Abstract

Our goal is to investigate the intrathymic genesis of autoimmunity. Specific investigations are based on a new concept of the role of the thymus in at least one form of autoimmunity, the neuromuscular disease myasthenia gravis (MG). Most thymic epithelial cells express Ia constitutively, and medullary epithelial cells express nicotinic acetylcholine receptors (AChR), the antigen of MG. Much is known about the role of anti-AChR autoantibodies in causing failure of neuromuscular transmission in MG, but nothing is known about why these antibodies arise. In MG the thymus is a major site of anti-AChR antibody production. Its removal frequently is followed by remission of the disease. The thymus undergoes neoplastic transformation in 15% of MG patients. Studies outlined in this proposal concern the role of thymic epithelial cells in initiating autoimmunity to AChR. Hypotheses to be tested are that: i) AChR associated with thymic epithelial cells is the primary immunogen of spontaneously acquired MG; ii) this immunogenicity is promoted by activation of vertically transmitted proviral genes; iii) production of anti-AChR autoantibodies reflects an anti-tumor/virus immune response that is progressing in situ in the thymus; iv) some epitopes of the AChR expressed on thymic epithelial cells are neuroectoderm-specific and are expressed selectively on cranial (oculobulbar) muscles. The long-term goal is to find a basis for new and more effective methods of treating MG. Materials to be tested include normal thymus tissues from mice, rats and humans, and cryopreserved thymus tissue and thymomas from MG patients. The AKR/J strain of mouse, which has a 90% incidence of thymic tumors and a paradoxical susceptibility to experimental autoimmune MG (EAMG), will be investigated as a novel model of the relationship between thymoma and MG. Methods include culture of thymic epithelial cells and thymomas, probing immunologically and with 32P-cDNA for coexpression of AChR and viral or onc gene products, generation of T cell clones, testing ability of thymic epithelial cells to present AChR, testing EAMG susceptibility in AKR/J mice with thymoma suppressed by neonatal treatment with anti-gp70 antibodies, serologic comparisons of the antigenicity of AChR in thymus and cranial and limb muscles.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
5R01NS023537-05
Application #
3407159
Study Section
Immunobiology Study Section (IMB)
Project Start
1986-09-01
Project End
1992-08-31
Budget Start
1990-09-01
Budget End
1992-08-31
Support Year
5
Fiscal Year
1990
Total Cost
Indirect Cost

  Institution

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

  Publications

Vernino, Steven; Lennon, Vanda A (2004) Autoantibody profiles and neurological correlations of thymoma. Clin Cancer Res 10:7270-5
Yoshikawa, Hiroaki; Lennon, Vanda A (2002) ACh receptor protein drives primary and memory autoantibody responses in chimeric human-SCID mice. Clin Immunol 104:128-37
Yoshikawa, H; Lambert, E H; Walser-Kuntz, D R et al. (1997) A 17-Mer self-peptide of acetylcholine receptor binds to B cell MHC class II, activates helper T cells, and stimulates autoantibody production and electrophysiologic signs of myasthenia gravis. J Immunol 159:1570-7
Yoshikawa, H; Lennon, V A (1997) Acetylcholine receptor autoantibody secretion by thymocytes: relationship to myasthenia gravis. Neurology 49:562-7
McCormick, D J; Liebenow, J A; Griesmann, G E et al. (1993) Nine residues influence the binding of alpha-bungarotoxin in alpha-subunit region 185-200 of human muscle acetylcholine receptor. J Neurochem 60:1906-14
Brimijoin, S; Moser, V; Hammond, P et al. (1993) Death of intermediolateral spinal cord neurons follows selective, complement-mediated destruction of peripheral preganglionic sympathetic terminals by acetylcholinesterase antibodies. Neuroscience 54:201-23
Sano, M; Lennon, V A (1993) Enzyme immunoassay of anti-human acetylcholine receptor autoantibodies in patients with myasthenia gravis reveals correlation with striational autoantibodies. Neurology 43:573-8
Sano, M; Lambert, E H; McCormick, D J et al. (1992) Muscle acetylcholine receptors complexed with autologous IgG reflect seropositivity but not necessarily in vivo binding. Neurology 42:218-22
Victor, K D; Pascual, V; Williams, C L et al. (1992) Human monoclonal striational autoantibodies isolated from thymic B lymphocytes of patients with myasthenia gravis use VH and VL gene segments associated with the autoimmune repertoire. Eur J Immunol 22:2231-6
Williams, C L; Hay, J E; Huiatt, T W et al. (1992) Paraneoplastic IgG striational autoantibodies produced by clonal thymic B cells and in serum of patients with myasthenia gravis and thymoma react with titin. Lab Invest 66:331-6

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