TY - JOUR
T1 - A new common mutation in the cardiac beta-myosin heavy chain gene in Finnish patients with hypertrophic cardiomyopathy
AU - Jääskeläinen, Pertti
AU - Heliö, Tiina
AU - Aalto-Setälä, Katriina
AU - Kaartinen, Maija
AU - Ilveskoski, Erkki
AU - Hämäläinen, Liisa
AU - Melin, John
AU - Kärkkäinen, Satu
AU - Peuhkurinen, Keijo
AU - Nieminen, Markku S.
AU - Laakso, Markku
AU - Kuusisto, Johanna
PY - 2014
Y1 - 2014
N2 - Background. In the nationwide FinHCM Study including 306 Finnish patients with hypertrophic cardiomyopathy (HCM), we have previously identified two founder mutations in the alpha-tropomyosin (TPM1-D175N) and myosin-binding protein C (MYBPC3-Q1061X) genes, accounting for 18% of all cases. Objective. To screen additional mutations, previously identified in eastern Finnish cohorts with HCM, in the FinHCM Study population. Patients and methods. Ten mutations in the beta-myosin heavy chain gene (MYH7), TPM1, and MYBPC3 were screened. Results. MYH7-R1053Q was found in 17 of 306 patients (5.6%). No carriers of MYH7-R719W or N696S were found. A novel TPM1-D175G mutation was found in a single patient. MYBPC3 mutations were found in 14 patients: IVS5-2A-C in two, IVS14-13G-A in two, K811del in six, and A851insT in four patients. Altogether, a HCM-causing mutation was identified in 32 patients, accounting for 10.5% of all cases. In addition, two MYBPC3 variants R326Q and V896M with uncertain pathogenicity were found in eight and in 10 patients, respectively. Conclusion. Combining the present findings with our previous results, a causative mutation was identified in 28% of the FinHCM cohort. MYH7-R1053Q was the third most common mutation, and should be screened in all new cases of HCM in Finland.
AB - Background. In the nationwide FinHCM Study including 306 Finnish patients with hypertrophic cardiomyopathy (HCM), we have previously identified two founder mutations in the alpha-tropomyosin (TPM1-D175N) and myosin-binding protein C (MYBPC3-Q1061X) genes, accounting for 18% of all cases. Objective. To screen additional mutations, previously identified in eastern Finnish cohorts with HCM, in the FinHCM Study population. Patients and methods. Ten mutations in the beta-myosin heavy chain gene (MYH7), TPM1, and MYBPC3 were screened. Results. MYH7-R1053Q was found in 17 of 306 patients (5.6%). No carriers of MYH7-R719W or N696S were found. A novel TPM1-D175G mutation was found in a single patient. MYBPC3 mutations were found in 14 patients: IVS5-2A-C in two, IVS14-13G-A in two, K811del in six, and A851insT in four patients. Altogether, a HCM-causing mutation was identified in 32 patients, accounting for 10.5% of all cases. In addition, two MYBPC3 variants R326Q and V896M with uncertain pathogenicity were found in eight and in 10 patients, respectively. Conclusion. Combining the present findings with our previous results, a causative mutation was identified in 28% of the FinHCM cohort. MYH7-R1053Q was the third most common mutation, and should be screened in all new cases of HCM in Finland.
KW - Alpha-tropomyosin
KW - Beta-myosin heavy chain
KW - Cardiac myosin-binding protein C
KW - Finland
KW - Genetics
KW - Hypertrophic cardiomyopathy
KW - Alpha-tropomyosin
KW - Beta-myosin heavy chain
KW - Cardiac myosin-binding protein C
KW - Finland
KW - Genetics
KW - Hypertrophic cardiomyopathy
U2 - 10.3109/07853890.2014.912834
DO - 10.3109/07853890.2014.912834
M3 - Article
AN - SCOPUS:84907044926
SN - 0785-3890
VL - 46
SP - 424
EP - 429
JO - Annals of Medicine
JF - Annals of Medicine
IS - 6
ER -