Different expressivity of a ventricular essential myosin light chain gene Ala57Gly mutation in familial hypertrophic cardiomyopathy

Background Familial hypertrophic cardiomyopathy (HCM) is a clinically and genetically heterogeneous disease of the sarcomere. Molecular genetic studies have shown that familial HCM involves mutations in 8 different genes that encode proteins of the myofibrillar apparatus. Methods We thoroughly searc...

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Published in:The American heart journal 2001-02, Vol.141 (2), p.184-189
Main Authors: Lee, Won-Ha, Hwang, Tae Hong, Kimura, Akinori, Park, Seung Woo, Satoh, Manatsu, Nishi, Hirofumi, Harada, Haruhito, Toyama, Junji, Park, Jeong-Euy
Format: Article
Language:English
Subjects:
Adult
Aged
Biological and medical sciences
Cardiology. Vascular system
Cardiomyopathy, Hypertrophic - genetics
Cardiomyopathy, Hypertrophic - metabolism
DNA - analysis
DNA Probes - chemistry
Female
Gene Expression
Genetic Predisposition to Disease
Heart
Heart Ventricles - metabolism
Humans
Male
Medical sciences
Middle Aged
Mutation, Missense
Myocarditis. Cardiomyopathies
Myocardium - metabolism
Myosin Light Chains - genetics
Myosin Light Chains - metabolism
Phenotype
Polymerase Chain Reaction
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Summary:Background Familial hypertrophic cardiomyopathy (HCM) is a clinically and genetically heterogeneous disease of the sarcomere. Molecular genetic studies have shown that familial HCM involves mutations in 8 different genes that encode proteins of the myofibrillar apparatus. Methods We thoroughly searched these genes to find the mutations in 38 probands of unrelated families with familial HCM. Results We found a novel missense mutation that resulted in Ala57Gly amino acid substitution of the ventricular essential myosin light chain (vMLC1) gene in two unrelated Korean families with familial HCM and one Japanese patient. The mutated site is located in the putative helix-loop-helix region (named EF-hand domain) of the calcium-binding site that is highly conserved in vMLC1 isoforms across the various species. The phenotype of this mutation in the affected families is a classic asymmetric septal hypertrophy, and the disease penetrance in genotyped members older than 18 years is 78%. In one Korean family a 42-year-old woman and two brothers (34 and 38 years old) with the mutation had fully expressed the disease, but two sisters (39 and 29 years old) with the mutation had no phenotypic expression of HCM. Conclusions Ala57Gly mutation in the vMLC1 gene may exhibit the classic form of familial HCM and widely different penetration of the disease phenotype in the family members with mutation, especially in women. (Am Heart J 2001;141:184-9.)
ISSN:0002-8703
1097-6744
DOI:10.1067/mhj.2001.112487