A new form of congenital muscular dystrophy with joint hyperlaxity maps to 3p23-21

doi:10.1093/brain/awl146

Brain Advance Access originally published online on June 7, 2006
Brain 2006 129(8):2077-2084; doi:10.1093/brain/awl146

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A new form of congenital muscular dystrophy with joint hyperlaxity maps to 3p23-21

M. Tétreault¹, A. Duquette¹, I. Thiffault¹, C. Bherer¹^,4, J. Jarry¹, L. Loisel¹, B. Banwell⁶, G. D'Anjou², J. Mathieu⁵, Y. Robitaille³, M. Vanasse² and B. Brais¹^,2^,5

¹ Laboratoire de neurogénétique, Center for the study of brain diseases, Centre de recherche du CHUM Montreal, Québec, Canada ² Clinique des maladies neuromusculaires, Centre de réadaptation Marie-Enfant, Hôpital Sainte-Justine Montreal, Québec, Canada ³ Département de pathologie, Hôpital Sainte-Justine Montreal, Québec, Canada ⁴ Démographie et épidémiologie génétique, Université du Québec à Chicoutimi Québec, Canada ⁵ Clinique des maladies neuromusculaires, Carrefour de Santé de Jonquière Saguenay, Québec, Canada ⁶ Division of Neurology, the Hospital for Sick Children Toronto, Ontario, Canada

Correspondence to: Bernard Brais, MD, MPhil, PhD, Laboratoire de neurogénétique, M4211-L3, Hôpital Notre-Dame-CHUM, 1560 Sherbrooke Est, Montreal, Quebec, Canada H2L 4M1 E-mail: Bernard.Brais{at}umontreal.ca

Congenital muscular dystrophies (CMDS) are a heterogeneous groupof disorders. A growing number of CMDS have been found to beassociated with joint hyperlaxity. We recruited 14 French–Canadiancases belonging to 11 families affected by a novel autosomalrecessive congenital muscular dystrophy with hyperlaxity (CMDH).All cases come from the southwestern part of Quebec, suggestinga new French–Canadian founder effect. All patients presentmuscle weakness, proximal contractures coexisting with distaljoint hyperlaxity. Pathological and genetic studies have excludedthat mutations in the three genes coding for collagen VI subunitsare responsible for this disease. A genome-wide scan establishedlinkage of two CMDH families to a region on chromosome 3p23-21.Further linkage analysis confirmed that all families are linkedto the same region (log of the odds score of 5.3). Haplotypeanalysis defines a 1.6-cM candidate interval and suggests thattwo common mutations may account for 78% of carrier chromosomes.This study describes and maps a new form of recessive CMD withjoint hyperlaxity distinct from Ullrich and Bethlem myopathieswith a founder effect in the French–Canadian population.

Key Words: congenital muscular dystrophy; hyperlaxity; linkage; family study

Abbreviations: CMD, congenital muscular dystrophy; CMDH, congenital muscular dystrophy with hyperlaxity; H & E, haematoxylin and eosin; LOD, log of the odds; PBS, phosphate-buffered saline; PCR, polymerase chain reaction; SNP, single nucleotide polymorphism; UCMD, Ullrich congenital muscular dystrophy

Received January 18, 2006. Revised April 25, 2006. Accepted May 8, 2006.

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