Abstract

This project will continue our studies on the soluble molecules produced by T cells which regulate T cell immunity in contact hypersensitivity to 2,4- dinitrofluorobenzene (DNFB) in mice. We have established a large panel of cloned suppressor T cell (Ts) hybridomas which produce a DNP-specific, class I MHC-restricted suppressor molecule. These Ts hybridomas have rearranged TcR alpha and beta chain genes and express a 80-90 kd alpha/beta heterodimer TcR. The suppressor molecule is a 100-11- kd heterodimer molecule and consists of a nonantigen-binding (NAgB) chain which expresses vbeta and cbeta determinants and an antigen-binding (AgB) chain which expresses Calpha determinants. The Nagb chain dictates MHC restriction and the AgB chain dictates antigen specificity. By these parameters the suppressor molecule is a soluble analogue of the TcR. This proposal will provide more definitive information concerning the biochemical properties of the suppressor molecule, its mechanism of action and its relationship to the TcR. Mechanisms will be studied by determining the effect of the suppressor molecule on various parameters of lymphokine production by DNFB- immune T cells in vitro. Studies will also be done to determine if the suppressor molecule is derived from a glycosyl-phosphatidylinositol (GPI)- linked form of the TcR. Ts hybridomas or cells expressing an engineered form of a GPI-linked TcR will be treated with phospholipase C and the supernatants tested for suppressor activity. Genes which encode the receptor and suppressor molecule will be cloned and sequenced and transfected into a panel of TcR alpha or beta chain deleted variants to restore receptor expression and suppressor molecule production. Finally, the suppressor molecule will be isolated from high titered bioreactor supernatants for biochemical characterization, sequence and crystalographic analysis. Results from these studies will enhance our understanding of how Ts cells function, how they regulate T cell-mediated immune responses and how the TcR interacts with antigen/MHC complexes. In addition, these results may provide important information useful for the development of therapeutic molecules which may be used for the antigen-specific regulation of debilitating T cell-mediated autoimmune disease

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
2R01AI012993-14A1
Application #
3125340
Study Section
Immunobiology Study Section (IMB)
Project Start
1976-06-01
Project End
1996-04-30
Budget Start
1992-07-01
Budget End
1993-04-30
Support Year
14
Fiscal Year
1992
Total Cost
Indirect Cost

  Institution

Name
University of Colorado Denver
Department
Type
Schools of Medicine
DUNS #
065391526
City
Aurora
State
CO
Country
United States
Zip Code
80045

  Publications

Moorhead, J W; Clayton, G H; Smith, R L et al. (1999) A replication-incompetent adenovirus vector with the preterminal protein gene deleted efficiently transduces mouse ears. J Virol 73:1046-53
Diiulio, N A; Fairchild, R L; Caulfield, M J (1997) The anti-erythrocyte autoimmune response of NZB mice. Identification of two distinct autoantigens. Immunology 91:246-51
Abe, M; Kondo, T; Xu, H et al. (1996) Interferon-gamma inducible protein (IP-10) expression is mediated by CD8+ T cells and is regulated by CD4+ T cells during the elicitation of contact hypersensitivity. J Invest Dermatol 107:360-6
Barbo, J V; McCormack, J E; Moorhead, J W et al. (1995) Reconstitution of TCR alpha-chain expression in deletion mutants restores dinitrophenyl-specific/class I MHC-restricted suppressor molecule production. J Immunol 154:1551-9
Fairchild, R L; Palmer, E; Moorhead, J W (1993) Production of DNP-specific/class I MHC-restricted suppressor molecules is linked to the expression of T cell receptor alpha- and beta-chain genes. J Immunol 150:67-77
Fairchild, R L; Moorhead, J W (1991) Soluble factors in tolerance and contact sensitivity to DNFB in mice. X. IL-2 is the activation signal mediating release of synthesized suppressor factor. Cell Immunol 133:147-60
Fairchild, R L; Kubo, R T; Moorhead, J W (1990) DNP-specific/class I MHC-restricted suppressor molecules bear determinants of the T cell receptor alpha- and beta-chains. The V beta 8+ chain dictates restriction to either K or D. J Immunol 145:2001-9
Fairchild, R L; Moorhead, J W (1988) Soluble factors in tolerance and contact sensitivity to DNFB in mice. VIII. Regulation of T suppressor cell function by autoreactive T helper cells. Cell Immunol 117:35-44
Fairchild, R L; Kubo, R T; Moorhead, J W (1988) Soluble factors in tolerance and contact sensitivity to 2,4-dinitro-fluorobenzene in mice. IX. A monoclonal T cell suppressor molecule is structurally and serologically related to the alpha/beta T cell receptor. J Immunol 141:3342-8
Chang, J C; Ishioka, G I; Moorhead, J W (1987) Re-presentation of the hapten dinitrophenol (DNP) to a DNP-specific T-cell line. Cell Immunol 106:1-11

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