Improving the diagnosis of cobalamin and related defects by genomic analysis, plus functional and structural assessment of novel variants

Sandra Brasil,Fátima Leal,Ana I. Vega,Rosa Navarrete,María Jesús Ecay,Lourdes R. Desviat,Casandra Riera,Natàlia Padilla,Xavier de la Cruz,Mari Luz Couce,Elena Martín-Hernández,A. Moráis,Consuelo Pedrón,Luis Peña-Quintana,Miriam Rigoldi,Norma Specola,Isabel Tavares de Almeida,Inmaculada Vives,Raquel Yahyaoui,Pilar Rodríguez-Pombo,Magdalena Ugarte,Celia Pérez-Cerdá,Begoña Merinero,Belén Pérez

Improving the diagnosis of cobalamin and related defects by genomic analysis, plus functional and structural assessment of novel variants

2018

Background Cellular cobalamin defects are a locus and allelic heterogeneous disorder. The gold standard for coming to genetic diagnoses of cobalamin defects has for some time been gene-by-gene Sanger sequencing of individual DNA fragments. Enzymatic and cellular methods are employed before such sequencing to help in the selection of the gene defects to be sought, but this is time-consuming and laborious. Furthermore some cases remain undiagnosed because no biochemical methods have been available to test for cobalamin absorption and transport defects.

Keywords:

Cobalamin
Genetics
Biology
Massive parallel sequencing
DNA
Gene
Locus (genetics)
Human genetics
Sanger sequencing
Allele
Exome

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