Identification of a New Locus for a Peculiar Form of Congenital Muscular Dystrophy with Early Rigidity of the Spine, on Chromosome 1p35-36

Classical congenital muscular dystrophies (CMDs) are autosomal recessive neuromuscular disorders characterized by early onset of hypotonia and weakness, atrophy of limbs and trunk muscles, contractures, and dystrophic changes in the muscle biopsy. So far, only one gene, LAMA2 (6q2), which encodes th...

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Bibliographic Details
Published in:American journal of human genetics 1998-06, Vol.62 (6), p.1439-1445
Main Authors: Moghadaszadeh, Behzad, Desguerre, Isabelle, Topaloglu, Haluk, Muntoni, Francesco, Pavek, Sylvana, Sewry, Caroline, Mayer, Michèle, Fardeau, Michel, Tomé, Fernando M.S., Guicheney, Pascale
Format: Article
Language:English
Subjects:
Adolescent
Biological and medical sciences
Child
Chromosome 1p
Chromosome Mapping
Chromosomes, Human, Pair 1
Congenital muscular dystrophy
Diseases of striated muscles. Neuromuscular diseases
Female
Genetic Linkage
Homozygosity mapping
Humans
Laminin - analysis
Male
Medical sciences
Muscular Dystrophies - congenital
Muscular Dystrophies - genetics
Muscular Dystrophies - physiopathology
Neurology
Pedigree
Respiratory failure
Rigid-spine syndrome
Spine - physiopathology
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Summary:Classical congenital muscular dystrophies (CMDs) are autosomal recessive neuromuscular disorders characterized by early onset of hypotonia and weakness, atrophy of limbs and trunk muscles, contractures, and dystrophic changes in the muscle biopsy. So far, only one gene, LAMA2 (6q2), which encodes the laminin α2 chain (or merosin), has been identified in these disorders. Mutations in LAMA2 cause CMD with complete or partial merosin deficiency, detectable by immunocytochemistry on muscle biopsies, and account for ∼50% of CMD cases. In a large consanguineous family (11 siblings) comprising three children affected by CMD without merosin deficiency, we undertook a genomewide search by homozygosity mapping and analyzed 380 microsatellite markers. The affected children were homozygous for several markers on chromosome 1p35-36. We identified two additional consanguineous families with affected children who also showed linkage to this locus. A maximum cumulative LOD score of 4.48, at a recombination fraction of .00, was obtained with D1S2885. A consistent feature in these three families was the presence of early rigidity of the spine, scoliosis, and reduced vital capacity, as found in rigid-spine syndrome (RSS). This study is the first description of a locus for a merosin-positive CMD and will help to better define the nosology of RSS.
ISSN:0002-9297
1537-6605
DOI:10.1086/301882