Abstract

During the last several years this laboratory has continued to be intimately involved in the development of human lymphocyte cell separation procedures, human lymphocyte functional assays, T cell cloning strategies, T cell hybridization and the assessment of T cell surface molecules using monoclonal antibodies that together permit precise analysis of human immune responses in vitro. More recently, our laboratory has begun to utilize DNA-mediated transfer of genes encoding human T cell surface molecules to further explore functional properties of human T cells. The thrust of the current proposal is to bring to bear these newer technologies to analyze the relationship of the function of T cell surface molecules to the cellular interactions important in antigen recognition, T cell triggering and immunoregulation. Recent data from our laboratory and others strongly suggest that many if not all of the already defined surface molecules on human T cells, including the T1, T3, T4, T8 and T11 molecules themselves, as well as recently defined activation antigens, serve as critical structures important in lymphocyte function.
Our specific aims are to: (1) further define the heterogeneity of cellular functions contained within the mutually exclusive T4+ and T8+ subsets of mature human T cells. In these studies we will also continue to analyze the T-T, T-B, and T-macrophage cellular imteractions important in the functions of isolated subsets; (2) further define the precise functional role of T4+ and T8+ glycoprotein molecules themselves in antigen recognition and MHC restriction as well as helper and suppressor functions; and (3) further define the functional role of T cell glycoproteins expressed on the majority of human T cells including T1, T3 and T11 antigens. This will involve functional studies to determine the importance of these molecules in T cell triggering, activation and recognition. In many of these studies we should emphasize that we plan to analyze not only freshly isolated populations of human T cells but also IL-2 dependent T cell clones and murine fibroblasts expressing human T cell glycoproteins after DNA mediated transfer of genes encoding these molecules. These studies will be essential to further the understanding of human diseases involving immunodeficiency and/or imbalances in the regulation of T cell function including AIDS, autoimmune states and neoplastic states.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI014969-11
Application #
3125951
Study Section
Immunological Sciences Study Section (IMS)
Project Start
1978-04-01
Project End
1989-03-31
Budget Start
1988-04-01
Budget End
1989-03-31
Support Year
11
Fiscal Year
1988
Total Cost
Indirect Cost

  Institution

Name
Columbia University (N.Y.)
Department
Type
Schools of Medicine
DUNS #
064931884
City
New York
State
NY
Country
United States
Zip Code
10027

  Publications

Lederman, S; Cleary, A M; Yellin, M J et al. (1996) The central role of the CD40-ligand and CD40 pathway in T-lymphocyte-mediated differentiation of B lymphocytes. Curr Opin Hematol 3:77-86
Cleary, A M; Fortune, S M; Yellin, M J et al. (1995) Opposing roles of CD95 (Fas/APO-1) and CD40 in the death and rescue of human low density tonsillar B cells. J Immunol 155:3329-37
Ware, R; Jiang, H; Braunstein, N et al. (1995) Human CD8+ T lymphocyte clones specific for T cell receptor V beta families expressed on autologous CD4+ T cells. Immunity 2:177-84
Jiang, H; Ware, R; Stall, A et al. (1995) Murine CD8+ T cells that specifically delete autologous CD4+ T cells expressing V beta 8 TCR: a role of the Qa-1 molecule. Immunity 2:185-94
Covey, L R; Cleary, A M; Yellin, M J et al. (1994) Isolation of cDNAs encoding T-BAM, a surface glycoprotein on CD4+ T cells mediating contact-dependent helper function for B cells: identity with the CD40-ligand. Mol Immunol 31:471-84
Yellin, M J; Sinning, J; Covey, L R et al. (1994) T lymphocyte T cell-B cell-activating molecule/CD40-L molecules induce normal B cells or chronic lymphocytic leukemia B cells to express CD80 (B7/BB-1) and enhance their costimulatory activity. J Immunol 153:666-74
Lederman, S; Yellin, M J; Cleary, A M et al. (1994) T-BAM/CD40-L on helper T lymphocytes augments lymphokine-induced B cell Ig isotype switch recombination and rescues B cells from programmed cell death. J Immunol 152:2163-71
Yellin, M J; Sippel, K; Inghirami, G et al. (1994) CD40 molecules induce down-modulation and endocytosis of T cell surface T cell-B cell activating molecule/CD40-L. Potential role in regulating helper effector function. J Immunol 152:598-608
Lederman, S; Yellin, M J; Covey, L R et al. (1993) Non-antigen signals for B-cell growth and differentiation to antibody secretion. Curr Opin Immunol 5:439-44
Lederman, S; Yellin, M J; Inghirami, G et al. (1992) Molecular interactions mediating T-B lymphocyte collaboration in human lymphoid follicles. Roles of T cell-B-cell-activating molecule (5c8 antigen) and CD40 in contact-dependent help. J Immunol 149:3817-26

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