Abstract

During the humoral immune response to T cell-dependent antigen, the combined processes of clonal selection and somatic hypermutation generate large clones of B cells that secrete abundant quantities of mutated antibodies. Recent studies from this laboratory have shown that antibody V regions are potentially immunogenic when viewed by the syngeneic T cell repertoire in the context of class II MHC molecules. This finding suggests that helper functions could be delivered to B cells through T cell recognition of antibody that is self-presented by the B cell. However, this would lead to a chronic state of unregulated antibody production. Therefore, we hypothesize that in the physiologic state tolerance is normally achieved to antibody V regions presented in the context of class II MHC structures. Experiments are proposed to test this hypothesis. Antibodies with well-defined V regions that are recurrently elicited in the immune response to a hapten will be tested as immunogenic substrates. T cell tolerance of these V regions in the context of class II MHC will be assessed in normal and transgenic mice that carry and express genes encoding mutated versions of these V regions known to be immunogenic. Tolerance will be assessed both before and after immune recruitment of B cells that synthesize the immunogenic V regions. The results of these experiments will advance our understanding of the role of T cell help in achieving specific humoral immunity without autoimmunity.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI033613-03
Application #
2068683
Study Section
Experimental Immunology Study Section (EI)
Project Start
1993-09-01
Project End
1996-08-31
Budget Start
1995-09-01
Budget End
1996-08-31
Support Year
3
Fiscal Year
1995
Total Cost
Indirect Cost

  Institution

Name
National Jewish Health
Department
Type
DUNS #
City
Denver
State
CO
Country
United States
Zip Code
80206

  Publications

Detanico, Thiago; St Clair, James B; Aviszus, Katja et al. (2013) Somatic mutagenesis in autoimmunity. Autoimmunity 46:102-14
Aviszus, Katja; Macleod, Megan K L; Kirchenbaum, Greg A et al. (2012) Antigen-specific suppression of humoral immunity by anergic Ars/A1 B cells. J Immunol 189:4275-83
Heiser, Ryan A; Snyder, Christopher M; St Clair, James et al. (2011) Aborted germinal center reactions and B cell memory by follicular T cells specific for a B cell receptor V region peptide. J Immunol 187:212-21
Detanico, Thiago; Heiser, Ryan A; Aviszus, Katja et al. (2011) Self-tolerance checkpoints in CD4 T cells specific for a peptide derived from the B cell antigen receptor. J Immunol 187:82-91
Guo, Wenzhong; Smith, Diana; Aviszus, Katja et al. (2010) Somatic hypermutation as a generator of antinuclear antibodies in a murine model of systemic autoimmunity. J Exp Med 207:2225-37
Guth, A; Detanico, T; Smith, D et al. (2009) Spontaneous autoimmunity in mice that carry an IghV partial transgene: a required arginine in VHCDR3. Lupus 18:299-308
Aviszus, Katja; Zhang, Xianghua; Wysocki, Lawrence J (2007) Silent development of memory progenitor B cells. J Immunol 179:5181-90
Wysocki, L J; Liu, A H; Jena, P K (1998) Somatic mutagenesis and evolution of memory B cells. Curr Top Microbiol Immunol 229:105-31
Portanova, J P; Creadon, G; Zhang, X et al. (1995) An early post-mutational selection event directs expansion of autoreactive B cells in murine lupus. Mol Immunol 32:117-35
Eyerman, M C; Wysocki, L (1994) T cell recognition of somatically-generated Ab diversity. J Immunol 152:1569-77

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