| Literature DB >> 26841830 |
Jorge Oliveira1,2, Ana Gonçalves1,2, Ricardo Taipa3, Manuel Melo-Pires3, Márcia E Oliveira1,2, José Luís Costa4,5, José Carlos Machado4,5, Elmira Medeiros6, Teresa Coelho7, Manuela Santos8, Rosário Santos1,2,9, Mário Sousa2,10,11.
Abstract
Congenital myopathies (CMs) are a heterogeneous group of muscle diseases characterized by hypotonia, delayed motor skills and muscle weakness with onset during the first years of life. The diagnostic workup of CM is highly dependent on the interpretation of the muscle histology, where typical pathognomonic findings are suggestive of a CM but are not necessarily gene specific. Over 20 loci have been linked to these myopathies, including three exceptionally large genes (TTN, NEB and RYR1), which are a challenge for molecular diagnosis. We developed a new approach using massive parallel sequencing (MPS) technology to simultaneously analyze 20 genes linked to CMs. Assay design was based on the Ion AmpliSeq strategy and sequencing runs were performed on an Ion PGM system. A total of 12 patients were analyzed in this study. Among the 2534 variants detected, 14 pathogenic mutations were successfully identified in the DNM2, NEB, RYR1, SEPN1 and TTN genes. Most of these had not been documented and/or fully characterized, hereby contributing to expand the CM mutational spectrum. The utility of this approach was demonstrated by the identification of mutations in 70% of the patients included in this study, which is relevant for CMs especially considering its wide phenotypic and genetic heterogeneity.Entities:
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Year: 2016 PMID: 26841830 DOI: 10.1038/jhg.2016.2
Source DB: PubMed Journal: J Hum Genet ISSN: 1434-5161 Impact factor: 3.172