Your search keyword '"Thiffault I"' showing total 2 results

1. Founder mutation for α-sarcoglycan-LGMD2D in a Magdalen Islands Acadian cluster.

Author

Tétreault M, Srour M, Allyson J, Thiffault I, Loisel L, Robitaille Y, Bouchard JP, and Brais B

Subjects

Adolescent, Adult, Aged, Canada epidemiology, Canada ethnology, Cohort Studies, Creatine Kinase metabolism, DNA Mutational Analysis, Disease Progression, Female, France ethnology, Gene Frequency, Genomics methods, Genotype, Humans, Lordosis etiology, Lung Diseases etiology, Male, Middle Aged, Muscle, Skeletal pathology, Muscular Dystrophies, Limb-Girdle complications, Spain ethnology, Muscular Dystrophies, Limb-Girdle ethnology, Muscular Dystrophies, Limb-Girdle genetics, Polymorphism, Single Nucleotide genetics, Sarcoglycans genetics

Abstract

Background: We have recruited a group of four living and reviewed the records of six deceased distantly related French-Canadians of Acadian descent affected by a childhood-onset form of recessive limb-girdle muscular dystrophy (LGMD). All cases originate from the small archipelago of the Magdalen Islands (population: 13,000) isolated in the Gulf of St-Lawrence., Methods: Based on the likely sharing of the same founder mutation we completed a 319K SNPs genome-wide scan to identify the disease locus and then screen candidate genes in this region., Results: All patients had normal initial motor milestones. They presented with limb girdle weakness at the average age of seven years (5-11). Progressive weakness led to loss of ambulation at a wide range of ages (10-39). Patients also developed macroglossia, large calves and mild to moderate contractures, hyperlordosis and decreased pulmonary function. Creatine kinase levels were elevated (1,800-10,000 U/L) in the first decades, but decreased with progression of disease. Homozygosity mapping uncovered a shared chromosomal region of 6.33Mb. The alpha sarcoglycan (SGCA) gene, mutated in LGMD2D, lay in this candidate interval. Sequencing of all SGCA exons uncovered a shared homozygous missense mutation (c. 229C>T, p.R77C), the most common SGCA mutation internationally reported. Using demographic data, we estimated a high carrier rate of 1/22., Conclusion: The p.R77C mutation has also been observed in many populations, including in France and Spain (Basques). This corresponds to the first reported recessive founder disease for the Magdalen Islands, an archipelago settled in the XIXth century, largely by Acadian immigrants.

Published

2011

2. A novel founder SCN4A mutation causes painful cold-induced myotonia in French-Canadians.

Author

Rossignol E, Mathieu J, Thiffault I, Tétreault M, Dicaire MJ, Chrestian N, Dupré N, Puymirat J, and Brais B

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Child, Child, Preschool, Female, France ethnology, Humans, Male, Middle Aged, Mutation, Myotonia complications, Myotonia diagnosis, NAV1.4 Voltage-Gated Sodium Channel, Pain complications, Pain diagnosis, Quebec, White People genetics, Cold Temperature adverse effects, Founder Effect, Myotonia genetics, Pain genetics, Sodium Channels genetics

Abstract

Background: Myotonia is observed in classic congenital myotonia caused by CLCN1 mutations and in sodium-channel myotonia (SCM) due to SCN4A mutations., Methods: We assessed 66 electrically proven cases of myotonia belonging to 17 French-Canadian families living in the Saguenay Lac St-Jean area of Quebec, a region well known for its genetic founder effects. The CLCN1 gene was sequenced in one affected member of each family. SCN4A exons with known SCM mutations were subsequently sequenced in families where no CLCN1 mutations were found., Results: Six families, 33% of cases (22/66), presenting classic congenital myotonia phenotypes were found to carry two previously identified CLCN1 mutations. In the other 11 families comprising 66% of cases (44/66), a new dominant SCN4A mutation in exon 24 (M1476I) was uncovered and segregated with a variable SCM phenotype. Although all carriers of this novel mutation had electrical myotonia, some were asymptomatic (25%) and age at onset was variable in the others (5 to 67, mean 21). Cold aggravated myotonia was observed in 41% of cases and painful myotonia in 18%. Additional features observed include aggravation of symptoms with pregnancies (7%), localized muscle swelling (2%), myotonic reactions to anesthesia (2%), and food-induced paralysis (2%)., Conclusions: This cohort is the largest described with a variable sodium-channel myotonia phenotype caused by a single SCN4A mutation. The clinical variability observed in this cohort underlines the phenotypic heterogeneity of SCN4A mutations and suggests that variants in other genes likely modulate clinical expression.

Published

2007