A Genome-Wide Association Study Identifies the Skin Color Genes IRF4, MC1R, ASIP, and BNC2 Influencing Facial Pigmented Spots

Jacobs, Leonie C.; Hamer, Merel A.; Gunn, David A.; Deelen, Joris; Lall, Jaspal S.; Heemst, Diana van; Uh, Hae‐Won; Hofman, Albert; Uitterlinden, André G.; Griffiths, C.E.M.; Beekman, Marian; Slagboom, P. Eline; Kayser, Manfred; Liu, Fan; Nijsten, Tamar

doi:10.1038/jid.2015.62

Cited by 118 publications

(163 citation statements)

References 55 publications

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“…In the analysis of skin cancer, variants in or near IRF4 (MIM: 601900), MC1R (MIM: 155555), RALY (MIM: 614663), and SLC45A2 (MIM: 606202) were significant at a ¼ 5 3 10 À8 , and all four of these genes were previously identified as associated with pigmentation traits and skin cancers. [31][32][33][34][35][36] In the other traits, variants in TCF7L2 (MIM:…”

Section: Analysis Of Mgi Datamentioning

confidence: 99%

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A Fast and Accurate Algorithm to Test for Binary Phenotypes and Its Application to PheWAS

Dey

Schmidt

Abecasis

et al. 2017

The American Journal of Human Genetics

128

113

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The availability of electronic health record (EHR)-based phenotypes allows for genome-wide association analyses in thousands of traits and has great potential to enable identification of genetic variants associated with clinical phenotypes. We can interpret the phenomewide association study (PheWAS) result for a single genetic variant by observing its association across a landscape of phenotypes. Because a PheWAS can test thousands of binary phenotypes, and most of them have unbalanced or often extremely unbalanced case-control ratios (1:10 or 1:600, respectively), existing methods cannot provide an accurate and scalable way to test for associations. Here, we propose a computationally fast score-test-based method that estimates the distribution of the test statistic by using the saddlepoint approximation. Our method is much ($100 times) faster than the state-of-the-art Firth's test. It can also adjust for covariates and control type I error rates even when the case-control ratio is extremely unbalanced. Through application to PheWAS data from the Michigan Genomics Initiative, we show that the proposed method can control type I error rates while replicating previously known association signals even for traits with a very small number of cases and a large number of controls.

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Section: Analysis Of Mgi Datamentioning

confidence: 99%

“…Zhang et al 31 Sulem et al, 32 Jacobs et al, 33 and Liu et al 34 5:33951693 rs16891982 SLC45A2 C>G 0.038 7 3 10…”

Section: à13mentioning

confidence: 99%

A Fast and Accurate Algorithm to Test for Binary Phenotypes and Its Application to PheWAS

Dey

Schmidt

Abecasis

et al. 2017

The American Journal of Human Genetics

128

113

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“…Loss-of-function MC1R alleles has been associated with the presence of solar lentigines, suggesting that melanocytes with reduced MC1R activity are expected to form these benign hyperpigmented lesions (37,97). Genetic variants in the SLC45A2 gene have also been found to be implicated in solar lentigines development (98), although this correlation was not found in a GWAS study using Caucasian individuals (30). This high-powered GWAS study demonstrated significant associations between variants in four pigmentation-related genes (IRF4, MC1R, ASIP and BNC2) and facial pigmented spots, including solar lentigines among others (30).…”

Section: Lentiginesmentioning

confidence: 99%

“…Furthermore, Jacobs and cols. (2015) showed that females presented a much higher prevalence of facial sun spots than males, suggesting that females are more severely affected by sun exposure than males independently of genotype (30). These differences could be the result of socio-cultural reasons, as males tend to spend more time outdoors; physiological reasons, as males have thicker skin and increased number of blood vessels; differential tanning, as no sex difference in basal skin pigmentation has been shown; and hormonal factors, as oestrogens stimulate pigmentation while androgens have an inhibitory effect on melanocytes (61,87).…”

Section: Letter To the Editormentioning

confidence: 99%

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The genetic basis of sunlight sensitivity and melanoma-risk pigmentation phenotypes: The role of sex-specific genetic effects, 3' untranslated regions and melanoma susceptibility genes

Fuster¹

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AGRADECIMIENTOSAntes de presentar este trabajo, es momento de agradecer el respaldo de todas aquellas personas que han hecho posible que hoy sea una finisher de esta carrera de larga distancia que es hacer una tesis doctoral.Mis primeras líneas de agradecimiento son para mi director, Conrado Martínez-Cadenas, y co-directora de tesis, Gloria Ribas; quienes con su dedicación, experiencia y profesionalidad me han guiado de manera excepcional durante las diferentes fases de este trabajo, tanto en el proceso puramente experimental como en el análisis, interpretación y presentación de los datos. A Conrado, gracias por darme la oportunidad de realizar la tesis en su grupo de investigación, además de por su apoyo personal, confianza, cercanía y dedicación. Gracias por mover cielo y tierra porque esto fuera posible. A Gloria, gracias por abrirme las puertas de su laboratorio y, sobre todo, por sus excepcionales consejos que, no sólo me han ayudado a desarrollar esta tesis, sino que también han permitido la publicación de los resultados obtenidos.Gracias a Maider Ibarrola-Villava y Maria Peña-Chilet, miembros del grupo de investigación del Departamento de Oncología del INCLIVA, por acompañarme en este largo camino, por su valiosa aportación y su gran compañerismo.Gracias a Zalfa Abdel-Malek por acogerme en su laboratorio y darme la oportunidad de participar en un ambicioso proyecto que ha enriquecido sustancialmente mi carrera investigadora. Gracias por su exigencia y crítica constructiva, pero también por su cariño durante mi estancia. Mención especial a Vicky Sope y Renny Starner por su incalculable ayuda, paciencia y amistad. Gracias de corazón por dejarme empapar de vuestra profesionalidad.Gracias a todo el personal de la Unidad Predepartamental de Medicina de la Universitat Jaume I de Castellón, por el buen humor y compañerismo demostrado. Mención especial para mis compañeros de batalla en el laboratorio. Gracias por esas largas conversaciones y hacerme sentir afortunada por compartir mi trabajo diario con vosotros. Gracias por todo lo compartido.Gracias también a todas esas personas anónimas que voluntariamente han donado una muestra, y al personal médico de los diferentes hospitales encargados de recoger dichas muestras, ya que sin su contribución este trabajo no habría existido.Finalmente, es necesario expresar mi mayor gratitud a todas esas personas que indirectamente también han sido partícipes de este trabajo. A mi familia, por creer en mí.A mi padre, por enseñarme el valor del esfuerzo, el trabajo duro y la disciplina. A mi madre, por enseñarme a tener paciencia. A mi hermana, por ser mi mejor amiga y consejera, especialmente en la estadística y el uso del R. A Manoli, porque todo lo vivido juntas es lo que me ha hecho ser lo que soy. A mi grupo de entrenamiento, por ayudarme a evadirme de todo en los momentos que más lo necesitaba. A Iván, por estar siempre a mi lado. Por no dejarme caer. Por saber cómo hacer que confiara en mi misma. Por hacerme ver que soy una privilegiada hasta en los momentos menos buenos...

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Benign Melanocytic Proliferations and Melanocytic Naevi

Stefanaki,

Sgouros,

Stratigos

2024

Rook's Textbook of Dermatology

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Benign cutaneous melanocytic proliferations are by far the most common neoplasms in humans. Although benign, they often concern the patient due to aesthetic reasons or their association with other medical conditions. For dermatologists, melanocytic naevi are generally considered risk factors and occasionally simulants of melanoma, posing significant diagnostic and management issues in clinical practice. This chapter describes in a comprehensive way the spectrum of benign melanocytic lesions, their divergent clinical presentation and dermoscopic features, the underlying pathogenetic pathways, their histological features, their association with other diseases – particularly melanoma – and their current management.

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A Genome-Wide Association Study Identifies the Skin Color Genes IRF4, MC1R, ASIP, and BNC2 Influencing Facial Pigmented Spots

Cited by 118 publications

References 55 publications

A Fast and Accurate Algorithm to Test for Binary Phenotypes and Its Application to PheWAS

A Fast and Accurate Algorithm to Test for Binary Phenotypes and Its Application to PheWAS

The genetic basis of sunlight sensitivity and melanoma-risk pigmentation phenotypes: The role of sex-specific genetic effects, 3' untranslated regions and melanoma susceptibility genes

Benign Melanocytic Proliferations and Melanocytic Naevi

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