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Neuropediatrics 2008; 39(1): 33-38
DOI: 10.1055/s-2008-1077085
Original Article

© Georg Thieme Verlag KG Stuttgart · New York

Two Novel Mutations in the GDAP1 and PRX Genes in Early Onset Charcot-Marie-Tooth Syndrome

M. Auer-Grumbach 1 , 5 , 10 , C. Fischer 1 , 10 , L. Papić 1 , 10 , E. John 1 , 10 , B. Plecko 2 , R. E. Bittner 3 , G. Bernert 4 , T. R. Pieber 5 , G. Miltenberger 6 , R. Schwarz 7 , C. Windpassinger 1 , F. Grill 8 , V. Timmerman 9 , M. R. Speicher 1 , A. R. Janecke 1
  • 1Institute of Human Genetics, Medical University of Graz, Austria
  • 2Department of Paediatrics, Medical University of Graz, Austria
  • 3Neuromuscular Research Department, Centre of Anatomy and Cell Biology, Medical University, Vienna, Austria
  • 4Department of Paediatrics, University of Vienna, Vienna, Austria
  • 5Department of Internal Medicine, Medical University of Graz, Austria
  • 6Division of Clinical Genetics, Medical University, Innsbruck, Austria
  • 7Landes Frauen- und Kinderklinik, Linz, Austria
  • 8Orthopaedic Hospital of Vienna, Speising, Austria
  • 9VIB - Department of Molecular Genetics, Peripheral Neuropathy Group, University of Antwerp, Antwerp, Belgium
  • 10Centre for Medical Research, Medical University of Graz, Graz, Austria
Further Information

Publication History

received 16.10.2007

accepted after revision 19.04.2008

Publication Date:
26 May 2008 (online)

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Abstract

Autosomal recessive Charcot-Marie-Tooth syndrome (AR-CMT) is often characterised by an infantile disease onset and a severe phenotype. Mutations in the ganglioside-induced differentiation-associated protein 1 (GDAP1) gene are thought to be a common cause of AR-CMT. Mutations in the periaxin (PRX) gene are rare. They are associated with severe demyelination of the peripheral nerves and sometimes lead to prominent sensory disturbances. To evaluate the frequency of GDAP1 and PRX mutations in early onset CMT, we examined seven AR-CMT families and 12 sporadic CMT patients, all presenting with progressive distal muscle weakness and wasting. In one family also prominent sensory abnormalities and sensory ataxia were apparent from early childhood. In three families we detected four GDAP1 mutations (L58LfsX4, R191X, L239F and P153L), one of which is novel and is predicted to cause a loss of protein function. In one additional family with prominent sensory abnormalities a novel homozygous PRX mutation was found (A700PfsX17). No mutations were identified in 12 sporadic cases. This study suggests that mutations in the GDAP1 gene are a common cause of early-onset AR-CMT. In patients with early-onset demyelinating AR-CMT and severe sensory loss PRX is one of the genes to be tested.

Key words

AR-CMT - GDAP1 - PRX - early onset peripheral neuropathy

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Correspondence

M. Auer-GrumbachMD 

Institute of Human Genetics and Department of Internal Medicine

Stiftingtalstraße 24

8010 Graz

Austria

Phone: +43/316/385 728 29

Fax: +43/316/385 730 09

Email: michaela.auer-grumbach@klinikum-graz.at

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