Abstract

Melanoma has a complex, multifactorial etiology that includes genetic predisposition, UV exposure and somatic genetic changes. This project is focused on the discovery of genetic alterations that play a role in the development of melanorna and the use of those genetic biomarkers in the development of two imodels. These two models will 1) provide information about risk factors tbr the probability of having melanoma and 2) risk of metastatic failure in those individuals who do develop melanoma. We will develop the genetic biomarkers for these models by: 1) analyzing the association between germline variants in DNA damage response genes and risk for melanoma; 2) evaluating the mutation spectrum of a panel of receptor tyrosine kinase genes that may play a role malignant transformation and genome instability in melanomas, and 3) identifying patterns of genomic instability in melanoma using a whole genome approach. We hypothesize that by combining established risk factors with novel genetic biomarkers from these three sources, accurate models for both risk of developing disease and risk of metastatic failure in patients who do develop melanoma can be defined for every individual. These risk profiles also will contain important biological information on melanoma initiation and progression that is needed to develop effective prevention, staging and treatment strategies.
The specific aims of this project are:
Specific Aim 1 : To identify low-penetrance melanoma susceptibility alleles in DNA damage response genes, evaluate their interaction with other genetic variants and risk factors in a case-control study and develop a multivariate melanoma etiology model.
Specific Aim 2 : To analyze a panel of 50 primary melanoma cell lines for mutations in candidate receptor tyrosine kinase genes and validate frequent mutations in 50 patient lesions.
Specific Aim 3 : To develop a novel molecular profile of melanoma using array-based comparative genomic hybridization (aCGH) to characterize amplifications and deletions across the entire genome at 1 Mb resolution.
Specific Aim 4 : To validate somatic genetic alterations as risk factors for use in prognostic models that will distinguish melanoma patients at minimal and high risk of metastasis, thus requiring different management strategies.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Specialized Center (P50)
Project #
5P50CA093372-07
Application #
7679457
Study Section
Special Emphasis Panel (ZCA1)
Project Start
Project End
Budget Start
2008-07-01
Budget End
2009-06-30
Support Year
7
Fiscal Year
2008
Total Cost
$288,392
Indirect Cost

  Institution

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

  Publications

Ojha, Rani; Leli, Nektaria M; Onorati, Angelique et al. (2018) ER translocation of the MAPK pathway drives therapy resistance in BRAF mutant melanoma. Cancer Discov :
Kugel 3rd, Curtis H; Douglass, Stephen M; Webster, Marie R et al. (2018) Age Correlates with Response to Anti-PD1, Reflecting Age-Related Differences in Intratumoral Effector and Regulatory T-Cell Populations. Clin Cancer Res 24:5347-5356
Nti, Akosua A; Serrano, Leona W; Sandhu, Harpal S et al. (2018) FREQUENT SUBCLINICAL MACULAR CHANGES IN COMBINED BRAF/MEK INHIBITION WITH HIGH-DOSE HYDROXYCHLOROQUINE AS TREATMENT FOR ADVANCED METASTATIC BRAF MUTANT MELANOMA: Preliminary Results From a Phase I/II Clinical Treatment Trial. Retina :
Onorati, Angelique V; Dyczynski, Matheus; Ojha, Rani et al. (2018) Targeting autophagy in cancer. Cancer 124:3307-3318
Noguera-Ortega, Estela; Amaravadi, Ravi K (2018) Autophagy in the Tumor or in the Host: Which Plays a Greater Supportive Role? Cancer Discov 8:266-268
Rebecca, Vito W; Nicastri, Michael C; Fennelly, Colin et al. (2018) PPT1 promotes tumor growth and is the molecular target of chloroquine derivatives in cancer. Cancer Discov :
Garman, Bradley; Anastopoulos, Ioannis N; Krepler, Clemens et al. (2017) Genetic and Genomic Characterization of 462 Melanoma Patient-Derived Xenografts, Tumor Biopsies, and Cell Lines. Cell Rep 21:1936-1952
Rebecca, Vito W; Nicastri, Michael C; McLaughlin, Noel et al. (2017) A Unified Approach to Targeting the Lysosome's Degradative and Growth Signaling Roles. Cancer Discov 7:1266-1283
Ndoye, Abibatou; Budina-Kolomets, Anna; Kugel 3rd, Curtis H et al. (2017) ATG5 Mediates a Positive Feedback Loop between Wnt Signaling and Autophagy in Melanoma. Cancer Res 77:5873-5885
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

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