Your search keyword '"Begg, Colin B"' showing total 47 results

1. Sex-Specific Associations of MDM2 and MDM4 Variants with Risk of Multiple Primary Melanomas and Melanoma Survival in Non-Hispanic Whites.

Author

Ward, Sarah V, Ward, Sarah V, Autuori, Isidora, Luo, Li, LaPilla, Emily, Yoo, Sarah, Sharma, Ajay, Busam, Klaus J, Olilla, David W, Dwyer, Terence, Anton-Culver, Hoda, Zanetti, Roberto, Sacchetto, Lidia, Cust, Anne E, Gallagher, Richard P, Kanetsky, Peter A, Rosso, Stefano, Begg, Colin B, Berwick, Marianne, Thomas, Nancy E, Orlow, Irene, GEM Study Group, Ward, Sarah V, Ward, Sarah V, Autuori, Isidora, Luo, Li, LaPilla, Emily, Yoo, Sarah, Sharma, Ajay, Busam, Klaus J, Olilla, David W, Dwyer, Terence, Anton-Culver, Hoda, Zanetti, Roberto, Sacchetto, Lidia, Cust, Anne E, Gallagher, Richard P, Kanetsky, Peter A, Rosso, Stefano, Begg, Colin B, Berwick, Marianne, Thomas, Nancy E, Orlow, Irene, and GEM Study Group

Abstract

MDM2-SNP309 (rs2279744), a common genetic modifier of cancer incidence in Li-Fraumeni syndrome, modifies risk, age of onset, or prognosis in a variety of cancers. Melanoma incidence and outcomes vary by sex, and although SNP309 exerts an effect on the estrogen receptor, no consensus exists on its effect on melanoma. MDM2 and MDM4 restrain p53-mediated tumor suppression, independently or together. We investigated SNP309, an a priori MDM4-rs4245739, and two coinherited variants, in a population-based cohort of 3663 primary incident melanomas. Per-allele and per-haplotype (MDM2_SNP309-SNP285; MDM4_rs4245739-rs1563828) odds ratios (OR) for multiple-melanoma were estimated with logistic regression models. Hazard ratios (HR) for melanoma death were estimated with Cox proportional hazards models. In analyses adjusted for covariates, females carrying MDM4-rs4245739*C were more likely to develop multiple melanomas (ORper-allele = 1.25, 95% CI 1.03-1.51, and Ptrend = 0.03), while MDM2-rs2279744*G was inversely associated with melanoma-death (HRper-allele = 0.63, 95% CI 0.42-0.95, and Ptrend = 0.03). We identified 16 coinherited expression quantitative loci that control the expression of MDM2, MDM4, and other genes in the skin, brain, and lungs. Our results suggest that MDM4/MDM2 variants are associated with the development of subsequent primaries and with the death of melanoma in a sex-dependent manner. Further investigations of the complex MDM2/MDM4 motif, and its contribution to the tumor microenvironment and observed associations, are warranted.

Published

2023

2. Association of Melanoma-Risk Variants with Primary Melanoma Tumor Prognostic Characteristics and Melanoma-Specific Survival in the GEM Study.

Author

Davari, Danielle R, Davari, Danielle R, Orlow, Irene, Kanetsky, Peter A, Luo, Li, Busam, Klaus J, Sharma, Ajay, Kricker, Anne, Cust, Anne E, Anton-Culver, Hoda, Gruber, Stephen B, Gallagher, Richard P, Zanetti, Roberto, Rosso, Stefano, Sacchetto, Lidia, Dwyer, Terence, Gibbs, David C, Ollila, David W, Begg, Colin B, Berwick, Marianne, Thomas, Nancy E, Davari, Danielle R, Davari, Danielle R, Orlow, Irene, Kanetsky, Peter A, Luo, Li, Busam, Klaus J, Sharma, Ajay, Kricker, Anne, Cust, Anne E, Anton-Culver, Hoda, Gruber, Stephen B, Gallagher, Richard P, Zanetti, Roberto, Rosso, Stefano, Sacchetto, Lidia, Dwyer, Terence, Gibbs, David C, Ollila, David W, Begg, Colin B, Berwick, Marianne, and Thomas, Nancy E

Abstract

Genome-wide association studies (GWAS) and candidate pathway studies have identified low-penetrant genetic variants associated with cutaneous melanoma. We investigated the association of melanoma-risk variants with primary melanoma tumor prognostic characteristics and melanoma-specific survival. The Genes, Environment, and Melanoma Study enrolled 3285 European origin participants with incident invasive primary melanoma. For each of 47 melanoma-risk single nucleotide polymorphisms (SNPs), we used linear and logistic regression modeling to estimate, respectively, the per allele mean changes in log of Breslow thickness and odds ratios for presence of ulceration, mitoses, and tumor-infiltrating lymphocytes (TILs). We also used Cox proportional hazards regression modeling to estimate the per allele hazard ratios for melanoma-specific survival. Passing the false discovery threshold (p = 0.0026) were associations of IRF4 rs12203592 and CCND1 rs1485993 with log of Breslow thickness, and association of TERT rs2242652 with presence of mitoses. IRF4 rs12203592 also had nominal associations (p < 0.05) with presence of mitoses and melanoma-specific survival, as well as a borderline association (p = 0.07) with ulceration. CCND1 rs1485993 also had a borderline association with presence of mitoses (p = 0.06). MX2 rs45430 had nominal associations with log of Breslow thickness, presence of mitoses, and melanoma-specific survival. Our study indicates that further research investigating the associations of these genetic variants with underlying biologic pathways related to tumor progression is warranted.

Published

2021

3. Disease-Associated Risk Variants in ANRIL Are Associated with Tumor-Infiltrating Lymphocyte Presence in Primary Melanomas in the Population-Based GEM Study.

Author

Davari, Danielle R, Davari, Danielle R, Orlow, Irene, Kanetsky, Peter A, Luo, Li, Edmiston, Sharon N, Conway, Kathleen, Parrish, Eloise A, Hao, Honglin, Busam, Klaus J, Sharma, Ajay, Kricker, Anne, Cust, Anne E, Anton-Culver, Hoda, Gruber, Stephen B, Gallagher, Richard P, Zanetti, Roberto, Rosso, Stefano, Sacchetto, Lidia, Dwyer, Terence, Ollila, David W, Begg, Colin B, Berwick, Marianne, Thomas, Nancy E, GEM Study Group, Davari, Danielle R, Davari, Danielle R, Orlow, Irene, Kanetsky, Peter A, Luo, Li, Edmiston, Sharon N, Conway, Kathleen, Parrish, Eloise A, Hao, Honglin, Busam, Klaus J, Sharma, Ajay, Kricker, Anne, Cust, Anne E, Anton-Culver, Hoda, Gruber, Stephen B, Gallagher, Richard P, Zanetti, Roberto, Rosso, Stefano, Sacchetto, Lidia, Dwyer, Terence, Ollila, David W, Begg, Colin B, Berwick, Marianne, Thomas, Nancy E, and GEM Study Group

Abstract

BackgroundGenome-wide association studies have reported that genetic variation at ANRIL (CDKN2B-AS1) is associated with risk of several chronic diseases including coronary artery disease, coronary artery calcification, myocardial infarction, and type 2 diabetes mellitus. ANRIL is located at the CDKN2A/B locus, which encodes multiple melanoma tumor suppressors. We investigated the association of these variants with melanoma prognostic characteristics.MethodsThe Genes, Environment, and Melanoma Study enrolled 3,285 European origin participants with incident invasive primary melanoma. For each of ten disease-associated SNPs at or near ANRIL, we used linear and logistic regression modeling to estimate, respectively, the per allele mean changes in log of Breslow thickness and ORs for presence of ulceration and tumor-infiltrating lymphocytes (TIL). We also assessed effect modification by tumor NRAS/BRAF mutational status.ResultsRs518394, rs10965215, and rs564398 passed false discovery and were each associated (P ≤ 0.005) with TILs, although only rs564398 was independently associated (P = 0.0005) with TILs. Stratified by NRAS/BRAF mutational status, rs564398*A was significantly positively associated with TILs among NRAS/BRAF mutant, but not wild-type, cases. We did not find SNP associations with Breslow thickness or ulceration.ConclusionsANRIL rs564398 was associated with TIL presence in primary melanomas, and this association may be limited to NRAS/BRAF-mutant cases.ImpactPathways related to ANRIL variants warrant exploration in relationship to TILs in melanoma, especially given the impact of TILs on immunotherapy and survival.

Published

2021

4. Differences in Melanoma Between Canada and New South Wales, Australia: A Population-Based Genes, Environment, and Melanoma (GEM) Study.

Author

Yardman-Frank, Joseph Michael, Yardman-Frank, Joseph Michael, Glassheim, Elyssa, Kricker, Anne, Armstrong, Bruce K, Marrett, Loraine D, Luo, Li, Cust, Anne E, Busam, Klaus J, Orlow, Irene, Gallagher, Richard P, Gruber, Stephen B, Anton-Culver, Hoda, Rosso, Stefano, Zanetti, Roberto, Sacchetto, Lidia, Kanetsky, Peter A, Dwyer, Terence, Venn, Alison, Lee-Taylor, Julia, Begg, Colin B, Thomas, Nancy E, Berwick, Marianne, Yardman-Frank, Joseph Michael, Yardman-Frank, Joseph Michael, Glassheim, Elyssa, Kricker, Anne, Armstrong, Bruce K, Marrett, Loraine D, Luo, Li, Cust, Anne E, Busam, Klaus J, Orlow, Irene, Gallagher, Richard P, Gruber, Stephen B, Anton-Culver, Hoda, Rosso, Stefano, Zanetti, Roberto, Sacchetto, Lidia, Kanetsky, Peter A, Dwyer, Terence, Venn, Alison, Lee-Taylor, Julia, Begg, Colin B, Thomas, Nancy E, and Berwick, Marianne

Published

2021

5. Disease-Associated Risk Variants in ANRIL Are Associated with Tumor-Infiltrating Lymphocyte Presence in Primary Melanomas in the Population-Based GEM Study.

Author

Davari, Danielle R, Davari, Danielle R, Orlow, Irene, Kanetsky, Peter A, Luo, Li, Edmiston, Sharon N, Conway, Kathleen, Parrish, Eloise A, Hao, Honglin, Busam, Klaus J, Sharma, Ajay, Kricker, Anne, Cust, Anne E, Anton-Culver, Hoda, Gruber, Stephen B, Gallagher, Richard P, Zanetti, Roberto, Rosso, Stefano, Sacchetto, Lidia, Dwyer, Terence, Ollila, David W, Begg, Colin B, Berwick, Marianne, Thomas, Nancy E, GEM Study Group, Davari, Danielle R, Davari, Danielle R, Orlow, Irene, Kanetsky, Peter A, Luo, Li, Edmiston, Sharon N, Conway, Kathleen, Parrish, Eloise A, Hao, Honglin, Busam, Klaus J, Sharma, Ajay, Kricker, Anne, Cust, Anne E, Anton-Culver, Hoda, Gruber, Stephen B, Gallagher, Richard P, Zanetti, Roberto, Rosso, Stefano, Sacchetto, Lidia, Dwyer, Terence, Ollila, David W, Begg, Colin B, Berwick, Marianne, Thomas, Nancy E, and GEM Study Group

Abstract

BackgroundGenome-wide association studies have reported that genetic variation at ANRIL (CDKN2B-AS1) is associated with risk of several chronic diseases including coronary artery disease, coronary artery calcification, myocardial infarction, and type 2 diabetes mellitus. ANRIL is located at the CDKN2A/B locus, which encodes multiple melanoma tumor suppressors. We investigated the association of these variants with melanoma prognostic characteristics.MethodsThe Genes, Environment, and Melanoma Study enrolled 3,285 European origin participants with incident invasive primary melanoma. For each of ten disease-associated SNPs at or near ANRIL, we used linear and logistic regression modeling to estimate, respectively, the per allele mean changes in log of Breslow thickness and ORs for presence of ulceration and tumor-infiltrating lymphocytes (TIL). We also assessed effect modification by tumor NRAS/BRAF mutational status.ResultsRs518394, rs10965215, and rs564398 passed false discovery and were each associated (P ≤ 0.005) with TILs, although only rs564398 was independently associated (P = 0.0005) with TILs. Stratified by NRAS/BRAF mutational status, rs564398*A was significantly positively associated with TILs among NRAS/BRAF mutant, but not wild-type, cases. We did not find SNP associations with Breslow thickness or ulceration.ConclusionsANRIL rs564398 was associated with TIL presence in primary melanomas, and this association may be limited to NRAS/BRAF-mutant cases.ImpactPathways related to ANRIL variants warrant exploration in relationship to TILs in melanoma, especially given the impact of TILs on immunotherapy and survival.

Published

2021

6. Association of Melanoma-Risk Variants with Primary Melanoma Tumor Prognostic Characteristics and Melanoma-Specific Survival in the GEM Study.

Author

Davari, Danielle R, Davari, Danielle R, Orlow, Irene, Kanetsky, Peter A, Luo, Li, Busam, Klaus J, Sharma, Ajay, Kricker, Anne, Cust, Anne E, Anton-Culver, Hoda, Gruber, Stephen B, Gallagher, Richard P, Zanetti, Roberto, Rosso, Stefano, Sacchetto, Lidia, Dwyer, Terence, Gibbs, David C, Ollila, David W, Begg, Colin B, Berwick, Marianne, Thomas, Nancy E, Davari, Danielle R, Davari, Danielle R, Orlow, Irene, Kanetsky, Peter A, Luo, Li, Busam, Klaus J, Sharma, Ajay, Kricker, Anne, Cust, Anne E, Anton-Culver, Hoda, Gruber, Stephen B, Gallagher, Richard P, Zanetti, Roberto, Rosso, Stefano, Sacchetto, Lidia, Dwyer, Terence, Gibbs, David C, Ollila, David W, Begg, Colin B, Berwick, Marianne, and Thomas, Nancy E

Abstract

Genome-wide association studies (GWAS) and candidate pathway studies have identified low-penetrant genetic variants associated with cutaneous melanoma. We investigated the association of melanoma-risk variants with primary melanoma tumor prognostic characteristics and melanoma-specific survival. The Genes, Environment, and Melanoma Study enrolled 3285 European origin participants with incident invasive primary melanoma. For each of 47 melanoma-risk single nucleotide polymorphisms (SNPs), we used linear and logistic regression modeling to estimate, respectively, the per allele mean changes in log of Breslow thickness and odds ratios for presence of ulceration, mitoses, and tumor-infiltrating lymphocytes (TILs). We also used Cox proportional hazards regression modeling to estimate the per allele hazard ratios for melanoma-specific survival. Passing the false discovery threshold (p = 0.0026) were associations of IRF4 rs12203592 and CCND1 rs1485993 with log of Breslow thickness, and association of TERT rs2242652 with presence of mitoses. IRF4 rs12203592 also had nominal associations (p < 0.05) with presence of mitoses and melanoma-specific survival, as well as a borderline association (p = 0.07) with ulceration. CCND1 rs1485993 also had a borderline association with presence of mitoses (p = 0.06). MX2 rs45430 had nominal associations with log of Breslow thickness, presence of mitoses, and melanoma-specific survival. Our study indicates that further research investigating the associations of these genetic variants with underlying biologic pathways related to tumor progression is warranted.

Published

2021

7. Differences in Melanoma Between Canada and New South Wales, Australia: A Population-Based Genes, Environment, and Melanoma (GEM) Study.

Author

Yardman-Frank, Joseph Michael, Yardman-Frank, Joseph Michael, Glassheim, Elyssa, Kricker, Anne, Armstrong, Bruce K, Marrett, Loraine D, Luo, Li, Cust, Anne E, Busam, Klaus J, Orlow, Irene, Gallagher, Richard P, Gruber, Stephen B, Anton-Culver, Hoda, Rosso, Stefano, Zanetti, Roberto, Sacchetto, Lidia, Kanetsky, Peter A, Dwyer, Terence, Venn, Alison, Lee-Taylor, Julia, Begg, Colin B, Thomas, Nancy E, Berwick, Marianne, Yardman-Frank, Joseph Michael, Yardman-Frank, Joseph Michael, Glassheim, Elyssa, Kricker, Anne, Armstrong, Bruce K, Marrett, Loraine D, Luo, Li, Cust, Anne E, Busam, Klaus J, Orlow, Irene, Gallagher, Richard P, Gruber, Stephen B, Anton-Culver, Hoda, Rosso, Stefano, Zanetti, Roberto, Sacchetto, Lidia, Kanetsky, Peter A, Dwyer, Terence, Venn, Alison, Lee-Taylor, Julia, Begg, Colin B, Thomas, Nancy E, and Berwick, Marianne

Abstract

In an effort to understand the difference between melanomas diagnosed in Australia (New South Wales) and Canada, where the incidence in New South Wales is almost three times greater than in Canada, and mortality is twice as high although survival is slightly more favorable, we had one pathologist review 1,271 melanomas from British Columbia and Ontario, Canada, to compare these to melanomas in New South Wales, Australia. We hypothesized that histopathologic characteristics might provide insight into divergent pathways to melanoma development. We found a number of differences in risk factors and tumor characteristics between the two geographic areas. There were higher mole counts and darker phenotypes in the Canadian patients, while the Australian patients had greater solar elastosis, more lentigo maligna melanomas, and more tumor infiltrating lymphocytes. We hypothesize that the differences observed may illustrate different etiologies – the cumulative exposure pathway among Australian patients and the nevus pathway among Canadian patients. This is one of the largest studies investigating the divergent pathway hypothesis and is particularly robust due to the evaluation of all lesions by one dermatopathologist.

Published

2021

8. Association of Known Melanoma Risk Factors with Primary Melanoma of the Scalp and Neck.

Author

Wood, Renee P, Wood, Renee P, Heyworth, Jane S, McCarthy, Nina S, Mauguen, Audrey, Berwick, Marianne, Thomas, Nancy E, Millward, Michael J, Anton-Culver, Hoda, Cust, Anne E, Dwyer, Terence, Gallagher, Richard P, Gruber, Stephen B, Kanetsky, Peter A, Orlow, Irene, Rosso, Stefano, Moses, Eric K, Begg, Colin B, Ward, Sarah V, Wood, Renee P, Wood, Renee P, Heyworth, Jane S, McCarthy, Nina S, Mauguen, Audrey, Berwick, Marianne, Thomas, Nancy E, Millward, Michael J, Anton-Culver, Hoda, Cust, Anne E, Dwyer, Terence, Gallagher, Richard P, Gruber, Stephen B, Kanetsky, Peter A, Orlow, Irene, Rosso, Stefano, Moses, Eric K, Begg, Colin B, and Ward, Sarah V

Abstract

BackgroundScalp and neck (SN) melanoma confers a worse prognosis than melanoma of other sites but little is known about its determinants. We aimed to identify associations between SN melanoma and known risk genes, phenotypic traits, and sun exposure patterns.MethodsParticipants were cases from the Western Australian Melanoma Health Study (n = 1,200) and the Genes, Environment, and Melanoma Study (n = 3,280). Associations between risk factors and SN melanoma, compared with truncal and arm/leg melanoma, were investigated using binomial logistic regression. Facial melanoma was also compared with the trunk and extremities, to evaluate whether associations were subregion specific, or reflective of the whole head/neck region.ResultsCompared with other sites, increased odds of SN and facial melanoma were observed in older individuals [SN: OR = 1.28, 95% confidence interval (CI) = 0.92-1.80, P trend = 0.016; Face: OR = 4.57, 95% CI = 3.34-6.35, P trend < 0.001] and those carrying IRF4-rs12203592*T (SN: OR = 1.35, 95% CI = 1.12-1.63, P trend = 0.002; Face: OR = 1.29, 95% CI = 1.10-1.50, P trend = 0.001). Decreased odds were observed for females (SN: OR = 0.49, 95% CI = 0.37-0.64, P < 0.001; Face: OR = 0.66, 95% CI = 0.53-0.82, P < 0.001) and the presence of nevi (SN: OR = 0.66, 95% CI = 0.49-0.89, P = 0.006; Face: OR = 0.65, 95% CI = 0.52-0.83, P < 0.001).ConclusionsDifferences observed between SN melanoma and other sites were also observed for facial melanoma. Factors previously associated with the broader head and neck region, notably older age, may be driven by the facial subregion. A novel finding was the association of IRF4-rs12203592 with both SN and facial melanoma.ImpactUnderstanding the epidemiology of site-specific melanoma will enable tailored strategies for risk factor reduction and site-specific screening campaigns.

Published

2020

9. MC1R variants in childhood and adolescent melanoma: a retrospective pooled analysis of a multicentre cohort.

Author

Pellegrini, Cristina, Pellegrini, Cristina, Botta, Francesca, Massi, Daniela, Martorelli, Claudia, Facchetti, Fabio, Gandini, Sara, Maisonneuve, Patrick, Avril, Marie-Françoise, Demenais, Florence, Bressac-de Paillerets, Brigitte, Hoiom, Veronica, Cust, Anne E, Anton-Culver, Hoda, Gruber, Stephen B, Gallagher, Richard P, Marrett, Loraine, Zanetti, Roberto, Dwyer, Terence, Thomas, Nancy E, Begg, Colin B, Berwick, Marianne, Puig, Susana, Potrony, Miriam, Nagore, Eduardo, Ghiorzo, Paola, Menin, Chiara, Manganoni, Ausilia Maria, Rodolfo, Monica, Brugnara, Sonia, Passoni, Emanuela, Sekulovic, Lidija Kandolf, Baldini, Federica, Guida, Gabriella, Stratigos, Alexandros, Ozdemir, Fezal, Ayala, Fabrizio, Fernandez-de-Misa, Ricardo, Quaglino, Pietro, Ribas, Gloria, Romanini, Antonella, Migliano, Emilia, Stanganelli, Ignazio, Kanetsky, Peter A, Pizzichetta, Maria Antonietta, García-Borrón, Jose Carlos, Nan, Hongmei, Landi, Maria Teresa, Little, Julian, Newton-Bishop, Julia, Sera, Francesco, Fargnoli, Maria Concetta, Raimondi, Sara, IMI Study Group, GEM Study Group, M-SKIP Study Group, Pellegrini, Cristina, Pellegrini, Cristina, Botta, Francesca, Massi, Daniela, Martorelli, Claudia, Facchetti, Fabio, Gandini, Sara, Maisonneuve, Patrick, Avril, Marie-Françoise, Demenais, Florence, Bressac-de Paillerets, Brigitte, Hoiom, Veronica, Cust, Anne E, Anton-Culver, Hoda, Gruber, Stephen B, Gallagher, Richard P, Marrett, Loraine, Zanetti, Roberto, Dwyer, Terence, Thomas, Nancy E, Begg, Colin B, Berwick, Marianne, Puig, Susana, Potrony, Miriam, Nagore, Eduardo, Ghiorzo, Paola, Menin, Chiara, Manganoni, Ausilia Maria, Rodolfo, Monica, Brugnara, Sonia, Passoni, Emanuela, Sekulovic, Lidija Kandolf, Baldini, Federica, Guida, Gabriella, Stratigos, Alexandros, Ozdemir, Fezal, Ayala, Fabrizio, Fernandez-de-Misa, Ricardo, Quaglino, Pietro, Ribas, Gloria, Romanini, Antonella, Migliano, Emilia, Stanganelli, Ignazio, Kanetsky, Peter A, Pizzichetta, Maria Antonietta, García-Borrón, Jose Carlos, Nan, Hongmei, Landi, Maria Teresa, Little, Julian, Newton-Bishop, Julia, Sera, Francesco, Fargnoli, Maria Concetta, Raimondi, Sara, IMI Study Group, GEM Study Group, and M-SKIP Study Group

Abstract

BackgroundGermline variants in the melanocortin 1 receptor gene (MC1R) might increase the risk of childhood and adolescent melanoma, but a clear conclusion is challenging because of the low number of studies and cases. We assessed the association of MC1R variants with childhood and adolescent melanoma in a large study comparing the prevalence of MC1R variants in child or adolescent patients with melanoma to that in adult patients with melanoma and in healthy adult controls.MethodsIn this retrospective pooled analysis, we used the M-SKIP Project, the Italian Melanoma Intergroup, and other European groups (with participants from Australia, Canada, France, Greece, Italy, the Netherlands, Serbia, Spain, Sweden, Turkey, and the USA) to assemble an international multicentre cohort. We gathered phenotypic and genetic data from children or adolescents diagnosed with sporadic single-primary cutaneous melanoma at age 20 years or younger, adult patients with sporadic single-primary cutaneous melanoma diagnosed at age 35 years or older, and healthy adult individuals as controls. We calculated odds ratios (ORs) for childhood and adolescent melanoma associated with MC1R variants by multivariable logistic regression. Subgroup analysis was done for children aged 18 or younger and 14 years or younger.FindingsWe analysed data from 233 young patients, 932 adult patients, and 932 healthy adult controls. Children and adolescents had higher odds of carrying MC1R r variants than did adult patients (OR 1·54, 95% CI 1·02-2·33), including when analysis was restricted to patients aged 18 years or younger (1·80, 1·06-3·07). All investigated variants, except Arg160Trp, tended, to varying degrees, to have higher frequencies in young patients than in adult patients, with significantly higher frequencies found for Val60Leu (OR 1·60, 95% CI 1·05-2·44; p=0·04) and Asp294His (2·15, 1·05-4·40; p=0·04). Compared with those of healthy controls, young patients with melanoma had significantly higher frequ

Published

2019

10. Inherited Genetic Variants Associated with Melanoma BRAF/NRAS Subtypes.

Author

Thomas, Nancy E, Thomas, Nancy E, Edmiston, Sharon N, Orlow, Irene, Kanetsky, Peter A, Luo, Li, Gibbs, David C, Parrish, Eloise A, Hao, Honglin, Busam, Klaus J, Armstrong, Bruce K, Kricker, Anne, Cust, Anne E, Anton-Culver, Hoda, Gruber, Stephen B, Gallagher, Richard P, Zanetti, Roberto, Rosso, Stefano, Sacchetto, Lidia, Dwyer, Terence, Ollila, David W, Begg, Colin B, Berwick, Marianne, Conway, Kathleen, GEM Study Group, Thomas, Nancy E, Thomas, Nancy E, Edmiston, Sharon N, Orlow, Irene, Kanetsky, Peter A, Luo, Li, Gibbs, David C, Parrish, Eloise A, Hao, Honglin, Busam, Klaus J, Armstrong, Bruce K, Kricker, Anne, Cust, Anne E, Anton-Culver, Hoda, Gruber, Stephen B, Gallagher, Richard P, Zanetti, Roberto, Rosso, Stefano, Sacchetto, Lidia, Dwyer, Terence, Ollila, David W, Begg, Colin B, Berwick, Marianne, Conway, Kathleen, and GEM Study Group

Abstract

BRAF and NRAS mutations arise early in melanoma development, but their associations with low-penetrance melanoma susceptibility loci remain unknown. In the Genes, Environment and Melanoma Study, 1,223 European-origin participants had their incident invasive primary melanomas screened for BRAF/NRAS mutations and germline DNA genotyped for 47 single-nucleotide polymorphisms identified as low-penetrant melanoma-risk variants. We used multinomial logistic regression to simultaneously examine each single-nucleotide polymorphism's relationship to BRAF V600E, BRAF V600K, BRAF other, and NRAS+ relative to BRAF-/NRAS- melanoma adjusted for study features. IRF4 rs12203592*T was associated with BRAF V600E (odds ratio [OR] = 0.59, 95% confidence interval [CI] = 0.43-0.79) and V600K (OR = 0.65, 95% CI = 0.41-1.03), but not BRAF other or NRAS+ melanoma. A global test of etiologic heterogeneity (Pglobal = 0.001) passed false discovery (Pglobal = 0.0026). PLA2G6 rs132985*T was associated with BRAF V600E (OR = 1.32, 95% CI = 1.05-1.67) and BRAF other (OR = 1.82, 95% CI = 1.11-2.98), but not BRAF V600K or NRAS+ melanoma. The test for etiologic heterogeneity (Pglobal) was 0.005. The IRF4 rs12203592 associations were slightly attenuated after adjustment for melanoma-risk phenotypes. The PLA2G6 rs132985 associations were independent of phenotypes. IRF4 and PLA2G6 inherited genotypes may influence melanoma BRAF/NRAS subtype development.

Published

2018

11. Inherited Genetic Variants Associated with Melanoma BRAF/NRAS Subtypes.

Author

Thomas, Nancy E, Thomas, Nancy E, Edmiston, Sharon N, Orlow, Irene, Kanetsky, Peter A, Luo, Li, Gibbs, David C, Parrish, Eloise A, Hao, Honglin, Busam, Klaus J, Armstrong, Bruce K, Kricker, Anne, Cust, Anne E, Anton-Culver, Hoda, Gruber, Stephen B, Gallagher, Richard P, Zanetti, Roberto, Rosso, Stefano, Sacchetto, Lidia, Dwyer, Terence, Ollila, David W, Begg, Colin B, Berwick, Marianne, Conway, Kathleen, GEM Study Group, Thomas, Nancy E, Thomas, Nancy E, Edmiston, Sharon N, Orlow, Irene, Kanetsky, Peter A, Luo, Li, Gibbs, David C, Parrish, Eloise A, Hao, Honglin, Busam, Klaus J, Armstrong, Bruce K, Kricker, Anne, Cust, Anne E, Anton-Culver, Hoda, Gruber, Stephen B, Gallagher, Richard P, Zanetti, Roberto, Rosso, Stefano, Sacchetto, Lidia, Dwyer, Terence, Ollila, David W, Begg, Colin B, Berwick, Marianne, Conway, Kathleen, and GEM Study Group

Abstract

BRAF and NRAS mutations arise early in melanoma development, but their associations with low-penetrance melanoma susceptibility loci remain unknown. In the Genes, Environment and Melanoma Study, 1,223 European-origin participants had their incident invasive primary melanomas screened for BRAF/NRAS mutations and germline DNA genotyped for 47 single-nucleotide polymorphisms identified as low-penetrant melanoma-risk variants. We used multinomial logistic regression to simultaneously examine each single-nucleotide polymorphism's relationship to BRAF V600E, BRAF V600K, BRAF other, and NRAS+ relative to BRAF-/NRAS- melanoma adjusted for study features. IRF4 rs12203592*T was associated with BRAF V600E (odds ratio [OR] = 0.59, 95% confidence interval [CI] = 0.43-0.79) and V600K (OR = 0.65, 95% CI = 0.41-1.03), but not BRAF other or NRAS+ melanoma. A global test of etiologic heterogeneity (Pglobal = 0.001) passed false discovery (Pglobal = 0.0026). PLA2G6 rs132985*T was associated with BRAF V600E (OR = 1.32, 95% CI = 1.05-1.67) and BRAF other (OR = 1.82, 95% CI = 1.11-2.98), but not BRAF V600K or NRAS+ melanoma. The test for etiologic heterogeneity (Pglobal) was 0.005. The IRF4 rs12203592 associations were slightly attenuated after adjustment for melanoma-risk phenotypes. The PLA2G6 rs132985 associations were independent of phenotypes. IRF4 and PLA2G6 inherited genotypes may influence melanoma BRAF/NRAS subtype development.

Published

2018

12. Inherited Genetic Variants Associated with Melanoma BRAF/NRAS Subtypes.

Author

Thomas, Nancy E, Thomas, Nancy E, Edmiston, Sharon N, Orlow, Irene, Kanetsky, Peter A, Luo, Li, Gibbs, David C, Parrish, Eloise A, Hao, Honglin, Busam, Klaus J, Armstrong, Bruce K, Kricker, Anne, Cust, Anne E, Anton-Culver, Hoda, Gruber, Stephen B, Gallagher, Richard P, Zanetti, Roberto, Rosso, Stefano, Sacchetto, Lidia, Dwyer, Terence, Ollila, David W, Begg, Colin B, Berwick, Marianne, Conway, Kathleen, GEM Study Group, Thomas, Nancy E, Thomas, Nancy E, Edmiston, Sharon N, Orlow, Irene, Kanetsky, Peter A, Luo, Li, Gibbs, David C, Parrish, Eloise A, Hao, Honglin, Busam, Klaus J, Armstrong, Bruce K, Kricker, Anne, Cust, Anne E, Anton-Culver, Hoda, Gruber, Stephen B, Gallagher, Richard P, Zanetti, Roberto, Rosso, Stefano, Sacchetto, Lidia, Dwyer, Terence, Ollila, David W, Begg, Colin B, Berwick, Marianne, Conway, Kathleen, and GEM Study Group

Abstract

BRAF and NRAS mutations arise early in melanoma development, but their associations with low-penetrance melanoma susceptibility loci remain unknown. In the Genes, Environment and Melanoma Study, 1,223 European-origin participants had their incident invasive primary melanomas screened for BRAF/NRAS mutations and germline DNA genotyped for 47 single-nucleotide polymorphisms identified as low-penetrant melanoma-risk variants. We used multinomial logistic regression to simultaneously examine each single-nucleotide polymorphism's relationship to BRAF V600E, BRAF V600K, BRAF other, and NRAS+ relative to BRAF-/NRAS- melanoma adjusted for study features. IRF4 rs12203592*T was associated with BRAF V600E (odds ratio [OR] = 0.59, 95% confidence interval [CI] = 0.43-0.79) and V600K (OR = 0.65, 95% CI = 0.41-1.03), but not BRAF other or NRAS+ melanoma. A global test of etiologic heterogeneity (Pglobal = 0.001) passed false discovery (Pglobal = 0.0026). PLA2G6 rs132985*T was associated with BRAF V600E (OR = 1.32, 95% CI = 1.05-1.67) and BRAF other (OR = 1.82, 95% CI = 1.11-2.98), but not BRAF V600K or NRAS+ melanoma. The test for etiologic heterogeneity (Pglobal) was 0.005. The IRF4 rs12203592 associations were slightly attenuated after adjustment for melanoma-risk phenotypes. The PLA2G6 rs132985 associations were independent of phenotypes. IRF4 and PLA2G6 inherited genotypes may influence melanoma BRAF/NRAS subtype development.

Published

2018

13. The interaction between vitamin D receptor polymorphisms and sun exposure around time of diagnosis influences melanoma survival.

Author

Orlow, Irene, Orlow, Irene, Shi, Yang, Kanetsky, Peter A, Thomas, Nancy E, Luo, Li, Corrales-Guerrero, Sergio, Cust, Anne E, Sacchetto, Lidia, Zanetti, Roberto, Rosso, Stefano, Armstrong, Bruce K, Dwyer, Terence, Venn, Alison, Gallagher, Richard P, Gruber, Stephen B, Marrett, Loraine D, Anton-Culver, Hoda, Busam, Klaus, Begg, Colin B, Berwick, Marianne, GEM Study Group, Orlow, Irene, Orlow, Irene, Shi, Yang, Kanetsky, Peter A, Thomas, Nancy E, Luo, Li, Corrales-Guerrero, Sergio, Cust, Anne E, Sacchetto, Lidia, Zanetti, Roberto, Rosso, Stefano, Armstrong, Bruce K, Dwyer, Terence, Venn, Alison, Gallagher, Richard P, Gruber, Stephen B, Marrett, Loraine D, Anton-Culver, Hoda, Busam, Klaus, Begg, Colin B, Berwick, Marianne, and GEM Study Group

Abstract

Evidence on the relationship between the vitamin D pathway and outcomes in melanoma is growing, although it is not always clear. We investigated the impact of measured levels of sun exposure at diagnosis on associations of vitamin D receptor gene (VDR) polymorphisms and melanoma death in 3336 incident primary melanoma cases. Interactions between six SNPs and a common 3'-end haplotype were significant (p < .05). These SNPs, and a haplotype, had a statistically significant association with survival among subjects exposed to high UVB in multivariable regression models and exerted their effect in the opposite direction among those with low UVB. SNPs rs1544410/BsmI and rs731236/TaqI remained significant after adjustment for multiple testing. These results suggest that the association between VDR and melanoma-specific survival is modified by sun exposure around diagnosis, and require validation in an independent study. Whether the observed effects are dependent or independent of vitamin D activation remains to be determined.

Published

2018

14. Associations of MC1R Genotype and Patient Phenotypes with BRAF and NRAS Mutations in Melanoma.

Author

Thomas, Nancy E, Thomas, Nancy E, Edmiston, Sharon N, Kanetsky, Peter A, Busam, Klaus J, Kricker, Anne, Armstrong, Bruce K, Cust, Anne E, Anton-Culver, Hoda, Gruber, Stephen B, Luo, Li, Orlow, Irene, Reiner, Anne S, Gallagher, Richard P, Zanetti, Roberto, Rosso, Stefano, Sacchetto, Lidia, Dwyer, Terence, Parrish, Eloise A, Hao, Honglin, Gibbs, David C, Frank, Jill S, Ollila, David W, Begg, Colin B, Berwick, Marianne, Conway, Kathleen, GEM Study Group, Thomas, Nancy E, Thomas, Nancy E, Edmiston, Sharon N, Kanetsky, Peter A, Busam, Klaus J, Kricker, Anne, Armstrong, Bruce K, Cust, Anne E, Anton-Culver, Hoda, Gruber, Stephen B, Luo, Li, Orlow, Irene, Reiner, Anne S, Gallagher, Richard P, Zanetti, Roberto, Rosso, Stefano, Sacchetto, Lidia, Dwyer, Terence, Parrish, Eloise A, Hao, Honglin, Gibbs, David C, Frank, Jill S, Ollila, David W, Begg, Colin B, Berwick, Marianne, Conway, Kathleen, and GEM Study Group

Abstract

Associations of MC1R with BRAF mutations in melanoma have been inconsistent between studies. We sought to determine for 1,227 participants in the international population-based Genes, Environment, and Melanoma (GEM) study whether MC1R and phenotypes were associated with melanoma BRAF/NRAS subtypes. We used logistic regression adjusted by age, sex, and study design features and examined effect modifications. BRAF+ were associated with younger age, blond/light brown hair, increased nevi, and less freckling, and NRAS+ with older age relative to the wild type (BRAF-/NRAS-) melanomas (all P < 0.05). Comparing specific BRAF subtypes to the wild type, BRAF V600E was associated with younger age, blond/light brown hair, and increased nevi and V600K with increased nevi and less freckling (all P < 0.05). MC1R was positively associated with BRAF V600E cases but only among individuals with darker phototypes or darker hair (Pinteraction < 0.05) but inversely associated with BRAF V600K (Ptrend = 0.006) with no significant effect modification by phenotypes. These results support distinct etiologies for BRAF V600E, BRAF V600K, NRAS+, and wild-type melanomas. MC1R's associations with BRAF V600E cases limited to individuals with darker phenotypes indicate that MC1R genotypes specifically provide information about BRAF V600E melanoma risk in those not considered high risk based on phenotype. Our results also suggest that melanin pathways deserve further study in BRAF V600E melanomagenesis.

Published

2017

15. Associations of MC1R Genotype and Patient Phenotypes with BRAF and NRAS Mutations in Melanoma.

Author

Thomas, Nancy E, Thomas, Nancy E, Edmiston, Sharon N, Kanetsky, Peter A, Busam, Klaus J, Kricker, Anne, Armstrong, Bruce K, Cust, Anne E, Anton-Culver, Hoda, Gruber, Stephen B, Luo, Li, Orlow, Irene, Reiner, Anne S, Gallagher, Richard P, Zanetti, Roberto, Rosso, Stefano, Sacchetto, Lidia, Dwyer, Terence, Parrish, Eloise A, Hao, Honglin, Gibbs, David C, Frank, Jill S, Ollila, David W, Begg, Colin B, Berwick, Marianne, Conway, Kathleen, GEM Study Group, Thomas, Nancy E, Thomas, Nancy E, Edmiston, Sharon N, Kanetsky, Peter A, Busam, Klaus J, Kricker, Anne, Armstrong, Bruce K, Cust, Anne E, Anton-Culver, Hoda, Gruber, Stephen B, Luo, Li, Orlow, Irene, Reiner, Anne S, Gallagher, Richard P, Zanetti, Roberto, Rosso, Stefano, Sacchetto, Lidia, Dwyer, Terence, Parrish, Eloise A, Hao, Honglin, Gibbs, David C, Frank, Jill S, Ollila, David W, Begg, Colin B, Berwick, Marianne, Conway, Kathleen, and GEM Study Group

Abstract

Associations of MC1R with BRAF mutations in melanoma have been inconsistent between studies. We sought to determine for 1,227 participants in the international population-based Genes, Environment, and Melanoma (GEM) study whether MC1R and phenotypes were associated with melanoma BRAF/NRAS subtypes. We used logistic regression adjusted by age, sex, and study design features and examined effect modifications. BRAF+ were associated with younger age, blond/light brown hair, increased nevi, and less freckling, and NRAS+ with older age relative to the wild type (BRAF-/NRAS-) melanomas (all P < 0.05). Comparing specific BRAF subtypes to the wild type, BRAF V600E was associated with younger age, blond/light brown hair, and increased nevi and V600K with increased nevi and less freckling (all P < 0.05). MC1R was positively associated with BRAF V600E cases but only among individuals with darker phototypes or darker hair (Pinteraction < 0.05) but inversely associated with BRAF V600K (Ptrend = 0.006) with no significant effect modification by phenotypes. These results support distinct etiologies for BRAF V600E, BRAF V600K, NRAS+, and wild-type melanomas. MC1R's associations with BRAF V600E cases limited to individuals with darker phenotypes indicate that MC1R genotypes specifically provide information about BRAF V600E melanoma risk in those not considered high risk based on phenotype. Our results also suggest that melanin pathways deserve further study in BRAF V600E melanomagenesis.

Published

2017

16. Association of Incident Amelanotic Melanoma With Phenotypic Characteristics, MC1R Status, and Prior Amelanotic Melanoma.

Author

Vernali, Steven, Vernali, Steven, Waxweiler, Weston T, Dillon, Patrick M, Kanetsky, Peter A, Orlow, Irene, Luo, Li, Busam, Klaus J, Kricker, Anne, Armstrong, Bruce K, Anton-Culver, Hoda, Gruber, Stephen B, Gallagher, Richard P, Zanetti, Roberto, Rosso, Stefano, Sacchetto, Lidia, Dwyer, Terence, Cust, Anne E, Ollila, David W, Begg, Colin B, Berwick, Marianne, Thomas, Nancy E, GEM Study Group, Vernali, Steven, Vernali, Steven, Waxweiler, Weston T, Dillon, Patrick M, Kanetsky, Peter A, Orlow, Irene, Luo, Li, Busam, Klaus J, Kricker, Anne, Armstrong, Bruce K, Anton-Culver, Hoda, Gruber, Stephen B, Gallagher, Richard P, Zanetti, Roberto, Rosso, Stefano, Sacchetto, Lidia, Dwyer, Terence, Cust, Anne E, Ollila, David W, Begg, Colin B, Berwick, Marianne, Thomas, Nancy E, and GEM Study Group

Abstract

ImportanceWe 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.ObjectiveTo determine whether phenotypic characteristics, carriage of MC1R variants, and history of amelanotic melanoma are associated with histopathologically amelanotic melanoma.Design, setting, and participantsThe 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 measuresAssociations 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.ResultsThis 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 los

Published

2017

17. Variants in autophagy-related genes and clinical characteristics in melanoma: a population-based study.

Author

White, Kirsten AM, White, Kirsten AM, Luo, Li, Thompson, Todd A, Torres, Salina, Hu, Chien-An Andy, Thomas, Nancy E, Lilyquist, Jenna, Anton-Culver, Hoda, Gruber, Stephen B, From, Lynn, Busam, Klaus J, Orlow, Irene, Kanetsky, Peter A, Marrett, Loraine D, Gallagher, Richard P, Sacchetto, Lidia, Rosso, Stefano, Dwyer, Terence, Cust, Anne E, Begg, Colin B, Berwick, Marianne, GEM Study Group, White, Kirsten AM, White, Kirsten AM, Luo, Li, Thompson, Todd A, Torres, Salina, Hu, Chien-An Andy, Thomas, Nancy E, Lilyquist, Jenna, Anton-Culver, Hoda, Gruber, Stephen B, From, Lynn, Busam, Klaus J, Orlow, Irene, Kanetsky, Peter A, Marrett, Loraine D, Gallagher, Richard P, Sacchetto, Lidia, Rosso, Stefano, Dwyer, Terence, Cust, Anne E, Begg, Colin B, Berwick, Marianne, and GEM Study Group

Abstract

Autophagy has been linked with melanoma risk and survival, but no polymorphisms in autophagy-related (ATG) genes have been investigated in relation to melanoma progression. We examined five single-nucleotide polymorphisms (SNPs) in three ATG genes (ATG5; ATG10; and ATG16L) with known or suspected impact on autophagic flux in an international population-based case-control study of melanoma. DNA from 911 melanoma patients was genotyped. An association was identified between (GG) (rs2241880) and earlier stage at diagnosis (OR 0.47; 95% Confidence Intervals (CI) = 0.27-0.81, P = 0.02) and a decrease in Breslow thickness (P = 0.03). The ATG16L heterozygous genotype (AG) (rs2241880) was associated with younger age at diagnosis (P = 0.02). Two SNPs in ATG5 were found to be associated with increased stage (rs2245214 CG, OR 1.47; 95% CI = 1.11-1.94, P = 0.03; rs510432 CC, OR 1.84; 95% CI = 1.12-3.02, P = 0.05). Finally, we identified inverse associations between ATG5 (GG rs2245214) and melanomas on the scalp or neck (OR 0.20, 95% CI = 0.05-0.86, P = 0.03); ATG10 (CC) (rs1864182) and brisk tumor infiltrating lymphocytes (TILs) (OR 0.42; 95% CI = 0.21-0.88, P = 0.02), and ATG5 (CC) (rs510432) with nonbrisk TILs (OR 0.55; 95% CI = 0.34-0.87, P = 0.01). Our data suggest that ATG SNPs might be differentially associated with specific host and tumor characteristics including age at diagnosis, TILs, and stage. These associations may be critical to understanding the role of autophagy in cancer, and further investigation will help characterize the contribution of these variants to melanoma progression.

Published

2016

18. Vitamin D receptor polymorphisms and survival in patients with cutaneous melanoma: a population-based study.

Author

Orlow, Irene, Orlow, Irene, Reiner, Anne S, Thomas, Nancy E, Roy, Pampa, Kanetsky, Peter A, Luo, Li, Paine, Susan, Armstrong, Bruce K, Kricker, Anne, Marrett, Loraine D, Rosso, Stefano, Zanetti, Roberto, Gruber, Stephen B, Anton-Culver, Hoda, Gallagher, Richard P, Dwyer, Terence, Busam, Klaus, Begg, Colin B, Berwick, Marianne, GEM Study Group, Orlow, Irene, Orlow, Irene, Reiner, Anne S, Thomas, Nancy E, Roy, Pampa, Kanetsky, Peter A, Luo, Li, Paine, Susan, Armstrong, Bruce K, Kricker, Anne, Marrett, Loraine D, Rosso, Stefano, Zanetti, Roberto, Gruber, Stephen B, Anton-Culver, Hoda, Gallagher, Richard P, Dwyer, Terence, Busam, Klaus, Begg, Colin B, Berwick, Marianne, and GEM Study Group

Abstract

Factors known to affect melanoma survival include age at presentation, sex and tumor characteristics. Polymorphisms also appear to modulate survival following diagnosis. Result from other studies suggest that vitamin D receptor (VDR) polymorphisms (SNPs) impact survival in patients with glioma, renal cell carcinoma, lung, breast, prostate and other cancers; however, a comprehensive study of VDR polymorphisms and melanoma-specific survival is lacking. We aimed to investigate whether VDR genetic variation influences survival in patients with cutaneous melanoma. The analysis involved 3566 incident single and multiple primary melanoma cases enrolled in the international population-based Genes, Environment, and Melanoma Study. Melanoma-specific survival outcomes were calculated for each of 38 VDR SNPs using a competing risk analysis after adjustment for covariates. There were 254 (7.1%) deaths due to melanoma during the median 7.6 years follow-up period. VDR SNPs rs7299460, rs3782905, rs2239182, rs12370156, rs2238140, rs7305032, rs1544410 (BsmI) and rs731236 (TaqI) each had a statistically significant (trend P values < 0.05) association with melanoma-specific survival in multivariate analysis. One functional SNP (rs2239182) remained significant after adjustment for multiple testing using the Monte Carlo method. None of the SNPs associated with survival were significantly associated with Breslow thickness, ulceration or mitosis. These results suggest that the VDR gene may influence survival from melanoma, although the mechanism by which VDR exerts its effect does not seem driven by tumor aggressiveness. Further investigations are needed to confirm our results and to understand the relationship between VDR and survival in the combined context of tumor and host characteristics.

Published

2016

19. Association of Interferon Regulatory Factor-4 Polymorphism rs12203592 With Divergent Melanoma Pathways.

Author

Gibbs, David C, Gibbs, David C, Orlow, Irene, Bramson, Jennifer I, Kanetsky, Peter A, Luo, Li, Kricker, Anne, Armstrong, Bruce K, Anton-Culver, Hoda, Gruber, Stephen B, Marrett, Loraine D, Gallagher, Richard P, Zanetti, Roberto, Rosso, Stefano, Dwyer, Terence, Sharma, Ajay, La Pilla, Emily, From, Lynn, Busam, Klaus J, Cust, Anne E, Ollila, David W, Begg, Colin B, Berwick, Marianne, Thomas, Nancy E, GEM Study Group, Gibbs, David C, Gibbs, David C, Orlow, Irene, Bramson, Jennifer I, Kanetsky, Peter A, Luo, Li, Kricker, Anne, Armstrong, Bruce K, Anton-Culver, Hoda, Gruber, Stephen B, Marrett, Loraine D, Gallagher, Richard P, Zanetti, Roberto, Rosso, Stefano, Dwyer, Terence, Sharma, Ajay, La Pilla, Emily, From, Lynn, Busam, Klaus J, Cust, Anne E, Ollila, David W, Begg, Colin B, Berwick, Marianne, Thomas, Nancy E, and GEM Study Group

Abstract

BackgroundSolar elastosis and neval remnants are histologic markers characteristic of divergent melanoma pathways linked to differences in age at onset, host phenotype, and sun exposure. However, the association between these pathway markers and newly identified low-penetrance melanoma susceptibility loci remains unknown.MethodsIn the Genes, Environment and Melanoma (GEM) Study, 2103 Caucasian participants had first primary melanomas that underwent centralized pathology review. For 47 single-nucleotide polymorphisms (SNPs) previously identified as low-penetrant melanoma risk variants, we used multinomial logistic regression to compare melanoma with solar elastosis and melanoma with neval remnants simultaneously to melanoma with neither of these markers, excluding melanomas with both markers. All statistical tests were two-sided.ResultsIRF4 rs12203592 was the only SNP to pass the false discovery threshold in baseline models adjusted for age, sex, and study center. rs12203592*T was associated positively with melanoma with solar elastosis (odds ratio [OR] = 1.47, 95% confidence interval [CI] = 1.18 to 1.82) and inversely with melanoma with neval remnants (OR = 0.65, 95% CI = 0.48 to 0.87) compared with melanoma with neither marker (P global = 3.78 x 10(-08)). Adjusting for phenotypic characteristics and total sun exposure hours did not materially affect rs12203592's associations. Distinct early- and late-onset age distributions were observed in patients with IRF4 rs12203592 [CC] and [TT] genotypes, respectively.ConclusionsOur findings suggest a role of IRF4 rs12203592 in pathway-specific risk for melanoma development. We hypothesize that IRF4 rs12203592 could underlie in part the bimodal age distribution reported for melanoma and linked to the divergent pathways.

Published

2016

20. Variants in autophagy-related genes and clinical characteristics in melanoma: a population-based study.

Author

White, Kirsten AM, White, Kirsten AM, Luo, Li, Thompson, Todd A, Torres, Salina, Hu, Chien-An Andy, Thomas, Nancy E, Lilyquist, Jenna, Anton-Culver, Hoda, Gruber, Stephen B, From, Lynn, Busam, Klaus J, Orlow, Irene, Kanetsky, Peter A, Marrett, Loraine D, Gallagher, Richard P, Sacchetto, Lidia, Rosso, Stefano, Dwyer, Terence, Cust, Anne E, Begg, Colin B, Berwick, Marianne, GEM Study Group, White, Kirsten AM, White, Kirsten AM, Luo, Li, Thompson, Todd A, Torres, Salina, Hu, Chien-An Andy, Thomas, Nancy E, Lilyquist, Jenna, Anton-Culver, Hoda, Gruber, Stephen B, From, Lynn, Busam, Klaus J, Orlow, Irene, Kanetsky, Peter A, Marrett, Loraine D, Gallagher, Richard P, Sacchetto, Lidia, Rosso, Stefano, Dwyer, Terence, Cust, Anne E, Begg, Colin B, Berwick, Marianne, and GEM Study Group

Abstract

Autophagy has been linked with melanoma risk and survival, but no polymorphisms in autophagy-related (ATG) genes have been investigated in relation to melanoma progression. We examined five single-nucleotide polymorphisms (SNPs) in three ATG genes (ATG5; ATG10; and ATG16L) with known or suspected impact on autophagic flux in an international population-based case-control study of melanoma. DNA from 911 melanoma patients was genotyped. An association was identified between (GG) (rs2241880) and earlier stage at diagnosis (OR 0.47; 95% Confidence Intervals (CI) = 0.27-0.81, P = 0.02) and a decrease in Breslow thickness (P = 0.03). The ATG16L heterozygous genotype (AG) (rs2241880) was associated with younger age at diagnosis (P = 0.02). Two SNPs in ATG5 were found to be associated with increased stage (rs2245214 CG, OR 1.47; 95% CI = 1.11-1.94, P = 0.03; rs510432 CC, OR 1.84; 95% CI = 1.12-3.02, P = 0.05). Finally, we identified inverse associations between ATG5 (GG rs2245214) and melanomas on the scalp or neck (OR 0.20, 95% CI = 0.05-0.86, P = 0.03); ATG10 (CC) (rs1864182) and brisk tumor infiltrating lymphocytes (TILs) (OR 0.42; 95% CI = 0.21-0.88, P = 0.02), and ATG5 (CC) (rs510432) with nonbrisk TILs (OR 0.55; 95% CI = 0.34-0.87, P = 0.01). Our data suggest that ATG SNPs might be differentially associated with specific host and tumor characteristics including age at diagnosis, TILs, and stage. These associations may be critical to understanding the role of autophagy in cancer, and further investigation will help characterize the contribution of these variants to melanoma progression.

Published

2016

21. Vitamin D receptor polymorphisms and survival in patients with cutaneous melanoma: a population-based study.

Author

Orlow, Irene, Orlow, Irene, Reiner, Anne S, Thomas, Nancy E, Roy, Pampa, Kanetsky, Peter A, Luo, Li, Paine, Susan, Armstrong, Bruce K, Kricker, Anne, Marrett, Loraine D, Rosso, Stefano, Zanetti, Roberto, Gruber, Stephen B, Anton-Culver, Hoda, Gallagher, Richard P, Dwyer, Terence, Busam, Klaus, Begg, Colin B, Berwick, Marianne, GEM Study Group, Orlow, Irene, Orlow, Irene, Reiner, Anne S, Thomas, Nancy E, Roy, Pampa, Kanetsky, Peter A, Luo, Li, Paine, Susan, Armstrong, Bruce K, Kricker, Anne, Marrett, Loraine D, Rosso, Stefano, Zanetti, Roberto, Gruber, Stephen B, Anton-Culver, Hoda, Gallagher, Richard P, Dwyer, Terence, Busam, Klaus, Begg, Colin B, Berwick, Marianne, and GEM Study Group

Abstract

Factors known to affect melanoma survival include age at presentation, sex and tumor characteristics. Polymorphisms also appear to modulate survival following diagnosis. Result from other studies suggest that vitamin D receptor (VDR) polymorphisms (SNPs) impact survival in patients with glioma, renal cell carcinoma, lung, breast, prostate and other cancers; however, a comprehensive study of VDR polymorphisms and melanoma-specific survival is lacking. We aimed to investigate whether VDR genetic variation influences survival in patients with cutaneous melanoma. The analysis involved 3566 incident single and multiple primary melanoma cases enrolled in the international population-based Genes, Environment, and Melanoma Study. Melanoma-specific survival outcomes were calculated for each of 38 VDR SNPs using a competing risk analysis after adjustment for covariates. There were 254 (7.1%) deaths due to melanoma during the median 7.6 years follow-up period. VDR SNPs rs7299460, rs3782905, rs2239182, rs12370156, rs2238140, rs7305032, rs1544410 (BsmI) and rs731236 (TaqI) each had a statistically significant (trend P values < 0.05) association with melanoma-specific survival in multivariate analysis. One functional SNP (rs2239182) remained significant after adjustment for multiple testing using the Monte Carlo method. None of the SNPs associated with survival were significantly associated with Breslow thickness, ulceration or mitosis. These results suggest that the VDR gene may influence survival from melanoma, although the mechanism by which VDR exerts its effect does not seem driven by tumor aggressiveness. Further investigations are needed to confirm our results and to understand the relationship between VDR and survival in the combined context of tumor and host characteristics.

Published

2016

22. Association of Interferon Regulatory Factor-4 Polymorphism rs12203592 With Divergent Melanoma Pathways.

Author

Gibbs, David C, Gibbs, David C, Orlow, Irene, Bramson, Jennifer I, Kanetsky, Peter A, Luo, Li, Kricker, Anne, Armstrong, Bruce K, Anton-Culver, Hoda, Gruber, Stephen B, Marrett, Loraine D, Gallagher, Richard P, Zanetti, Roberto, Rosso, Stefano, Dwyer, Terence, Sharma, Ajay, La Pilla, Emily, From, Lynn, Busam, Klaus J, Cust, Anne E, Ollila, David W, Begg, Colin B, Berwick, Marianne, Thomas, Nancy E, GEM Study Group, Gibbs, David C, Gibbs, David C, Orlow, Irene, Bramson, Jennifer I, Kanetsky, Peter A, Luo, Li, Kricker, Anne, Armstrong, Bruce K, Anton-Culver, Hoda, Gruber, Stephen B, Marrett, Loraine D, Gallagher, Richard P, Zanetti, Roberto, Rosso, Stefano, Dwyer, Terence, Sharma, Ajay, La Pilla, Emily, From, Lynn, Busam, Klaus J, Cust, Anne E, Ollila, David W, Begg, Colin B, Berwick, Marianne, Thomas, Nancy E, and GEM Study Group

Abstract

Solar elastosis and neval remnants are histologic markers characteristic of divergent melanoma pathways linked to differences in age at onset, host phenotype, and sun exposure. However, the association between these pathway markers and newly identified low-penetrance melanoma susceptibility loci remains unknown. In the Genes, Environment and Melanoma (GEM) Study, 2103 Caucasian participants had first primary melanomas that underwent centralized pathology review. For 47 single-nucleotide polymorphisms (SNPs) previously identified as low-penetrant melanoma risk variants, we used multinomial logistic regression to compare melanoma with solar elastosis and melanoma with neval remnants simultaneously to melanoma with neither of these markers, excluding melanomas with both markers. All statistical tests were two-sided. IRF4 rs12203592 was the only SNP to pass the false discovery threshold in baseline models adjusted for age, sex, and study center. rs12203592*T was associated positively with melanoma with solar elastosis (odds ratio [OR] = 1.47, 95% confidence interval [CI] = 1.18 to 1.82) and inversely with melanoma with neval remnants (OR = 0.65, 95% CI = 0.48 to 0.87) compared with melanoma with neither marker (P global = 3.78 x 10(-08)). Adjusting for phenotypic characteristics and total sun exposure hours did not materially affect rs12203592's associations. Distinct early- and late-onset age distributions were observed in patients with IRF4 rs12203592 [CC] and [TT] genotypes, respectively. Our findings suggest a role of IRF4 rs12203592 in pathway-specific risk for melanoma development. We hypothesize that IRF4 rs12203592 could underlie in part the bimodal age distribution reported for melanoma and linked to the divergent pathways.

Published

2016

23. Nevus count associations with pigmentary phenotype, histopathological melanoma characteristics and survival from melanoma.

Author

Taylor, Nicholas J, Taylor, Nicholas J, Thomas, Nancy E, Anton-Culver, Hoda, Armstrong, Bruce K, Begg, Colin B, Busam, Klaus J, Cust, Anne E, Dwyer, Terence, From, Lynn, Gallagher, Richard P, Gruber, Stephen B, Nishri, Diane E, Orlow, Irene, Rosso, Stefano, Venn, Alison J, Zanetti, Roberto, Berwick, Marianne, Kanetsky, Peter A, GEM Study Group, Taylor, Nicholas J, Taylor, Nicholas J, Thomas, Nancy E, Anton-Culver, Hoda, Armstrong, Bruce K, Begg, Colin B, Busam, Klaus J, Cust, Anne E, Dwyer, Terence, From, Lynn, Gallagher, Richard P, Gruber, Stephen B, Nishri, Diane E, Orlow, Irene, Rosso, Stefano, Venn, Alison J, Zanetti, Roberto, Berwick, Marianne, Kanetsky, Peter A, and GEM Study Group

Abstract

Although nevus count is an established risk factor for melanoma, relationships between nevus number and patient and tumor characteristics have not been well studied and the influence of nevus count on melanoma-specific survival is equivocal. Using data from the Genes, Environment and Melanoma (GEM) study, a large population-based study of primary cutaneous melanoma, we evaluated associations between number of nevi and patient features, including sun-sensitivity summarized in a phenotypic index, and tumor characteristics. We also assessed the association of nevus count with melanoma-specific survival. Higher nevus counts were independently and positively associated with male gender and younger age at diagnosis, and they were inversely associated with lentigo maligna histology. We observed a borderline significant trend of poorer melanoma-specific survival with increasing quartile of nevus count, but little or no association between number of nevi and pigmentary phenotypic characteristics or prognostic tumor features.

Published

2016

24. A design for cancer case-control studies using only incident cases: experience with the GEM study of melanoma.

Author

Begg, Colin B, Begg, Colin B, Hummer, Amanda J, Mujumdar, Urvi, Armstrong, Bruce K, Kricker, Anne, Marrett, Loraine D, Millikan, Robert C, Gruber, Stephen B, Culver, Hoda Anton, Zanetti, Roberto, Gallagher, Richard P, Dwyer, Terrence, Rebbeck, Timothy R, Busam, Klaus, From, Lynn, Berwick, Marianne, GEM Study Group, Begg, Colin B, Begg, Colin B, Hummer, Amanda J, Mujumdar, Urvi, Armstrong, Bruce K, Kricker, Anne, Marrett, Loraine D, Millikan, Robert C, Gruber, Stephen B, Culver, Hoda Anton, Zanetti, Roberto, Gallagher, Richard P, Dwyer, Terrence, Rebbeck, Timothy R, Busam, Klaus, From, Lynn, Berwick, Marianne, and GEM Study Group

Abstract

BackgroundThe population-based case-control study is not suited to the evaluation of rare genetic (or environmental) factors. The use of a novel case-control design in which cases have second primaries and controls are cancer survivors has been proposed for this purpose.MethodsWe report results from an international study of melanoma that involved population-based ascertainment of incident cases of second or subsequent primary melanoma as the 'case' group and incident cases of first primary melanoma as the 'control' group. We evaluate the validity of the study design by comparing the results obtained for phenotypic factors that have been shown consistently to be associated with melanoma in previous conventional studies with the results from a conventional case-control study conducted in Connecticut and from literature reviews.ResultsAll but one of the known risk factors for melanoma were shown to be significantly associated with melanoma in our study, though the individual odds ratios appear to be somewhat attenuated relative to the magnitudes typically observed in the literature.ConclusionsPatients with a second or subsequent primary cancer of a single type represent a potentially valuable and under-utilized resource for the study of cancer aetiology.

Published

2006

25. A design for cancer case-control studies using only incident cases: experience with the GEM study of melanoma.

Author

Begg, Colin B, Begg, Colin B, Hummer, Amanda J, Mujumdar, Urvi, Armstrong, Bruce K, Kricker, Anne, Marrett, Loraine D, Millikan, Robert C, Gruber, Stephen B, Culver, Hoda Anton, Zanetti, Roberto, Gallagher, Richard P, Dwyer, Terrence, Rebbeck, Timothy R, Busam, Klaus, From, Lynn, Berwick, Marianne, GEM Study Group, Begg, Colin B, Begg, Colin B, Hummer, Amanda J, Mujumdar, Urvi, Armstrong, Bruce K, Kricker, Anne, Marrett, Loraine D, Millikan, Robert C, Gruber, Stephen B, Culver, Hoda Anton, Zanetti, Roberto, Gallagher, Richard P, Dwyer, Terrence, Rebbeck, Timothy R, Busam, Klaus, From, Lynn, Berwick, Marianne, and GEM Study Group

Abstract

BackgroundThe population-based case-control study is not suited to the evaluation of rare genetic (or environmental) factors. The use of a novel case-control design in which cases have second primaries and controls are cancer survivors has been proposed for this purpose.MethodsWe report results from an international study of melanoma that involved population-based ascertainment of incident cases of second or subsequent primary melanoma as the 'case' group and incident cases of first primary melanoma as the 'control' group. We evaluate the validity of the study design by comparing the results obtained for phenotypic factors that have been shown consistently to be associated with melanoma in previous conventional studies with the results from a conventional case-control study conducted in Connecticut and from literature reviews.ResultsAll but one of the known risk factors for melanoma were shown to be significantly associated with melanoma in our study, though the individual odds ratios appear to be somewhat attenuated relative to the magnitudes typically observed in the literature.ConclusionsPatients with a second or subsequent primary cancer of a single type represent a potentially valuable and under-utilized resource for the study of cancer aetiology.

Published

2006

26. Lifetime risk of melanoma in CDKN2A mutation carriers in a population-based sample.

Author

Begg, Colin B, Begg, Colin B, Orlow, Irene, Hummer, Amanda J, Armstrong, Bruce K, Kricker, Anne, Marrett, Loraine D, Millikan, Robert C, Gruber, Stephen B, Anton-Culver, Hoda, Zanetti, Roberto, Gallagher, Richard P, Dwyer, Terence, Rebbeck, Timothy R, Mitra, Nandita, Busam, Klaus, From, Lynn, Berwick, Marianne, Genes Environment and Melanoma Study Group, Begg, Colin B, Begg, Colin B, Orlow, Irene, Hummer, Amanda J, Armstrong, Bruce K, Kricker, Anne, Marrett, Loraine D, Millikan, Robert C, Gruber, Stephen B, Anton-Culver, Hoda, Zanetti, Roberto, Gallagher, Richard P, Dwyer, Terence, Rebbeck, Timothy R, Mitra, Nandita, Busam, Klaus, From, Lynn, Berwick, Marianne, and Genes Environment and Melanoma Study Group

Abstract

BackgroundGermline mutations in the CDKN2A gene have been linked to melanoma incidence in many families with multiple cases of the disease. Previous studies of multiple-case families have indicated that the lifetime risk (i.e., penetrance) of melanoma in CDKN2A mutation carriers is very high, ranging from 58% in Europe to 91% in Australia by age 80 years. In this study, we examined lifetime melanoma risk among CDKN2A mutation carriers using carriers who were identified in a population-based study of melanoma.MethodsProbands for the study were incident case patients with either first or subsequent melanoma who were identified in nine geographic regions in Australia, Canada, the United States, and Italy. A total of 3626 probands (53% participation rate) with adequate DNA for analysis were recruited and genotyped for CDKN2A mutations. From the 3550 probands whose DNA could be amplified by polymerase chain reaction of CDKN2A exons 1alpha, 2, and 3 and surrounding regions, 65 mutation carriers were identified. Melanoma histories in first-degree relatives of these probands were used to calculate the lifetime risk in CDKN2A mutation carriers using the kin-cohort method.ResultsThe risk of melanoma in CDKN2A mutation carriers was approximately 14% (95% CI = 8% to 22%) by age 50 years, 24% (95% CI = 15% to 34%) by age 70 years, and 28% (95% CI = 18% to 40%) by age 80 years. Eighteen probands had three or more first-degree relatives with melanoma, but only one was a carrier of a CDKN2A mutation.ConclusionsCDKN2A mutation carriers in the general population have a much lower risk of melanoma than that suggested by estimates obtained from multiple-case families. The preponderance of familial clustering of melanoma occurs in families without identifiable mutations in CDKN2A.

Published

2005

27. Lifetime risk of melanoma in CDKN2A mutation carriers in a population-based sample.

Author

Begg, Colin B, Begg, Colin B, Orlow, Irene, Hummer, Amanda J, Armstrong, Bruce K, Kricker, Anne, Marrett, Loraine D, Millikan, Robert C, Gruber, Stephen B, Anton-Culver, Hoda, Zanetti, Roberto, Gallagher, Richard P, Dwyer, Terence, Rebbeck, Timothy R, Mitra, Nandita, Busam, Klaus, From, Lynn, Berwick, Marianne, Genes Environment and Melanoma Study Group, Begg, Colin B, Begg, Colin B, Orlow, Irene, Hummer, Amanda J, Armstrong, Bruce K, Kricker, Anne, Marrett, Loraine D, Millikan, Robert C, Gruber, Stephen B, Anton-Culver, Hoda, Zanetti, Roberto, Gallagher, Richard P, Dwyer, Terence, Rebbeck, Timothy R, Mitra, Nandita, Busam, Klaus, From, Lynn, Berwick, Marianne, and Genes Environment and Melanoma Study Group

Abstract

BackgroundGermline mutations in the CDKN2A gene have been linked to melanoma incidence in many families with multiple cases of the disease. Previous studies of multiple-case families have indicated that the lifetime risk (i.e., penetrance) of melanoma in CDKN2A mutation carriers is very high, ranging from 58% in Europe to 91% in Australia by age 80 years. In this study, we examined lifetime melanoma risk among CDKN2A mutation carriers using carriers who were identified in a population-based study of melanoma.MethodsProbands for the study were incident case patients with either first or subsequent melanoma who were identified in nine geographic regions in Australia, Canada, the United States, and Italy. A total of 3626 probands (53% participation rate) with adequate DNA for analysis were recruited and genotyped for CDKN2A mutations. From the 3550 probands whose DNA could be amplified by polymerase chain reaction of CDKN2A exons 1alpha, 2, and 3 and surrounding regions, 65 mutation carriers were identified. Melanoma histories in first-degree relatives of these probands were used to calculate the lifetime risk in CDKN2A mutation carriers using the kin-cohort method.ResultsThe risk of melanoma in CDKN2A mutation carriers was approximately 14% (95% CI = 8% to 22%) by age 50 years, 24% (95% CI = 15% to 34%) by age 70 years, and 28% (95% CI = 18% to 40%) by age 80 years. Eighteen probands had three or more first-degree relatives with melanoma, but only one was a carrier of a CDKN2A mutation.ConclusionsCDKN2A mutation carriers in the general population have a much lower risk of melanoma than that suggested by estimates obtained from multiple-case families. The preponderance of familial clustering of melanoma occurs in families without identifiable mutations in CDKN2A.

Published

2005

28. Inherited variation at MC1R and histological characteristics of primary melanoma.

Author

Taylor, Nicholas J, Taylor, Nicholas J, Busam, Klaus J, From, Lynn, Groben, Pamela A, Anton-Culver, Hoda, Cust, Anne E, Begg, Colin B, Dwyer, Terence, Gallagher, Richard P, Gruber, Stephen B, Orlow, Irene, Rosso, Stefano, Thomas, Nancy E, Zanetti, Roberto, Rebbeck, Timothy R, Berwick, Marianne, Kanetsky, Peter A, Taylor, Nicholas J, Taylor, Nicholas J, Busam, Klaus J, From, Lynn, Groben, Pamela A, Anton-Culver, Hoda, Cust, Anne E, Begg, Colin B, Dwyer, Terence, Gallagher, Richard P, Gruber, Stephen B, Orlow, Irene, Rosso, Stefano, Thomas, Nancy E, Zanetti, Roberto, Rebbeck, Timothy R, Berwick, Marianne, and Kanetsky, Peter A

Abstract

Variation in the melanocortin-1receptor (MC1R) gene is associated with pigmentary phenotypes and risk of malignant melanoma. Few studies have reported on MC1R variation with respect to tumor characteristics, especially clinically important prognostic features. We examined associations between MC1R variants and histopathological melanoma characteristics. Study participants were enrolled from nine geographic regions in Australia, Canada, Italy and the United States and were genotyped for MC1R variants classified as high-risk [R] (D84E, R142H, R151C, R160W, and D294H, all nonsense and insertion/deletion) or low-risk [r] (all other nonsynonymous) variants. Tissue was available for 2,160 white participants of the Genes, Environment and Melanoma (GEM) Study with a first incident primary melanoma diagnosis, and underwent centralized pathologic review. No statistically significant associations were observed between MC1R variants and AJCC established prognostic tumor characteristics: Breslow thickness, presence of mitoses or presence of ulceration. However, MC1R was significantly associated with anatomic site of melanoma (p = 0.002) and a positive association was observed between carriage of more than one [R] variant and melanomas arising on the arms (OR = 2.39; 95% CI: 1.40, 4.09). We also observed statistically significant differences between sun-sensitive and sun-resistant individuals with respect to associations between MC1R genotype and AJCC prognostic tumor characteristics. Our results suggest inherited variation in MC1R may play an influential role in anatomic site presentation of melanomas and may differ with respect to skin pigmentation phenotype.

Published

2015

29. Inherited variation at MC1R and histological characteristics of primary melanoma.

Author

Taylor, Nicholas J, Dadras, Soheil S1, Taylor, Nicholas J, Busam, Klaus J, From, Lynn, Groben, Pamela A, Anton-Culver, Hoda, Cust, Anne E, Begg, Colin B, Dwyer, Terence, Gallagher, Richard P, Gruber, Stephen B, Orlow, Irene, Rosso, Stefano, Thomas, Nancy E, Zanetti, Roberto, Rebbeck, Timothy R, Berwick, Marianne, Kanetsky, Peter A, Taylor, Nicholas J, Dadras, Soheil S1, Taylor, Nicholas J, Busam, Klaus J, From, Lynn, Groben, Pamela A, Anton-Culver, Hoda, Cust, Anne E, Begg, Colin B, Dwyer, Terence, Gallagher, Richard P, Gruber, Stephen B, Orlow, Irene, Rosso, Stefano, Thomas, Nancy E, Zanetti, Roberto, Rebbeck, Timothy R, Berwick, Marianne, and Kanetsky, Peter A

Abstract

Variation in the melanocortin-1receptor (MC1R) gene is associated with pigmentary phenotypes and risk of malignant melanoma. Few studies have reported on MC1R variation with respect to tumor characteristics, especially clinically important prognostic features. We examined associations between MC1R variants and histopathological melanoma characteristics. Study participants were enrolled from nine geographic regions in Australia, Canada, Italy and the United States and were genotyped for MC1R variants classified as high-risk [R] (D84E, R142H, R151C, R160W, and D294H, all nonsense and insertion/deletion) or low-risk [r] (all other nonsynonymous) variants. Tissue was available for 2,160 white participants of the Genes, Environment and Melanoma (GEM) Study with a first incident primary melanoma diagnosis, and underwent centralized pathologic review. No statistically significant associations were observed between MC1R variants and AJCC established prognostic tumor characteristics: Breslow thickness, presence of mitoses or presence of ulceration. However, MC1R was significantly associated with anatomic site of melanoma (p = 0.002) and a positive association was observed between carriage of more than one [R] variant and melanomas arising on the arms (OR = 2.39; 95% CI: 1.40, 4.09). We also observed statistically significant differences between sun-sensitive and sun-resistant individuals with respect to associations between MC1R genotype and AJCC prognostic tumor characteristics. Our results suggest inherited variation in MC1R may play an influential role in anatomic site presentation of melanomas and may differ with respect to skin pigmentation phenotype.

Published

2015

30. Inherited variation at MC1R and ASIP and association with melanoma-specific survival.

Author

Taylor, Nicholas J, Taylor, Nicholas J, Reiner, Anne S, Begg, Colin B, Cust, Anne E, Busam, Klaus J, Anton-Culver, Hoda, Dwyer, Terence, From, Lynn, Gallagher, Richard P, Gruber, Stephen B, Rosso, Stefano, White, Kirsten A, Zanetti, Roberto, Orlow, Irene, Thomas, Nancy E, Rebbeck, Timothy R, Berwick, Marianne, Kanetsky, Peter A, GEM Study Group, Taylor, Nicholas J, Taylor, Nicholas J, Reiner, Anne S, Begg, Colin B, Cust, Anne E, Busam, Klaus J, Anton-Culver, Hoda, Dwyer, Terence, From, Lynn, Gallagher, Richard P, Gruber, Stephen B, Rosso, Stefano, White, Kirsten A, Zanetti, Roberto, Orlow, Irene, Thomas, Nancy E, Rebbeck, Timothy R, Berwick, Marianne, Kanetsky, Peter A, and GEM Study Group

Abstract

Melanocortin-1 receptor (MC1R) is a marker of melanoma risk in populations of European ancestry. However, MC1R effects on survival are much less studied. We investigated associations between variation at MC1R and survival in an international, population-based series of single primary melanoma patients enrolled into the Genes, Environment, and Melanoma study. MC1R genotype data was available for 2,200 participants with a first incident primary melanoma diagnosis. We estimated the association of MC1R genotypes with melanoma-specific survival (i.e., death caused by melanoma) and overall survival using COX proportional hazards modeling, adjusting for established prognostic factors for melanoma. We also conducted stratified analyses by Breslow thickness, tumor site, phenotypic index, and age. In addition, we evaluated haplotypes involving polymorphisms near the Agouti signaling protein gene (ASIP) locus for their impacts on survival. Melanoma-specific survival was inversely associated with carriage of MC1R variants in the absence of consensus alleles compared to carriage of at least one consensus allele (hazard ratio (HR) = 0.60; 95% confidence interval (CI): 0.40, 0.90). MC1R results for overall survival were consistent with no association. We did not observe any statistical evidence of heterogeneity of effect estimates in stratified analyses. We observed increased hazard of melanoma-specific death among carriers of the risk haplotype TG near the ASIP locus (HR = 1.37; 95% CI: 0.91, 2.04) when compared to carriers of the most common GG haplotype. Similar results were noted for overall survival. Upon examining the ASIP TG/TG diplotype, we observed considerably increased hazard of melanoma-specific death (HR = 5.11; 95% CI: 1.88, 13.88) compared to carriers of the most common GG/GG diplotype. Our data suggest improved melanoma-specific survival among carriers of two inherited MC1R variants.

Published

2015

31. Inherited genetic variants associated with occurrence of multiple primary melanoma.

Author

Gibbs, David C, Gibbs, David C, Orlow, Irene, Kanetsky, Peter A, Luo, Li, Kricker, Anne, Armstrong, Bruce K, Anton-Culver, Hoda, Gruber, Stephen B, Marrett, Loraine D, Gallagher, Richard P, Zanetti, Roberto, Rosso, Stefano, Dwyer, Terence, Sharma, Ajay, La Pilla, Emily, From, Lynn, Busam, Klaus J, Cust, Anne E, Ollila, David W, Begg, Colin B, Berwick, Marianne, Thomas, Nancy E, GEM Study Group, Gibbs, David C, Gibbs, David C, Orlow, Irene, Kanetsky, Peter A, Luo, Li, Kricker, Anne, Armstrong, Bruce K, Anton-Culver, Hoda, Gruber, Stephen B, Marrett, Loraine D, Gallagher, Richard P, Zanetti, Roberto, Rosso, Stefano, Dwyer, Terence, Sharma, Ajay, La Pilla, Emily, From, Lynn, Busam, Klaus J, Cust, Anne E, Ollila, David W, Begg, Colin B, Berwick, Marianne, Thomas, Nancy E, and GEM Study Group

Abstract

Recent studies, including genome-wide association studies, have identified several putative low-penetrance susceptibility loci for melanoma. We sought to determine their generalizability to genetic predisposition for multiple primary melanoma in the international population-based Genes, Environment, and Melanoma (GEM) Study. GEM is a case-control study of 1,206 incident cases of multiple primary melanoma and 2,469 incident first primary melanoma participants as the control group. We investigated the odds of developing multiple primary melanoma for 47 SNPs from 21 distinct genetic regions previously reported to be associated with melanoma. ORs and 95% confidence intervals were determined using logistic regression models adjusted for baseline features (age, sex, age by sex interaction, and study center). We investigated univariable models and built multivariable models to assess independent effects of SNPs. Eleven SNPs in 6 gene neighborhoods (TERT/CLPTM1L, TYRP1, MTAP, TYR, NCOA6, and MX2) and a PARP1 haplotype were associated with multiple primary melanoma. In a multivariable model that included only the most statistically significant findings from univariable modeling and adjusted for pigmentary phenotype, back nevi, and baseline features, we found TERT/CLPTM1L rs401681 (P = 0.004), TYRP1 rs2733832 (P = 0.006), MTAP rs1335510 (P = 0.0005), TYR rs10830253 (P = 0.003), and MX2 rs45430 (P = 0.008) to be significantly associated with multiple primary melanoma, while NCOA6 rs4911442 approached significance (P = 0.06). The GEM Study provides additional evidence for the relevance of these genetic regions to melanoma risk and estimates the magnitude of the observed genetic effect on development of subsequent primary melanoma.

Published

2015

32. Association Between NRAS and BRAF Mutational Status and Melanoma-Specific Survival Among Patients With Higher-Risk Primary Melanoma.

Author

Thomas, Nancy E, Thomas, Nancy E, Edmiston, Sharon N, Alexander, Audrey, Groben, Pamela A, Parrish, Eloise, Kricker, Anne, Armstrong, Bruce K, Anton-Culver, Hoda, Gruber, Stephen B, From, Lynn, Busam, Klaus J, Hao, Honglin, Orlow, Irene, Kanetsky, Peter A, Luo, Li, Reiner, Anne S, Paine, Susan, Frank, Jill S, Bramson, Jennifer I, Marrett, Lorraine D, Gallagher, Richard P, Zanetti, Roberto, Rosso, Stefano, Dwyer, Terence, Cust, Anne E, Ollila, David W, Begg, Colin B, Berwick, Marianne, Conway, Kathleen, GEM Study Group, Thomas, Nancy E, Thomas, Nancy E, Edmiston, Sharon N, Alexander, Audrey, Groben, Pamela A, Parrish, Eloise, Kricker, Anne, Armstrong, Bruce K, Anton-Culver, Hoda, Gruber, Stephen B, From, Lynn, Busam, Klaus J, Hao, Honglin, Orlow, Irene, Kanetsky, Peter A, Luo, Li, Reiner, Anne S, Paine, Susan, Frank, Jill S, Bramson, Jennifer I, Marrett, Lorraine D, Gallagher, Richard P, Zanetti, Roberto, Rosso, Stefano, Dwyer, Terence, Cust, Anne E, Ollila, David W, Begg, Colin B, Berwick, Marianne, Conway, Kathleen, and GEM Study Group

Abstract

ImportanceNRAS and BRAF mutations in melanoma inform current treatment paradigms, but their role in survival from primary melanoma has not been established. Identification of patients at high risk of melanoma-related death based on their primary melanoma characteristics before evidence of recurrence could inform recommendations for patient follow-up and eligibility for adjuvant trials.ObjectiveTo determine tumor characteristics and survival from primary melanoma by somatic NRAS and BRAF status.Design, setting, and participantsA population-based study with a median follow-up of 7.6 years (through 2007), including 912 patients from the United States and Australia in the Genes, Environment, and Melanoma (GEM) Study, with first primary cutaneous melanoma diagnosed in the year 2000 and analyzed for NRAS and BRAF mutations.Main outcomes and measuresTumor characteristics and melanoma-specific survival of primary melanoma by NRAS and BRAF mutational status.ResultsThe melanomas were 13% NRAS+, 30% BRAF+, and 57% with neither NRAS nor BRAF mutation (wildtype [WT]). In a multivariable model including clinicopathologic characteristics, relative to WT melanoma (with results reported as odds ratios [95% CIs]), NRAS+ melanoma was associated with presence of mitoses (1.8 [1.0-3.3]), lower tumor-infiltrating lymphocyte (TIL) grade (nonbrisk, 0.5 [0.3-0.8]; and brisk, 0.3 [0.5-0.7] [vs absent TILs]), and anatomic site other than scalp/neck (0.1 [0.01-0.6] for scalp/neck vs trunk/pelvis), and BRAF+ melanoma was associated with younger age (ages 50-69 years, 0.7 [0.5-1.0]; and ages >70 years, 0.5 [0.3-0.8] [vs <50 years]), superficial spreading subtype (nodular, 0.5 [0.2-1.0]; lentigo maligna, 0.4 [0.2-0.7]; and unclassified/other, 0.2 [0.1-0.5] [vs superficial spreading]), and presence of mitoses (1.7 [1.1-2.6]) (P < .05 for all). There was no significant difference in melanoma-specific survival (reported as hazard ratios [95% CIs]) for melanoma harboring mutations in NRAS (1

Published

2015

33. MITF E318K's effect on melanoma risk independent of, but modified by, other risk factors.

Author

Berwick, Marianne, Berwick, Marianne, MacArthur, Jamie, Orlow, Irene, Kanetsky, Peter, Begg, Colin B, Luo, Li, Reiner, Anne, Sharma, Ajay, Armstrong, Bruce K, Kricker, Anne, Cust, Anne E, Marrett, Loraine D, Gruber, Stephen B, Anton-Culver, Hoda, Zanetti, Roberto, Rosso, Stefano, Gallagher, Richard P, Dwyer, Terence, Venn, Alison, Busam, Klaus, From, Lynn, White, Kirsten, Thomas, Nancy E, GEM Study Group, Berwick, Marianne, Berwick, Marianne, MacArthur, Jamie, Orlow, Irene, Kanetsky, Peter, Begg, Colin B, Luo, Li, Reiner, Anne, Sharma, Ajay, Armstrong, Bruce K, Kricker, Anne, Cust, Anne E, Marrett, Loraine D, Gruber, Stephen B, Anton-Culver, Hoda, Zanetti, Roberto, Rosso, Stefano, Gallagher, Richard P, Dwyer, Terence, Venn, Alison, Busam, Klaus, From, Lynn, White, Kirsten, Thomas, Nancy E, and GEM Study Group

Abstract

A rare germline variant in the microphthalmia-associated transcription factor (MITF) gene, E318K, has been reported as associated with melanoma. We confirmed its independent association with melanoma [odds ratio (OR) 1.7, 95% confidence interval (CI) = 1.1, 2.7, P = 0.03]; adjusted for age, sex, center, age × sex interaction, pigmentation characteristics, family history of melanoma, and nevus density). In stratified analyses, carriage of MITF E318K was associated with melanoma more strongly in people with dark hair than fair hair (P for interaction, 0.03) and in those with no moles than some or many moles (P for interaction, <0.01). There was no evidence of interaction between MC1R 'red hair variants' and MITF E318K. Moreover, risk of melanoma among carriers with 'low risk' phenotypes was as great or greater than among those with 'at risk' phenotypes with few exceptions.

Published

2014

34. Sun exposure and melanoma survival: a GEM study.

Author

Berwick, Marianne, Berwick, Marianne, Reiner, Anne S, Paine, Susan, Armstrong, Bruce K, Kricker, Anne, Goumas, Chris, Cust, Anne E, Thomas, Nancy E, Groben, Pamela A, From, Lynn, Busam, Klaus, Orlow, Irene, Marrett, Loraine D, Gallagher, Richard P, Gruber, Stephen B, Anton-Culver, Hoda, Rosso, Stefano, Zanetti, Roberto, Kanetsky, Peter A, Dwyer, Terry, Venn, Alison, Lee-Taylor, Julia, Begg, Colin B, GEM Study Group, Berwick, Marianne, Berwick, Marianne, Reiner, Anne S, Paine, Susan, Armstrong, Bruce K, Kricker, Anne, Goumas, Chris, Cust, Anne E, Thomas, Nancy E, Groben, Pamela A, From, Lynn, Busam, Klaus, Orlow, Irene, Marrett, Loraine D, Gallagher, Richard P, Gruber, Stephen B, Anton-Culver, Hoda, Rosso, Stefano, Zanetti, Roberto, Kanetsky, Peter A, Dwyer, Terry, Venn, Alison, Lee-Taylor, Julia, Begg, Colin B, and GEM Study Group

Abstract

BackgroundWe previously reported a significant association between higher UV radiation exposure before diagnosis and greater survival with melanoma in a population-based study in Connecticut. We sought to evaluate the hypothesis that sun exposure before diagnosis was associated with greater survival in a larger, international population-based study with more detailed exposure information.MethodsWe conducted a multicenter, international population-based study in four countries-Australia, Italy, Canada, and the United States-with 3,578 cases of melanoma with an average of 7.4 years of follow-up. Measures of sun exposure included sunburn, intermittent exposure, hours of holiday sun exposure, hours of water-related outdoor activities, ambient ultraviolet B (280-320 nm) dose, histologic solar elastosis, and season of diagnosis.ResultsResults were not strongly supportive of the earlier hypothesis. Having had any sunburn in 1 year within 10 years of diagnosis was inversely associated with survival; solar elastosis-a measure of lifetime cumulative exposure-was not. In addition, none of the intermittent exposure measures-water-related activities and sunny holidays-were associated with melanoma-specific survival. Estimated ambient UVB dose was not associated with survival.ConclusionAlthough there was an apparent protective effect of sunburns within 10 years of diagnosis, there was only weak evidence in this large, international, population-based study of melanoma that sun exposure before diagnosis is associated with greater melanoma-specific survival.ImpactThis study adds to the evidence that sun exposure before melanoma diagnosis has little effect on survival with melanoma.

Published

2014

35. Comparison of clinicopathologic features and survival of histopathologically amelanotic and pigmented melanomas: a population-based study.

Author

Thomas, Nancy E, Thomas, Nancy E, Kricker, Anne, Waxweiler, Weston T, Dillon, Patrick M, Busman, Klaus J, From, Lynn, Groben, Pamela A, Armstrong, Bruce K, Anton-Culver, Hoda, Gruber, Stephen B, Marrett, Loraine D, Gallagher, Richard P, Zanetti, Roberto, Rosso, Stefano, Dwyer, Terence, Venn, Alison, Kanetsky, Peter A, Orlow, Irene, Paine, Susan, Ollila, David W, Reiner, Anne S, Luo, Li, Hao, Honglin, Frank, Jill S, Begg, Colin B, Berwick, Marianne, Genes, Environment, and Melanoma (GEM) Study Group, Thomas, Nancy E, Thomas, Nancy E, Kricker, Anne, Waxweiler, Weston T, Dillon, Patrick M, Busman, Klaus J, From, Lynn, Groben, Pamela A, Armstrong, Bruce K, Anton-Culver, Hoda, Gruber, Stephen B, Marrett, Loraine D, Gallagher, Richard P, Zanetti, Roberto, Rosso, Stefano, Dwyer, Terence, Venn, Alison, Kanetsky, Peter A, Orlow, Irene, Paine, Susan, Ollila, David W, Reiner, Anne S, Luo, Li, Hao, Honglin, Frank, Jill S, Begg, Colin B, Berwick, Marianne, and Genes, Environment, and Melanoma (GEM) Study Group

Abstract

IMPORTANCE Previous studies have reported that histopathologically amelanotic melanoma is associated with poorer survival than pigmented melanoma; however, small numbers of amelanotic melanomas, selected populations, lack of centralized pathologic review, or no adjustment for stage limit the interpretation or generalization of results from prior studies.OBJECTIVE To compare melanoma-specific survival between patients with histopathologically amelanotic and those with pigmented melanoma in a large international population-based study.DESIGN, SETTING, AND PARTICIPANTS Survival analysis with a median follow-up of 7.6 years.The study population comprised 2995 patients with 3486 invasive primary melanomas centrally scored for histologic pigmentation from the Genes, Environment, and Melanoma(GEM) Study, which enrolled incident cases of melanoma diagnosed in 1998 through 2003 from international population-based cancer registries.MAIN OUTCOMES AND MEASURES Clinicopathologic predictors and melanoma-specific survival of histologically amelanotic and pigmented melanoma were compared using generalized estimating equations and Cox regression models, respectively.RESULTS Of 3467 melanomas, 275 (8%) were histopathologically amelanotic. Female sex,nodular and unclassified or other histologic subtypes, increased Breslow thickness, presence of mitoses, severe solar elastosis, and lack of a coexisting nevus were independently associated with amelanotic melanoma (each P < .05). Amelanotic melanoma was generally ofa higher American Joint Committee on Cancer (AJCC) tumor stage at diagnosis (odds ratios[ORs] [95%CIs] between 2.9 [1.8-4.6] and 11.1 [5.8-21.2] for tumor stages between T1b and T3b and ORs [95%CIs] of 24.6 [13.6-44.4] for T4a and 29.1 [15.5-54.9] for T4b relative to T1a;P value for trend, <.001) than pigmented melanoma. Hazard of death from melanoma was higher for amelanotic than for pigmented melanoma (hazard ratio [HR], 2.0; 95%CI, 1.4-3.0)(P < .001), adjusted for

Published

2014

36. Tumor-infiltrating lymphocyte grade in primary melanomas is independently associated with melanoma-specific survival in the population-based genes, environment and melanoma study.

Author

Thomas, Nancy E, Thomas, Nancy E, Busam, Klaus J, From, Lynn, Kricker, Anne, Armstrong, Bruce K, Anton-Culver, Hoda, Gruber, Stephen B, Gallagher, Richard P, Zanetti, Roberto, Rosso, Stefano, Dwyer, Terence, Venn, Alison, Kanetsky, Peter A, Groben, Pamela A, Hao, Honglin, Orlow, Irene, Reiner, Anne S, Luo, Li, Paine, Susan, Ollila, David W, Wilcox, Homer, Begg, Colin B, Berwick, Marianne, Thomas, Nancy E, Thomas, Nancy E, Busam, Klaus J, From, Lynn, Kricker, Anne, Armstrong, Bruce K, Anton-Culver, Hoda, Gruber, Stephen B, Gallagher, Richard P, Zanetti, Roberto, Rosso, Stefano, Dwyer, Terence, Venn, Alison, Kanetsky, Peter A, Groben, Pamela A, Hao, Honglin, Orlow, Irene, Reiner, Anne S, Luo, Li, Paine, Susan, Ollila, David W, Wilcox, Homer, Begg, Colin B, and Berwick, Marianne

Abstract

PurposeAlthough most hospital-based studies suggest more favorable survival with tumor-infiltrating lymphocytes (TILs) present in primary melanomas, it is uncertain whether TILs provide prognostic information beyond existing melanoma staging definitions. We addressed the issue in an international population-based study of patients with single and multiple primary melanomas.Patients and methodsOn the basis of the Genes, Environment and Melanoma (GEM) study, we conducted follow-up of 2,845 patients diagnosed from 1998 to 2003 with 3,330 invasive primary melanomas centrally reviewed for TIL grade (absent, nonbrisk, or brisk). The odds of TIL grades associated with clinicopathologic features and survival by TIL grade were examined.ResultsIndependent predictors (P < .05) for nonbrisk TIL grade were site, histologic subtype, and Breslow thickness, and for brisk TIL grade, they were age, site, Breslow thickness, and radial growth phase. Nonbrisk and brisk TIL grades were each associated with lower American Joint Committee on Cancer (AJCC) tumor stage compared with TIL absence (P(trend) < .001). Death as a result of melanoma was 30% less with nonbrisk TIL grade (hazard ratio [HR], 0.7; 95% CI, 0.5 to 1.0) and 50% less with brisk TIL grade (HR, 0.5; 95% CI, 0.3 to 0.9) relative to TIL absence, adjusted for age, sex, site, and AJCC tumor stage.ConclusionAt the population level, higher TIL grade of primary melanoma is associated with a lower risk of death as a result of melanoma independently of tumor characteristics currently used for AJCC tumor stage. We conclude that TIL grade deserves further prospective investigation to determine whether it should be included in future AJCC staging revisions.

Published

2013

37. Tumor-infiltrating lymphocyte grade in primary melanomas is independently associated with melanoma-specific survival in the population-based genes, environment and melanoma study.

Author

Thomas, Nancy E, Thomas, Nancy E, Busam, Klaus J, From, Lynn, Kricker, Anne, Armstrong, Bruce K, Anton-Culver, Hoda, Gruber, Stephen B, Gallagher, Richard P, Zanetti, Roberto, Rosso, Stefano, Dwyer, Terence, Venn, Alison, Kanetsky, Peter A, Groben, Pamela A, Hao, Honglin, Orlow, Irene, Reiner, Anne S, Luo, Li, Paine, Susan, Ollila, David W, Wilcox, Homer, Begg, Colin B, Berwick, Marianne, Thomas, Nancy E, Thomas, Nancy E, Busam, Klaus J, From, Lynn, Kricker, Anne, Armstrong, Bruce K, Anton-Culver, Hoda, Gruber, Stephen B, Gallagher, Richard P, Zanetti, Roberto, Rosso, Stefano, Dwyer, Terence, Venn, Alison, Kanetsky, Peter A, Groben, Pamela A, Hao, Honglin, Orlow, Irene, Reiner, Anne S, Luo, Li, Paine, Susan, Ollila, David W, Wilcox, Homer, Begg, Colin B, and Berwick, Marianne

Abstract

PurposeAlthough most hospital-based studies suggest more favorable survival with tumor-infiltrating lymphocytes (TILs) present in primary melanomas, it is uncertain whether TILs provide prognostic information beyond existing melanoma staging definitions. We addressed the issue in an international population-based study of patients with single and multiple primary melanomas.Patients and methodsOn the basis of the Genes, Environment and Melanoma (GEM) study, we conducted follow-up of 2,845 patients diagnosed from 1998 to 2003 with 3,330 invasive primary melanomas centrally reviewed for TIL grade (absent, nonbrisk, or brisk). The odds of TIL grades associated with clinicopathologic features and survival by TIL grade were examined.ResultsIndependent predictors (P < .05) for nonbrisk TIL grade were site, histologic subtype, and Breslow thickness, and for brisk TIL grade, they were age, site, Breslow thickness, and radial growth phase. Nonbrisk and brisk TIL grades were each associated with lower American Joint Committee on Cancer (AJCC) tumor stage compared with TIL absence (P(trend) < .001). Death as a result of melanoma was 30% less with nonbrisk TIL grade (hazard ratio [HR], 0.7; 95% CI, 0.5 to 1.0) and 50% less with brisk TIL grade (HR, 0.5; 95% CI, 0.3 to 0.9) relative to TIL absence, adjusted for age, sex, site, and AJCC tumor stage.ConclusionAt the population level, higher TIL grade of primary melanoma is associated with a lower risk of death as a result of melanoma independently of tumor characteristics currently used for AJCC tumor stage. We conclude that TIL grade deserves further prospective investigation to determine whether it should be included in future AJCC staging revisions.

Published

2013

38. Interaction of CDKN2A and sun exposure in the etiology of melanoma in the general population.

Author

Berwick, Marianne, Berwick, Marianne, Begg, Colin B, Armstrong, Bruce K, Reiner, Anne S, Thomas, Nancy E, Cook, Linda S, Orlow, Irene, Kricker, Anne, Marrett, Loraine D, Gruber, Stephen B, Anton-Culver, Hoda, Millikan, Robert C, Gallagher, Richard P, Dwyer, Terry, Rosso, Stefano, Kanetsky, Peter A, Lee-Taylor, Julia, Berwick, Marianne, Berwick, Marianne, Begg, Colin B, Armstrong, Bruce K, Reiner, Anne S, Thomas, Nancy E, Cook, Linda S, Orlow, Irene, Kricker, Anne, Marrett, Loraine D, Gruber, Stephen B, Anton-Culver, Hoda, Millikan, Robert C, Gallagher, Richard P, Dwyer, Terry, Rosso, Stefano, Kanetsky, Peter A, and Lee-Taylor, Julia

Published

2011

39. Interaction of CDKN2A and sun exposure in the etiology of melanoma in the general population.

Author

Berwick, Marianne, Berwick, Marianne, Begg, Colin B, Armstrong, Bruce K, Reiner, Anne S, Thomas, Nancy E, Cook, Linda S, Orlow, Irene, Kricker, Anne, Marrett, Loraine D, Gruber, Stephen B, Anton-Culver, Hoda, Millikan, Robert C, Gallagher, Richard P, Dwyer, Terry, Rosso, Stefano, Kanetsky, Peter A, Lee-Taylor, Julia, Berwick, Marianne, Berwick, Marianne, Begg, Colin B, Armstrong, Bruce K, Reiner, Anne S, Thomas, Nancy E, Cook, Linda S, Orlow, Irene, Kricker, Anne, Marrett, Loraine D, Gruber, Stephen B, Anton-Culver, Hoda, Millikan, Robert C, Gallagher, Richard P, Dwyer, Terry, Rosso, Stefano, Kanetsky, Peter A, and Lee-Taylor, Julia

Published

2011

40. Reproductive factors and risk of contralateral breast cancer by BRCA1 and BRCA2 mutation status: results from the WECARE study.

Author

Poynter, Jenny N, Poynter, Jenny N, Langholz, Bryan, Largent, Joan, Mellemkjaer, Lene, Bernstein, Leslie, Malone, Kathleen E, Lynch, Charles F, Borg, Ake, Concannon, Patrick, Teraoka, Sharon N, Xue, Shanyan, Diep, Anh T, Törngren, Therese, Begg, Colin B, Capanu, Marinela, Haile, Robert W, WECARE Study Collaborative Group, Bernstein, Jonine L, Poynter, Jenny N, Poynter, Jenny N, Langholz, Bryan, Largent, Joan, Mellemkjaer, Lene, Bernstein, Leslie, Malone, Kathleen E, Lynch, Charles F, Borg, Ake, Concannon, Patrick, Teraoka, Sharon N, Xue, Shanyan, Diep, Anh T, Törngren, Therese, Begg, Colin B, Capanu, Marinela, Haile, Robert W, WECARE Study Collaborative Group, and Bernstein, Jonine L

Abstract

ObjectiveReproductive factors, such as early age at menarche, late age at menopause, and nulliparity are known risk factors for breast cancer. Previously, we reported these factors to be associated with risk of developing contralateral breast cancer (CBC). In this study, we evaluated the association between these factors and CBC risk among BRCA1 and BRCA2 (BRCA1/2) mutation carriers and non-carriers.MethodsThe WECARE Study is a population-based multi-center case-control study of 705 women with CBC (cases) and 1,397 women with unilateral breast cancer (controls). All participants were screened for BRCA1/2 mutations and 181 carriers were identified. Conditional logistic regression models were used to evaluate associations between reproductive factors and CBC for mutation carriers and non-carriers.ResultsNone of the associations between reproductive factors and CBC risk differed between mutation carriers and non-carriers. The increase in risk with younger age at menarche and decrease in risk in women with more than two full-term pregnancies seen in non-carriers were not significantly different in carriers (adjusted RRs = 1.31, 95% CI 0.65-2.65 and 0.53, 95% CI 0.19-1.51, respectively). No significant associations between the other reproductive factors and CBC risk were observed in mutation carriers or non-carriers.ConclusionFor two reproductive factors previously shown to be associated with CBC risk, we observed similar associations for BRCA1/2 carriers. This suggests that reproductive variables that affect CBC risk may have similar effects in mutation carriers and non-carriers.

Published

2010

41. Adjuvant systemic therapy for breast cancer in BRCA1/BRCA2 mutation carriers in a population-based study of risk of contralateral breast cancer.

Author

Reding, Kerryn W, Reding, Kerryn W, Bernstein, Jonine L, Langholz, Bryan M, Bernstein, Leslie, Haile, Robert W, Begg, Colin B, Lynch, Charles F, Concannon, Patrick, Borg, Ake, Teraoka, Sharon N, Törngren, Therese, Diep, Anh, Xue, Shanyan, Bertelsen, Lisbeth, Liang, Xiaolin, Reiner, Anne S, Capanu, Marinela, Malone, Kathleen E, WECARE Collaborative Study Group, Reding, Kerryn W, Reding, Kerryn W, Bernstein, Jonine L, Langholz, Bryan M, Bernstein, Leslie, Haile, Robert W, Begg, Colin B, Lynch, Charles F, Concannon, Patrick, Borg, Ake, Teraoka, Sharon N, Törngren, Therese, Diep, Anh, Xue, Shanyan, Bertelsen, Lisbeth, Liang, Xiaolin, Reiner, Anne S, Capanu, Marinela, Malone, Kathleen E, and WECARE Collaborative Study Group

Abstract

Given the greatly elevated risks of contralateral breast cancer (CBC) observed in breast cancer patients who carry mutations in BRCA1 and BRCA2, it is critical to determine the effectiveness of standard adjuvant therapies in preventing CBC in mutation carriers. The WECARE study is a matched, case-control study of 708 women with CBC as cases and 1,399 women with unilateral breast cancer (UBC) as controls, including 181 BRCA1/BRCA2 mutation carriers. Interviews and medical record reviews provided detailed information on risk factors and breast cancer therapy. All study participants were screened for BRCA1 and BRCA2 mutations using denaturing high-performance liquid chromatography (DHPLC) to detect genetic variants in the coding and flanking regions of the genes. Conditional logistic regression was used to compare the risk of CBC associated with chemotherapy and tamoxifen in BRCA1/BRCA2 mutation carriers and non-carriers. Chemotherapy was associated with lower CBC risk both in non-carriers (RR = 0.6 [95% CI: 0.5-0.7]) and carriers (RR = 0.5 [95% CI: 0.2-1.0]; P value = 0.04). Tamoxifen was associated with a reduced CBC risk in non-carriers (RR = 0.7 [95% CI: 0.6-1.0]; P value = 0.03). We observed a similar but non-significant reduction associated with tamoxifen in mutation carriers (RR = 0.7 [95% CI: 0.3-1.8]). The tests of heterogeneity comparing carriers to non-carriers did not provide evidence for a difference in the associations with chemotherapy (P value = 0.51) nor with tamoxifen (P value = 0.15). Overall, we did not observe a difference in the relative risk reduction associated with adjuvant treatment between BRCA1/BRCA2 mutation carriers and non-carriers. However, given the higher absolute CBC risk in mutation carriers, the potentially greater impact of adjuvant therapy in reducing CBC risk among mutation carriers should be considered when developing treatment plans for these patients.

Published

2010

42. Reproductive factors and risk of contralateral breast cancer by BRCA1 and BRCA2 mutation status: results from the WECARE study.

Author

Poynter, Jenny N, Poynter, Jenny N, Langholz, Bryan, Largent, Joan, Mellemkjaer, Lene, Bernstein, Leslie, Malone, Kathleen E, Lynch, Charles F, Borg, Ake, Concannon, Patrick, Teraoka, Sharon N, Xue, Shanyan, Diep, Anh T, Törngren, Therese, Begg, Colin B, Capanu, Marinela, Haile, Robert W, WECARE Study Collaborative Group, Bernstein, Jonine L, Poynter, Jenny N, Poynter, Jenny N, Langholz, Bryan, Largent, Joan, Mellemkjaer, Lene, Bernstein, Leslie, Malone, Kathleen E, Lynch, Charles F, Borg, Ake, Concannon, Patrick, Teraoka, Sharon N, Xue, Shanyan, Diep, Anh T, Törngren, Therese, Begg, Colin B, Capanu, Marinela, Haile, Robert W, WECARE Study Collaborative Group, and Bernstein, Jonine L

Abstract

ObjectiveReproductive factors, such as early age at menarche, late age at menopause, and nulliparity are known risk factors for breast cancer. Previously, we reported these factors to be associated with risk of developing contralateral breast cancer (CBC). In this study, we evaluated the association between these factors and CBC risk among BRCA1 and BRCA2 (BRCA1/2) mutation carriers and non-carriers.MethodsThe WECARE Study is a population-based multi-center case-control study of 705 women with CBC (cases) and 1,397 women with unilateral breast cancer (controls). All participants were screened for BRCA1/2 mutations and 181 carriers were identified. Conditional logistic regression models were used to evaluate associations between reproductive factors and CBC for mutation carriers and non-carriers.ResultsNone of the associations between reproductive factors and CBC risk differed between mutation carriers and non-carriers. The increase in risk with younger age at menarche and decrease in risk in women with more than two full-term pregnancies seen in non-carriers were not significantly different in carriers (adjusted RRs = 1.31, 95% CI 0.65-2.65 and 0.53, 95% CI 0.19-1.51, respectively). No significant associations between the other reproductive factors and CBC risk were observed in mutation carriers or non-carriers.ConclusionFor two reproductive factors previously shown to be associated with CBC risk, we observed similar associations for BRCA1/2 carriers. This suggests that reproductive variables that affect CBC risk may have similar effects in mutation carriers and non-carriers.

Published

2010

43. Effect of systemic adjuvant treatment on risk for contralateral breast cancer in the Women's Environment, Cancer and Radiation Epidemiology Study.

Author

Bertelsen, Lisbeth, Bertelsen, Lisbeth, Bernstein, Leslie, Olsen, Jørgen H, Mellemkjaer, Lene, Haile, Robert W, Lynch, Charles F, Malone, Kathleen E, Anton-Culver, Hoda, Christensen, Jane, Langholz, Bryan, Thomas, Duncan C, Begg, Colin B, Capanu, Marinela, Ejlertsen, Bent, Stovall, Marilyn, Boice, John D, Shore, Roy E, Women's Environment, Cancer and Radiation Epidemiology Study Collaborative Group, Bernstein, Jonine L, Bertelsen, Lisbeth, Bertelsen, Lisbeth, Bernstein, Leslie, Olsen, Jørgen H, Mellemkjaer, Lene, Haile, Robert W, Lynch, Charles F, Malone, Kathleen E, Anton-Culver, Hoda, Christensen, Jane, Langholz, Bryan, Thomas, Duncan C, Begg, Colin B, Capanu, Marinela, Ejlertsen, Bent, Stovall, Marilyn, Boice, John D, Shore, Roy E, Women's Environment, Cancer and Radiation Epidemiology Study Collaborative Group, and Bernstein, Jonine L

Abstract

BackgroundResults from randomized trials indicate that treatment with tamoxifen or chemotherapy for primary breast cancer reduces the risk for contralateral breast cancer. However, less is known about how long the risk is reduced and the impact of factors such as age and menopausal status.MethodsThe study included 634 women with contralateral breast cancer (case patients) and 1158 women with unilateral breast cancer (control subjects) from the Women's Environment, Cancer and Radiation Epidemiology Study. The women were younger than age 55 when they were first diagnosed with breast cancer during 1985-1999. Rate ratios (RRs) and 95% confidence intervals (CIs) for contralateral breast cancer after treatment with chemotherapy or tamoxifen were assessed by multivariable adjusted conditional logistic regression analyses.ResultsChemotherapy was associated with a lower risk for contralateral breast cancer (RR = 0.57, 95% CI = 0.42 to 0.75) than no chemotherapy. A statistically significant association between chemotherapy and reduced risk for contralateral breast cancer persisted up to 10 years after the first breast cancer diagnosis and was stronger among women who became postmenopausal within 1 year of the first breast cancer diagnosis (RR = 0.28, 95% CI = 0.11 to 0.76). Tamoxifen use was also associated with reduced risk for contralateral breast cancer (RR = 0.66, 95% CI = 0.50 to 0.88) compared with no use, and the association was statistically significant for 5 years after the first diagnosis.ConclusionThe associations between chemotherapy and tamoxifen treatment and reduced risk for contralateral breast cancer appear to continue for 10 and 5 years, respectively, after the initial breast cancer is diagnosed. Ovarian suppression may have a role in the association between chemotherapy and reduced risk for contralateral breast cancer.

Published

2008

44. Effect of systemic adjuvant treatment on risk for contralateral breast cancer in the Women's Environment, Cancer and Radiation Epidemiology Study.

Author

Bertelsen, Lisbeth, Bertelsen, Lisbeth, Bernstein, Leslie, Olsen, Jørgen H, Mellemkjaer, Lene, Haile, Robert W, Lynch, Charles F, Malone, Kathleen E, Anton-Culver, Hoda, Christensen, Jane, Langholz, Bryan, Thomas, Duncan C, Begg, Colin B, Capanu, Marinela, Ejlertsen, Bent, Stovall, Marilyn, Boice, John D, Shore, Roy E, Women's Environment, Cancer and Radiation Epidemiology Study Collaborative Group, Bernstein, Jonine L, Bertelsen, Lisbeth, Bertelsen, Lisbeth, Bernstein, Leslie, Olsen, Jørgen H, Mellemkjaer, Lene, Haile, Robert W, Lynch, Charles F, Malone, Kathleen E, Anton-Culver, Hoda, Christensen, Jane, Langholz, Bryan, Thomas, Duncan C, Begg, Colin B, Capanu, Marinela, Ejlertsen, Bent, Stovall, Marilyn, Boice, John D, Shore, Roy E, Women's Environment, Cancer and Radiation Epidemiology Study Collaborative Group, and Bernstein, Jonine L

Abstract

BackgroundResults from randomized trials indicate that treatment with tamoxifen or chemotherapy for primary breast cancer reduces the risk for contralateral breast cancer. However, less is known about how long the risk is reduced and the impact of factors such as age and menopausal status.MethodsThe study included 634 women with contralateral breast cancer (case patients) and 1158 women with unilateral breast cancer (control subjects) from the Women's Environment, Cancer and Radiation Epidemiology Study. The women were younger than age 55 when they were first diagnosed with breast cancer during 1985-1999. Rate ratios (RRs) and 95% confidence intervals (CIs) for contralateral breast cancer after treatment with chemotherapy or tamoxifen were assessed by multivariable adjusted conditional logistic regression analyses.ResultsChemotherapy was associated with a lower risk for contralateral breast cancer (RR = 0.57, 95% CI = 0.42 to 0.75) than no chemotherapy. A statistically significant association between chemotherapy and reduced risk for contralateral breast cancer persisted up to 10 years after the first breast cancer diagnosis and was stronger among women who became postmenopausal within 1 year of the first breast cancer diagnosis (RR = 0.28, 95% CI = 0.11 to 0.76). Tamoxifen use was also associated with reduced risk for contralateral breast cancer (RR = 0.66, 95% CI = 0.50 to 0.88) compared with no use, and the association was statistically significant for 5 years after the first diagnosis.ConclusionThe associations between chemotherapy and tamoxifen treatment and reduced risk for contralateral breast cancer appear to continue for 10 and 5 years, respectively, after the initial breast cancer is diagnosed. Ovarian suppression may have a role in the association between chemotherapy and reduced risk for contralateral breast cancer.

Published

2008

45. CDKN2A germline mutations in individuals with cutaneous malignant melanoma.

Author

Orlow, Irene, Orlow, Irene, Begg, Colin B, Cotignola, Javier, Roy, Pampa, Hummer, Amanda J, Clas, Brian A, Mujumdar, Urvi, Canchola, Rebecca, Armstrong, Bruce K, Kricker, Anne, Marrett, Loraine D, Millikan, Robert C, Gruber, Stephen B, Anton-Culver, Hoda, Zanetti, Roberto, Gallagher, Richard P, Dwyer, Terence, Rebbeck, Timothy R, Kanetsky, Peter A, Wilcox, Homer, Busam, Klaus, From, Lynn, Berwick, Marianne, GEM Study Group, Orlow, Irene, Orlow, Irene, Begg, Colin B, Cotignola, Javier, Roy, Pampa, Hummer, Amanda J, Clas, Brian A, Mujumdar, Urvi, Canchola, Rebecca, Armstrong, Bruce K, Kricker, Anne, Marrett, Loraine D, Millikan, Robert C, Gruber, Stephen B, Anton-Culver, Hoda, Zanetti, Roberto, Gallagher, Richard P, Dwyer, Terence, Rebbeck, Timothy R, Kanetsky, Peter A, Wilcox, Homer, Busam, Klaus, From, Lynn, Berwick, Marianne, and GEM Study Group

Abstract

Cyclin-dependent kinase inhibitor type 2A (CDKN2A) has been identified as a major melanoma susceptibility gene based on the presence of germline mutations in high-risk melanoma families. In this study, we sought to identify and characterize the spectrum of CDKN2A mutations affecting p16 inhibitor of cyclin-dependent kinase type 4 (INK4a) in individuals with melanoma using a population-based study design. DNA samples from 1189 individuals with incident multiple primary melanoma (MPM) and 2424 with incident single primary melanoma unselected for family history of melanoma were available for screening of CDKN2A (p16INK4a) mutations. Variants were classified for functional impact based on intragenic position, existing functional data, sequence, and structural analysis. The impact of individual mutations and functional groupings was assessed by comparing frequencies in cases of MPM versus cases with a single first primary melanoma, and by comparing the reported incidence rates in first-degree relatives. Our results show that mutations occur infrequently in these high-risk groups, and that they occur mainly in exons 1alpha and 2. Rare coding variants with putative functional impact are observed to increase substantially the risk of melanoma. With the exception of the variant in position -34 of CDKN2A of known functional consequence, the remaining rare variants in the non-coding region have no apparent impact on risk.

Published

2007

46. CDKN2A germline mutations in individuals with cutaneous malignant melanoma.

Author

Orlow, Irene, Orlow, Irene, Begg, Colin B, Cotignola, Javier, Roy, Pampa, Hummer, Amanda J, Clas, Brian A, Mujumdar, Urvi, Canchola, Rebecca, Armstrong, Bruce K, Kricker, Anne, Marrett, Loraine D, Millikan, Robert C, Gruber, Stephen B, Anton-Culver, Hoda, Zanetti, Roberto, Gallagher, Richard P, Dwyer, Terence, Rebbeck, Timothy R, Kanetsky, Peter A, Wilcox, Homer, Busam, Klaus, From, Lynn, Berwick, Marianne, GEM Study Group, Orlow, Irene, Orlow, Irene, Begg, Colin B, Cotignola, Javier, Roy, Pampa, Hummer, Amanda J, Clas, Brian A, Mujumdar, Urvi, Canchola, Rebecca, Armstrong, Bruce K, Kricker, Anne, Marrett, Loraine D, Millikan, Robert C, Gruber, Stephen B, Anton-Culver, Hoda, Zanetti, Roberto, Gallagher, Richard P, Dwyer, Terence, Rebbeck, Timothy R, Kanetsky, Peter A, Wilcox, Homer, Busam, Klaus, From, Lynn, Berwick, Marianne, and GEM Study Group

Abstract

Cyclin-dependent kinase inhibitor type 2A (CDKN2A) has been identified as a major melanoma susceptibility gene based on the presence of germline mutations in high-risk melanoma families. In this study, we sought to identify and characterize the spectrum of CDKN2A mutations affecting p16 inhibitor of cyclin-dependent kinase type 4 (INK4a) in individuals with melanoma using a population-based study design. DNA samples from 1189 individuals with incident multiple primary melanoma (MPM) and 2424 with incident single primary melanoma unselected for family history of melanoma were available for screening of CDKN2A (p16INK4a) mutations. Variants were classified for functional impact based on intragenic position, existing functional data, sequence, and structural analysis. The impact of individual mutations and functional groupings was assessed by comparing frequencies in cases of MPM versus cases with a single first primary melanoma, and by comparing the reported incidence rates in first-degree relatives. Our results show that mutations occur infrequently in these high-risk groups, and that they occur mainly in exons 1alpha and 2. Rare coding variants with putative functional impact are observed to increase substantially the risk of melanoma. With the exception of the variant in position -34 of CDKN2A of known functional consequence, the remaining rare variants in the non-coding region have no apparent impact on risk.

Published

2007

47. Mejora de la calidad de los informes de los ensayos clínicos aleatorio controlados. Recomendaciones del grupo de trabajo CONSORT

Author

Begg, Colin B., Cho, Mildred, Eastwood, Susan, Horton, Richard C., Pitkin, Roy, Rennie, Drummond, Schulz, Kenneth F., Simel, David, Stroup, Donna F., Moher, David, Olkin, Ingram, Begg, Colin B., Cho, Mildred, Eastwood, Susan, Horton, Richard C., Pitkin, Roy, Rennie, Drummond, Schulz, Kenneth F., Simel, David, Stroup, Donna F., Moher, David, and Olkin, Ingram

Abstract

This summary corresponds to the translation into Spanish of the Special Communication published in the Journal of the American Medical Association in August 1996, along with the editorial published in the same issue "How to report Randomized Controlled Trials. The Consort Statement". It describes the Consolidated Standars for Preparation of Controlled Clinical Trials, prepared by a work group made up of members of the SORT Group and of the Asilomar Work Group, along with the editor of a magazine and the author of the report on a clinical trial. The work was carried out by means of a Delphy process and the result was a check list and a process diagram. The check list is made up of 21 items that mainly refer to methods, results and discussions on the report of a controlled clinical trial, identifying the necessary information in order to be able to evaluate the internal and external value of the report, judging the improvement to be positive for the patient, the editors and the reviewers of the magazines., Este trabajo corresponde a la traducción al español de la Colaboración Especial publicada en The Journal of the American Medical Association en agosto de 1996, junto con el editorial How to report Randomized Controlled Trials. The Consort Statement, publicada en el mismo número. En ella se describe la elaboración de las Normas Consolidadas para la elaboración de los Informes de los Ensayos Clínicos Controlados, por un grupo de trabajo formado por los componentes del grupo SORT y del Grupo de Trabajo Asilomar, junto con el director de una revista y el autor del informe de un ensayo clínico. El trabajo se realizó mediante un proceso Delphi y el resultado fue una lista de comprobación (checklist) y un diagrama de flujo. La primera está compuesta por 21 puntos que se refieren principalmente a los métodos, resultados y discusión del informe de un ensayo clínico controlado, identificándose la información necesaria para poder evaluar la validez interna y externa del ensayo, valorándose la mejora como positiva, tanto para los pacientes, como para los editores de las revistas y los revisores de las mismas.

Published

1998