, Yoichi; Tsuji, Kunikazu et al. (2006) Osteopontin is associated with nuclear factor kappaB gene expression during tail-suspension-induced bone loss. Exp Cell Res 312:3075-83
Vetrano, Anna M; Heck, Diane E; Mariano, Thomas M et al. (2005) Characterization of the oxidase activity in mammalian catalase. J Biol Chem 280:35372-81
Martey, Christine A; Vetrano, Anna M; Whittemore, Marilyn S et al. (2005) Inhibition of interferon-gamma signaling by a mercurio-substituted dihydropsoralen in murine keratinocytes. Biochem Pharmacol 70:1726-34
Heck, Diane E; Kagan, Valerian E; Shvedova, Anna A et al. (2005) An epigrammatic (abridged) recounting of the myriad tales of astonishing deeds and dire consequences pertaining to nitric oxide and reactive oxygen species in mitochondria with an ancillary missive concerning the origins of apoptosis. Toxicology 208:259-71
Fakhrzadeh, Ladan; Laskin, Jeffrey D; Gardner, Carol R et al. (2004) Superoxide dismutase-overexpressing mice are resistant to ozone-induced tissue injury and increases in nitric oxide and tumor necrosis factor-alpha. Am J Respir Cell Mol Biol 30:280-7
Heck, Diane E; Gerecke, Donald R; Vetrano, Anna M et al. (2004) Solar ultraviolet radiation as a trigger of cell signal transduction. Toxicol Appl Pharmacol 195:288-97

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