Abstract

This program project seeks to identify the genes, mRNAs and proteins that establish the phenotypic characteristics that distinguish the cellular elements (i.e., neuron subsets, or """"""""types"""""""") within defined regions and nuclei of the rodent brian. Many brain-specific or enriched genes and gene products await discovery and characterization. Therefore, the goals of this continuation application are focussed upon discovery strategies that will optimize detection of functionally responsive genes and gene products. To reach this objective we will apply recombinant DNa, and genetic technologies to isolate the cDNA clones of brain mRNAs identified through their spatial distribution or through their sequence-specific hybridization with nucleic acid probes devised within the Buchmeier, Milner, Peterson and Sutcliffe Components to reflect unique functional properties according to their individual strategic protocols. The Bloom component will employ immunological, immunocytochemical, and in situ hybridization methods to map the mRNAs and their gene products at the regionally selective developmental expression and extend these subtractive hybridization approaches to the rodent hypothalamus and to the repair processes that follow central axotomy or cns infection with the Mouse Hepatitis Virus, or its reduced virulence deletion mutants. We shall identify and characterize the rodent substance K receptor gene and compare it with other tachykinin and G-protein coupled receptors. We will employ stem cell gene disruption and transgeneic expression to evaluate changes in brain structure or function when cells that normally express selected genes are prevented from doing so. We will characterize the altered gene products and spatially map the affected cells. We will relate our data to known brain molecules and cells, and seek to define the functional properties of the molecules identified and the cell types and cell systems that express them. We view the identification of functionally unknown brain specific genes and gene products as a critical step in fully understanding brain physiology and the pathophysiology of presently isoluble neurologic and psychiatric disorders.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Program Projects (P01)
Project #
2P01NS022347-04
Application #
3099916
Study Section
Neurological Disorders Program Project Review B Committee (NSPB)
Project Start
1986-08-01
Project End
1994-07-31
Budget Start
1989-08-01
Budget End
1990-07-31
Support Year
4
Fiscal Year
1989
Total Cost
Indirect Cost

  Institution

Name
Scripps Research Institute
Department
Type
DUNS #
City
San Diego
State
CA
Country
United States
Zip Code
92037

  Publications

O'Shaughnessy, W S; Murthy, S K; Edell, D J et al. (2007) Stable biopassive insulation synthesized by initiated chemical vapor deposition of poly(1,3,5-trivinyltrimethylcyclotrisiloxane). Biomacromolecules 8:2564-70
O'Shaughnessy, W Shannan; Gao, Meiling; Gleason, Karen K (2006) Initiated chemical vapor deposition of trivinyltrimethylcyclotrisiloxane for biomaterial coatings. Langmuir 22:7021-6
Murthy, Shashi K; Olsen, Bradley D; Gleason, Karen K (2004) Peptide attachment to vapor deposited polymeric thin films. Langmuir 20:4774-6
Trembleau, A; Melia, K R; Bloom, F E (1995) BC1 RNA and vasopressin mRNA in rat neurohypophysis: axonal compartmentalization and differential regulation during dehydration and rehydration. Eur J Neurosci 7:2249-60
Chowdhury, D; Travis, G H; Sutcliffe, J G et al. (1995) Synaptotagmin I and 1B4 are identical: implications for synaptotagmin distribution in the primate brain. Neurosci Lett 190:9-12
Trembleau, A; Bloom, F E (1995) Enhanced sensitivity for light and electron microscopic in situ hybridization with multiple simultaneous non-radioactive oligodeoxynucleotide probes. J Histochem Cytochem 43:829-41
Gerendasy, D D; Herron, S R; Jennings, P A et al. (1995) Calmodulin stabilizes an amphiphilic alpha-helix within RC3/neurogranin and GAP-43/neuromodulin only when Ca2+ is absent. J Biol Chem 270:6741-50
de Lecea, L; Soriano, E; Criado, J R et al. (1994) Transcripts encoding a neural membrane CD26 peptidase-like protein are stimulated by synaptic activity. Brain Res Mol Brain Res 25:286-96
Di Simone, C; Zandonatti, M A; Buchmeier, M J (1994) Acidic pH triggers LCMV membrane fusion activity and conformational change in the glycoprotein spike. Virology 198:455-65
Watson, J B; Coulter 2nd, P M; Margulies, J E et al. (1994) G-protein gamma 7 subunit is selectively expressed in medium-sized neurons and dendrites of the rat neostriatum. J Neurosci Res 39:108-16

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