Abstract

This renewal application to study the structure and function of the major histocompatibility complex (MHC) class II genes in vivo focuses on a recently produced strain of class II MHC-deficient mice. We have recently been successful in producing mice deficient for all class II MHC expression, using the approach of gene disruption in embryonal stem cells. It is our goal to use the class II-deficient mice in ways that will allow us to study the structure and function of class II molecules in T cell development, antigen presentation and processes of positive and negative selection, to evaluate the role of the cytoplasmic domain in vivo, and to determine the function of different cellular populations as antigen- presenting cells in vivo. This involves using these mice as recipients for A beta transgenes which have been altered by mutagenesis, or are driven by heterologous promoters which target to selected tissues. We also wish to use them as mating partners to produce and study MHC class I and II double- deficient animals. We have three Specific Aims.
In Aim 1, we wish to explore the role of the A beta cytoplasmic domain in T cell-mediated responses, antigen presentation and transmembrane signalling, as a continuation of studies currently funded by this grant. Introduction of an A beta transgene with a truncated cytoplasmic domain into the class II- deficient mice whose only class II molecule will be an I-A molecule formed by the pairing of the endogenous wild-type Aalpha b with the mutated truncated Abeta transgene. The ability of these transgenic mice to respond to foreign protein antigens, tumor antigens, viral antigens and allogeneic and xenogeneic antigens can then be evaluated. The role of the CD 28/B7 pathway and the integrity of transmembrane signalling will also be examined.
In Aim 2, we will determine which cell types are involved in antigen presentation, positive selection and tolerance by selective targeting of class II. By using the class II-deficient mice as recipients for an Abetab transgene driven by selected promoters, or as mating partners to existing I-E transgenics, tissue-specific expression of class II in B cells, macrophages and epithelial cells should by possible.
In Aim 3, will produce and analyze MHC class I and II double deficient mice by mating the class II-deficient mice with the homozygous Beta2 microglobulin-deficient 129/Sv strain developed by Jaenisch and colleagues. The analysis of these double-deficient mice will be similar to the analysis of the mice expressing a tailless I-A molecule, with special emphasis on the use of these double-deficient animals for solid organ and islet cell transplantation.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Method to Extend Research in Time (MERIT) Award (R37)
Project #
5R37AI021569-10
Application #
3481148
Study Section
Immunological Sciences Study Section (IMS)
Project Start
1984-01-01
Project End
1997-04-30
Budget Start
1993-05-01
Budget End
1994-04-30
Support Year
10
Fiscal Year
1993
Total Cost
Indirect Cost

  Institution

Name
Harvard University
Department
Type
Schools of Public Health
DUNS #
082359691
City
Boston
State
MA
Country
United States
Zip Code
02115

  Publications

Erlebacher, A (2001) Why isn't the fetus rejected? Curr Opin Immunol 13:590-3
de Bont, E S; Reilly, C R; Lo, D et al. (1999) A minimal level of MHC class II expression is sufficient to abrogate autoreactivity. Int Immunol 11:1295-306
Laufer, T M; Fan, L; Glimcher, L H (1999) Self-reactive T cells selected on thymic cortical epithelium are polyclonal and are pathogenic in vivo. J Immunol 162:5078-84
Laufer, T M; Glimcher, L H; Lo, D (1999) Using thymus anatomy to dissect T cell repertoire selection. Semin Immunol 11:65-70
Laufer, T M; Smiley, S T; Ranger, A et al. (1997) Single amino acid mutations in the murine MHC class II A beta cytoplasmic domain abrogate antigen presentation. J Immunol 159:5914-20
Tarleton, R L; Grusby, M J; Postan, M et al. (1996) Trypanosoma cruzi infection in MHC-deficient mice: further evidence for the role of both class I- and class II-restricted T cells in immune resistance and disease. Int Immunol 8:13-22
Zhao, J; Freeman, G J; Gray, G S et al. (1996) A cell type-specific enhancer in the human B7.1 gene regulated by NF-kappaB. J Exp Med 183:777-89
Steele, D J; Laufer, T M; Smiley, S T et al. (1996) Two levels of help for B cell alloantibody production. J Exp Med 183:699-703
Chakkalath, H R; Theodos, C M; Markowitz, J S et al. (1995) Class II major histocompatibility complex-deficient mice initially control an infection with Leishmania major but succumb to the disease. J Infect Dis 171:1302-8
Kuchroo, V K; Das, M P; Brown, J A et al. (1995) B7-1 and B7-2 costimulatory molecules activate differentially the Th1/Th2 developmental pathways: application to autoimmune disease therapy. Cell 80:707-18

Showing the most recent 10 out of 39 publications