Risk of cardiac manifestations in adult mitochondrial disease caused by nuclear genetic defects

ObjectiveRegular cardiac surveillance is advocated for patients with primary mitochondrial DNA disease. However, there is limited information to guide clinical practice in mitochondrial conditions caused by nuclear DNA defects. We sought to determine the frequency and spectrum of cardiac abnormaliti...

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Published in:Open heart 2021-04, Vol.8 (1), p.e001510
Main Authors: Lim, Albert Zishen, Jones, Daniel M, Bates, Matthew G D, Schaefer, Andrew M, O'Sullivan, John, Feeney, Catherine, Farrugia, Maria E, Bourke, John P, Turnbull, Doug M, Gorman, Gráinne S, McFarland, Robert, Ng, Yi Shiau
Format: Article
Language:English
Subjects:
Adults
Asymptomatic
Ataxia
Blood pressure
Body mass index
Cardiology
Cardiomyopathy
Cholesterol
Clinical medicine
Deoxyribonucleic acid
Diabetes
Disease
DNA
epidemiology
Genes
genetic association studies
genetic diseases
genetics
Heart transplants
Hypertension
inborn
Mitochondrial DNA
Obesity
Patients
Peripheral neuropathy
Risk factors
Special Populations
Statistical analysis
Surveillance
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Summary:ObjectiveRegular cardiac surveillance is advocated for patients with primary mitochondrial DNA disease. However, there is limited information to guide clinical practice in mitochondrial conditions caused by nuclear DNA defects. We sought to determine the frequency and spectrum of cardiac abnormalities identified in adult mitochondrial disease originated from the nuclear genome.MethodsAdult patients with a genetically confirmed mitochondrial disease were identified and followed up at the national clinical service for mitochondrial disease in Newcastle upon Tyne, UK (January 2009 to December 2018). Case notes, molecular genetics reports, laboratory data and cardiac investigations, including serial electrocardiograms and echocardiograms, were reviewed.ResultsIn this cohort-based observational study, we included 146 adult patients (92 women) (mean age 53.6±18.7 years, 95% CI 50.6 to 56.7) with a mean follow-up duration of 7.9±5.1 years (95% CI 7.0 to 8.8). Eleven different nuclear genotypes were identified: TWNK, POLG, RRM2B, OPA1, GFER, YARS2, TYMP, ETFDH, SDHA, TRIT1 and AGK. Cardiac abnormalities were detected in 14 patients (9.6%). Seven of these patients (4.8%) had early-onset cardiac manifestations: hypertrophic cardiomyopathy required cardiac transplantation (AGK; n=2/2), left ventricular (LV) hypertrophy and bifascicular heart block (GFER; n=2/3) and mild LV dysfunction (GFER; n=1/3, YARS2; n=1/2, TWNK; n=1/41). The remaining seven patients had acquired heart disease most likely related to conventional cardiovascular risk factors and presented later in life (14.6±12.8 vs 55.1±8.9 years, p
ISSN:2053-3624
2398-595X
2053-3624
DOI:10.1136/openhrt-2020-001510