Abstract

Due to the escalating incidence rate of melanoma in the USA and its high frequency to metastasize to the brain, melanoma brain metastasis (MBM) poses an increasingly significant clinical problem. In the absence of predictive biomarkers for MBM, early recognition and effective management of MBM remain inadequate to the detriment of the nation's healthcare economy and patients' quality of life. We will identify genomic and epigenomic aberrations that are signatures of MBM. We will then develop and verify these molecular aberrations as predictive molecular MBM biomarker signature(s) of stage III and IV melanomas for high-risk of MBM occurrence. Our main hypothesis is that specific genomic and epigenomic biomarkers can be identified as signatures of MBM and utilized for stage III and early stage IV melanoma metastasis for MBM occurrence.
The specific Aims are based on our strong preliminary studies on genomic and epigenomic aberrations identified in MBM.
The Specific Aims are as follows:
Aim I. Identify and develop a signature panel of MBM genomic biomarkers that can be used as predictive biomarkers in stage III and IV melanoma for MBM occurrence. Single-nucleotide polymorphism (SNP) will be used to identify copy number variations (CNV) for losses and gains as predictive biomarkers using customized quantitative PCR assays. Prioritized MBM genomic biomarkers will then be assessed as predictors of MBM occurrence.
Aim II. Identify and develop a signature panel of epigenomic MBM biomarkers that can be used as predictive biomarkers in stage III and early stage IV for MBM occurrence. Methylation array and quantitative methylation-specific PCR assays have been used to screen and identify biomarker signatures of MBM. These predictive MBM epigenomic biomarkers will then be developed and analyzed by optimized quantitative methylation-specific PCR assays. Prioritized MBM epigenomic biomarkers will then be assessed as predictors of MBM occurrence.
Aim III. Verify a MBM predictive signature(s) of genomic and/or epigenomic MBM biomarkers for stage III and IV metastasis. The optimal MBM biomarker signature panel identified in Aims I and II will be tested in patients with stage III and IV metastases, respectivey, for their ability to predict MBM occurrence using phase III multicenter clinical trial patients who have undergone surgical resection to be rendered disease-free. The studies will verify high-risk stage III and IV patients' melanoma subtypes developing into MBM, identification of new targets for therapy, and identification of MBM molecular signatures.

Public Health Relevance

The objective of this proposal is to develop MBM molecular signatures that can be used to classify MBM and used as predictive biomarkers in stage III and stage IV metastatic melanomas at high-risk MBM occurrence. The optimal predictive biomarker signature(s) will be used to identify high-risk stage III/IV melanomas for metastasis to the brain. The MBM biomarker signature will also be used to identify potential therapeutic target characteristics of MBM.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
4R01CA167967-04
Application #
9043824
Study Section
Cancer Biomarkers Study Section (CBSS)
Program Officer
Thurin, Magdalena
Project Start
2013-03-01
Project End
2018-02-28
Budget Start
2016-03-01
Budget End
2017-02-28
Support Year
4
Fiscal Year
2016
Total Cost
Indirect Cost

  Institution

Name
John Wayne Cancer Institute
Department
Type
DUNS #
556074458
City
Santa Monica
State
CA
Country
United States
Zip Code
90404

  Publications

Orozco, Javier I J; Knijnenburg, Theo A; Manughian-Peter, Ayla O et al. (2018) Epigenetic profiling for the molecular classification of metastatic brain tumors. Nat Commun 9:4627
Iida, Yuuki; Salomon, Matthew P; Hata, Keisuke et al. (2018) Predominance of triple wild-type and IGF2R mutations in mucosal melanomas. BMC Cancer 18:1054
Salomon, Matthew P; Orozco, Javier I J; Wilmott, James S et al. (2018) Brain metastasis DNA methylomes, a novel resource for the identification of biological and clinical features. Sci Data 5:180245
Klein, Anat; Sagi-Assif, Orit; Meshel, Tsipi et al. (2017) CCR4 is a determinant of melanoma brain metastasis. Oncotarget 8:31079-31091
Wang, Jinhua; Hirose, Hajime; Du, Guanhua et al. (2017) P-REX1 amplification promotes progression of cutaneous melanoma via the PAK1/P38/MMP-2 pathway. Cancer Lett 407:66-75
Iida, Yuuki; Ciechanover, Aaron; Marzese, Diego M et al. (2017) Epigenetic Regulation of KPC1 Ubiquitin Ligase Affects the NF-?B Pathway in Melanoma. Clin Cancer Res 23:4831-4842
Huynh, Kelly; Hoon, Dave S B (2016) Liquid Biopsies for Assessing Metastatic Melanoma Progression. Crit Rev Oncog 21:141-54
Huang, Sharon K; Hoon, Dave S B (2016) Liquid biopsy utility for the surveillance of cutaneous malignant melanoma patients. Mol Oncol 10:450-63
Ekmekcioglu, Suhendan; Davies, Michael A; Tanese, Keiji et al. (2016) Inflammatory Marker Testing Identifies CD74 Expression in Melanoma Tumor Cells, and Its Expression Associates with Favorable Survival for Stage III Melanoma. Clin Cancer Res 22:3016-24
Leung, Felix; Kulasingam, Vathany; Diamandis, Eleftherios P et al. (2016) Circulating Tumor DNA as a Cancer Biomarker: Fact or Fiction? Clin Chem 62:1054-60

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