Autosomal recessive Bethlem myopathy

Bethlem myopathy is a well-defined clinical entity among collagen VI disorders, featuring proximal muscle weakness and contractures of the fingers, wrists, and ankles. It is an early-onset, slowly progressive, and relatively mild disease, invariably associated to date with heterozygous dominant muta...

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Published in	Neurology Vol. 73; no. 22; p. 1883
Main Authors	Gualandi, F, Urciuolo, A, Martoni, E, Sabatelli, P, Squarzoni, S, Bovolenta, M, Messina, S, Mercuri, E, Franchella, A, Ferlini, A, Bonaldo, P, Merlini, L
Format	Journal Article
Language	English
Published	United States 01.12.2009
Subjects	Adult Cells, Cultured Codon, Nonsense - genetics Collagen Diseases - complications Collagen Diseases - genetics Collagen Diseases - pathology Collagen Type VI - genetics Collagen Type VI - metabolism Female Fibroblasts - metabolism Fibroblasts - ultrastructure Genetic Association Studies Genetic Predisposition to Disease Glutamine - genetics Humans Male Microscopy, Electron - methods Middle Aged Molecular Sequence Data Muscle, Skeletal - pathology Muscle, Skeletal - ultrastructure Muscular Diseases - complications Muscular Diseases - genetics Muscular Diseases - pathology Tomography, X-Ray Computed - methods
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Abstract	Bethlem myopathy is a well-defined clinical entity among collagen VI disorders, featuring proximal muscle weakness and contractures of the fingers, wrists, and ankles. It is an early-onset, slowly progressive, and relatively mild disease, invariably associated to date with heterozygous dominant mutations in the 3 collagen VI genes. We have characterized the clinical, laboratory, and genetic features of autosomal recessive Bethlem myopathy in 2 unrelated patients. This study is based on clinical, histochemical, immunocytochemical, and electron microscope evaluation of the muscle and dermal fibroblasts, CT imaging of the muscles, and biochemical and molecular analysis. Both patients carry a truncating COL6A2 mutation (Q819X; R366X) associated with missense changes in the partnering allele lying within the C2 domain of the alpha2(VI) chain (D871N; R843W-R830Q). They show decreased amounts of collagen VI in the basal lamina of muscle fibers and in dermal fibroblast cultures and altered behavior of collagen VI tetramers. Biochemical studies supported the pathogenic effect of identified amino acid substitutions, which involve strictly conserved residues. The reported patients illustrate the occurrence of Bethlem myopathy with a recessive mode of inheritance. This observation completes the hereditary pattern in collagen VI myopathies with both Ullrich congenital muscular dystrophy and Bethlem myopathy underlined by either recessive or dominant effecting mutations. This finding has relevant implications for genetic counseling and molecular characterization of patients with Bethlem myopathy, as well as for genotype-phenotype correlations in collagen VI disorders.
AbstractList	Bethlem myopathy is a well-defined clinical entity among collagen VI disorders, featuring proximal muscle weakness and contractures of the fingers, wrists, and ankles. It is an early-onset, slowly progressive, and relatively mild disease, invariably associated to date with heterozygous dominant mutations in the 3 collagen VI genes. We have characterized the clinical, laboratory, and genetic features of autosomal recessive Bethlem myopathy in 2 unrelated patients. This study is based on clinical, histochemical, immunocytochemical, and electron microscope evaluation of the muscle and dermal fibroblasts, CT imaging of the muscles, and biochemical and molecular analysis. Both patients carry a truncating COL6A2 mutation (Q819X; R366X) associated with missense changes in the partnering allele lying within the C2 domain of the alpha2(VI) chain (D871N; R843W-R830Q). They show decreased amounts of collagen VI in the basal lamina of muscle fibers and in dermal fibroblast cultures and altered behavior of collagen VI tetramers. Biochemical studies supported the pathogenic effect of identified amino acid substitutions, which involve strictly conserved residues. The reported patients illustrate the occurrence of Bethlem myopathy with a recessive mode of inheritance. This observation completes the hereditary pattern in collagen VI myopathies with both Ullrich congenital muscular dystrophy and Bethlem myopathy underlined by either recessive or dominant effecting mutations. This finding has relevant implications for genetic counseling and molecular characterization of patients with Bethlem myopathy, as well as for genotype-phenotype correlations in collagen VI disorders.
Author	Urciuolo, A Franchella, A Ferlini, A Sabatelli, P Squarzoni, S Bovolenta, M Gualandi, F Messina, S Martoni, E Mercuri, E Bonaldo, P Merlini, L
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SubjectTerms	Adult Cells, Cultured Codon, Nonsense - genetics Collagen Diseases - complications Collagen Diseases - genetics Collagen Diseases - pathology Collagen Type VI - genetics Collagen Type VI - metabolism Female Fibroblasts - metabolism Fibroblasts - ultrastructure Genetic Association Studies Genetic Predisposition to Disease Glutamine - genetics Humans Male Microscopy, Electron - methods Middle Aged Molecular Sequence Data Muscle, Skeletal - pathology Muscle, Skeletal - ultrastructure Muscular Diseases - complications Muscular Diseases - genetics Muscular Diseases - pathology Tomography, X-Ray Computed - methods
Title	Autosomal recessive Bethlem myopathy
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