Abstract

Experimental allergic encephalomyelitis (EAE), an animal model of multiple sclerosis, is induced by generating T-cell mediated immunity to central nervous system antigens. The primary autoantigen in EAE in B10.PL mice is myelin basic protein (MBP). The immune response to MBP is predominantly directed toward residues MBP 1-11, with minor responses detected to MBP 31-50 and MBP 121-140. The basis for the dominance of MBP 1-11 and the extent to which tolerance mechanisms influence immunodominance are not understood. The role played by subdominant epitopes in autoimmune disease is also not well characterized. The extent to which subdominant epitopes participate in determinant spreading in the later stages of autoimmune disease may depend on the mechanisms responsible for their subdominance. Preliminary experiments show that endogenous expression of MBP significantly influences immunodominance of particular epitopes. In mice lacking endogenous MBP (MBP-/-), the strongest immune response is now directed toward MBP 121-140, with MBP 1-11 responses comparable to those observed in wild-type mice. Thus, wild-type mice induce tolerance in most MBP 121-140 specific T-cells while MBP 1-11 specific T-cells escape tolerance. The proposed research investigates the mechanisms underlying this differential tolerance. The investigators' hypothesis is that interactions between MBP 121-140/I-Au complexes and T-cells are of sufficient avidity to induce tolerance by clonal deletion, while interactions between MBP 1-11/I-Au complexes and T-cells are lower avidity and less able to induce tolerance. To test this hypothesis, kinetic experiments to compare both the binding affinities of MBP 1-11 and 121-140 for I-Au MHC protein as well as the effective affinities of MBP 1-11 and 121-140 specific T-cells for their respective ligands will be performed. Two possibilities for incomplete tolerance to MBP 121-140 will be addressed using both kinetic experiments and a comparison of T-cell receptor repertoires in MBP 121-140 specific T-cells from MBP+/+ (""""""""wild-type"""""""") and MBP -/- mice: 1) the minor response in wild-type mice consists of clones that escaped tolerance induction because they express lower affinity T-cell receptors than those found in MBP -/- mice, or 2) some MBP 121-140 specific T-cells in wild type mice randomly escape tolerance mechanisms and are few in number but still highly reactive to antigen. T-cell receptor transgenic models will also be developed to define the mechanisms and the site of tolerance induction to MBP 121-140.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
1R01NS035126-01A1
Application #
2038267
Study Section
Immunological Sciences Study Section (IMS)
Program Officer
Kerza-Kwiatecki, a P
Project Start
1996-12-01
Project End
2000-11-30
Budget Start
1996-12-01
Budget End
1997-11-30
Support Year
1
Fiscal Year
1997
Total Cost
Indirect Cost

  Institution

Name
University of Washington
Department
Biochemistry
Type
Schools of Medicine
DUNS #
135646524
City
Seattle
State
WA
Country
United States
Zip Code
98195

  Publications

Simmons, Sarah B; Pierson, Emily R; Lee, Sarah Y et al. (2013) Modeling the heterogeneity of multiple sclerosis in animals. Trends Immunol 34:410-22
Pierson, Emily; Simmons, Sarah B; Castelli, Luca et al. (2012) Mechanisms regulating regional localization of inflammation during CNS autoimmunity. Immunol Rev 248:205-15
Goverman, Joan M (2011) Immune tolerance in multiple sclerosis. Immunol Rev 241:228-40
McBeth, Christine; Seamons, Audrey; Pizarro, Juan C et al. (2008) A new twist in TCR diversity revealed by a forbidden alphabeta TCR. J Mol Biol 375:1306-19
Seamons, Audrey; Perchellet, Antoine; Goverman, Joan (2006) Endogenous myelin basic protein is presented in the periphery by both dendritic cells and resting B cells with different functional consequences. J Immunol 177:2097-106
Perchellet, Antoine; Stromnes, Ingunn; Pang, Jennifer M et al. (2004) CD8+ T cells maintain tolerance to myelin basic protein by 'epitope theft'. Nat Immunol 5:606-14
Seamons, Audrey; Sutton, Jennifer; Bai, Dina et al. (2003) Competition between two MHC binding registers in a single peptide processed from myelin basic protein influences tolerance and susceptibility to autoimmunity. J Exp Med 197:1391-7
Huseby, E S; Sather, B; Huseby, P G et al. (2001) Age-dependent T cell tolerance and autoimmunity to myelin basic protein. Immunity 14:471-81
Goverman, J (1999) Tolerance and autoimmunity in TCR transgenic mice specific for myelin basic protein. Immunol Rev 169:147-59
Loftus, C; Huseby, E; Gopaul, P et al. (1999) Highly cross-reactive T cell responses to myelin basic protein epitopes reveal a nonpredictable form of TCR degeneracy. J Immunol 162:6451-7

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