Dobutamine stress for evaluation of right ventricular reserve in pulmonary arterial hypertension
- Tripura Sharma1,2,5,
- Edmund M.T. Lau1,3,5,
- Preeti Choudhary1,2,
- Paul J. Torzillo1,3,
- Phillip A. Munoz3,
- Lisa R. Simmons2,
- Robert Naeije4 and
- David S. Celermajer1,2⇑
- 1Discipline of Medicine, Sydney Medical School, University of Sydney, Sydney, Australia
- 2Dept of Cardiology, Royal Prince Alfred Hospital, Sydney, Australia
- 3Dept of Respiratory Medicine, Royal Prince Alfred Hospital, Sydney, Australia
- 4Dept of Pathophysiology, Free University of Brussels, Brussels, Belgium
- 5Both authors contributed equally
- David S. Celermajer, Dept of Cardiology, Royal Prince Alfred Hospital, Camperdown, NSW 2050, Australia. E-mail: david.celermajer{at}email.cs.nsw.gov.au
Abstract
Right ventricular contractile response to pharmacological stress in pulmonary arterial hypertension (PAH) has not been characterised. We evaluated right ventricular contractile reserve in adults with PAH using dobutamine stress echocardiography.
16 PAH patients and 18 age-matched controls underwent low-dose dobutamine stress echocardiography. Contractile reserve was assessed by the change (Δ; peak stress minus rest value) in tricuspid annular plane systolic excursion (TAPSE) and tricuspid annular systolic velocity (S′). A subgroup of 13 PAH patients underwent treadmill cardiopulmonary exercise testing for peak oxygen uptake (V′O2peak).
At rest, TAPSE and S′ were reduced in the PAH group compared with controls (1.7±0.4 versus 2.4±0.2 cm and 9.7±2.6 versus 12.5±1.2 cm·s−1, respectively; p<0.05). Contractile reserve was markedly attenuated in PAH compared to controls (ΔTAPSE 0.1±0.2 versus 0.6±0.3 cm and ΔS′ 4.6±2.8 versus 11.2±3.6 cm·s−1; p<0.0001). In the sub-group of PAH patients with preserved right ventricular systolic function at rest, contractile reserve remained depressed compared to controls. V′O2peak was significantly correlated with ΔS′ (r=0.87, p=0.0003) and change in stroke volume (r=0.59, p=0.03).
Dobutamine stress can reveal sub-clinical reduction in right ventricular contractile reserve in patients with PAH. A correlation with exercise capacity suggests potential clinical value beyond resting measurements.
Abstract
Dobutamine-induced right ventricular contractile reserve is impaired in PAH and correlates with exercise capacity http://ow.ly/zVg0r
Introduction
Although pulmonary arterial hypertension (PAH) is a disease of the distal pulmonary arteries, the ability of the right ventricle (RV) to adapt to the increased afterload is the main determinant of clinical outcomes in this condition [1]. RV failure is the main cause of death in patients with PAH [2], and most identified prognostic indices have consistently been derived from either direct measurements of RV function or surrogate indicators of RV dysfunction, such as right atrial pressure (RAP) and cardiac output [3–6].
Despite severe elevation of RV afterload in PAH, symptoms of RV failure do not occur at rest until the latter stages of the disease. Thus, it is rational that measurement of RV function under stress may provide incremental value in the clinical assessment of PAH patients. This notion is supported by a recent study where right ventricular contractile reserve was indirectly assessed by the increase in pulmonary artery pressure (PAP) during exercise, and the inability to augment PAP was associated with poorer survival [7].
Inotropic stimulation with dobutamine is an accepted alternative to exercise stress in the evaluation of left ventricular contractile reserve across a range of underlying pathologies including ischaemic heart disease, idiopathic dilated cardiomyopathy and valvular heart disease [8–10]. In contrast, only limited studies have addressed RV contractile reserve and these have predominantly been in the setting of biventricular failure [7, 11–17]. Specifically, assessment of RV contractile reserve using dobutamine stress has not been investigated in PAH. Exercise echocardiography is technically demanding and requires rapid acquisition of images in tachypnoeic patients. Thus, assessment of RV contractile reserve using pharmacological stress is an appealing alternative to exercise stress.
Our study sought to assess RV contractile reserve using low-dose dobutamine stress echocardiography in patients with PAH. We also assessed the association between indices of RV contractile reserve and exercise capacity.
Materials and methods
A total of 35 subjects participated in the study; 17 subjects with PAH and 18 age-matched healthy controls. The diagnosis of PAH was established according to published guidelines. All PAH patients had invasive confirmation with right heart catheterisation demonstrating mean PAP ≥25 mmHg, pulmonary artery wedge pressure ≤15 mmHg and pulmonary vascular resistance >3 Wood units. Healthy controls had no history of cardiorespiratory conditions, no risk factors for pulmonary vascular disease, <10 pack-years smoking history and normal baseline transthoracic echocardiography. Pulmonary haemodynamic responses from these study subjects during dobutamine stress have been reported previously [18]. This study was approved by the Local Institutional Ethics Review Committee (Sydney Local Health District, Australia: X10-0260) and all participants provided written informed consent.
Dobutamine stress echocardiography
Echocardiography images were acquired by either a Vivid 9 system (GE Healthcare, Little Chalfont, UK) or iE33 (Philips Healthcare, Amsterdam, the Netherlands) with a 3.5 MHz transducer by an experienced cardiac sonographer. All patients underwent continuous dobutamine infusion using a low-dose protocol. Dobutamine was increased at increments of 5 μg·kg−1·min−1 at 3-min intervals up to a maximum of 20 μg·kg−1·min−1. The pre-specified infusion end-points were either reaching the maximum dobutamine dose, heart rate >120 beats·min−1 or side-effects requiring cessation. A heart rate of 120 beats·min−1 was chosen for safety reasons to ensure that very high heart rates were not induced in patients with PAH, which could precipitate RV ischaemia. Side-effects requiring cessation of infusion were defined as: 1) hypotension (systolic blood pressure <85 mmHg); 2) chest pain; 3) new onset arrhythmias; or 4) intolerable symptoms experienced by subject. All control subjects completed the dobutamine stress echocardiography protocol but one PAH patient developed self-limiting atrial fibrillation at a dobutamine dose of 10 μg·kg−1·min−1. This patient was excluded from the final data analysis resulting in a final total of 16 assessable PAH patients. No adverse events occurred in any of the other PAH patients.
A standard echocardiogram was performed at baseline. Two-dimensional, M-mode, Doppler echocardiography measurements were performed according to recommendation of the American Society of Echocardiography [19, 20]. Systolic PAP was measured by peak gradient between the RV and the right atrium from the peak tricuspid regurgitation velocity (TRV) using the Bernoulli equation (systolic PAP = (TRV)2 + RAP). RAP was assigned at 5 mmHg for all healthy controls and estimated from the inferior vena cava diameter and collapsibility in PAH subjects. Stroke volume was estimated from the left ventricular outflow tract (LVOT) diameter and LVOT velocity time integral (stroke volume = LVOT velocity time integral × π(LVOT diameter/2)2). Left ventricular ejection fraction was calculated using Simpson’s biplane method. Left atrial and right atrial areas were measured in end-systole from apical four-chamber view. Left ventricular diastolic function was assessed by measuring early (E) and late (A) transmitral flow velocity, and the early diastolic velocity of the medial mitral valve annulus (e′) in order to derive E/A and E/e′ ratios.
Right ventricular systolic function was assessed at baseline and during dobutamine stress using two established indices of longitudinal contraction: 1) tricuspid annular plane systolic excursion (TAPSE); and 2) pulse tissue Doppler peak tricuspid annular systolic velocity at the lateral annulus (S′). RV contractile reserve was defined as the difference between these values obtained at baseline and peak stress (ΔTAPSE and ΔS′, respectively). At baseline we defined a depressed TAPSE as <1.6 cm and S′ as <10 cm·s−1, using reference ranges published in the American Society of Echocardiography guidelines [19]. All values were measured in duplicate for each condition and the average was taken.
Cardiopulmonary exercise testing
A subgroup of 13 out of 16 patients with PAH consented to treadmill cardiopulmonary exercise testing (CPET). The remaining three did not provide consent due to lower limb joint disease (n = 1) and refusal to participate in exercise testing (n=2). All CPET were performed within 1 week of dobutamine stress echocardiography on a treadmill using either a Naughton or Modified Bruce protocol according to the subject’s estimated exercise capacity. Oxygen uptake (V′O2), carbon dioxide production and minute ventilation were measured breath-by-breath together with continuous ECG monitoring and blood pressure via cuff sphygmomanometer.
Statistical analysis
Continuous variables were presented as mean±sd, unless otherwise stated. RV systolic function at rest and peak stress were compared using two-way ANOVA with repeated measures, with post hoc Bonferroni correction for multiple comparisons. Spearman’s correlation was performed to assess correlation in the PAH group. A two-sided p-value <0.05 was considered statistically significant. Statistical analysis was performed using the Prism 6 package (GraphPad, La Jolla, CA, USA).
Results
Baseline demographics of the PAH and control groups are shown in table 1. There was a greater proportion of females in the PAH group, but the two groups were otherwise well matched for age and body mass index. The diagnostic categories of PAH included idiopathic PAH (n=6), scleroderma-associated PAH (n=9) and portopulmonary hypertension (n=1). Baseline disease characteristics encompassed a range of severity as demonstrated by invasive haemodynamics, 6-min walk distance and New York Heart Association (NYHA) functional class. All patients were receiving targeted PAH therapies at the time of study according to a guideline treatment algorithm [21].
The peak dobutamine dose reached was not significantly different between the two groups (PAH 18.4±2.9 μg·kg−1·min−1 versus controls 19.7±1.2 μg·kg−1·min−1; p=0.10). Resting heart rate, as well as peak stress heart rate, were both higher in PAH compared to controls (baseline heart rate: 80±12 versus 65±9 beats·min−1, p=0.004; peak heart rate: 113±17 versus 96±12 beats·min−1, p=0.003). Peak stress resulted in augmentation of systolic PAP from 21±5 to 31±7 mmHg and from 79±24 to 108±30 mmHg in controls and PAH patients, respectively.
Right ventricular contractile reserve
Baseline echocardiographic parameters are summarised in table 2. Resting RV systolic function was reduced in PAH compared to controls. Resting TAPSE in PAH patients was 1.7±0.4 cm and S′ was 9.7±2.6 cm·s−1. In controls, resting TAPSE and S′ were both higher at 2.4±0.2 cm and 12.5±1.2 cm·s−1, respectively (both p<0.05 compared to PAH) (fig. 1). However, 10 (63%) out of the 16 and seven out of (44%) the 16 PAH patients had resting TAPSE and S′, respectively, within the normal range as defined by TAPSE ≥1.6 cm and S′ ≥10 cm·s−1 [19].
RV contractile reserve was markedly reduced in PAH patients compared to controls (ΔTAPSE: 0.1±0.2 versus 0.6±0.3 cm, p<0.0001; ΔS′: 4.6±2.8 versus 11.2±3.6 cm·s−1, p<0.0001) (fig. 2). Of the 10 PAH subjects with a preserved TAPSE at rest, ΔTAPSE was depressed at 0.1±0.3 cm (p<0.0001 compared to controls). Similarly, of the seven PAH patients with a preserved resting S′, ΔS′ was similarly depressed at 5.7±3.0 cm·s−1 (p=0.0012 compared to controls).
Relationship between contractile reserve and exercise capacity
The mean (range) peak V′O2 in the PAH group was 16.2±7.2 (9.0–32.9) mL·kg−1·min−1. There was a significant positive correlation between ΔS′ and peak V′O2 (r=0.87, p=0.0003) but not between ΔTAPSE and peak V′O2 (r=0.21, p=0.49). Change in stroke volume also correlated with exercise capacity (r=0.59, p=0.03). When PAH subjects were stratified by NYHA functional class status, those in functional class 1–2 (n=8) had better contractile reserve compared to those in functional class 3–4 (n=8) when measured by ΔS′ (6.4±2.5 versus 2.8±1.8 cm·s−1, p=0.005). Resting TAPSE and S′ also correlated significantly with peak V′O2 (r=0.60, p=0.034 and r=0.62, p=0.026, respectively), although less strongly than ΔS′ (fig. 3).
Discussion
To the best of our knowledge this is the first study to assess RV contractile reserve using dobutamine stress echocardiography in patients with PAH. We found that the RV contractile reserve following dobutamine stimulation was markedly reduced in subjects with PAH and contractile reserve using systolic myocardial velocity at the tricuspid annulus (ΔS′) correlated significantly with reduced exercise capacity. Furthermore, we found that even in PAH patients where RV parameters were within the “normal range” at baseline, contractile reserve remained significantly depressed compared to healthy controls. This suggests that the use of dobutamine stress may potentially unmask latent RV dysfunction that is not apparent at rest. A significant correlation between indices of RV contractile reserve and exercise capacity in PAH patients supports the potential clinical utility of dobutamine stress echocardiography, given that exercise capacity is a powerful predictor of prognosis in this condition [22].
Due to the complex geometry of the RV, accurate volumetric assessment with two-dimensional echocardiography is difficult. Even with three-dimensional echocardiography, volumetrics can be inaccurate [23]. Magnetic resonance imaging is the gold standard for assessing RV volumes but its expense limits its current role in the routine bedside assessment of RV function, and exercise magnetic resonance imaging for RV function is currently not well established. Due to the unique myocardial fibre orientation of the RV, base-to-apex longitudinal contraction is considered to be particularly important in RV emptying [24, 25]. TAPSE and S′ represent two of the most commonly used, reproducible and validated indices of RV systolic function in clinical practice [19]. Furthermore, measures of longitudinal RV systolic function have been demonstrated to predict prognosis in PAH [3, 26]. For this reason, we elected to study these two particular RV indices for the present study, for both simplicity and potential clinical application.
The assessment of left ventricular contractile reserve using stress echocardiography is a well-established technique for left heart disease [27]. The incremental prognostic value of left ventricular contractile reserve over resting measurements has been demonstrated for ischaemic heart disease, valvular heart disease and idiopathic dilated cardiomyopathy [13, 28, 29]. Only two previous studies have specifically evaluated RV contractile reserve in PAH and employed exercise Doppler echocardiography protocols [7, 17]. In the study by Grunig et al. [7], RV contractile reserve was assessed indirectly by the augmentation of PAP during exercise, rather than by direct measurements of RV function. PAH patients who were able to augment PAP above the median value of 30 mmHg had a significantly improved prognosis on follow-up. The physiological basis of exercised-induced PAP augmentation as a surrogate parameter of contractile reserve is based on the premise that any increase in PAP during exercise results from an increase in cardiac output, which in turn is a reflection of the ability of the RV to increase its stroke volume under stress. In another study, Almeida et al. [17] made direct measurements of RV systolic function during treadmill exercise. They found ΔS′ and ΔTAPSE augmentations in PAH patients of 4.3±3.3 cm·s−1 and 0.06±0.25 cm, respectively; values very similar to those disclosed by dobutamine stress in our study.
The use of low-dose dobutamine stress echocardiography is potentially a simpler and more appealing modality for the bedside assessment of RV contractile reserve, compared to exercise stress. Exercise echocardiography is technically challenging for the RV and particularly so in the breathless patient due to respiratory motion and the need for rapid image acquisition during exercise. With dobutamine stress echocardiography we were able to obtain, with sufficient quality, direct measurements of RV function in all subjects at peak stress, rather than rely on a surrogate marker such as exercise-induced PAP augmentation. Furthermore, direct measurement of RV function is likely to be preferable, as PAP augmentation during exercise is not only on dependent RV stroke volume reserve, but also on the individual patient’s chronotropic response and the slope of the pressure–flow relationship of the pulmonary circulation during exercise [30].
It was of interest that we found a significant correlation between contractile reserve measured by ΔS′ and peak V′O2. Even though patients with PAH may present with mild-to-moderate ventilation/perfusion mismatch abnormalities, the main determinant of exercise capacity is right ventricular function (and cardiac output) [31]. In PAH, exercise capacity is dependent on the ability of the RV to respond to the increase in cardiac output required for the metabolic requirements of exercise [32]. Thus, it is perceivable that measures of RV contractile reserve may, therefore, be coupled with exercise capacity. The lack of correlation between ΔTAPSE with exercise capacity may be due to a number of factors. Although TAPSE and S′ both represent measures of longitudinal contraction at the tricuspid annulus, they are fundamentally different in that TAPSE measures the distance and S′ measures the peak velocity of systolic contraction. For this reason, it is likely that S′ may be more sensitive to the inotropic effects of dobutamine and, thus, may better reflect augmentation of RV stroke volume compared to TAPSE. Furthermore, studies in healthy subjects indicate that exercise stress augments TAPSE by ∼20% relative to baseline (∼0.5 cm) but S′ increases by ∼80% (∼10 cm·s−1) [17]. Thus, the relatively small augmentation in TAPSE (even in normal subjects) suggests that assessment of RV reserve using TAPSE may suffer from larger noise-to signal ratio compared to S′. In fact, our study found that TAPSE did not change significantly following dobutamine stress in PAH patients, which is concordant with the findings of the recent exercise study by Almeida et al. [17].
Limitations
The major limitation of our study was a relatively small number of subjects. However, this was an exploratory study to determine the feasibility, safety and potential utility of low dose dobutamine stress echocardiography for the assessment of RV contractive reserve in PAH and had sufficient power for clear separation of groups. We acknowledge that both TAPSE and S′ have drawbacks as measurements of RV function, as ideal measures of ventricular contractility should be load independent, such as end-systolic ventricular elastance derived from invasively measured pressure–volume loops. Nevertheless, longitudinal measures of RV systolic function are simple and reproducible parameters that are utilised widely in clinical practice and, at present, there remains no ideal load-independent measurement of RV function using two-dimensional echocardiography. It remains to be determined whether such longitudinal measures of RV systolic function are sufficient to characterise RV contractile reserve.
We did not assess contractile reserve using other RV parameters, such as fractional area change, Tei-index or tricuspid annulus isovolumic acceleration. Our own experience and that of other authors has found fractional area change to suffer from large interobserver variations [33], often the result of difficulty in clearly defining endocardial borders due to RV trabeculations. Furthermore, accurate measurement of RV area is limited by the complex geometry of this chamber. Both Tei-index and isovolumic acceleration have large variability depending on heart rate and, thus, we avoided these parameters due to the chronotropic effects of dobutamine (as would also apply to exercise).
Our dobutamine stress echocardiography protocol represents a modification of the protocol used for assessment of myocardial ischaemia, which conventionally employs dobutamine doses up to 40 μg·kg−1·min−1 with or without additional atropine [34]. Patients with severe PAH may not tolerate extreme heart rates and induction of arrhythmias is also of particular concern in this study. Our protocol, with a peak dose of 20 μg·kg−1·min−1 and limiting heart rate to a maximum of 120 beats·min−1, appeared generally safe and well tolerated. It has been demonstrated that a heart rate of around ∼120 beats·min−1 is also close to the maximum response in severe PAH patients because of decreased chronotropic response [35]. The optimal dosing protocol of dobutamine stress for the assessment of RV contractile reserve in PAH requires further clarification.
Not all PAH patients underwent cardiopulmonary exercise testing, which could have had an influence on our overall results concerning the relationship between RV contractile reserve and exercise capacity. Finally, larger prospective studies are required to determine the clinical relevance of different echocardiography derived parameters of RV contractile reserve, the limits of normal contractile reserve in healthy individuals, and whether threshold values of RV contractile reserve can be predictive of poorer outcomes in PAH.
Conclusions
We demonstrate that patients with PAH exhibit markedly diminished RV contractile reserve during dobutamine stress echocardiography, and abnormal stress responses occur even in those with relatively preserved resting RV systolic function. RV contractile reserve correlates with exercise capacity, suggesting the potential clinical value of measures of RV contractile reserve beyond resting measurements.
Footnotes
For editorial comments see Eur Respir J 2015; 45: 604–607 [DOI: 10.1183/09031936.00233614].
Support statement: Funding for this study was received from the National Health and Medical Research Council of Australia Project awarded to D.S. Celermajer (grant no. 1022141), and a National Health and Medical Research Council Post-Graduate Scholarship to E. Lau (no. 633136) and P. Choudhary (no. 1055773).
Conflict of interest: None declared.
- Received May 15, 2014.
- Accepted July 9, 2014.
- Copyright ©ERS 2015