Phenotypic variability in giant axonal neuropathy |
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| Authors: | Meriem Tazir Sonia Nouioua Laurent Magy Kathrin Huehne Salima Assami Andoni Urtizberea Djamel Grid Tarik Hamadouche Bernd Rautenstrauss Jean-Michel Vallat |
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| Affiliation: | 1. Department of Neurology, University Hospital Mustapha Bacha, Algiers, Algeria;2. Laboratoire de Neurosciences, University of Algiers 1, Algiers, Algeria;3. Laboratoire de Biologie Moléculaire, University of Boumerdes, Boumerdes, Algeria;4. Department of Neurology, CHU Poitiers, University of Poitiers, France;5. Centre de Référence Neuropathies Périphériques Rares, Service et Laboratoire de Neurologie, University Hospital, Limoges, France |
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| Abstract: | Giant axonal neuropathy (GAN), a severe childhood disorder affecting both the peripheral nerves and the central nervous system, is due to mutations in the GAN gene encoding gigaxonin, a protein implicated in the cytoskeletal functions and dynamics. In the majority of the GAN series reported to date, patients had the classical clinical phenotype characterized by a severe axonal neuropathy with kinky hair and early onset CNS involvement including cerebellar and pyramidal signs. We present 12 patients (6 families) with GAN mutations and different clinical phenotypes. Four families were harbouring an identical homozygous nonsense mutation but with different severe clinical phenotypes, one patient had a novel missense homozygous mutation with a peculiar moderate phenotype and prominent skeletal deformations. The last family (4 patients) harbouring a homozygous missense mutation had the mildest form of the disease. In contrast with recent reported series of patients with typical GAN clinical features, the present series demonstrate obvious clinical heterogeneity. |
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