Genetic variants in PARP1 (rs3219090) and IRF4 (rs12203592) genes associated with melanoma susceptibility in a Spanish population

BACKGROUND: Few high penetrance genes are known in Malignant Melanoma (MM), however, the involvement of low-penetrance genes such as MC1R, OCA2, ASIP, SLC45A2 and TYR has been observed. Lately, genome-wide association studies (GWAS) have been the ideal strategy to identify new common, low-penetrance...

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Autores principales: Peña-Chilet, Maria, Blanquer-Maceiras, Maite, Ibarrola-Villava, Maider, Martinez-Cadenas, Conrado, Martin-Gonzalez, Manuel, Gomez-Fernandez, Cristina, Mayor, Matias, Aviles, Juan Antonio, Lluch, Ana, Ribas, Gloria
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2013
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3704782/
https://www.ncbi.nlm.nih.gov/pubmed/23537197
http://dx.doi.org/10.1186/1471-2407-13-160
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author Peña-Chilet, Maria
Blanquer-Maceiras, Maite
Ibarrola-Villava, Maider
Martinez-Cadenas, Conrado
Martin-Gonzalez, Manuel
Gomez-Fernandez, Cristina
Mayor, Matias
Aviles, Juan Antonio
Lluch, Ana
Ribas, Gloria
author_facet Peña-Chilet, Maria
Blanquer-Maceiras, Maite
Ibarrola-Villava, Maider
Martinez-Cadenas, Conrado
Martin-Gonzalez, Manuel
Gomez-Fernandez, Cristina
Mayor, Matias
Aviles, Juan Antonio
Lluch, Ana
Ribas, Gloria
author_sort Peña-Chilet, Maria
collection PubMed
description BACKGROUND: Few high penetrance genes are known in Malignant Melanoma (MM), however, the involvement of low-penetrance genes such as MC1R, OCA2, ASIP, SLC45A2 and TYR has been observed. Lately, genome-wide association studies (GWAS) have been the ideal strategy to identify new common, low-penetrance susceptibility loci. In this case–control study, we try to validate in our population nine melanoma associated markers selected from published GWAS in melanoma predisposition. METHODS: We genotyped the 9 markers corresponding to 8 genes (PARP1, MX2, ATM, CCND1, NADSYN1, CASP8, IRF4 and CYP2R1) in 566 cases and 347 controls from a Spanish population using KASPar probes. Genotypes were analyzed by logistic regression and adjusted by phenotypic characteristics. RESULTS: We confirm the protective role in MM of the rs3219090 located on the PARP1 gene (p-value 0.027). Additionally, this SNP was also associated with eye color (p-value 0.002). A second polymorphism, rs12203592, located on the IRF4 gene was associated with protection to develop MM for the dominant model (p-value 0.037). We have also observed an association of this SNP with both lentigines (p-value 0.014) and light eye color (p-value 3.76 × 10(-4)). Furthermore, we detected a novel association with rs1485993, located on the CCND1 gene, and dark eye color (p-value 4.96 × 10(-4)). Finally, rs1801516, located on the ATM gene, showed a trend towards a protective role in MM similar to the one firstly described in a GWAS study. CONCLUSIONS: To our knowledge, this is the first time that these SNPs have been associated with MM in a Spanish population. We confirmed the proposed role of rs3219090, located on the PARP1 gene, and rs12203592, located on the IRF4 gene, as protective to MM along the same lines as have previous genome-wide associated works. Finally, we have seen associations between IRF4, PARP1, and CCND1 and phenotypic characteristics, confirming previous results for the IRF4 gene and presenting novel data for the last two, suggesting that pigmentation characteristics correlated with eye color are potential mediators between PARP1 and MM protection.
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spelling pubmed-37047822013-07-10 Genetic variants in PARP1 (rs3219090) and IRF4 (rs12203592) genes associated with melanoma susceptibility in a Spanish population Peña-Chilet, Maria Blanquer-Maceiras, Maite Ibarrola-Villava, Maider Martinez-Cadenas, Conrado Martin-Gonzalez, Manuel Gomez-Fernandez, Cristina Mayor, Matias Aviles, Juan Antonio Lluch, Ana Ribas, Gloria BMC Cancer Research Article BACKGROUND: Few high penetrance genes are known in Malignant Melanoma (MM), however, the involvement of low-penetrance genes such as MC1R, OCA2, ASIP, SLC45A2 and TYR has been observed. Lately, genome-wide association studies (GWAS) have been the ideal strategy to identify new common, low-penetrance susceptibility loci. In this case–control study, we try to validate in our population nine melanoma associated markers selected from published GWAS in melanoma predisposition. METHODS: We genotyped the 9 markers corresponding to 8 genes (PARP1, MX2, ATM, CCND1, NADSYN1, CASP8, IRF4 and CYP2R1) in 566 cases and 347 controls from a Spanish population using KASPar probes. Genotypes were analyzed by logistic regression and adjusted by phenotypic characteristics. RESULTS: We confirm the protective role in MM of the rs3219090 located on the PARP1 gene (p-value 0.027). Additionally, this SNP was also associated with eye color (p-value 0.002). A second polymorphism, rs12203592, located on the IRF4 gene was associated with protection to develop MM for the dominant model (p-value 0.037). We have also observed an association of this SNP with both lentigines (p-value 0.014) and light eye color (p-value 3.76 × 10(-4)). Furthermore, we detected a novel association with rs1485993, located on the CCND1 gene, and dark eye color (p-value 4.96 × 10(-4)). Finally, rs1801516, located on the ATM gene, showed a trend towards a protective role in MM similar to the one firstly described in a GWAS study. CONCLUSIONS: To our knowledge, this is the first time that these SNPs have been associated with MM in a Spanish population. We confirmed the proposed role of rs3219090, located on the PARP1 gene, and rs12203592, located on the IRF4 gene, as protective to MM along the same lines as have previous genome-wide associated works. Finally, we have seen associations between IRF4, PARP1, and CCND1 and phenotypic characteristics, confirming previous results for the IRF4 gene and presenting novel data for the last two, suggesting that pigmentation characteristics correlated with eye color are potential mediators between PARP1 and MM protection. BioMed Central 2013-03-27 /pmc/articles/PMC3704782/ /pubmed/23537197 http://dx.doi.org/10.1186/1471-2407-13-160 Text en Copyright © 2013 Peña-Chilet et al.; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Peña-Chilet, Maria
Blanquer-Maceiras, Maite
Ibarrola-Villava, Maider
Martinez-Cadenas, Conrado
Martin-Gonzalez, Manuel
Gomez-Fernandez, Cristina
Mayor, Matias
Aviles, Juan Antonio
Lluch, Ana
Ribas, Gloria
Genetic variants in PARP1 (rs3219090) and IRF4 (rs12203592) genes associated with melanoma susceptibility in a Spanish population
title Genetic variants in PARP1 (rs3219090) and IRF4 (rs12203592) genes associated with melanoma susceptibility in a Spanish population
title_full Genetic variants in PARP1 (rs3219090) and IRF4 (rs12203592) genes associated with melanoma susceptibility in a Spanish population
title_fullStr Genetic variants in PARP1 (rs3219090) and IRF4 (rs12203592) genes associated with melanoma susceptibility in a Spanish population
title_full_unstemmed Genetic variants in PARP1 (rs3219090) and IRF4 (rs12203592) genes associated with melanoma susceptibility in a Spanish population
title_short Genetic variants in PARP1 (rs3219090) and IRF4 (rs12203592) genes associated with melanoma susceptibility in a Spanish population
title_sort genetic variants in parp1 (rs3219090) and irf4 (rs12203592) genes associated with melanoma susceptibility in a spanish population
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3704782/
https://www.ncbi.nlm.nih.gov/pubmed/23537197
http://dx.doi.org/10.1186/1471-2407-13-160
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