Log in to MyACC
Natural History of MYH7-Related Dilated Cardiomyopathy
Quick Takes
- Among individuals with MYH7 mutations, phenotypic manifestation was dilated cardiomyopathy (DCM), commonly with LV noncompaction morphology, and malignant ventricular arrhythmias were rare and only in individuals with EF ≤35%.
- Phenotypic expression rate in the form of DCM was high (99% by age 80 years) and up to 16% had DCM prior to age 18 years.
- Carriers with conduction disease were more likely to develop DCM and individuals with MYH7 mutations classified as variant of uncertain significance showed similar phenotype, suggesting that these variants are likely to be reclassified as pathogenic in the future.
Study Questions:
What is the clinical course and what are the long-term outcomes associated with dilated cardiomyopathy (DCM) related to MYH7 variants and its asymptomatic carriers?
Methods:
An international cohort of DCM patients from Europe, Argentina, and Australia was studied retrospectively. These patients had pathogenic or likely pathogenic variants of MYH7. Carriers identified through cascade screening were also included irrespective of phenotype expression. Patients with coronary artery disease, valvular disease, hypertrophic cardiomyopathy, and with other pathogenic/likely pathogenic mutations were also excluded.
Results:
A total of 147 patients were included, comprised of 106 patients with DCM at initial evaluation and 41 patients as asymptomatic carriers. Mean age of 106 patients with DCM at first evaluation was 39 years, 42% were female, and one-half had New York Heart Association class II symptoms or worse. Mean ejection fraction (EF) was 40% and 58% had left ventricular (LV) noncompaction (LVNC) morphology by magnetic resonance imaging (MRI). Atrial arrhythmias were noted in 6%, ventricular arrhythmias in 21%, and conduction disease in 21%. Carriers were younger at first evaluation with a mean age of 27 years and 71% had LVNC by MRI. Over a median follow-up duration of 4.5 years, 24% developed DCM. The strongest predictor of DCM was presence of intraventricular conduction delay and LVNC was not associated with DCM onset.
Overall, mean age at DCM onset among all patients was 37 years. Males were younger than females at age of onset and most patients were diagnosed between 20-60 years and phenotypic expression rate was 99% by age 80 years. Occurrence of DCM before the age of 18 years occurred in 16%. Incidence of LV reverse remodeling was similar to the LMNA cohort but lower than the TTN cohort. Overall incidence of malignant ventricular arrhythmias (MVAs) at 5 years was 1% and all these patients had an EF ≤35%. Incidence of end-stage heart failure (HF) at 5 years was 12%, similar to the TTN cohort. Most mutations were in the head region of the protein (65%) and these were more likely to be affected with LVNC than mutations elsewhere in the protein. The mutation location was not associated with MVA or end-stage HF. Patients with MYH7 variants classified as variant of uncertain significance (VUS) had a similar prevalence of MVA and end-stage HF and more likely to have LV reverse remodeling compared with individuals with pathogenic MYH7 variants.
Conclusions:
In an international cohort of individuals with MYH7 variants, incidence of phenotypic expression as DCM was high and LVNC was common. Overall, 16% of individuals had DCM prior to the age of 18 years. Incidence of malignant arrhythmias was low and only in individuals with EF ≤35%. Incidence of end-stage HF was 12%.
Perspective:
Genetic causes for DCM are identified in up to 40% of individuals. Pathogenic MYH7 mutations are identified in up to 5% of DCM cases, making it one of the most common genes implicated. This study is the largest cohort of patients and carriers of MYH7 mutations. The resultant phenotype was DCM, and MVAs were rare and only in patients with EF ≤35%. LVNC was common. Notable features include the high phenotypic expression rate with up to 99% of individuals having DCM by age 80 years. In addition, DCM was noted in up to 16% of individuals below age 18 years, suggesting the need to begin screening earlier in childhood for carriers of this mutation, especially among individuals with evidence of conduction disease. Since MVA was rare and occurred in only individuals with EF ≤35%, standard guidelines for implantable cardioverter-defibrillator implantation should be followed. In addition, individuals with MYH7 VUS were just as likely to develop DCM and MVA as individuals with pathogenic MYH7 variants, suggesting that most VUS are likely to be reclassified as pathogenic.
Clinical Topics: Arrhythmias and Clinical EP, Heart Failure and Cardiomyopathies, Noninvasive Imaging, Implantable Devices, Genetic Arrhythmic Conditions, SCD/Ventricular Arrhythmias, Atrial Fibrillation/Supraventricular Arrhythmias, Acute Heart Failure, Magnetic Resonance Imaging
Keywords: Arrhythmias, Cardiac, Cardiomyopathy, Dilated, Defibrillators, Implantable, Diagnostic Imaging, ESC22, ESC Congress, Genetics, Heart Failure, Magnetic Resonance Imaging, Cine, Mutation, Outcome Assessment, Health Care, Phenotype, Stroke Volume
< Back to Listings
