Abstract

The research proposed here is an ongoing inquiry into the immunogenicity, host response and natural history of human melanoma and its precursor lesions. Central to this effort is a large, well studied group of patients with melanoma and a variety of its precursors. This research utilizes both patient-derived cell lines and monoclonal antibodies directed to melanoma-associated antigens. With these materials, we have found a fundamental difference in the behavior of cell lines established from biologically early melanoma and advanced disease. Cells cultured from early melanoma (in """"""""radial growth phase"""""""") stimulate the proliferation of autologous lymphocytes. These, in turn, generate autologous tumor cytotoxicity and produce relevant lymphokines (e.g., Gamma-interferon). Expression of HLA-DR histocompatibility antigens is necesssary but insuffcient of the melanoma cells to stimulate. Melanoma cells derived from advanced disease (""""""""vertical growth phase"""""""" and metastases) are not stimulatory. Current and proposed studies are directed to: 1) identifying the antigen(s) on melanoma which, in concert with HLA-DR, provoke lymphocyte stimulation or, conversely, which are lost from those cells which do not stimulate; 2) characterizing the phenotype and function of host cells, particularly T cells, responding in vitro to autologous melanoma; 3) identifying the antigen(s) on melanoma which are the targets of specifically cytotoxic T cells; and 4) extending studies of lymphocyte stimulation and the responsible antigens to cells cultured from melanoma precursors. These studies should contribute to an understanding of the role of host cellular imunity in the developmental biology of melanoma. Such studies are of general importance to tumor immunology as melanoma (because of its easy detection and accessibility in the skin) can be investigated while the early, and presumably most important, host-tumor interactions are taking place. An understanding of these interactons should lead to strategies to manipulate the immune response to melanoma and may well lead to the development of novel therapies.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA029200-05
Application #
3168579
Study Section
Experimental Immunology Study Section (EI)
Project Start
1980-12-01
Project End
1987-12-31
Budget Start
1986-01-01
Budget End
1986-12-31
Support Year
5
Fiscal Year
1986
Total Cost
Indirect Cost

  Institution

Name
University of Pennsylvania
Department
Type
Schools of Medicine
DUNS #
042250712
City
Philadelphia
State
PA
Country
United States
Zip Code
19104

  Publications

Bennicelli, J L; Guerry 4th, D (1993) Production of multiple cytokines by cultured human melanomas. Exp Dermatol 2:186-90
Shabon, U; Bennicelli, J L; Guerry 4th, D P et al. (1991) Human melanoma cells transcribe interleukin 1 genes identical to those of monocytes. Cancer Res 51:3334-5
Bennicelli, J L; Elias, J; Kern, J et al. (1989) Production of interleukin 1 activity by cultured human melanoma cells. Cancer Res 49:930-5
Alexander, M A; Bennicelli, J; Guerry 4th, D (1989) Defective antigen presentation by human melanoma cell lines cultured from advanced, but not biologically early, disease. J Immunol 142:4070-8
Mancianti, M L; Herlyn, M; Weil, D et al. (1988) Growth and phenotypic characteristics of human nevus cells in culture. J Invest Dermatol 90:134-41
Rakowicz-Szulczynska, E M; Herlyn, M; Koprowski, H (1988) Nerve growth factor receptors in chromatin of melanoma cells, proliferating melanocytes, and colorectal carcinoma cells in vitro. Cancer Res 48:7200-6
Guerry 4th, D; Alexander, M A; Elder, D E et al. (1987) Interferon-gamma regulates the T cell response to precursor nevi and biologically early melanoma. J Immunol 139:305-12
Herlyn, M; Rodeck, U; Mancianti, M et al. (1987) Expression of melanoma-associated antigens in rapidly dividing human melanocytes in culture. Cancer Res 47:3057-61
Herlyn, D; Elder, D E; Bondi, E et al. (1986) Human cutaneous nevi transplanted onto nude mice: a model for the study of the lesional steps in tumor progression. Cancer Res 46:1339-43
Greene, M H; Clark Jr, W H; Tucker, M A et al. (1985) Acquired precursors of cutaneous malignant melanoma. The familial dysplastic nevus syndrome. N Engl J Med 312:91-7

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