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MC1Rgenotype as a predictor of early-onset melanoma, compared with self-reported and physician-measured traditional risk factors: an Australian case-control-family study
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MC1Rgenotype as a predictor of early-onset melanoma, compared with self-reported and physician-measured traditional risk factors: an Australian case-control-family study
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MC1Rgenotype as a predictor of early-onset melanoma, compared with self-reported and physician-measured traditional risk factors: an Australian case-control-family study
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Journal Article
MC1Rgenotype as a predictor of early-onset melanoma, compared with self-reported and physician-measured traditional risk factors: an Australian case-control-family study
2013
Overview
Background
Melanocortin-1 receptor (
MC1R
) gene variants are very common and are associated with melanoma risk, but their contribution to melanoma risk prediction compared with traditional risk factors is unknown. We aimed to 1) evaluate the separate and incremental contribution of
MC1R
genotype to prediction of early-onset melanoma, and compare this with the contributions of physician-measured and self-reported traditional risk factors, and 2) develop risk prediction models that include
MC1R
, and externally validate these models using an independent dataset from a genetically similar melanoma population.
Methods
Using data from an Australian population-based, case-control-family study, we included 413 case and 263 control participants with sequenced
MC1R
genotype, clinical skin examination and detailed questionnaire. We used unconditional logistic regression to estimate predicted probabilities of melanoma. Results were externally validated using data from a similar study in England.
Results
When added to a base multivariate model containing only demographic factors,
MC1R
genotype improved the area under the receiver operating characteristic curve (AUC) by 6% (from 0.67 to 0.73;
P
< 0.001) and improved the quartile classification by a net 26% of participants. In a more extensive multivariate model, the factors that contributed significantly to the AUC were
MC1R
genotype, number of nevi and previous non-melanoma skin cancer; the AUC was 0.78 (95% CI 0.75-0.82) for the model with self-reported nevi and 0.83 (95% CI 0.80-0.86) for the model with physician-counted nevi. Factors that did not further contribute were sun and sunbed exposure and pigmentation characteristics. Adding
MC1R
to a model containing pigmentation characteristics and other self-reported risk factors increased the AUC by 2.1% (
P
= 0.01) and improved the quartile classification by a net 10% (95% CI 1-18%,
P
= 0.03).
Conclusions
Although
MC1R
genotype is strongly associated with skin and hair phenotype, it was a better predictor of early-onset melanoma than was pigmentation characteristics. Physician-measured nevi and previous non-melanoma skin cancer were also strong predictors. There might be modest benefit to measuring
MC1R
genotype for risk prediction even if information about traditional self-reported or clinically measured pigmentation characteristics and nevi is already available.
Publisher
BioMed Central,BioMed Central Ltd
Subject
