Your browser doesn't support javascript.
loading
Natural history of Charcot-Marie-Tooth disease type 2A: a large international multicentre study.
Pipis, Menelaos; Feely, Shawna M E; Polke, James M; Skorupinska, Mariola; Perez, Laura; Shy, Rosemary R; Laura, Matilde; Morrow, Jasper M; Moroni, Isabella; Pisciotta, Chiara; Taroni, Franco; Vujovic, Dragan; Lloyd, Thomas E; Acsadi, Gyula; Yum, Sabrina W; Lewis, Richard A; Finkel, Richard S; Herrmann, David N; Day, John W; Li, Jun; Saporta, Mario; Sadjadi, Reza; Walk, David; Burns, Joshua; Muntoni, Francesco; Ramchandren, Sindhu; Horvath, Rita; Johnson, Nicholas E; Züchner, Stephan; Pareyson, Davide; Scherer, Steven S; Rossor, Alexander M; Shy, Michael E; Reilly, Mary M.
Afiliación
  • Pipis M; MRC Centre for Neuromuscular Diseases, UCL Queen Square Institute of Neurology, London, UK.
  • Feely SME; Department of Neurology, Carver College of Medicine, University of Iowa, Iowa City, Iowa, USA.
  • Polke JM; MRC Centre for Neuromuscular Diseases, UCL Queen Square Institute of Neurology, London, UK.
  • Skorupinska M; MRC Centre for Neuromuscular Diseases, UCL Queen Square Institute of Neurology, London, UK.
  • Perez L; Department of Neurology, Carver College of Medicine, University of Iowa, Iowa City, Iowa, USA.
  • Shy RR; Department of Neurology, Carver College of Medicine, University of Iowa, Iowa City, Iowa, USA.
  • Laura M; MRC Centre for Neuromuscular Diseases, UCL Queen Square Institute of Neurology, London, UK.
  • Morrow JM; MRC Centre for Neuromuscular Diseases, UCL Queen Square Institute of Neurology, London, UK.
  • Moroni I; Department of Pediatric Neurosciences, Fondazione IRCCS Istituto Neurologico Carlo Besta, Milan, Italy.
  • Pisciotta C; Unit of Rare Neurodegenerative and Neurometabolic Diseases, Department of Clinical Neurosciences, Fondazione IRCCS Istituto Neurologico Carlo Besta, Milan, Italy.
  • Taroni F; Unit of Medical Genetics and Neurogenetics, Department of Diagnostics and Technology, Fondazione IRCCS Istituto Neurologico Carlo Besta, Milan, Italy.
  • Vujovic D; Department of Neurology, The Perelman School of Medicine at the University of Pennsylvania, Philadelphia, PA, USA.
  • Lloyd TE; Department of Neurology, The Johns Hopkins University School of Medicine, Baltimore, Maryland, USA.
  • Acsadi G; Connecticut Children's Medical Center, Hartford, CT, USA.
  • Yum SW; The Children's Hospital of Philadelphia, and Perelman School of Medicine at the University of Pennsylvania, Philadelphia, PA, USA.
  • Lewis RA; Department of Neurology, Cedars-Sinai Medical Center, Los Angeles, CA, USA.
  • Finkel RS; Center for Experimental Neurotherapeutics, St. Jude Children's Research Hospital, Memphis, TN, USA.
  • Herrmann DN; Department of Neurology, University of Rochester, Rochester, NY, USA.
  • Day JW; Department of Neurology, Stanford Health Care, Stanford, CA, USA.
  • Li J; Department of Neurology, Wayne State University School of Medicine, Detroit, MI, USA.
  • Saporta M; Department of Neurology, University of Miami Miller School of Medicine, Miami, Florida, USA.
  • Sadjadi R; Massachusetts General Hospital, Boston, Massachusetts, USA.
  • Walk D; Department of Neurology, University of Minnesota, Minneapolis, Minnesota, USA.
  • Burns J; University of Sydney School of Health Sciences and Children's Hospital at Westmead, Sydney, Australia.
  • Muntoni F; Dubowitz Neuromuscular Centre, NIHR Biomedical Research Centre at UCL Great Ormond Street Institute of Child Health and Great Ormond Street Hospital, London, UK.
  • Ramchandren S; PRA Health Services, Raleigh, NC, USA.
  • Horvath R; Department of Clinical Neurosciences, University of Cambridge, Cambridge Biomedical Campus, Cambridge, UK.
  • Johnson NE; Virginia Commonwealth University, Richmond, VA, USA.
  • Züchner S; Dr. John T. Macdonald Foundation Department of Human Genetics and John P. Hussman Institute for Human Genomics, University of Miami Miller School of Medicine, Miami, FL, USA.
  • Pareyson D; Unit of Rare Neurodegenerative and Neurometabolic Diseases, Department of Clinical Neurosciences, Fondazione IRCCS Istituto Neurologico Carlo Besta, Milan, Italy.
  • Scherer SS; Department of Neurology, The Perelman School of Medicine at the University of Pennsylvania, Philadelphia, PA, USA.
  • Rossor AM; MRC Centre for Neuromuscular Diseases, UCL Queen Square Institute of Neurology, London, UK.
  • Shy ME; Department of Neurology, Carver College of Medicine, University of Iowa, Iowa City, Iowa, USA.
  • Reilly MM; MRC Centre for Neuromuscular Diseases, UCL Queen Square Institute of Neurology, London, UK.
Brain ; 143(12): 3589-3602, 2020 12 01.
Article en En | MEDLINE | ID: mdl-33415332
ABSTRACT
Mitofusin-2 (MFN2) is one of two ubiquitously expressed homologous proteins in eukaryote cells, playing a critical role in mitochondrial fusion. Mutations in MFN2 (most commonly autosomal dominant) cause Charcot-Marie-Tooth disease type 2A (CMT2A), the commonest axonal form of CMT, with significant allelic heterogeneity. Previous, moderately-sized, cross sectional genotype-phenotype studies of CMT2A have described the phenotypic spectrum of the disease, but longitudinal natural history studies are lacking. In this large multicentre prospective cohort study of 196 patients with dominant and autosomal recessive CMT2A, we present an in-depth genotype-phenotype study of the baseline characteristics of patients with CMT2A and longitudinal data (1-2 years) to describe the natural history. A childhood onset of autosomal dominant CMT2A is the most predictive marker of significant disease severity and is independent of the disease duration. When compared to adult onset autosomal dominant CMT2A, it is associated with significantly higher rates of use of ankle-foot orthoses, full-time use of wheelchair, dexterity difficulties and also has significantly higher CMT Examination Score (CMTESv2) and CMT Neuropathy Score (CMTNSv2) at initial assessment. Analysis of longitudinal data using the CMTESv2 and its Rasch-weighted counterpart, CMTESv2-R, show that over 1 year, the CMTESv2 increases significantly in autosomal dominant CMT2A (mean change 0.84 ± 2.42; two-tailed paired t-test P = 0.039). Furthermore, over 2 years both the CMTESv2 (mean change 0.97 ± 1.77; two-tailed paired t-test P = 0.003) and the CMTESv2-R (mean change 1.21 ± 2.52; two-tailed paired t-test P = 0.009) increase significantly with respective standardized response means of 0.55 and 0.48. In the paediatric CMT2A population (autosomal dominant and autosomal recessive CMT2A grouped together), the CMT Pediatric Scale increases significantly both over 1 year (mean change 2.24 ± 3.09; two-tailed paired t-test P = 0.009) and over 2 years (mean change 4.00 ± 3.79; two-tailed paired t-test P = 0.031) with respective standardized response means of 0.72 and 1.06. This cross-sectional and longitudinal study of the largest CMT2A cohort reported to date provides guidance for variant interpretation, informs prognosis and also provides natural history data that will guide clinical trial design.
Asunto(s)
Palabras clave
Texto completo
Imprimir
XML
PubMed Links
Buscar en Google

Texto completo: 1 Colección: 01-internacional Banco de datos: MEDLINE Asunto principal: Enfermedad de Charcot-Marie-Tooth Tipo de estudio: Clinical_trials / Etiology_studies / Guideline / Incidence_studies / Observational_studies / Prognostic_studies / Risk_factors_studies Límite: Adolescent / Adult / Child / Child, preschool / Female / Humans / Infant / Male Idioma: En Revista: Brain Año: 2020 Tipo del documento: Article País de afiliación: Reino Unido
Texto completo
Imprimir
XML
PubMed Links
Buscar en Google

Texto completo: 1 Colección: 01-internacional Banco de datos: MEDLINE Asunto principal: Enfermedad de Charcot-Marie-Tooth Tipo de estudio: Clinical_trials / Etiology_studies / Guideline / Incidence_studies / Observational_studies / Prognostic_studies / Risk_factors_studies Límite: Adolescent / Adult / Child / Child, preschool / Female / Humans / Infant / Male Idioma: En Revista: Brain Año: 2020 Tipo del documento: Article País de afiliación: Reino Unido