Exercise Training in Hypertrophic Cardiomyopathy: (SAFE-HCM)

Sponsor

St George's, University of London (Other)

Overall Status

Completed

CT.gov ID

NCT05459467

Collaborator

Guy's and St Thomas' NHS Foundation Trust (Other), King's College Hospital NHS Trust (Other)

Enrollment

Locations

Arms

Actual Duration (Months)

26.7

Patients Per Site

Patients Per Site Per Month

Study Details

Study Description

Brief Summary

To explore the feasibility, safety, health and psychological benefits of a 12-week high intensity exercise programme in a young group of individuals with hypertrophic cardiomyopathy (HCM). This will pave the way for a large-scale randomised study of safety of exercise in HCM, the results of which will strengthen the evidence base for exercise recommendations.

Condition or Disease	Intervention/Treatment	Phase
Hypertrophic Cardiomyopathy	Other: Exercise	N/A

Detailed Description

A greater understanding of the pathogenic mechanisms underpinning HCM has translated to improved medical care and better survival of affected individuals. Historically these patients were considered to be at high risk of sudden cardiac death during exercise, therefore exercise recommendations were highly conservative and promoted a sedentary life style. There is emerging evidence which suggests that exercise in HCM has a favourable effect on cardiovascular remodelling and moderate exercise programmes have not raised any safety concerns. Furthermore, individuals with HCM have a similar burden of atherosclerotic risk factors as the general population in whom exercise has been associated with a reduction in myocardial infarction, stroke and heart failure, especially among those with a high-risk burden.

Small studies have revealed that athletes who choose to continue with regular competition do not demonstrate adverse outcomes when compared to those who discontinue sport, and active individuals implanted with an implantable cardioverter defibrillator (ICD) do not have an increased risk of appropriate shocks or other adverse events. The recently published exercise recommendations from the European Society of Cardiology account for more contemporary evidence and adopt a more liberal stance regarding competitive and high intensity sport in individuals with low-risk HCM.

However, further work is required into exercise prescription in younger non competitive individuals participating in higher intensity exercise. Moreover low/moderate intensity exercise may be appropriate for older HCM patients, it is unlikely to attract younger, often asymptomatic patients, who wish to engage in higher intensity regimes.Therefore this study aims to assess the feasibility, safety and outcomes of an individually tailored, high intensity exercise programme in young patients with HCM.

Study Design

Study Type:

Interventional

Actual Enrollment :

80 participants

Allocation:

Randomized

Intervention Model:

Parallel Assignment

Masking:

Single (Investigator)

Masking Description:

Masking for randomisation and analysis

Primary Purpose:

Other

Official Title:

Safety and Outcomes of a Structured Exercise Programme in Young Patients With Hypertrophic Cardiomyopathy: the SAFE HCM Trial

Actual Study Start Date :

Jan 1, 2018

Actual Primary Completion Date :

Mar 3, 2020

Actual Study Completion Date :

Mar 3, 2020

Arms and Interventions

Arm	Intervention/Treatment
Experimental: Exercise Participants began exercising at 70% of their heart rate reserve (HRR). The Borg scale was used to monitor exertion during the programme. Participants were provided with watches to monitor their HR and also wore ECG monitors to assess for arrhythmias during exercise classes. Sessions consisted of a circuit of set exercises alternating between aerobic/cardiovascular and resistance exercises. Participants were progressed in a graded fashion (up to a maximum of 85% HRR). Participants were also expected to participate in a predefined exercise session remotely. Educational session took place in the half an hour following the exercise session. Examples of topics covered included: living with HCM, medications, diet, stress/anxiety management and mindfulness, ICD therapy- what to expect?.	Other: Exercise 12 weeks high intensity exercise programme
No Intervention: Usual care Patients exercised as per usual.

Arm

Intervention/Treatment

Experimental: Exercise

Participants began exercising at 70% of their heart rate reserve (HRR). The Borg scale was used to monitor exertion during the programme. Participants were provided with watches to monitor their HR and also wore ECG monitors to assess for arrhythmias during exercise classes. Sessions consisted of a circuit of set exercises alternating between aerobic/cardiovascular and resistance exercises. Participants were progressed in a graded fashion (up to a maximum of 85% HRR). Participants were also expected to participate in a predefined exercise session remotely. Educational session took place in the half an hour following the exercise session. Examples of topics covered included: living with HCM, medications, diet, stress/anxiety management and mindfulness, ICD therapy- what to expect?.

Other: Exercise

12 weeks high intensity exercise programme

No Intervention: Usual care

Patients exercised as per usual.

Outcome Measures

Primary Outcome Measures

Safety composite outcome [6 months]
This will be reported as the number of people who reach the composite safety outcome (the occurrence of at least one) of the following measured variables 1)cardiovascular death; 2)cardiac arrest; 3) appropriate or inappropriate ICD therapy; 4)exercise induced syncope; 5)sustained ventricular tachycardia; 6) non-sustained ventricular tachycardia; or 7)sustained atrial arrhythmias >30seconds post testing and at 6 months.
Feasibility (qualitative outcome) [12 weeks]
Feasibility will be reported qualitatively using an open ended questionnaire through analysis of the following a) response to invitation to participate and reasons for refusal; b) adherence to the cardiac rehabilitation programme; c) practical issues related to the programme including staffing and resource assessment; d) acceptability of the intervention and educational materials provided to patients and families

Secondary Outcome Measures

Impact on exercise capacity; time to anaerobic threshold (tAT) (seconds) [6 months]
This variable will be assessed individually and compared to baseline values post testing and at 6 months.
Impact on exercise capacity; total exercise time (tMax) (seconds) [6 months]
This variable will be assessed individually and compared to baseline values post testing and at 6 months.
Impact on exercise capacity; VO2(ml/kg/min) at AT (VO2/kgAT) (ml/kg/min) [6 months]
The anaerobic threshold (AT) was calculated initially using the V slope method (visual estimation from the VCO2 and VO2 graphs at the point where the slope of the VCO2 curve exceeded the slope of the VO2 curve). This was checked manually using the raw data and 10 second averaging. All data was additionally averaged over 10 seconds at this point and the averaged VO2 ml/kg/min value used as the VO2 at the AT. This variable will be assessed individually and compared to baseline values post testing and at 6 months.
Impact on exercise capacity; peak VO2(ml/kg/min) (VO2/kgMax) (ml/kg/min) [6 months]
CPET analysis was performed using COSMED Quark CPET metabolic cart (Rome, Italy). This automatically calculated peak VO2 ml/min and converted it to ml/kg/min using the patient's weight which had been inputted into the program prior to commencing the CPET. This variable will be assessed individually and compared to baseline values post testing and at 6 months.
Impact on exercise capacity; VE/VCO2 slope (ratio) [6 months]
This variable will be assessed individually and compared to baseline values post testing and at 6 months.
Impact on exercise capacity; physical activity levels (hours/week) [6 months]
This variable will be assessed individually and compared to baseline values post testing and at 6 months.
Impact on cardiovascular risk factors; blood pressure (BP) (mmHg) [6 months]
This variable will be assessed individually and compared to baseline values post testing and at 6 months.
Impact on cardiovascular risk factors; body mass index (BMI) (kg/m2) [6 months]
This variable will be assessed individually and compared to baseline post testing and at 6 months.
Impact on cardiovascular risk factors; lipid profile (mmol/l) [12 weeks]
This variable will be assessed individually and compared to baseline values post testing.
Impact on cardiovascular risk factors; HbA1c (mmol/mol) [12 weeks]
This variable will be assessed individually and compared to baseline values post testing.
Impact on QoL and psychological parameters; Short form 36 (SF36) scores [6 months]
This variable will be assessed individually and compared to baseline values post testing and at 6 months. The SF-36 is comprised of eight scaled scores, which are the weighted sums of the questions in their section. Each scale is converted into a 0-100 scale, with a lower score denoting greater disability.
Impact on QoL and psychological parameters; Hospital anxiety and depression scale (HADS) scores [6 months]
This variable will be assessed individually and compared to baseline values post testing and at 6 months. The HADS questionnaire consists of seven items each for depression and anxiety. Each item is scored from zero to three, with three the highest anxiety or depression level. Either an anxiety or depression score of >8 points (total 21) denotes considerable symptoms of anxiety or depression.
Impact on QoL and psychological parameters; WHO disability assessment scale II (WHODAS II) scores [6 months]
This variable will be assessed individually and compared to baseline values post testing and at 6 months. The WHODAS II score can be calculated using simple scoring where the following scores are assigned to each item - none (1), mild (2) moderate (3), severe (4) and extreme (5). The scores are then summed, with a higher score denoting greater disability.
Impact on disease phenotype-cardiac biomarkers; troponin (ng/l) [12 weeks]
This variable will be assessed individually and compared to baseline values post testing.
Impact on disease phenotype-cardiac biomarkers; BNP (ng/l) [12 weeks]
This variable will be assessed individually and compared to baseline values post testing.
Impact on disease phenotype-echocardiographic outcomes; LA volume (ml) [12 weeks]
This variable will be assessed individually and compared to baseline values post testing.
Impact on disease phenotype-echocardiographic outcomes; LVEDD (mm) [12 weeks]
This variable will be assessed individually and compared to baseline values post testing.
Impact on disease phenotype-echocardiographic outcomes; LVWT (mm) [12 weeks]
This variable will be assessed individually and compared to baseline values post testing.
Impact on disease phenotype-echocardiographic outcomes; diastolic parameters (E/E', E/A)) [12 weeks]
This variable will be assessed individually and compared to baseline values post testing.
Impact on disease phenotype-ventricular ectopic burden; [6 months]
The absolute number of ventricular ectopics will be assessed and compared to baseline values post testing post testing and at 6 months.

Eligibility Criteria

Criteria

Ages Eligible for Study:

16 Years to 60 Years

Sexes Eligible for Study:

All

Accepts Healthy Volunteers:

Inclusion Criteria:

HCM*
Age range (16-60 years)
All genders
All ethnicities
Symptomatic and/or asymptomatic HCM patients (NYHA functional class I-II) stable on medication over the preceding 3 months
Patients may have ICDs
Patients able to exercise
Patients able to commit to the full duration of the exercise programme
Patients able to lie flat

Exclusion Criteria:

Competitive athletes (individuals who participate in team or individual sports that require systematic training to participate in regular competition against others)
Exercise induced syncope
Uncontrolled ventricular arrhythmias (arrhythmias which cause distracting/disabling symptoms or have caused or may cause incapacity)
NYHA class III-IV
Severe LV failure (ejection fraction <35%)
Exercise limited by a non-cardiac (unrelated to HCM) cause
Surgical myectomy
Awaiting or recent device implantation (within the last 3 months if due to an arrhythmic events, 4 weeks for primary prevention)
Known coronary artery disease - defined as a coronary artery lesion of >50% on coronary angiography or known coronary intervention
Renal failure (eGFR <30ml/min, chronic kidney disease stage 4 and 5 or acute renal failure)
Patients with Friedrich's ataxia, Noonan syndrome, Anderson-Fabry disease and other disorders associated with cardiac hypertrophy
Pregnancy

Contacts and Locations

Locations

	Site	City	Country	Postal Code
1	Guys and St Thomas's Hospital	London	United Kingdom	SE1 9RT
2	Kings College Hospital	London	United Kingdom	SE5 9RS
3	St George's Hospital	London	United Kingdom	SW17 0QT