Abstract

The objectives of this research are to provide insight into: 1) the relation of membrane sterol composition to biochemical expressions of glial differentiation and to ionic flux, 2) the relation of cytoskeletal structures to HMG-CoA reductase and cholesterol biosynthesis, 3) the relation of fatty acyl alterations to cholesterol biosynthesis, membrane lipid composition and oligodendroglial differentiation, and 4) the interrelations of lipid synthesis and specific events in brain development. The relation of membrane sterol composition to biochemical expressions of glial differentiation and to ionic flux will be studied in cultured C-6 glial cells, which can be induced to exhibit oligodendroglial or astrocytic properties. Membrane sterol composition will be altered by specific inhibitors of cholesterol biosynthesis, e.g., compactin and U18666A, which operate at different sites in the biosynthetic pathway. Correction of the lipid defects by addition of exogenous sources of sterol will help determine the precise relationships between membrane lipid alterations and the observed effects. The relation of cytoskeletal structures to HMG-CoA reductase and cholesterol biosynthesis will be studied principally in cultured C-6 glia. We will determine: 1) the relationships between tubulin polymerization and the activity of HMG-CoA reductase, 2) the cellular specificity of the relationships, 3) the mechanism of the changes in reductase activity, and 4) the consequences of alterations in reductase activity re: synthesis of nonsterol isoprenoid compounds, as well as sterol, and re: membrane lipid composition. The relations of fatty acyl alterations to cholesterol biosynthesis, membrane lipid composition and oligodendroglial differentiation will be studied in cultured C-6 glia. Fatty acyl alterations will be produced by providing the fatty acids to cells in serum-free medium. The interrelations of lipid synthesis, cellular proliferation, neuronal and glial differentiation, and myelination will be studied in aggregating brain cell cultures. We will determine the major correlates of these specific developmental events re: sterol and fatty acid (de novo and chain elongation systems) synthesis and re: the regulation of these pathways at the enzyme level. The specific roles of sterols in these events will be determined by utilization of specific inhibitors.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Research Project (R01)
Project #
5R01HD007464-12
Application #
3310682
Study Section
Metabolism Study Section (MET)
Project Start
1976-12-01
Project End
1986-11-30
Budget Start
1984-12-01
Budget End
1985-11-30
Support Year
12
Fiscal Year
1985
Total Cost
Indirect Cost

  Institution

Name
Washington University
Department
Type
Schools of Medicine
DUNS #
062761671
City
Saint Louis
State
MO
Country
United States
Zip Code
63130

  Publications

Oka, A; Belliveau, M J; Rosenberg, P A et al. (1993) Vulnerability of oligodendroglia to glutamate: pharmacology, mechanisms, and prevention. J Neurosci 13:1441-53
Ishii, S; Volpe, J J (1992) Glycoprotein processing is required for completion but not initiation of oligodendroglial differentiation from its bipotential progenitor cell. Dev Neurosci 14:221-9
Ishii, S; Volpe, J J (1992) Establishment of a culture system for the study of oligodendroglial development: complementary effects of boiled serum and astrocyte extract. Dev Neurosci 14:230-7
Callahan, D J; Engle, M J; Volpe, J J (1990) Hypoxic injury to developing glial cells: protective effect of high glucose. Pediatr Res 27:186-90
Ishii, S; Volpe, J J (1990) N-linked glycoprotein synthesis and transport during G1 are necessary for astrocytic proliferation. J Neurosci Res 26:419-27
Ishii, S; Volpe, J J (1990) Specific N-linked oligosaccharides are required for oligodendroglial differentiation but probably not for astrocytic differentiation. Dev Neurosci 12:46-60
Bass, T; Volpe, J J (1989) Ethanol in clinically relevant concentrations enhances expression of oligodendroglial differentiation but has no effect on astrocytic differentiation or DNA synthesis in primary cultures. Dev Neurosci 11:52-64
Ishii, S; Volpe, J J (1988) Dolichol-linked oligosaccharide and glycoprotein biosyntheses in glial cells in primary culture: development and enzymatic correlates. J Neurosci Res 20:463-72
Volpe, J J; Sakakihara, Y; Ishii, S (1987) Dolichol-linked glycoprotein synthesis in developing mammalian brain: maturational changes of the N-acetylglucosaminylphosphotransferase. Brain Res 430:277-84
Langan, T J; Volpe, J J (1987) Cell cycle-specific requirement for mevalonate, but not for cholesterol, for DNA synthesis in glial primary cultures. J Neurochem 49:513-21

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