Abstract

Cutaneous melanomas arise through causal pathways involving interplay between exposure to UV radiation and host factors, resulting in characteristic patterns of driver mutations in BRAF, NRAS, and other genes. To gain clearer insights into the factors contributing to somatic mutation genotypes in melanoma, we collected clinical and epidemiologic data, performed skin examinations, and collected saliva and tumor samples from a community-based series of 414 patients aged 18 to 79, newly diagnosed with cutaneous melanoma. We assessed constitutional DNA for nine common polymorphisms in melanocortin-1 receptor gene (MC1R). Tumor DNA was assessed for somatic mutations in 25 different genes. We observed mutually exclusive mutations in BRAF(V600E) (26%), BRAF(V600K) (8%), BRAF(other) (5%), and NRAS (9%). Compared to patients with BRAF wild-type melanomas, those with BRAF(V600E) mutants were significantly younger, had more nevi but fewer actinic keratoses, were more likely to report a family history of melanoma, and had tumors that were more likely to harbor neval remnants. BRAF(V600K) mutations were also associated with high nevus counts. Both BRAF(V600K) and NRAS mutants were associated with older age but not with high sun exposure. We also found no association between MC1R status and any somatic mutations in this community sample of cutaneous melanomas, contrary to earlier reports.

Authors	Hacker, Elke; Olsen, Catherine M.; Kvaskoff, Marina; Pandeya, Nirmala; Yeo, Abrey; Green, Adele C.; Williamson, Richard M.; Triscott, Joe; Wood, Dominic; Mortimore, Rohan; Hayward, Nicholas K.; Whiteman, David C.
Journal	JOURNAL OF INVESTIGATIVE DERMATOLOGY
Pages	829-837
Volume	136
Date	1/04/2016
Grant ID
Funding Body	Sullivan and Nicolaides Pathology, Queensland Medical Laboratory
URL	http://www.ncbi.nlm.nih.gov/pubmed/?term=10.1016/j.jid.2015.12.035
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