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Whole-Exome Sequencing Enables Rapid Determination of Xeroderma Pigmentosum Molecular Etiology

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Ortega-Recalde, Oscar-Javier
Ine´s Vergara, Jéssica
Fonseca Mendoza, Dora Janeth
Ríos, Xiomara
Mosquera, Hernando
Bermúdez, Olga
Medina, Claudia Liliana
Vargas, Clara
Pallares, Argemiro Enrique
Restrepo Fernández, Carlos Martín

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Fecha
2013

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Universidad del Rosario

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Resumen
Abstract
Xeroderma pigmentosum (XP) is a rare autosomal recessive disorder haracterized by extreme sensitivity to actinic pigmentation changes in the skin and increased incidence of skin cancer. In some cases, patients are affected by neurological alterations. XP is caused by mutations in 8 distinct genes (XPA through XPG and XPV). The XP-V (variant) subtype of the disease results from mutations in a gene (XPV, also named POLH) which encodes for Polg, a member of the Y-DNA polymerase family. Although the presence and severity of skin and neurological dysfunctions differ between XP subtypes, there are overlapping clinical features among subtypes such that the sub-type cannot be deduced from the clinical features. In this study, in order to overcome this drawback, we undertook whole-exome sequencing in two XP sibs and their father. We identified a novel homozygous nonsense mutation (c.897T.G, p.Y299X) in POLH which causes the disease. Our results demonstrate that next generation sequencing is a powerful approach to rapid determination of XP genetic etiology.
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Unidad de Genética , Universidad Autonoma de Bucaramanga , Genética Molecular de Colombia , Escuela de Medicina y Ciencias de la Salud , Departamento de Dermatologia , Universidad Industrial de Santander , Departamento de Biología Molecular
Keywords
Clınica Carlos Ardila Lulle , Dermatology Unit , Molecular Genetics of Colombia , Dermatology Department , Department of Molecular Biology
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