• Title of article

    Myosin binding protein C mutations and compound heterozygosity in hypertrophic cardiomyopathy Original Research Article

  • Author/Authors

    Sara L. Van Driest، نويسنده , , Vlad C. Vasile، نويسنده , , Steve R. Ommen، نويسنده , , Melissa L. Will، نويسنده , , A.Jamil Tajik، نويسنده , , Bernard J. Gersh، نويسنده , , Michael J. Ackerman، نويسنده ,

  • Issue Information
    روزنامه با شماره پیاپی سال 2004
  • Pages
    8
  • From page
    1903
  • To page
    1910
  • Abstract
    Objectives We sought to determine the frequency and phenotype of mutations in myosin binding protein C (MYBPC3) in a large outpatient cohort of patients with hypertrophic cardiomyopathy (HCM) seen at our tertiary referral center. Background Mutations in MYBPC3 are one of the most frequent genetic causes of HCM and have been associated with variable onset of disease and prognosis. However, the frequency of mutations and associated clinical presentation have not been established in a large, unrelated cohort of patients. Methods Using deoxyribonucleic acid from 389 unrelated patients with HCM, each protein coding exon of MYBPC3 was analyzed for mutations by polymerase chain reaction, denaturing high-performance liquid chromatography, and direct deoxyribonucleic acid sequencing. Clinical data were extracted from patient records blinded to patient genotype. Results Of 389 patients with HCM, 71 (18%) had mutations in MYBPC3. In all, 46 mutations were identified, 33 of which were novel (72%). Patients with MYBPC3 mutations did not differ significantly from patients with thick filament-HCM, thin filament-HCM, or genotype-negative HCM with respect to age at diagnosis, degree of hypertrophy, incidence of myectomy, or family history of HCM or sudden death. Patients with multiple mutations (n = 10, 2.6%) had the most severe disease presentation. Conclusions This study defines the frequency and associated phenotype for MYBPC3 and/or multiple mutations in HCM in the largest cohort to date. In this cohort, unrelated patients with MYBPC3-HCM virtually mimicked the phenotype of those with mutations in the beta-myosin heavy chain. Patients with multiple mutations had the most severe phenotype.
  • Keywords
    DNA , deoxyribonucleic acid , hypertrophic cardiomyopathy , Sudden cardiac death , SCD , ICD , DHPLC , HCM , implantable cardioverter-defibrillator , denaturing high-performance liquid chromatography , LVWT , left ventricular wall thickness , MYH7 , LVOTO , left ventricular outflow tract obstruction , MYBPC3 , myosin binding protein C , beta-myosin heavy chain
  • Journal title
    JACC (Journal of the American College of Cardiology)
  • Serial Year
    2004
  • Journal title
    JACC (Journal of the American College of Cardiology)
  • Record number

    459546