| Literature DB >> 27476724 |
Jianxin Shi1, Weiyin Zhou2, Bin Zhu1, Paula L Hyland1, Hunter Bennett1, Yanzi Xiao1, Xijun Zhang2, Laura S Burke3, Lei Song1, Chih Hao Hsu4, Chunhua Yan4, Qingrong Chen4, Daoud Meerzaman4, Casey L Dagnall2, Laurie Burdette2, Belynda Hicks2, Neal D Freedman1, Stephen J Chanock1, Meredith Yeager2, Margaret A Tucker1, Alisa M Goldstein1, Xiaohong R Yang5.
Abstract
Mounting evidence suggests that copy number variations (CNVs) can contribute to cancer susceptibility. The main goal of this study was to evaluate the role of germline CNVs in melanoma predisposition in high-risk melanoma families. We used genome-wide tiling comparative genomic hybridization and single nucleotide polymorphism arrays to characterize CNVs in 335 individuals (240 melanoma cases) from American melanoma-prone families (22 with germline CDKN2A or CDK4 mutations). We found that the global burden of overall CNVs (or deletions or duplications separately) was not significantly associated with case-control or CDKN2A/CDK4 mutation status after accounting for the familial dependence. However, we identified several rare CNVs that either involved known melanoma genes (e.g., PARP1, CDKN2A) or cosegregated with melanoma (duplication on 10q23.23, 3p12.2 and deletions on 8q424.3, 2q22.1) in families without mutations in known melanoma high-risk genes. Some of these CNVs were correlated with expression changes in disrupted genes based on RNASeq data from a subset of melanoma cases included in the CNV study. These results suggest that rare cosegregating CNVs may influence melanoma susceptibility in some melanoma-prone families and genes found in our study warrant further evaluation in future genetic analyses of melanoma.Entities:
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Year: 2016 PMID: 27476724 PMCID: PMC5123914 DOI: 10.1016/j.jid.2016.07.023
Source DB: PubMed Journal: J Invest Dermatol ISSN: 0022-202X Impact factor: 8.551