A genome-wide association study identifies multiple loci for variation in human ear morphology
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Adhikari, Kaustubh
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Reales, Guillermo
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Smith, Andrew J.P.
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Konka, Esra
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Palmen, Jutta
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Quinto Sánchez, Mirsha
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Acuña Alonzo, Víctor
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Jaramillo, Claudia
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Arias, William
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Fuentes, Macarena
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Pizarro, María
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Barquera Lozano, Rodrigo
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Macín Pérez, Gastón
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Gómez Valdés, Jorge
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Villamil Ramírez, Hugo
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Hunemeier, Tábita
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Ramallo, Virginia
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Silva de Cerqueira, Caio C.
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Hurtado, Malena
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Villegas, Valeria
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Granja, Vanessa
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Gallo, Carla
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Poletti, Giovanni
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Schuler Faccini, Lavinia
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Salzano, Francisco M.
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Bortolini, Maria Cátira
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Canizales Quinteros, Samuel
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Rothhammer Engel, Francisco
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Bedoya, Gabriel
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Calderón, Rosario
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Rosique, Javier
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Cheeseman, Michael
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Bhutta, Mahmood F.
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Humphries, Steve E.
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González José, Rolando
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Headon, Denis
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Balding, David
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Ruiz Linares, Andrés
Admission date
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2015-09-23T12:37:12Z
Available date
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2015-09-23T12:37:12Z
Publication date
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2015
Cita de ítem
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Nature Communications. Volumen: 6 Número de artículo: 7500 Jun 2015
en_US
Identifier
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DOI: 10.1038/ncomms8500
Identifier
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https://repositorio.uchile.cl/handle/2250/133776
General note
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Artículo de publicación ISI
en_US
Abstract
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Here we report a genome-wide association study for non-pathological pinna morphology in over 5,000 Latin Americans. We find genome-wide significant association at seven genomic regions affecting: lobe size and attachment, folding of antihelix, helix rolling, ear protrusion and antitragus size (linear regression P values 2 x 10(-8) to 3 x 10(-14)). Four traits are associated with a functional variant in the Ectodysplasin A receptor (EDAR) gene, a key regulator of embryonic skin appendage development. We confirm expression of Edar in the developing mouse ear and that Edar-deficient mice have an abnormally shaped pinna. Two traits are associated with SNPs in a region overlapping the T-Box Protein 15 (TBX15) gene, a major determinant of mouse skeletal development. Strongest association in this region is observed for SNP rs17023457 located in an evolutionarily conserved binding site for the transcription factor Cartilage paired-class homeoprotein 1 (CART1), and we confirm that rs17023457 alters in vitro binding of CART1.