| Literature DB >> 28685322 |
Valérie Biancalana1,2,3,4,5, Sophie Scheidecker6, Marguerite Miguet6, Annie Laquerrière7, Norma B Romero8,9, Tanya Stojkovic9, Osorio Abath Neto10, Sandra Mercier11,12,13, Nicol Voermans14, Laura Tanner15, Curtis Rogers16, Elisabeth Ollagnon-Roman17, Helen Roper18, Célia Boutte19, Shay Ben-Shachar20, Xavière Lornage21,22,23,24, Nasim Vasli21,22,23,24, Elise Schaefer25, Pascal Laforet26, Jean Pouget27, Alexandre Moerman28, Laurent Pasquier29, Pascale Marcorelle30,31, Armelle Magot13, Benno Küsters32, Nathalie Streichenberger33, Christine Tranchant34, Nicolas Dondaine6, Raphael Schneider21,22,23,24,35, Claire Gasnier6, Nadège Calmels6, Valérie Kremer36, Karine Nguyen37, Julie Perrier13, Erik Jan Kamsteeg38, Pierre Carlier39, Robert-Yves Carlier40, Julie Thompson35, Anne Boland41, Jean-François Deleuze41, Michel Fardeau8,9, Edmar Zanoteli10, Bruno Eymard26, Jocelyn Laporte21,22,23,24.
Abstract
X-linked myotubular myopathy (XLMTM), a severe congenital myopathy, is caused by mutations in the MTM1 gene located on the X chromosome. A majority of affected males die in the early postnatal period, whereas female carriers are believed to be usually asymptomatic. Nevertheless, several affected females have been reported. To assess the phenotypic and pathological spectra of carrier females and to delineate diagnostic clues, we characterized 17 new unrelated affected females and performed a detailed comparison with previously reported cases at the clinical, muscle imaging, histological, ultrastructural and molecular levels. Taken together, the analysis of this large cohort of 43 cases highlights a wide spectrum of clinical severity ranging from severe neonatal and generalized weakness, similar to XLMTM male, to milder adult forms. Several females show a decline in respiratory function. Asymmetric weakness is a noteworthy frequent specific feature potentially correlated to an increased prevalence of highly skewed X inactivation. Asymmetry of growth was also noted. Other diagnostic clues include facial weakness, ptosis and ophthalmoplegia, skeletal and joint abnormalities, and histopathological signs that are hallmarks of centronuclear myopathy such as centralized nuclei and necklace fibers. The histopathological findings also demonstrate a general disorganization of muscle structure in addition to these specific hallmarks. Thus, MTM1 mutations in carrier females define a specific myopathy, which may be independent of the presence of an XLMTM male in the family. As several of the reported affected females carry large heterozygous MTM1 deletions not detectable by Sanger sequencing, and as milder phenotypes present as adult-onset limb-girdle myopathy, the prevalence of this myopathy is likely to be greatly underestimated. This report should aid diagnosis and thus the clinical management and genetic counseling of MTM1 carrier females. Furthermore, the clinical and pathological history of this cohort may be useful for therapeutic projects in males with XLMTM, as it illustrates the spectrum of possible evolution of the disease in patients surviving long term.Entities:
Keywords: Centronuclear myopathy; Congenital myopathy; MTM1; X inactivation; X-linked myotubular myopathy
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Year: 2017 PMID: 28685322 DOI: 10.1007/s00401-017-1748-0
Source DB: PubMed Journal: Acta Neuropathol ISSN: 0001-6322 Impact factor: 17.088