Abstract

Recent investigations have identified a novel mutation in the B-RAF gene in the majority of human melanomas but a clear understanding of genetic and biologic events leading to melanoma remains elusive. Experimental investigations on melanoma development have been hampered by two major difficulties: i) the mouse is not an ideal experimental animal for melanoma-related studies because normal melanocytes are differently located in mouse versus human skin; ii) biologically early lesions cannot be obtained from pathologists because of their small size and the necessity for histologic scanning of the entire lesion. Our laboratory has developed a model of human melanoma in which human skin from healthy donors is grafted to immunodeficient mice, followed by intradermal adenovirus vector-mediated expression of three growth factors, bFGF (FGF 2), SCF (c-kit ligand) and ET-3 (endothelin-3) and concomitant irradiation with UVB (ultraviolet light in the B range). After a treatment period of only three to four weeks, highly invasive lesions developed in the human skin grafts that histologically resembled primary melanomas in patients. However, the lesions regressed in the absence of growth factors and cells cultured from the lesions showed limited life span.
The first aim proposes to induce tumorigenic melanomas using a novel skin reconstruction model for transduction of genes in melanocytes and stromal fibroblasts. We will test whether melanomas develop when melanocytes are activated by stromal and environmental stimuli, and whether they become immortal and growth factor independent when mutated genes such as mutated B-RAF are introduced.
The second aim i nvestigates the mechanisms of transformation of melanocytes to melanoma, testing the hypothesis that the growth factors bFGF, SCF, and ET-3, when produced by stromal fibroblasts, cooperate with UVB to activate critical pathways for growth, survival, and anti-apoptosis. We will focus our investigations on the MAPK, AKT, PKC, and NFKappaB signaling pathways, because we expect that their activation, together with aberrations in defined genes, leads to growth autonomy and limitless proliferative potential. Our unique model allows a systematic dissection of the biological and molecular events leading to human melanoma formation.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA080999-08
Application #
7025010
Study Section
Pathology B Study Section (PTHB)
Program Officer
Okano, Paul
Project Start
1999-04-01
Project End
2009-02-28
Budget Start
2006-04-01
Budget End
2007-02-28
Support Year
8
Fiscal Year
2006
Total Cost
$398,003
Indirect Cost

  Institution

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

  Publications

Desai, Brijal M; Villanueva, Jessie; Nguyen, Thierry-Thien K et al. (2013) The anti-melanoma activity of dinaciclib, a cyclin-dependent kinase inhibitor, is dependent on p53 signaling. PLoS One 8:e59588
Li, Ling; Fukunaga-Kalabis, Mizuho; Yu, Hong et al. (2010) Human dermal stem cells differentiate into functional epidermal melanocytes. J Cell Sci 123:853-60
Smalley, K S M; Xiao, M; Villanueva, J et al. (2009) CRAF inhibition induces apoptosis in melanoma cells with non-V600E BRAF mutations. Oncogene 28:85-94
Pinnix, Chelsea C; Lee, John T; Liu, Zhao-Jun et al. (2009) Active Notch1 confers a transformed phenotype to primary human melanocytes. Cancer Res 69:5312-20
Fukunaga-Kalabis, M; Martinez, G; Telson, S M et al. (2008) Downregulation of CCN3 expression as a potential mechanism for melanoma progression. Oncogene 27:2552-60
Smalley, Keiran S M; Contractor, Rooha; Nguyen, Thiennga K et al. (2008) Identification of a novel subgroup of melanomas with KIT/cyclin-dependent kinase-4 overexpression. Cancer Res 68:5743-52
Smalley, Keiran S M; Lioni, Mercedes; Dalla Palma, Maurizia et al. (2008) Increased cyclin D1 expression can mediate BRAF inhibitor resistance in BRAF V600E-mutated melanomas. Mol Cancer Ther 7:2876-83
Xie, Peng; Williams, Douglas S; Atilla-Gokcumen, G Ekin et al. (2008) Structure-based design of an organoruthenium phosphatidyl-inositol-3-kinase inhibitor reveals a switch governing lipid kinase potency and selectivity. ACS Chem Biol 3:305-16
Kalabis, Jiri; Oyama, Kenji; Okawa, Takaomi et al. (2008) A subpopulation of mouse esophageal basal cells has properties of stem cells with the capacity for self-renewal and lineage specification. J Clin Invest 118:3860-9
Oyama, K; Okawa, T; Nakagawa, H et al. (2007) AKT induces senescence in primary esophageal epithelial cells but is permissive for differentiation as revealed in organotypic culture. Oncogene 26:2353-64

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