04222nas a2200529 4500000000100000008004100001653001000042653001100052653001100063653000900074653000900083653001600092653001900108653002000127653001400147653003500161653001900196653002500215653001700240100001400257700001200271700001700283700001900300700001600319700001700335700002000352700001400372700002200386700001900408700001100427700001600438700002200454700002000476700001800496700002000514700001700534700001500551700002100566700001900587700002100606700001900627245012500646300001400771490000800785520288500793022001403678 2017 d10aAdult10aFemale10aHumans10aAged10aMale10aMiddle Aged10aCohort Studies10aLogistic Models10aPhenotype10aReceptor, Melanocortin, Type 110aSkin Neoplasms10aMelanoma, Amelanotic10aPigmentation1 aGroup GEM1 aDwyer T1 aThomas Nancy1 aKanetsky Peter1 aBusam Klaus1 aKricker Anne1 aArmstrong Bruce1 aCust Anne1 aAnton-Culver Hoda1 aGruber Stephen1 aLuo Li1 aOrlow Irene1 aGallagher Richard1 aZanetti Roberto1 aRosso Stefano1 aSacchetto Lidia1 aOllila David1 aBegg Colin1 aBerwick Marianne1 aVernali Steven1 aWaxweiler Weston1 aDillon Patrick00aAssociation of Incident Amelanotic Melanoma With Phenotypic Characteristics, MC1R Status, and Prior Amelanotic Melanoma. a1026-10310 v1533 a
Importance: We previously reported that survival is poorer from histopathologically amelanotic than pigmented melanoma because of more advanced stage at diagnosis. Identifying patients at risk of amelanotic melanoma might enable earlier diagnosis and improved survival; however, the phenotypic characteristics and underlying genetics associated with amelanotic melanoma are unknown.
Objective: To determine whether phenotypic characteristics, carriage of MC1R variants, and history of amelanotic melanoma are associated with histopathologically amelanotic melanoma.
Design, Setting, and Participants: The Genes, Environment, and Melanoma (GEM) study is an international cohort study that enrolled patients with incident primary cutaneous melanomas from population-based and hospital-based cancer registries (1998 to 2003). The GEM participants included here were 2387 patients with data for phenotypes, MC1R genotype, and primary melanomas scored for histopathologic pigmentation. Of these 2387 patients with incident melanomas scored for pigmentation, 527 had prior primary melanomas also scored for pigmentation.
Main Outcomes and Measures: Associations of phenotypic characteristics (freckles, nevi, phenotypic index) and MC1R status with incident amelanotic melanomas were evaluated using logistic regression models adjusted for age, sex, study center, and primary status (single or multiple primary melanoma); odds ratios (ORs) and 95% CIs are reported. Association of histopathologic pigmentation between incident and prior melanomas was analyzed using an exact logistic regression model.
Results: This study included 2387 patients (1065 women, 1322 men; mean [SD] age at diagnosis, 58.3 [16.1] years) and 2917 primary melanomas. In a multivariable model including phenotypic characteristics, absence of back nevi, presence of many freckles, and a sun-sensitive phenotypic index were independently associated with amelanotic melanoma. Carriage of MC1R variants was associated with amelanotic melanoma but lost statistical significance in a model with phenotype. Further, patients with incident primary amelanotic melanomas were more likely to have had a prior primary amelanotic melanoma (OR, 4.62; 95% CI, 1.25-14.13) than those with incident primary pigmented melanomas.
Conclusions and Relevance: Absence of back nevi, presence of many freckles, a sun-sensitive phenotypic index, and prior amelanotic melanoma increase odds for development of amelanotic melanoma. An increased index of suspicion for melanoma in presenting nonpigmented lesions and more careful examination for signs of amelanotic melanoma during periodic skin examination in patients at increased odds of amelanotic melanoma might lead to earlier diagnosis and improved survival.
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