AI Article Synopsis
- - We studied germline changes in CDK4 exon 2, CDKN2A, and MC1R in 89 families with multiple members affected by melanoma and found that 30% carried CDKN2A variants, including three known alleles present in Mediterranean populations.
- - The prevalence of nonsynonymous MC1R variants was significantly higher (72%) in these Spanish melanoma families compared to the general population (60%).
- - Our new classification of MC1R variants linked loss of function types to an increased risk of multiple melanoma cases in families, suggesting they play a significant role in melanoma risk in areas with lower incidence rates.
Article Abstract
We explored the presence of germline alterations in CDK4 exon 2, CDKN2A and MC1R in a hospital-based study of 89 melanoma cases from 89 families with at least two members affected by cutaneous melanoma. A total of 30% of the melanoma kindreds studied were carriers of CDKN2A variants, and three of these variants were known predominant alleles that have been identified earlier in Mediterranean populations (p.G101W, p.V59G and c.358delG). We observed a higher frequency of nonsynonymous MC1R variants in these Spanish melanoma kindreds (72%) with respect to the general population (60%). We observed a higher frequency of nonsynonymous MC1R variants in this Spanish melanoma kindred (72%) respect to general population (60%). A new classification of MC1R variants based on their functional effects over melanocortin-1 receptor, including the dominant-negative effect of some of them in heterozygotes, suggested an association of loss of function MC1R variants and multiple primary melanoma cases from melanoma kindred (odds ratio: 6.07, 95% confidence interval: 1.35-27.20). This study proposes the relevance of loss of function MC1R variants in the risk of melanoma in multiple primary melanoma cases with family history from areas with low melanoma incidence rate.
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| http://dx.doi.org/10.1097/CMR.0b013e32833b159d | DOI Listing |
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