Two novel mutations in the {beta}-myosin heavy chain gene associated with dilated cardiomyopathy

doi:10.1016/j.ejheart.2004.04.017

European Journal of Heart Failure 2004 6(7):861-868; doi:10.1016/j.ejheart.2004.04.017

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Two novel mutations in the β-myosin heavy chain gene associated with dilated cardiomyopathy

Satu Kärkkäinen^a, Tiina Heliö^b, Pertti Jääskeläinen^a, Raija Miettinen^a, Petri Tuomainen^a, Kari Ylitalo^c, Maija Kaartinen^b, Eeva Reissell^b, Lauri Toivonen^b, Markku S. Nieminen^b, Johanna Kuusisto^a, Markku Laakso^a and Keijo Peuhkurinen^a^,*

^a Department of Medicine, Kuopio University Hospital P.O. Box 1777, 70211 Kuopio, Finland
^b Department of Medicine, University of Helsinki Helsinki, Finland
^c Department of Medicine, University of Oulu Oulu, Finland

^* Corresponding author. Tel.: +358-17-173956; Fax: +358-17-173959. E-mail address: Keijo.Peuhkurinen{at}kuh.fi

Abstract

Background: Dilated cardiomyopathy (DCM) is familial in approximately 20–35%of cases of idiopathic DCM. Several mutations in the differentsarcomere protein genes have been reported to cause DCM.

Aims: We wanted to investigate the role of sarcomere protein genevariants in Finnish DCM patients.

Methods and results: We screened all coding exons of five sarcomere protein genes(β-myosin heavy chain, ${alpha}$ -tropomyosin, troponin C, troponinI and troponin T) in a well-characterized population of 52 DCMpatients in Eastern Finland by the PCR-SSCP and sequencing method.Two novel mutations, Arg1053Gln and Arg1500Trp, in the β-myosinheavy chain gene in two index patients were detected. The probandwith the Arg1053Gln mutation had a dilated left ventricle andimpaired systolic function, but other family members carryingthis mutation presented with septal hypertrophy. It thus seemsthat the Arg1053Gln mutation is primarily a HCM mutation, whichcan also lead to DCM. The other mutation, Arg1500Trp, was associatedwith a typical DCM phenotype. The Arg1500Trp mutation carrierhad only one family member alive, but she did not carry themutation and, therefore, cosegregation of the mutation and thedisease in this family could not be reliably verified. No disease-causingmutations were found in the other sarcomere protein genes.

Conclusions: Two novel mutations in the β-myosin heavy chain gene weredetected in patients with DCM. Overall, mutations in the β-myosinheavy chain gene seem to be relatively uncommon in Finnish DCMpatients.

Key Words: Dilated • Hypertrophy cardiomyopathy • Sarcomere protein gene

Received December 4, 2003; Revised March 28, 2004; Accepted April 2, 2004

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