| Literature DB >> 29792937 |
Reda Zenagui1, Delphine Lacourt1, Henri Pegeot1, Kevin Yauy1, Raul Juntas Morales2, Corine Theze1, François Rivier3, Claude Cances4, Guilhem Sole5, Dimitri Renard6, Ulrike Walther-Louvier7, Xavier Ferrer-Monasterio5, Caroline Espil8, Marie-Christine Arné-Bes9, Pascal Cintas9, Emmanuelle Uro-Coste10, Marie-Laure Martin Negrier11, Valérie Rigau12, Eric Bieth13, Cyril Goizet14, Mireille Claustres15, Michel Koenig16, Mireille Cossée17.
Abstract
Myopathies and muscular dystrophies (M-MDs) are genetically heterogeneous diseases, with >100 identified genes, including the giant and complex titin (TTN) and nebulin (NEB) genes. Next-generation sequencing technology revolutionized M-MD diagnosis and revealed high frequency of TTN and NEB variants. We developed a next-generation sequencing diagnostic strategy targeted to the coding sequences of 135 M-MD genes. Comparison of two targeted capture technologies (SeqCap EZ Choice library capture kit and Nextera Rapid Capture Custom Enrichment kit) and of two whole-exome sequencing kits (SureSelect V5 and TruSeq RapidExome capture) revealed best coverage with the SeqCap EZ Choice protocol. A marked decrease in coverage was observed with the other kits, affecting mostly the first exons of genes and the repeated regions of TTN and NEB. Bioinformatics analysis strategy was fine-tuned to achieve optimal detection of variants, including small insertions/deletions (INDELs) and copy number variants (CNVs). Analysis of a cohort of 128 patients allowed the detection of 52 substitutions, 13 INDELs (including a trinucleotide repeat expansion), and 3 CNVs. Two INDELs were localized in the repeated regions of NEB, suggesting that these mutations may be frequent but underestimated. A large deletion was also identified in TTN that is, to our knowledge, the first published CNV in this gene.Entities:
Mesh:
Substances:
Year: 2018 PMID: 29792937 DOI: 10.1016/j.jmoldx.2018.04.001
Source DB: PubMed Journal: J Mol Diagn ISSN: 1525-1578 Impact factor: 5.568