Abstract

Malignant melanoma (MM) is a singular challenge to modern oncology as it is one of the few human cancers in which the age-adjusted incidence has increased throughout the last decade, and it is notoriously refractory to therapy. The genetics of MM in humans suggest two general classes of lesions, receptor tyrosine kinase (RTK) activation, and deletion of the Ink4a/Arf locus at 9p21. Mice with melanocyte specific overexpression of H-Ras (a signaling intermediate of several RTKs) and Ink4a/Arf loss have been previously shown to develop melanoma with high penetrance and short latency. The Ink4a/Arf locus, conserved in mouse and humans, encodes two distinct proteins, p16INK4a and p19ARF, both of which regulate critical tumor suppressor pathways, and each may play a substantive role in human melanoma. Mutational analysis of human tumors and melanoma- prone kindreds clearly establish p16INK4a as a suppressor of melanoma formation, while the role of p19ARF in human tumors is less clear. Previous work in the mouse, however, shows p19ARF, through its regulation of p53, to be a critical tumor suppressor gene in a wide range of tissues. I propose to define genetically the relative importance of these two proteins in murine melanoma using two novel but as of yet uncharacterized strains of knockout mice. Using standard gene targeting techniques coupled with CRE recombinase mediated excision of the remnant selectable marker (PGK-Neo), I have produced two independent knockout (KO) strains with specific deletion of either p16INK4a or p19ARF. The work described in this proposal involves the characterization in vitro and in vivo of the p16INK4a specific KO, with a particular emphasis on melanocyte biology and melanoma formation. To c o mplement the in vivo analysis of the effect of p16INK4a loss on tumorigenesis, I will cross the p16INK4a KO to a p53-deficient background to look for increased tumor formation and change in tumor spectrum. Melanocyte growth from both p16INK4a and p19ARF null mice will be characterized in vitro, with particular emphasis on their relative transformability. Finally, I will attempt to develop a well-defined murine model of melanoma by crossing the p16INK4a and p19ARF specific KO mice to H-RAS overexpressing mice, in the hope of establishing which of the proteins, or perhaps both, is the critical mediator of melanoma susceptibility in mice in vivo. Such a model could then serve as a foundation for future studies of melanoma progression and therapy, and the results of this work will have implications for the treatment of human MM.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Clinical Investigator Award (CIA) (K08)
Project #
5K08CA090679-03
Application #
6666921
Study Section
Subcommittee G - Education (NCI)
Program Officer
Myrick, Dorkina C
Project Start
2002-02-15
Project End
2006-11-30
Budget Start
2003-03-01
Budget End
2003-11-30
Support Year
3
Fiscal Year
2003
Total Cost
$130,918
Indirect Cost

  Institution

Name
University of North Carolina Chapel Hill
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
608195277
City
Chapel Hill
State
NC
Country
United States
Zip Code
27599

  Publications

Rozenberg, Gabriela I; Monahan, Kimberly B; Torrice, Chad et al. (2010) Metastasis in an orthotopic murine model of melanoma is independent of RAS/RAF mutation. Melanoma Res 20:361-71
Shields, Janiel M; Thomas, Nancy E; Cregger, Melissa et al. (2007) Lack of extracellular signal-regulated kinase mitogen-activated protein kinase signaling shows a new type of melanoma. Cancer Res 67:1502-12
Petermann, Kimberly B; Rozenberg, Gabriela I; Zedek, Daniel et al. (2007) CD200 is induced by ERK and is a potential therapeutic target in melanoma. J Clin Invest 117:3922-9
Penland, Shannon K; Keku, Temitope O; Torrice, Chad et al. (2007) RNA expression analysis of formalin-fixed paraffin-embedded tumors. Lab Invest 87:383-91
Ji, Hongbin; Wang, Zhenxiong; Perera, Samanthi A et al. (2007) Mutations in BRAF and KRAS converge on activation of the mitogen-activated protein kinase pathway in lung cancer mouse models. Cancer Res 67:4933-9
Ji, Hongbin; Li, Danan; Chen, Liang et al. (2006) The impact of human EGFR kinase domain mutations on lung tumorigenesis and in vivo sensitivity to EGFR-targeted therapies. Cancer Cell 9:485-95
Shimamura, Takeshi; Ji, Hongbin; Minami, Yuko et al. (2006) Non-small-cell lung cancer and Ba/F3 transformed cells harboring the ERBB2 G776insV_G/C mutation are sensitive to the dual-specific epidermal growth factor receptor and ERBB2 inhibitor HKI-272. Cancer Res 66:6487-91
Ji, Hongbin; Sharpless, Norman E; Wong, Kwok-Kin (2006) EGFR targeted therapy: view from biological standpoint. Cell Cycle 5:2072-6
Krishnamurthy, Janakiraman; Torrice, Chad; Ramsey, Matthew R et al. (2004) Ink4a/Arf expression is a biomarker of aging. J Clin Invest 114:1299-307