Abstract

Clinical, histopathological, and experimental biological investigations have defined the characteristics of human melanocytes as they progress from benign to malignant lesions. Each of the five clinicopathologic steps of progression has been delineated in its relation to others and in its clinical significance. However, the molecular mechanisms of melanoma development and progression are still poorly understood. This program project has three major objectives which are investigated with unique models and tools: 1. Delineate the role of the microenvironment in melanocyte transformation, melanoma progression and host response. Project 1 investigates the microenvironment that controls melanocyte stem cell differentiation. When stem cells are activated to divide and differentiate they are likely highly susceptible to UV-induced DNA damage, which then leads to genetic aberrations (Project 2). The group determines the endogenous and exogenous mechanisms of cells escaping from the normal homeostatic environment in skin and of subsequent transformation to melanoma. Likely, the microenvironment also controls attraction of T cells to the tumor and determines their specificity and biological activity (Project 3). 2. Identify molecular mechanisms of transformation and progression. The group is testing the hypothesis that UV response genes are causatively involved in lentigo maligna melanoma (LMM) development from lentigo maligna, based on epidemiological data and our findings that chromosomal deletions in LMM include the XPG and HUS1 genes that are part of the replication checkpoint and nucleotide excision repair pathways (Project 2). The functional significance of the contribution of the replication checkpoint genes for melanoma development and maintenance is tested in Projects 2 using models of human melanoma development and progression developed in Projects 1 and 3. 3. Develop new targets for melanoma therapy. The group will identify new targets for therapy through genetic, biological, and immunological approaches. Comparative genomic hybridization (CGH) analyses of melanoma lesions (Project 2) will identify chromosomal regions with aberrations. T helper cells from melanoma patients will define new antigens that are immunogenic in patients (Project 3). Immunological approaches to melanoma marker identification have characterized in recent years a variety of proteins that are coded by mutated genes. The biological models developed in projects 1 and 3 will be utilized to select, verify and validate new targets for a growing pipeline of novel strategies for melanoma diagnosis, prognosis, prevention and therapy.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
5P01CA025874-28
Application #
7384411
Study Section
Subcommittee G - Education (NCI)
Program Officer
Sathyamoorthy, Neeraja
Project Start
1990-04-06
Project End
2010-03-31
Budget Start
2008-04-01
Budget End
2009-03-31
Support Year
28
Fiscal Year
2008
Total Cost
$1,319,037
Indirect Cost

  Institution

Name
Wistar Institute
Department
Type
DUNS #
075524595
City
Philadelphia
State
PA
Country
United States
Zip Code
19104

  Publications

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
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
Krepler, Clemens; Sproesser, Katrin; Brafford, Patricia et al. (2017) A Comprehensive Patient-Derived Xenograft Collection Representing the Heterogeneity of Melanoma. Cell Rep 21:1953-1967
Somasundaram, Rajasekharan; Zhang, Gao; Fukunaga-Kalabis, Mizuho et al. (2017) Tumor-associated B-cells induce tumor heterogeneity and therapy resistance. Nat Commun 8:607

Showing the most recent 10 out of 382 publications