Abstract

Genetic factors govern the susceptibility of individuals to a variety of human autoimmune diseases. The role of genetic factors in MS is significant. Polygenic inheritance likely characterizes MS, and it has been estimated that 1 to 3 susceptibility loci would predict the different rates of MS occurrence in studied populations. It is important to understand the nature and impact of the genes critical for susceptibility in MS, but this is problematic in any polygenic human disease, given the low general incidence, the low number of multiplex families, the small size of informative families and in the genetic diversity of the human population. Dissection of these traits in animal models is much more feasible because inbred strains may be used to control for genetic heterogeneity and even polygenic phenotypes can be understood at the genetic level. While it is not a perfect model, the genetic loci that have been found to be important in susceptibility to autoimmunity in animal models are proving useful in identifying relevant genes or pathways that are generalizable to the human conditions for which etiologic agents are unknown. We study the mechanisms and genetic control of EAE-susceptibility in inbred rats, with the goal of elucidating why certain rat strains show relatively strong resistance to the induction of this animal model of human multiple sclerosis. The ultimate goal of our research is to shed light on the genetic control autoimmunity, with possible extension to understanding the mechanisms of heritability of MS. We have now identified genetic markers that are useful for genomic screening of EAE-informative rat strain combinations and have performed the necessary preliminary genome exclusion mapping. We now propose to identify and physically map two EAE-modifying (Eaem) genes in relevant segments of rat chromosomes 4 and 5. Our results have shown that at least one gene is responsible for the EAE-susceptibility difference between F344 EAE-resistant and LEW EAE-susceptible rats; and three genes distinguish LER EAE-resistant rat from LEW rats for this trait. Our results show substantial support for the hypothesis that genes linked to the T cell receptor beta chain complex play a significant role in resistance to this autoimmune disease. In the next support period we propose to extend our genome exclusion mapping results to identify other Eae-m loci, to isolate the chromosomal segments containing these susceptibility loci in congenics, and to test the congenics for the presence of one hallmark characteristic of EAE-(MS-) susceptibility: the polarization of myelin-responsive T cells to the encephalitogenic Th1 phenotype.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
5R01NS025519-09
Application #
2702980
Study Section
Special Emphasis Panel (ZRG2-IVP (02))
Program Officer
Kerza-Kwiatecki, a P
Project Start
1988-02-01
Project End
1998-11-10
Budget Start
1998-05-01
Budget End
1998-11-10
Support Year
9
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
Allegheny University of Health Sciences
Department
Microbiology/Immun/Virology
Type
Schools of Medicine
DUNS #
City
Philadelphia
State
PA
Country
United States
Zip Code
19129

  Publications

Blankenhorn, E P; Butterfield, R J; Rigby, R et al. (2000) Genetic analysis of the influence of pertussis toxin on experimental allergic encephalomyelitis susceptibility: an environmental agent can override genetic checkpoints. J Immunol 164:3420-5
Teuscher, C; Butterfield, R J; Ma, R Z et al. (1999) Sequence polymorphisms in the chemokines Scya1 (TCA-3), Scya2 (monocyte chemoattractant protein (MCP)-1), and Scya12 (MCP-5) are candidates for eae7, a locus controlling susceptibility to monophasic remitting/nonrelapsing experimental allergic encephalomy J Immunol 163:2262-6
Bourque, M M; Martin, A M; Desquennes-Clark, L et al. (1996) Possible mechanism for the TCR beta-chain associated EAE resistance of LER rats. J Neurosci Res 45:714-22
Blankenhorn, E P; Stranford, S A; Martin, A M et al. (1995) Cloning of myelin basic protein-reactive T cells from the experimental allergic encephalomyelitis-resistant rat strain, LER. J Neuroimmunol 59:173-83
Livingstone, K D; Sudweeks, J D; Blankenhorn, E P et al. (1995) Susceptibility to actively-induced murine experimental allergic encephalomyelitis is not linked to genes of the T cell receptor or CD3 complexes. Autoimmunity 21:195-201
Wardell, B B; Michael, S D; Tung, K S et al. (1995) Aod1, the immunoregulatory locus controlling abrogation of tolerance in neonatal thymectomy-induced autoimmune ovarian dysgenesis, maps to mouse chromosome 16. Proc Natl Acad Sci U S A 92:4758-62
Sudweeks, J D; Todd, J A; Blankenhorn, E P et al. (1993) Locus controlling Bordetella pertussis-induced histamine sensitization (Bphs), an autoimmune disease-susceptibility gene, maps distal to T-cell receptor beta-chain gene on mouse chromosome 6. Proc Natl Acad Sci U S A 90:3700-4
Fu, Y; Blankenhorn, E P (1992) Nitric oxide-induced anti-mitogenic effects in high and low responder rat strains. J Immunol 148:2217-22
Blankenhorn, E P; Smith, P D; Williams, C B et al. (1992) Alleles of the rat T-cell receptor beta chain gene complex. Immunogenetics 35:324-31
Williams, C B; Blankenhorn, E P; Byrd, K E et al. (1991) Organization and nucleotide sequence of the rat T cell receptor beta-chain complex. J Immunol 146:4406-13

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