Defining cardiac adaptations and safety of endurance training in patients with m.3243A>G-related mitochondrial disease

Matthew G D Bates; Jane H Newman; Djordje G Jakovljevic; Kieren G Hollingsworth; Charlotte L Alston; Pawel Zalewski; Jacek J Klawe; Andrew M Blamire; Guy A MacGowan; Bernard D Keavney; John P Bourke; Andrew Schaefer; Robert McFarland; Julia L Newton; Douglass M Turnbull; Robert W Taylor; Michael I Trenell; Gráinne S Gorman

doi:10.1016/j.ijcard.2013.05.062

Defining cardiac adaptations and safety of endurance training in patients with m.3243A>G-related mitochondrial disease

Int J Cardiol. 2013 Oct 9;168(4):3599-608. doi: 10.1016/j.ijcard.2013.05.062. Epub 2013 Jun 3.

Authors

Matthew G D Bates¹, Jane H Newman, Djordje G Jakovljevic, Kieren G Hollingsworth, Charlotte L Alston, Pawel Zalewski, Jacek J Klawe, Andrew M Blamire, Guy A MacGowan, Bernard D Keavney, John P Bourke, Andrew Schaefer, Robert McFarland, Julia L Newton, Douglass M Turnbull, Robert W Taylor, Michael I Trenell, Gráinne S Gorman

Affiliation

¹ Wellcome Trust Centre for Mitochondrial Research, Institute for Ageing and Health, Newcastle University, Newcastle upon Tyne NE2 4HH, UK; Cardiothoracic Centre, Freeman Hospital, Newcastle upon Tyne Hospitals NHS Foundation Trust, Newcastle upon Tyne NE7 7DN, UK. Electronic address: m.g.d.bates@newcastle.ac.uk.

Abstract

Background: Cardiac hypertrophic remodelling and systolic dysfunction are common in patients with mitochondrial disease and independent predictors of morbidity and early mortality. Endurance exercise training improves symptoms and skeletal muscle function, yet cardiac adaptations are unknown.

Methods and results: Before and after 16-weeks of training, exercise capacity, cardiac magnetic resonance imaging and phosphorus-31 spectroscopy, disease burden, fatigue, quality of life, heart rate variability (HRV) and blood pressure variability (BPV) were assessed in 10 adult patients with m.3243A>G-related mitochondrial disease, and compared to age- and gender-matched sedentary control subjects. At baseline, patients had increased left ventricular mass index (LVMI, p<0.05) and LV mass to end-diastolic volume ratio, and decreased longitudinal shortening and myocardial phosphocreatine/adenosine triphosphate ratio (all p<0.01). Peak arterial-venous oxygen difference (p<0.05), oxygen uptake (VO2) and power were decreased in patients (both p<0.01) with no significant difference in cardiac power output. All patients remained stable and completed ≥80% sessions. With training, there were similar proportional increases in peak VO2, anaerobic threshold and work capacity in patients and controls. LVMI increased in both groups (p<0.01), with no significant effect on myocardial function or bioenergetics. Pre- and post-exercise training, HRV and BPV demonstrated increased low frequency and decreased high frequency components in patients compared to controls (all p<0.05).

Conclusion: Patients with mitochondrial disease and controls achieved similar proportional benefits of exercise training, without evidence of disease progression, or deleterious effects on cardiac function. Reduced exercise capacity is largely mediated through skeletal muscle dysfunction at baseline and sympathetic over-activation may be important in pathogenesis.

Keywords: Autonomic function; Cardiac magnetic resonance imaging; Cardiac magnetic resonance spectroscopy; Cardio-pulmonary exercise testing; Endurance exercise; Mitochondrial DNA.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adaptation, Physiological / physiology*
Adult
Cardiac Output / physiology
Cohort Studies
Exercise Test / methods*
Exercise Tolerance / physiology
Female
Follow-Up Studies
Humans
Male
Middle Aged
Mitochondrial Diseases / genetics*
Mitochondrial Diseases / physiopathology
Mitochondrial Diseases / therapy*
Physical Endurance / physiology*
Point Mutation / genetics*

Abstract

Publication types

MeSH terms

Grants and funding