Abstract

Astrocytes play critical roles in the biology and diseases of the central nervous system, yet much remains to be learned about their function. Recent advances in the molecular biology of astrocyte-specific genes offer new opportunities for genetic manipulation of astrocyte function in vivo through transgenic techniques. Our goals are to understand how the glial- specific intermediate filament, glial fibrillary acidic protein (GFAP), contributes to the development and reactions to injury of astrocytes in the central nervous system. We propose to test the hypothesis that GFAP expression itself directly influences the ability of astrocytes to form processes in vivo, and to form gliotic scars following injury, by generation of two kinds of transgenic mice. First, we will force over- expression of GFAP in astrocytes by adding multiple copies of functional GFAP genes to the mouse germ-line. These mice will demonstrate whether up- regulation of GFAP itself can initiate astrocyte hypertrophy. Second, we will prevent GFAP expression by generation of mice specifically mutated at the GFAP locus. These mice will demonstrate whether GFAP is necessary for astrocyte development and gliosis. In each case the entire nervous system will be surveyed by light microscopy, but particular attention will be focussed on the cerebellum, spinal cord, optic nerve, and retina. Finally, we will examine whether changes in astrocyte expression of GFAP result in altered responses to injuries such as trauma. The proposed experiments promise further understanding of the molecular and cell biological properties of GFAP in astrocytes, and ultimately the functions of astrocytes in normal development and diseases of the central nervous system.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
2R01NS022475-07A3
Application #
2264522
Study Section
Neurology C Study Section (NEUC)
Project Start
1985-09-23
Project End
1998-01-31
Budget Start
1995-04-01
Budget End
1996-01-31
Support Year
7
Fiscal Year
1995
Total Cost
Indirect Cost

  Institution

Name
University of Wisconsin Madison
Department
Pathology
Type
Schools of Veterinary Medicine
DUNS #
161202122
City
Madison
State
WI
Country
United States
Zip Code
53715

  Publications

Messing, Albee; Li, Rong; Naidu, Sakkubai et al. (2012) Archetypal and new families with Alexander disease and novel mutations in GFAP. Arch Neurol 69:208-14
Messing, Albee; Brenner, Michael; Feany, Mel B et al. (2012) Alexander disease. J Neurosci 32:5017-23
Hagemann, Tracy L; Gaeta, Stephen A; Smith, Mark A et al. (2005) Gene expression analysis in mice with elevated glial fibrillary acidic protein and Rosenthal fibers reveals a stress response followed by glial activation and neuronal dysfunction. Hum Mol Genet 14:2443-58
van der Knaap, Marjo S; Salomons, Gajja S; Li, Rong et al. (2005) Unusual variants of Alexander's disease. Ann Neurol 57:327-38
Su, Mu; Hu, Huimin; Lee, Youngjin et al. (2004) Expression specificity of GFAP transgenes. Neurochem Res 29:2075-93
Messing, Albee; Brenner, Michael (2003) GFAP: functional implications gleaned from studies of genetically engineered mice. Glia 43:87-90
Lesche, Ralf; Groszer, Matthias; Gao, Jing et al. (2002) Cre/loxP-mediated inactivation of the murine Pten tumor suppressor gene. Genesis 32:148-9
Li, Rong; Messing, Albee; Goldman, James E et al. (2002) GFAP mutations in Alexander disease. Int J Dev Neurosci 20:259-68
Gorospe, J R; Naidu, S; Johnson, A B et al. (2002) Molecular findings in symptomatic and pre-symptomatic Alexander disease patients. Neurology 58:1494-500
Zhuo, L; Theis, M; Alvarez-Maya, I et al. (2001) hGFAP-cre transgenic mice for manipulation of glial and neuronal function in vivo. Genesis 31:85-94

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