Abstract

Breast adenocarcinomas arise from malignant transformation of normal ductal epithelial cells. In the process of characterizing specificity of T cell lines derived from breast cancer patients and cytotoxic for breast tumors, we identified ductal epithelial cell mucin as the antigen on the tumor capable of stimulating patients' T cell immunity. We further identified one epitope on this antigen which serves as a target for tumor specific CTL. Normal mucin producing cells do not express this epitope and its presence correlates with the susceptibility to lysis of tumor cells by the CTL. This epitope and several others are preferentially expressed on tumor mucin due to incomplete glycosylation of this molecule by the tumor. We have determined that transfection of EBV immortalized B cells or primary fibroblast cultures with mucin cDNA plasmid expression vector and treatment of transfected cells with inhibitors of O-linked glycosylation results in tumorlike processing of the mucin molecule and high level expression of these epitopes. The overall goals of this proposal are to utilize the knowledge of one tumor specific epitope we have identified so far on breast cancer mucin, capable of stimulating human T cells, and our ability to recreate this epitope, as well as several others, in mucin transfected normal cells, to explore the possibility of constructing breast tumor specific vaccine. Sequence identity between the chimpanzee and human mucin allows us to test this mucin-based vaccine in vivo. 1) We will utilize plasmid expression vectors to express mucin in autochthonous antigen presenting cells(APC), (human as well as chimpanzee), and glycosylation inhibitors to expose tumor specific mucin epitopes, and perform in vitro analysis of T cell responses to these epitopes. 2) We will test the ability of glycosylation-inhibited, mucin transfected autochthonous APC to stimulate specific T cell responses in vivo, in chimpanzees immunized with these cells. 3) We will construct and test in vitro and in vivo new expression vectors containing partial mucin polypeptide core sequences with glycosylation sites mutated in order to ensure incomplete glycosylation and constitutive expression of tumor specific mucin epitopes.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA057820-04
Application #
2098561
Study Section
AIDS and Related Research Study Section 4 (ARRD)
Project Start
1992-08-07
Project End
1997-05-31
Budget Start
1995-06-01
Budget End
1996-05-31
Support Year
4
Fiscal Year
1995
Total Cost
Indirect Cost

  Institution

Name
University of Pittsburgh
Department
Genetics
Type
Schools of Medicine
DUNS #
053785812
City
Pittsburgh
State
PA
Country
United States
Zip Code
15213

  Publications

Kirii, Y; Magarian-Blander, J; Alter, M D et al. (1998) Functional and molecular analysis of T cell receptors used by pancreatic- and breast tumor- (mucin-) specific cytotoxic T cells. J Immunother 21:188-97
Henderson, R A; Konitsky, W M; Barratt-Boyes, S M et al. (1998) Retroviral expression of MUC-1 human tumor antigen with intact repeat structure and capacity to elicit immunity in vivo. J Immunother 21:247-56
Magarian-Blander, J; Ciborowski, P; Hsia, S et al. (1998) Intercellular and intracellular events following the MHC-unrestricted TCR recognition of a tumor-specific peptide epitope on the epithelial antigen MUC1. J Immunol 160:3111-20
Poland, P A; Kinlough, C L; Rokaw, M D et al. (1997) Differential glycosylation of MUC1 in tumors and transfected epithelial and lymphoblastoid cell lines. Glycoconj J 14:89-96
Barratt-Boyes, S M; Watkins, S C; Finn, O J (1997) Migration of cultured chimpanzee dendritic cells following intravenous and subcutaneous injection. Adv Exp Med Biol 417:71-5
Magarian-Blander, J; Hughey, R P; Kinlough, C et al. (1996) Differential expression of MUC1 on transfected cell lines influences its recognition by MUC1 specific T cells. Glycoconj J 13:749-56
Finn, O J; Debruyne, L A; Bishop, D K (1996) T cell receptor (TCR) repertoire in alloimmune responses. Int Rev Immunol 13:187-207
Pecher, G; Finn, O J (1996) Induction of cellular immunity in chimpanzees to human tumor-associated antigen mucin by vaccination with MUC-1 cDNA-transfected Epstein-Barr virus-immortalized autologous B cells. Proc Natl Acad Sci U S A 93:1699-704
Henderson, R A; Finn, O J (1996) Human tumor antigens are ready to fly. Adv Immunol 62:217-56
Ciborowski, P; Finn, O J (1995) Recombinant epithelial cell mucin (MUC-1) expressed in baculovirus resembles antigenically tumor associated mucin, target for cancer immunotherapy. Biomed Pept Proteins Nucleic Acids 1:193-8

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