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. 2011 May;21(5):338-44.
doi: 10.1016/j.nmd.2011.02.008. Epub 2011 Mar 3.

Four new Finnish families with LGMD1D; refinement of the clinical phenotype and the linked 7q36 locus

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Four new Finnish families with LGMD1D; refinement of the clinical phenotype and the linked 7q36 locus

Peter Hackman et al. Neuromuscul Disord. 2011 May.

Abstract

The objective is to refine the clinical and morphological phenotype and the chromosomal region of interest, in the recently reported 7q36 linked autosomal dominant limb-girdle muscular dystrophy (LGMD1 D/E), by describing four new informative Finnish families. Examinations of the patients included serum CK, neurophysiological studies, cardiac and respiratory function examinations, muscle biopsies and muscle imaging. DNA samples were analyzed by genotyping. Patients in all families had very similar phenotypes with onset of muscle weakness in the pelvic girdle muscles between the fourth and sixth decade, later involvement of the shoulder girdle, and marked walking difficulties in the eighth decade. Muscle biopsies showed myopathic and/or dystrophic features. Genotyping confirmed linkage to the same locus at chromosome 7q36 in all families by one identically segregating haplotype. The linked region was narrowed down from <6.3 to <3.4Mb. Sequencing of the genes in the area is ongoing, aiming to identify the genetic defect.

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