Abstract

Using a case series of 600 patients with melanoma, we will perform an integrated molecular epidemiologic study to correlate genetic susceptibility phenotype and genotype data from lymphocytes and to extend these findings in surrogate tissue to the tumor tissue. We will measure functional nucleotide excision repair (NER) capacity by using the host cell reactivation assay with plasmids damaged by ultraviolet light and determine the frequencies of polymorphisms in the DNA repair genes (ERCC1, XPA, XPB, XPC, XPD, XPF, and XPG) implicated in the NER pathway. We will correlate the genotypes with functional NER activity. We hypothesize that individuals with """"""""adverse"""""""" genotypes of the NER pathway will have poorer DNA repair capacity (DRC) than individuals with wild-type genotypes. In a subset of 400 patients, we will also determine the frequencies of mutations in the newly described BRAF gene and loss of heterozygosity (LOH) at lp36, 6q22-23, 8p22-24, 9p21-22, 10q23, and 1lq23 in tumor tissues and compare these tumor markers with sunlight exposure levels and constitutional markers of genomic instability (DRC and genotypes measured in lymphocytes). We hypothesize that the severity of mutations and loci-specific alterations in tumor tissues will be correlated with adverse susceptibility markers in surrogate tissue and with degree of exposure. The overarching goal of these studies is to determine whether the lymphocyte markers that we have already shown to be significant predictors of cancer risk (DRC and DNA repair gene polymorphisms) are an adequate reflection of genetic events in the target organ tissue. This finding will have substantial implications for future large-scale population-based molecular epidemiology studies and risk assessment for prevention and early detection of melanoma. Surrogate markers that best predict carcinogenic events in the target tissue will be useful for identifying high-risk subgroups for intensive screening and chemopreventive interventions. The ability to rapidly screen individuals for risk using minimally invasive procedures (blood analysis) has immense clinical implication.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Specialized Center (P50)
Project #
1P50CA093459-01A1
Application #
6993420
Study Section
Special Emphasis Panel (ZCA1-GRB-V (O1))
Project Start
2004-07-09
Project End
2009-05-31
Budget Start
2004-07-09
Budget End
2005-05-31
Support Year
1
Fiscal Year
2004
Total Cost
$191,918
Indirect Cost

  Institution

Name
University of Texas MD Anderson Cancer Center
Department
Type
DUNS #
800772139
City
Houston
State
TX
Country
United States
Zip Code
77030

  Publications

(2018) Genome-wide association analyses identify 44 risk variants and refine the genetic architecture of major depression. Nat Genet 50:668-681
Shah, Maitri Y; Ferracin, Manuela; Pileczki, Valentina et al. (2018) Cancer-associated rs6983267 SNP and its accompanying long noncoding RNA CCAT2 induce myeloid malignancies via unique SNP-specific RNA mutations. Genome Res 28:432-447
Huckins, L M; Hatzikotoulas, K; Southam, L et al. (2018) Investigation of common, low-frequency and rare genome-wide variation in anorexia nervosa. Mol Psychiatry 23:1169-1180
Kim, Sun-Hee; Roszik, Jason; Cho, Sung-Nam et al. (2018) The COX2 effector microsomal PGE2 synthase-1 is a regulator of immunosuppression in cutaneous melanoma. Clin Cancer Res :
Zhang, Tongwu; Choi, Jiyeon; Kovacs, Michael A et al. (2018) Cell-type-specific eQTL of primary melanocytes facilitates identification of melanoma susceptibility genes. Genome Res 28:1621-1635
Velazquez-Torres, Guermarie; Shoshan, Einav; Ivan, Cristina et al. (2018) A-to-I miR-378a-3p editing can prevent melanoma progression via regulation of PARVA expression. Nat Commun 9:461
Cascone, Tina; McKenzie, Jodi A; Mbofung, Rina M et al. (2018) Increased Tumor Glycolysis Characterizes Immune Resistance to Adoptive T Cell Therapy. Cell Metab 27:977-987.e4
Li, Bo; Wang, Yanru; Xu, Yinghui et al. (2018) Genetic variants in RORA and DNMT1 associated with cutaneous melanoma survival. Int J Cancer 142:2303-2312
Teerlink, Craig C; Huff, Chad; Stevens, Jeff et al. (2018) A Nonsynonymous Variant in the GOLM1 Gene in Cutaneous Malignant Melanoma. J Natl Cancer Inst :
Bezrookove, Vladimir; Nosrati, Mehdi; Miller 3rd, James R et al. (2018) Role of Elevated PHIP Copy Number as a Prognostic and Progression Marker for Cutaneous Melanoma. Clin Cancer Res 24:4119-4125

Showing the most recent 10 out of 290 publications