Clinical, histopathological, and experimental biological investigations have defined the characteristics of human melanocytes as they progress from benign to malignant lesions. Each of 5 steps of progression has been delineated in its relation to others and in its clinical significance. However, the molecular mechanisms of melanoma progression are still poorly understood. Similarly, the functions of most molecules that are overexpressed on melanoma cells have not been clarified nor has a useful approach been defined to use patients' anti-tumor response for melanoma therapy. This program focuses on 3 research areas: molecular genetics of melanoma; biology of melanoma progression; and immune response to melanoma. These areas are all interrelated and each project contributes to and benefits from the other projects. In molecular genetics of melanoma (project #1), the hypothesis is tested that chromosome 10 contains a melanoma suppressor gene. These studies will complement ongoing research efforts to isolate a melanoma susceptibility gene on chromosome arm 9p. The biology of melanoma development and progression is addressed in four projects (#2-5). Project #2 uses two experimental approaches to drive cells from one step of tumor progression to the next. The first employs one-step and two-step carcinogenesis models in human/mouse chimeras in which ultraviolet (UV) light in the UV-B range is tested for its tumor promoting activity in normal human skin, benign nevi and biological early melanomas. The second uses a skin reconstruction model in which melanocytic cells ar engineered to overexpress an adhesion receptor (MUC18) or growth factors (pleiotrophin and PDGF). In project #3, a pleiotropic cytokine, TGF-beta, is tested for its paracrine activities during tumor growth and invasion, and for its immunosuppressive role using a melanoma model in immunocompetent mice. In project #4, three adhesion receptors MUC18, vitronectin receptor, and ICAM-1 are characterized for their ability to assess the risk for recurrence in primary melanoma. Because of its potential clinical significance, the cellular adhesion molecule MUC18 is structurally and functionally analyzed in project #5. The immune response to melanoma is investigated in project #6 through a molecular dissection of patients; B and T cell responses with the goal of developing cancer vaccines specific for individual melanoma-associated antigens, and through evolution of a therapeutic strategy based on stimulation of T cell responses to a variety of melanoma-associated antigens in melanoma patients by engineering metastatic melanoma cells to express the co-stimulatory molecule B-7-1 and the multifunctional cytokine IL-12 (project #7). This program continues to function as a focal group for progress in melanoma research in molecular biology , biology, and immunology.

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
5P01CA025874-22
Application #
6375617
Study Section
Subcommittee G - Education (NCI)
Project Start
1990-04-06
Project End
2004-04-30
Budget Start
2001-05-01
Budget End
2002-04-30
Support Year
22
Fiscal Year
2001
Total Cost
$1,303,630
Indirect Cost
Name
Wistar Institute
Department
Type
DUNS #
042250712
City
Philadelphia
State
PA
Country
United States
Zip Code
19104
Perego, M; Maurer, M; Wang, J X et al. (2018) A slow-cycling subpopulation of melanoma cells with highly invasive properties. Oncogene 37:302-312
Heppt, Markus V; Wang, Joshua X; Hristova, Denitsa M et al. (2018) MSX1-Induced Neural Crest-Like Reprogramming Promotes Melanoma Progression. J Invest Dermatol 138:141-149
Cañadas, Israel; Thummalapalli, Rohit; Kim, Jong Wook et al. (2018) Tumor innate immunity primed by specific interferon-stimulated endogenous retroviruses. Nat Med 24:1143-1150
Jenkins, Russell W; Aref, Amir R; Lizotte, Patrick H et al. (2018) Ex Vivo Profiling of PD-1 Blockade Using Organotypic Tumor Spheroids. Cancer Discov 8:196-215
Liu, Shujing; Zhang, Gao; Guo, Jianping et al. (2018) Loss of Phd2 cooperates with BRAFV600E to drive melanomagenesis. Nat Commun 9:5426
Reyes-Uribe, Patricia; Adrianzen-Ruesta, Maria Paz; Deng, Zhong et al. (2018) Exploiting TERT dependency as a therapeutic strategy for NRAS-mutant melanoma. Oncogene 37:4058-4072
Chen, Gang; Huang, Alexander C; Zhang, Wei et al. (2018) Exosomal PD-L1 contributes to immunosuppression and is associated with anti-PD-1 response. Nature 560:382-386
Taylor, Laura A; Abraham, Ronnie M; Tahirovic, Emin et al. (2017) High ALDH1 expression correlates with better prognosis in tumorigenic malignant melanoma. Mod Pathol 30:634-639
Lu, Hezhe; Liu, Shujing; Zhang, Gao et al. (2017) PAK signalling drives acquired drug resistance to MAPK inhibitors in BRAF-mutant melanomas. Nature 550:133-136
Vitiello, Marianna; Tuccoli, Andrea; D'Aurizio, Romina et al. (2017) Context-dependent miR-204 and miR-211 affect the biological properties of amelanotic and melanotic melanoma cells. Oncotarget 8:25395-25417

Showing the most recent 10 out of 382 publications