Abstract

The immune response to tumors arising from a chemically induced adenocarcinoma in inbred rats ('13762') has been characterized. 13762 cells express Tumor Rejection Antigens (TRA) and a T cell-mediated immune response to 13762 cells can be induced by immunization with irradiated cells. Syngeneic Rat1 fibroblasts transformed by expression of activated ras oncogene ('Rat1/ras') can immunize rats to resist tumorigenic challenges of 13762 cells and also induce anti-tumor T cells which crossreact with 13762 cells in Winn assays. The proposed research shall: identify TRA molecules expressed by 13762 adenocarcinoma and also shall investigate the mechanism by which these antigenic tumorigenic cells escape immune response. Two hypotheses will be tested: that TRA expressed by 13762 tumor is derived from activated ras protein, and that expression of the immunomodulatory cytokine Transforming Growth Factor beta-1 by 13762 tumor is responsible for selective immunosuppression of anti-tumor immune response. To pursue the hypothesis that cross-reactive TRA molecules expressed by 13762 (and Rat1/ras) cells are derived from ras protein, in vitro proliferation and IL-2 or IFN release assays will be performed using anti-tumor T cells and synthetic peptides corresponding to selected regions of the ras protein sequence. In addition, the ability to directly immunize rats with synthetic peptides to resist 13762 (or Rat1/ras) tumorigenic challenges will be tested. In addition,TRA molecules shall be purified from 13762 cells. Anti-tumor T cells will be prepared, T-T hybridomas made by in vitro fusion with BW 5147 and tumor reactive T cell hybridomas will be cloned. Anti-tumor T cell hybridomas will form the basis of an in vitro antigen presenting system that shall be used to screen HPLC chromatography fractions derived from 13762 tumor. Purified TRA molecules will be characterized in biochemical terms and identified by deriving a partial amino acid sequence. The hypothesis that 13762 cells express Transforming Growth Factor beta-1 (TGF) which down-regulates anti-tumor immune response will be tested. Cell lines will be made in which TGF expression will be extinguished by means of antisense technology. Using the derived TGF-minus 13762 cells tumorigenicity will be correlated with TGF expression. The mechanism of activation of latent TGF elaborated by tumorigenic cells will be investigated.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA057797-03
Application #
2098543
Study Section
AIDS and Related Research Study Section 4 (ARRD)
Project Start
1992-08-01
Project End
1996-07-31
Budget Start
1994-08-01
Budget End
1995-07-31
Support Year
3
Fiscal Year
1994
Total Cost
Indirect Cost

  Institution

Name
New York University
Department
Anatomy/Cell Biology
Type
Schools of Medicine
DUNS #
004514360
City
New York
State
NY
Country
United States
Zip Code
10012

  Publications

Saio, Masanao; Teicher, Matt; Campbell, Gaynor et al. (2004) Immunocytochemical demonstration of down regulation of HLA class-I molecule expression in human metastatic breast carcinoma. Clin Exp Metastasis 21:243-9
Lee, C K; Rao, D T; Gertner, R et al. (2000) Distinct requirements for IFNs and STAT1 in NK cell function. J Immunol 165:3571-7
Radoja, S; Frey, A B (2000) Cancer-induced defective cytotoxic T lymphocyte effector function: another mechanism how antigenic tumors escape immune-mediated killing. Mol Med 6:465-79
Rao, T D; Frey, A B (1998) Administration of silica sensitizes lipopolysaccharide responsiveness of murine macrophages but inhibits T and B cell priming by inhibition of antigen presenting function. Immunol Invest 27:181-99
Frey, A B (1997) Study of immune response to tumors in the rat. Methods 12:173-88
Frey, A B; Cestari, S (1997) Killing of rat adenocarcinoma 13762 in situ by adoptive transfer of CD4+ anti-tumor T cells requires tumor expression of cell surface MHC class II molecules. Cell Immunol 178:79-90
Appleman, L J; Frey, A B (1996) Tumors antigens encoded by oncogenes and the impact of oncogenes upon the immune responses. Cell Immunol 170:1-10
Frey, A B (1996) Role of host antigen receptor-bearing and antigen receptor-negative cells in immune response to rat adenocarcinoma 13762. J Immunol 156:3841-9
Frey, A B (1995) Rat mammary adenocarcinoma 13762 expressing IFN-gamma elicits antitumor CD4+ MHC class II-restricted T cells that are cytolytic in vitro and tumoricidal in vivo. J Immunol 154:4613-22
Frey, A B; Cestari, S (1995) Expression of activated H-rasval12 in nontumorigenic and non-cross-reactive syngeneic cells induces tumor antigens cross-reactive with rat mammary adenocarcinoma 13762. J Immunol 155:4783-9

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