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a Institute of
Neurology , b Department of Human Genetics, University
Hospital Nijmegen, The Netherlands , c INSERM U289, Hôpital de la
Salpêtrière, Paris, France
Correspondence to: Dr A Gabreëls-Festen, Institute of Neurology, University Hospital Nijmegen, PO Box 9101, 6500 HB, Nijmegen, The Netherlands. Telephone 0031 24 3615291; fax 0031 24 3541122; email a.gabreels-festen{at}czzorlnm.azn.nl
Received 20 February
1998 and in revised form 2 October 1998;
Accepted 16
October 1998
OBJECTIVES
To report
the occurrence of the autosomal recessive form of demyelinating
Charcot-Marie-Tooth disease (CMT) with a locus on chromosome 5q23-33
in six non-related European families, to refine gene mapping, and to
define the disease phenotype.
METHODSIn an Algerian
patient with autosomal recessive
demyelinating CMT mapped to chromosome 5q23-q33 the same unique nerve
pathology was established as previously described in families with a
special form of autosomal recessive
demyelinating CMT. Subsequently, the DNA of patients with this
phenotype was tested from five Dutch families and one Turkish family
for the 5q23-q33 locus.
RESULTSThese patients
and the Algerian families showed a similar and highly typical
combination of clinical and morphological features, suggesting a common
genetic defect. A complete cosegregation for markers D5S413, D5S434,
D5S636, and D5S410 was found in the families. Haplotype construction
located the gene to a 7 cM region between D5S643 and D5S670. In the
present Dutch families linkage disequilibrium could be shown for
various risk alleles and haplotypes indicating that most of these
families may have inherited the underlying genetic defect form a common
distant ancestor.
CONCLUSIONSThis study
refines the gene localisation of autosomal
recessive demyelinating CMT, mapping to chromosome 5q23-33 and defines the phenotype characterised by a precocious and rapidly progressive scoliosis in combination with a relatively mild neuropathy and a unique
pathology. Morphological alterations in Schwann cells of the myelinated
and unmyelinated type suggest the involvement of a protein present in
both Schwann cell types or an extracellular matrix protein rather than
a myelin protein. The combination of pathological features possibly
discerns autosomal recessive demyelinating CMT with a gene locus on chromosome 5q23-33 from other demyelinating forms of CMT disease.
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