Abstract

It has now been successfully shown in a number of animal and human tumors that a specific immune response can be generated against the tumor. This foreshadows an era of immune manipulation of tumor growth and eventual recruitment of the immune system in the process of tumor destruction. The success of immunotherapy depends on further understanding of the multitude of reasons why the observed anti-tumor response is seldom effective. At the root of that understanding is the need to know the target antigen on the tumor cell. Patients with pancreatic and breast adenocarcinomas mount a specific T cell response to their tumors. CD8+ as well as CD4+ T cells can be isolated from tumor draining lymph nodes, both populations specifically recognizing epithelial mucin as the target antigen. This antigen coats the tumor cells and is also present on normal ductal epithelial cells but not recognized by the T cells until malignant transformation unmasks specific T cell epitopes. The epitopes recognized by the two T cell populations reside on a 20aa tandemly repeated peptide which comprises the mucin polypeptide core. The tandem repeat structure endows this antigen with antigenic multivalency, potentially useful in immunotherapy, which gives it the ability under certain circumstances to activate T cells directly. The ability of this antigen to stimulate both helper and cytotoxic T cells fulfills a critical requirement for establishment of an efficient immune response. Yet, the patient succumbs to the tumor. Potential reasons may be insufficient numbers of tumor-specific CTL and anergy in the helper T cell compartment. In this application we propose: I. To investigate MHC-restricted and MHC-unrestricted activation of CTL by mucin antigen in order to validate methods for in vitro and in vivo generation of large numbers of CD8+, tumor specific CTL. II. To investigate routes of antigen presentation which can lead to generation of large numbers of functional CD4+, tumor specific T helper cells. III. To investigate the state of anergy of the CD4+ T cells and ways in which this anergy may be broken, or the cells otherwise altered to provide functional help. The long term goals of the project are to fully understand the anti-tumor mucin response and its potential for immunotherapy.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA056103-02
Application #
3200604
Study Section
Experimental Therapeutics Subcommittee 1 (ET)
Project Start
1991-06-01
Project End
1996-05-31
Budget Start
1992-06-01
Budget End
1993-05-31
Support Year
2
Fiscal Year
1992
Total Cost
Indirect Cost

  Institution

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

  Publications

Cascio, Sandra; Faylo, Jacque L; Sciurba, Joshua C et al. (2017) Abnormally glycosylated MUC1 establishes a positive feedback circuit of inflammatory cytokines, mediated by NF-?B p65 and EzH2, in colitis-associated cancer. Oncotarget 8:105284-105298
Lohmueller, Jason J; Sato, Shuji; Popova, Lana et al. (2016) Antibodies elicited by the first non-viral prophylactic cancer vaccine show tumor-specificity and immunotherapeutic potential. Sci Rep 6:31740
Finn, Olivera J; Beatty, Pamela L (2016) Cancer immunoprevention. Curr Opin Immunol 39:52-8
Finn, Olivera J; Khleif, Samir N; Herberman, Ronald B (2015) The FDA guidance on therapeutic cancer vaccines: the need for revision to include preventive cancer vaccines or for a new guidance dedicated to them. Cancer Prev Res (Phila) 8:1011-6
Marvel, Douglas M; Finn, Olivera J (2014) Global Inhibition of DC Priming Capacity in the Spleen of Self-Antigen Vaccinated Mice Requires IL-10. Front Immunol 5:59
Finn, Olivera J (2014) Vaccines for cancer prevention: a practical and feasible approach to the cancer epidemic. Cancer Immunol Res 2:708-13
Iheagwara, Uzoma K; Beatty, Pamela L; Van, Phu T et al. (2014) Influenza virus infection elicits protective antibodies and T cells specific for host cell antigens also expressed as tumor-associated antigens: a new view of cancer immunosurveillance. Cancer Immunol Res 2:263-73
Kimura, Takashi; Finn, Olivera J (2013) MUC1 immunotherapy is here to stay. Expert Opin Biol Ther 13:35-49
Zhang, Lixin; Vlad, Anda; Milcarek, Christine et al. (2013) Human mucin MUC1 RNA undergoes different types of alternative splicing resulting in multiple isoforms. Cancer Immunol Immunother 62:423-35
Cascio, Sandra; Farkas, Adam M; Hughey, Rebecca P et al. (2013) Altered glycosylation of MUC1 influences its association with CIN85: the role of this novel complex in cancer cell invasion and migration. Oncotarget 4:1686-97

Showing the most recent 10 out of 62 publications