A novel nonsense mutation in the ABC1 gene causes a severe syringomyelia-like phenotype of Tangier disease

doi:10.1093/brain/awg074

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Brain, Vol. 126, No. 4, 920-927, April 2003
© 2003 Guarantors of Brain
doi: 10.1093/brain/awg074

A novel nonsense mutation in the ABC1 gene causes a severe syringomyelia-like phenotype of Tangier disease

Stephan Züchner¹, Anne D. Sperfeld³, Jan Senderek², Bernd Sellhaus¹, Clemens Oliver Hanemann³ and J. Michael Schröder¹

Departments of ¹ Neuropathology and ² Human Genetics, University Hospital, Technical University of Aachen, Aachen and ³ Department of Neurology, University of Ulm, Ulm, Germany

Correspondence to: Professor Dr J. Michael Schröder, Institut für Neuropathologie, Universitätsklinikum der RWTH Aachen, Pauwelsstrasse 32, 52074 Aachen, Germany E-mail: jmschroder{at}ukaachen.de

Tangier disease is a rare autosomal recessive disorder causedby mutations in the recently identified ATP-binding cassettetransporter 1 gene (ABC1). A typical clinical manifestationof Tangier disease is peripheral neuropathy. Former studiesdifferentiated between two manifestations: the more frequentmono- or polyneuropathic form and a syringomyelia-like type.It is unknown whether specific mutations in the ABC1 gene ora particular genetic background are responsible for either ofthese forms. A family is presented comprising a case with asevere syringomyelia-like phenotype of Tangier disease and absenceof cardiovascular disease. Sequencing analysis of the ABC1 genewas performed. A new homozygous C $->$ T transition in exon 18was found in the index patient. This mutation results in a stopcodon at position 909 (R909X) leading to premature terminationof translation. Her clinically asymptomatic daughters, her sisterand one of her nieces were heterozygous. Sural nerve biopsieswere studied in the index patient at the age of 45 and54 years; both revealed a severe neuropathy, characterizedby a subtotal and finally complete loss of nerve fibres. Theentire loss of Schwann cells resulted in an extraordinary formof endoneurial sclerosis. Only rare capillaries, lipid-ladenmacrophages and fibroblasts had survived in the endoneurium.This case appears to be unique in respect to the underlyingnovel mutation in the ABC1 gene and its association with completeendoneurial sclerosis of all fascicles in the sural nerve andabsence of cardiovascular disease.

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