Clinical predominance of proximal upper limb weakness in CMT1A syndrome
Autor: | Klaus Wagner, Michaela Auer-Grumbach, Wolfgang Löscher, Hans-Peter Hartung, S. Strasser-Fuchs, Michael M. Millner, Franz Fazekas |
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Rok vydání: | 2000 |
Předmět: |
Proximal muscle weakness
Physiology business.industry Motor nerve Anatomy medicine.disease Nerve conduction velocity Cellular and Molecular Neuroscience medicine.anatomical_structure Physiology (medical) Peripheral myelin protein 22 Chromosomal region medicine Facioscapulohumeral muscular dystrophy Neurology (clinical) Reduced tendon reflexes business Sensory nerve |
Zdroj: | Muscle & Nerve. 23:1243-1249 |
ISSN: | 1097-4598 0148-639X |
Popis: | We report an Austrian family with proximal muscle weakness and wasting predominantly of the shoulder girdle musculature, normal or slightly reduced distal muscle power, mild foot deformity, absent or reduced tendon reflexes in the lower limbs, and normal or slightly diminished sensation. Electrophysiologically, motor nerve conduction velocities were slowed to less than 33 m/s, distal latencies were prolonged, and compound motor action potentials were low. Sensory nerve conduction velocities were extremely reduced or no sensory potentials were recordable. Genetic testing in three affected individuals revealed a duplication of the chromosomal region 17p11.2. In addition, genetic testing for facioscapulohumeral muscular dystrophy (FSHD) revealed a 33 kb EcoRI fragment on chromosome 4q35 in one affected individual and in the clinically normal parent, whereas in a second affected person normal DNA-sizes were observed. These clinical findings define a new phenotypic variant associated with the Charcot-Marie-Tooth 1A duplication. This may be due to a mutation in another gene contained in the 1.5 Mb duplication although mutations in the peripheral myelin protein 22 gene have been excluded. Alternatively, the genetic background of other genes in the family may modify the phenotypic expression, as found in other inherited diseases. The unusual phenotype cannot be explained by the concomitant presence of FSHD despite some evidence for coexistance in one individual. |
Databáze: | OpenAIRE |
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