Oculopharyngodistal myopathy is a distinct entity
Clinical and genetic features of 47 patients
- H. Durmus, MD,
- S.H. Laval, DPhil,
- F. Deymeer, MD,
- Y. Parman, MD,
- E. Kiyan, MD,
- M. Gokyigiti, MD,
- C. Ertekin, MD,
- I. Ercan, MD,
- S. Solakoglu, MD,
- V. Karcagi, PhD,
- V. Straub, MD,
- K. Bushby, MD,
- H. Lochmüller, MD and
- P. Serdaroglu-Oflazer, MD
- From the Departments of Neurology (H.D., F.D., Y.P., P.S.-O.), Pneumology (E.K.), and Histology and Embryology (S.S.), Istanbul University, Faculty of Medicine, Istanbul, Turkey; Institute of Human Genetics (S.H.L., V.S., K.B., H.L.), Newcastle University, Newcastle upon Tyne, UK; Sisli Etfal Research and Training Hospital (M.G., I.E.), Istanbul; Department of Neurology (C.E.), Ege University Medical Faculty, Izmir, Turkey; and Department of Molecular Genetics and Diagnostics (V.K.), NIEH, Budapest, Hungary.
- Address correspondence and reprint requests to Prof. Dr. Piraye Serdaroglu-Oflazer, Department of Neurology, Istanbul University, Istanbul Faculty of Medicine, 34390, Capa, Istanbul, Turkey pirayes{at}istanbul.edu.tr
Abstract
Background: Oculopharyngodistal myopathy (OPDM) has been reported as a rare, adult-onset hereditary muscle disease with putative autosomal dominant and autosomal recessive inheritance. Patients with OPDM present with progressive ocular, pharyngeal, and distal limb muscle involvement. The genetic defect causing OPDM has not been elucidated.
Methods: Clinical and genetic findings of 47 patients from 9 unrelated Turkish families diagnosed with OPDM at the Department of Neurology, Istanbul Faculty of Medicine, between 1982 and 2009 were evaluated.
Results: The mean age at onset was around 22 years. Both autosomal dominant and autosomal recessive traits were observed, without any clear difference in clinical phenotype or severity. The most common initial symptom was ptosis, followed by oropharyngeal symptoms and distal weakness, which started after the fifth disease year. Intrafamilial variability of disease phenotype and severity was notable in the largest autosomal dominant family. Atypical presentations, such as absence of limb weakness in long-term follow-up in 9, proximal predominant weakness in 4, and asymmetric ptosis in 3 patients, were observed. Swallowing difficulty was due to oropharyngeal dysphagia with myopathic origin. Serum creatine kinase levels were slightly increased and EMG revealed myopathic pattern with occasional myotonic discharges. Myopathologic findings included rimmed and autophagic vacuoles and chronic myopathic changes. Importantly, a considerable proportion of patients developed respiratory muscle weakness while still ambulant. Linkage to the genetic loci for all known muscular dystrophies, and for distal and myofibrillar myopathies, was excluded in the largest autosomal dominant and autosomal recessive OPDM families.
Conclusions: We suggest that OPDM is a clinically and genetically distinct myopathy.
Footnotes
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Study funding: Supported by the American Academy of Neurology through an International Scholarship Award to H.D., the European Neurological Society (ENS) through a fellowship to H.D., Science City Newcastle, the Medical Research Council (MRC) through the Centre for Neuromuscular Diseases, and the Association Francaise contes les Myopathies (AFM, France). Newcastle University is the coordinating partner of the TREAT-NMD network of excellence (EC 036825).
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- CP
- cricopharyngeal
- FEV1
- forced expiratory volume in 1 second
- FSHD
- facioscapulohumeral dystrophy
- FVC
- forced vital capacity
- NCV
- nerve conduction study
- OPDM
- oculopharyngodistal myopathy
- OPMD
- oculopharyngeal muscular dystrophy
- TA
- thyroarytenoid
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Supplemental data at www.neurology.org
- Received April 19, 2010.
- Accepted September 17, 2010.
- Copyright © 2011 by AAN Enterprises, Inc.
