Abstract

A major question in multiple sclerosis research is the mechanism responsible for the development of neurologic deficits following demyelination. The goal of this proposal is to test the hypothesis that effector molecules released by CD8+ T cells cause neurologic deficits following demyelination by destroying or disrupting the function of axons and neurons. We have used the Theiler's virus model of demyelination to dissect the components of the MHC-restricted class I (CD8 T cells) versus MHC-restricted class II (CD4 T cells) responses to neurologic dysfunction following demyelination. Infection of class I- deficient mice results in prominent demyelination in the absence of neurologic deficits, whereas infection of class 11-deficient mice of identical genotype results in demyelination with severe neurologic dysfunction. Our first specific aim is to determine the effector molecules produced by cytotoxic T cells (IFN-gamma, Fas, TNF, and perforin) critical for induction of neurologic deficits by examining neurologic function and electrophysiology in immune knockout mice (IFN- gamma-/-, IFN-gammaR -/-, TNF -/-, TNFR -/-, PFP -/-, Fas -/-, FasL -/- )in mice of genotype resistant or susceptible to demyelination. We will also do adoptive transfer experiments into immunodeficient RAG -/- mice to determine the contribution of effector molecules with CD8 and CD4 cells to demyelination and neurologic deficit. Our specific second aim is to define the morphologic basis for functional deficits by determining whether axons are destroyed or injured in mice with immune effector deficiency following virus infection. We will assess degree of axonal dropout in normal and demyelinated white matter, perform neurofilament staining by immunofluorescence, count neurons in nuclei by retrograde labeling, and assess sodium channel distribution by [H3] saxitoxin autoradiography and fluorescence immunocytochemistry. These experiments are expected to provide new insights into the effector molecules released by the inflammatory response responsible for neurologic deficits in demyelinating disease.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
5R01NS032129-07
Application #
6187908
Study Section
Special Emphasis Panel (ZRG1-BDCN-4 (01))
Program Officer
Kerza-Kwiatecki, a P
Project Start
1994-08-01
Project End
2004-07-31
Budget Start
2000-08-01
Budget End
2001-07-31
Support Year
7
Fiscal Year
2000
Total Cost
$258,962
Indirect Cost

  Institution

Name
Mayo Clinic, Rochester
Department
Type
DUNS #
City
Rochester
State
MN
Country
United States
Zip Code
55905

  Publications

Watzlawik, Jens O; Painter, Meghan M; Wootla, Bharath et al. (2015) A human anti-polysialic acid antibody as a potential treatment to improve function in multiple sclerosis patients. J Nat Sci 1:
Paz Soldán, M Mateo; Novotna, Martina; Abou Zeid, Nuhad et al. (2015) Relapses and disability accumulation in progressive multiple sclerosis. Neurology 84:81-8
Painter, Meghan M; Morrison, James H; Zoecklein, Laurie J et al. (2015) Antiviral Protection via RdRP-Mediated Stable Activation of Innate Immunity. PLoS Pathog 11:e1005311
Perschbacher, Katherine; Smestad, John A; Peters, Justin P et al. (2015) Quantitative PCR analysis of DNA aptamer pharmacokinetics in mice. Nucleic Acid Ther 25:11-9
Wootla, Bharath; Denic, Aleksandar; Rodriguez, Moses (2014) Polyclonal and monoclonal antibodies in clinic. Methods Mol Biol 1060:79-110
Waubant, Emmanuelle; Mowry, Ellen M; Krupp, Lauren et al. (2013) Antibody response to common viruses and human leukocyte antigen-DRB1 in pediatric multiple sclerosis. Mult Scler 19:891-5
Tutuncu, Melih; Tang, Junger; Zeid, Nuhad Abou et al. (2013) Onset of progressive phase is an age-dependent clinical milestone in multiple sclerosis. Mult Scler 19:188-98
Xu, Xiaohua; Denic, Aleksandar; Warrington, Arthur E et al. (2013) Therapeutics to promote CNS repair: a natural human neuron-binding IgM regulates membrane-raft dynamics and improves motility in a mouse model of multiple sclerosis. J Clin Immunol 33 Suppl 1:S50-6
Watzlawik, Jens O; Warrington, Arthur E; Rodriguez, Moses (2013) PDGF is required for remyelination-promoting IgM stimulation of oligodendrocyte progenitor cell proliferation. PLoS One 8:e55149
Nastasijevic, Branislav; Wright, Brent R; Smestad, John et al. (2012) Remyelination induced by a DNA aptamer in a mouse model of multiple sclerosis. PLoS One 7:e39595

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