Early Onset Collagen Vi Myopathies: Genetic and Clinical Correlations
Göster/ Aç
Tarih
2010Yazar
Brinas, Laura
Richard, Pascale
Quijano-Roy, Susana
Gartioux, Corine
Ledeuil, Celine
Lacene, Emmanuelle
Makri, Samira
Ferreiro, Ana
Maugenre, Svetlana
Topaloglu, Haluk
Haliloglu, Goknur
Penisson-Besnier, Isabelle
Jeannet, Pierre-Yves
Merlini, Luciano
Navarro, Carmen
Toutain, Annick
Chaigne, Denys
Desguerre, Isabelle
de Die-Smulders, Christine
Dunand, Murielle
Echenne, Bernard
Eymard, Bruno
Kuntzer, Thierry
Maincent, Kim
Mayer, Michele
Plessis, Ghislaine
Rivier, Francois
Roelens, Filip
Stojkovic, Tanya
Lia Taratuto, Ana
Lubieniecki, Fabiana
Monges, Soledad
Tranchant, Christine
Viollet, Louis
Romero, Norma B.
Estournet, Brigitte
Guicheney, Pascale
Allamand, Valerie
Üst veri
Tüm öğe kaydını gösterÖzet
Objective: Mutations in the genes encoding the extracellular matrix protein collagen VI (ColVI) cause a spectrum of disorders with variable inheritance including Ullrich congenital muscular dystrophy, Bethlem myopathy, and intermediate phenotypes. We extensively characterized, at the clinical, cellular, and molecular levels, 49 patients with onset in the first 2 years of life to investigate genotype-phenotype correlations. Methods: Patients were classified into 3 groups: early-severe (18%), moderate-progressive (53%), and mild (29%). ColVI secretion was analyzed in patient-derived skin fibroblasts. Chain-specific transcript levels were quantified by quantitative reverse transcriptase polymerase chain reaction (qRT-PCR), and mutation identification was performed by sequencing of complementary DNA. Results: ColVI secretion was altered in all fibroblast cultures studied. We identified 56 mutations, mostly novel and private. Dominant de novo mutations were detected in 61% of the cases. Importantly, mutations causing premature termination codons (PTCs) or in-frame insertions strikingly destabilized the corresponding transcripts. Homozygous PTC-causing mutations in the triple helix domains led to the most severe phenotypes (ambulation never achieved), whereas dominant de novo in-frame exon skipping and glycine missense mutations were identified in patients of the moderate-progressive group (loss of ambulation). Interpretation: This work emphasizes that the diagnosis of early onset ColVI myopathies is arduous and time-consuming, and demonstrates that quantitative RT-PCR is a helpful tool for the identification of some mutation-bearing genes. Moreover, the clinical classification proposed allowed genotype-phenotype relationships to be explored, and may be useful in the design of future clinical trials. ANN NEUROL 2010;68:511-520