Abstract

This proposal is designed to delineate and characterize the regulatory mechanism involved in the control of murine immunoglobulin class expression employing B cell cloning assays that facilitate the class switch and restricted or cloned helper T cell populations. Initially, we will continue to examine the role of the B cell in determining isotype expression by analyzing the extent to which B cells exhibit class commitment. This will be done by reducing problems associated with B cell heterogeneity through the separation of primed and unprimed B cells into defined B cell subsets based on s-Ig (e.g. s-IgA, s-IgE), Lyb surface antigens, and Fc receptors. In addition, we will examine the potential for isotype expression of these defined B cell subsets depending upon the nature of the stimulus by using T-dependent and T-independent forms of the antigen. We will then explore the functional relationship between these defined B cell subsets and helper T cells that are involved in the regulation of isotype expression. The parasite-infected mouse model provides a biological system whereby isotypic regulation by T cells may be maximal since these mice produce abnormally high levels of IgE. We will characterize the helper T cell population from such mice with particular emphasis on helper T cells that may be functionally restricted for the IgE isotype. The most powerful approach for determining the role of T cells in the class switch is the use of clonally derived helper T cells. We intend to clone helper T cells to a variety of carriers including parasite antigens and use these lines in B cell cloning assays with defined B cell subsets. Moreover, employing enrichment procedures we will try to generate isotype-specific T cells from both antigen-primed and parasite-infected mice. We will then define the nature of the target B cells as well as possible recognition elements involved when these functionally-restricted T cells are operative. The proposed studies should substantially contribute to our knowledge of the control mechanisms involved in immunoglobulin class production.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI020313-03
Application #
3129873
Study Section
Immunological Sciences Study Section (IMS)
Project Start
1984-09-01
Project End
1987-08-31
Budget Start
1986-09-01
Budget End
1987-08-31
Support Year
3
Fiscal Year
1986
Total Cost
Indirect Cost

  Institution

Name
University of Texas Health Science Center San Antonio
Department
Type
Overall Medical
DUNS #
800772162
City
San Antonio
State
TX
Country
United States
Zip Code
78229

  Publications

Estes, D M; Turaga, P S; Sievers, K M et al. (1993) Characterization of an unusual cell type (CD4+ CD3-) expanded by helminth infection and related to the parasite stress response. J Immunol 150:1846-56
Medina, C A; Teale, J M (1993) Restricted kappa chain expression in early ontogeny: biased utilization of V kappa exons and preferential V kappa-J kappa recombinations. J Exp Med 177:1317-30
Teale, J M; Medina, C A (1992) Comparative expression of adult and fetal V gene repertoires. Int Rev Immunol 8:95-111
Yeh, T M; Korsmeyer, S J; Teale, J M (1991) Skewed B cell VH family repertoire in Bcl-2-Ig transgenic mice. Int Immunol 3:1329-33
Estes, D M; Teale, J M (1991) In vivo effects of anticytokine antibodies on isotype restriction in Mesocestoides corti-infected BALB/c mice. Infect Immun 59:836-42
Bangs, L A; Sanz, I E; Teale, J M (1991) Comparison of D, JH, and junctional diversity in the fetal, adult, and aged B cell repertoires. J Immunol 146:1996-2004
Estes, D M; Teale, J M (1991) Biochemical and functional analysis of extracellular stress proteins of Mesocestoides corti. J Immunol 147:3926-34
Jeong, H D; Teale, J M (1990) Contribution of the CD5+ B cell to D-proximal VH family expression early in ontogeny. J Immunol 145:2725-9
Jones, S L; Teale, J M; Riley, S C et al. (1990) Molecular analysis of neonatal IgA expression: implications for class switching, allelic polymorphism and somatic mutation. Immunol Res 9:147-56
Desai, B B; Abraham, K M; Teale, J M (1990) The isotype potential of B cells present in BALB/c mice chronically infected with Mesocestoides corti. Cell Immunol 130:139-49

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