Yoga and breathing technique training in patients with heart failure and preserved ejection fraction: study protocol for a randomized clinical trial

Active protocol with yoga body movements (àsanas) performed along with respiratory technique without contentions, current and vigorous (ujjayi), observing a respiratory frequency of 15–20 respiratory cycles per minute. This session should last around 45 min.

A standardized 7-min final relaxation will be performed and will be common to both study intervention protocols.

Patients will be oriented to keep their pharmacological routine and daily activities with no structured exercises. They will have to return to the hospital for post-testing after 8 weeks of randomization. After final assessment, all patients, including those in the control group, will be invited to participate in the study breathing activities at the outpatient wards of this trial.

Intervention will last 8 weeks (16 sessions). The post-intervention tests will be performed at the end of the intervention period for the evaluation of endpoints (Fig. 2). To ensure security, data will be stored both in the main researcher’s and study coordinator’s computers, as well as being added to a virtual drive. Researchers, study coordinators, doctors, and statisticians will be allowed data access. Interventions will occur at specific facilities in HCPA (physiatrist sector) and in ULBRA University hospital (medical school) according to patient enrollment. Protocol deviation and adverse events involving individual participants in clinical studies in the HCPA are recorded in the strategic adviser system available in the hospital intranet. Deviations and adverse events occurring at ULBRA will be recorded in the same system as the HCPA. The auditing procedures will occur randomly or designated by the ethical committee for research analysis.

The HFpEF diagnosis will be performed by trained cardiologist experts in the HF field according to the following criteria: HF patient showing an ejection fraction ≥ 50% and E/E’ index of > 8. In addition, other data will be considered for diagnosis, such as left atrial volume > 40 mL/m², atrial fibrillation, and left ventricular mass index. The diagnosis will be confirmed by B-type natriuretic peptide (BNP) levels > 200 pg/mL or NT-proBNP > 220 pg/mL. Patients will be classified either as HFpEF with pseudonormal filling pattern (moderate, grade II) when 8 < E/E’ < 15; or as HFpEF with restrictive left ventricular filling pattern (severe, grade III) when E/E’ > 15. The HF functional classification will be assessed by the New York Heart Association (NYHA) classification system.

Inspiratory muscle function testing will be performed using a pressure transducer (MVD-500 V.1.1 Microhard System, Globalmed, Porto Alegre, RS, Brazil) connected to a system with two unidirectional valves (DHD Inspiratory Muscle Trainer, Chicago, Illinois, USA). Maximal static inspiratory pressure will be determined in deep inspiration from residual volume against an occluded airway, with a minor air leak (2 mm). The highest pressure within six measurements will be used for analysis. The PI_max measurement will be performed at rest and at the 5th and 10th min after CPET. Predicted values will be corrected for age, sex, and weight [14]. Additionally, in order to determine the inspiratory muscle endurance, an incremental test will be used in which patients will breathe continuously through a mouthpiece connected to a measure device. The patients will use an initial load of 50% PI_max, and increments of 10% PI_max will be added every 3 min until the patient is unable to continue breathing. The highest inspiratory pressure that the individual is able to sustain for at least 1 min (Pth_max) will be considered as the measure for inspiratory muscle endurance and will be expressed as a rate of maximal inspiratory pressure (Pth_max/PI_max). In the second stage of the protocol, individuals will breathe against a constant inspiratory submaximal load equivalent to 80% Pth_max, and the time elapsed to task failure will be defined as the inspiratory endurance time. The Powerbreathe K5 will be used for patients with IMW and for those with normal respiratory fraction, for age and sex [15, 16].

The maximum distance covered during the walk test will be used to assess submaximal functional capacity [19]. Patients will self-grade their degree of dyspnea during the test using the Borg scale [20].

Maximal functional capacity will be evaluated using an incremental exercise test, with expired gas analysis, on a treadmill (INBRAMED10200, Porto Alegre, RS, Brazil), using a ramp protocol, starting at a speed of 2.4 km·h^− 1 and 2% slope, with 20-s increments of speed (0.1 to 0.2 km·h^− 1) and 60-s increments in slope (0.5% to 1.0%) to reach volitional fatigue at approximately 10 min. Twelve-lead electrocardiographic tracings will be obtained every minute (Nihon Khoden Corp., Tokyo, Japan). Blood pressure will be measured every 2 min with a standard cuff sphygmomanometer. Metabolic and ventilatory variables will be measured along and after exercise by 20-s mean aliquots, by a computer-aided gas analyzer (Total Metabolic Analysis System, TEEM 100, Aero Sport, Ann Arbor, Michigan, USA), previously validated [21]. Peak oxygen uptake (VO₂ peak) will be considered as the highest VO₂ value calculated in a 20-s period exercise. Maximal circulatory power will be calculated as the product of VO₂ peak and peak systolic pressure [22]. Throughout incremental exercise, oxygen uptake will be plotted against the logarithm of total ventilation, and the oxygen uptake efficiency slope will be determined [23].

QoL will be assessed using the Minnesota Living with Heart Failure Questionnaire [24]. Overall scores and the separate effects of physical and psychological perceptions of QoL will be analyzed.

Twenty-four-hour ECG recordings will be obtained with a SEER Light digital recorder (GE Medical Systems Information Technologies, Milwaukee, WI, USA). The recorded data will be analyzed using a MARS 8000 analyzer (Marquete Medical Systems, Milwaukee, WI, USA) [25, 26]. Briefly, time domain and frequency domain analyses of HRV will be performed according to the recommended by the European Society of Cardiology and North American Society of Pacing and Electrophysiology [27]. For time domain analysis, the following 24-h indices will be calculated: mean of all normal inter-beat (RR) intervals, standard deviation of all normal RR intervals, root mean square of successive differences of adjacent RR intervals, and rate of successive differences between normal adjacent RR intervals above 50 ms. For frequency domain analysis, the following spectral components will be calculated: low frequency (0.04–0.15 Hz), high frequency (0.15–0.5 Hz), and low-to-high frequency ratio. Spectral components will be expressed in absolute values (ms² Hz) and in normalized units. Heart rate spectral analysis and time domain indices will be calculated using 5-min segments at rest during active breathing (ujjayi) and passive breathing (pranàyama).

Since this trial will be performed at two centers, both BNP or NT-proBNP methods will be used, yet the same biomarker (either BNP or NT-proBNP) will be employed for pre- and post-tests in any given patient. The BNP test will be performed on the clinical specimen using blood serum and a chemiluminescence analysis method (Advia Centaursiemens). The NT-proBNP test will be performed on a clinical specimen using blood serum and a sandwich-type electrochemiluminescence analysis method (Cobas E601-Roche).

Usual and additional echocardiographic measures, such as volumetric gradients and diastolic parameters, will be analyzed in the selection of eligible patients (ejection fraction calculated by Teichholz method, ≥ 50%) [16] and after intervention by using two-dimensional echocardiograms (Philips IEE 33).