Background
Hypertension is associated with a significantly increased risk for adverse cardiac and cerebrovascular events, as well as chronic kidney disease [
1]. Despite optimal medical treatment, blood pressure control often remains poor and the risk for cardiovascular disease remains high. With prevalence ranging between 15 and 30%, treatment-resistant hypertension remains an important medical challenge and leads to intrinsic changes in the heart muscle and is associated with left ventricular (LV) hypertrophy and diastolic dysfunction [
2,
3].
Catheter-based renal denervation (RDN) has been introduced as a treatment modality to optimise blood pressure control in patients with treatment-resistant hypertension by reducing sympathetic nerve activity. Unfortunately, the exact blood pressure-lowering effect of renal sympathetic denervation remains disputed, demonstrated by non-responder rates varying between 8 and 37%, depending on study-specific cohorts and definitions used [
4]. However, sympathetic hyperactivity has been directly associated with LV remodelling and heart rate, which makes it imperative to look at the effects of renal sympathetic denervation beyond blood pressure [
5]. Speckle tracking echocardiography (STE) is a new echocardiography modality that is able to measure LV characteristics, including rotation, strain and strain rate. Strain measures myocardial fibre contraction and relaxation [
6]. This study aims to assess the effect of RDN on functional myocardial parameters, including STE, and to identify potential differences between responders and non-responders.
Methods
Study population
The study population consisted of 31 consecutive patients undergoing RDN in the context of treatment for resistant hypertension according to recent recommendations [
7]. Patients were included between December 2012 and June 2014. All patients underwent non-invasive pre-procedural renal artery imaging and were discussed in a multi-disciplinary team including interventional cardiologists, radiologists and hypertension specialists. As part of routine practice, all patients referred for RDN underwent extensive blood and urine analyses, 24-h ambulatory blood pressure measurement (24 h ABPM), echocardiography, echocardiogram (ECG) and magnetic resonance imaging (MRI) to assess renal artery eligibility and exclude renal artery stenosis in order to be able to exclude secondary causes of hypertension. Informed consent was obtained from all patients.
Definitions and end-points
Office blood pressure measurements were recorded three times in a resting situation with intervals of 5 min using an Omron automated blood pressure monitor. Patients were classified as responders in case the drop in 6 months office systolic blood pressure was 10 mmHg or higher. In order to identify subtle changes in LV function, STE was used to obtain apical rotation, basal rotation, LV twist, twist velocity, peak untwisting velocity, time to peak untwisting velocity, global longitudinal strain (GLS), global circumferential strain (GCS), peak early and late longitudinal diastolic strain rate, and peak early and late circumferential diastolic strain rate. LV twist is defined as the maximal value of the apical systolic rotation–basal systolic rotation [
8].
Transthoracic echocardiography
Echocardiography measurements were performed before the RDN procedure (baseline) and 6 months after the RDN procedure. Two-dimensional grey-scale images were obtained in the left lateral decubitus position using a commercially available ultrasound system (iE33, Philips, Best, The Netherlands), equipped with a broadband (1–5 MHz) S5-1 transducer (frequency transmitted 1.7 MHz, received 3.4 MHz). Data were analysed by two experienced echocardiographers according to the recent recommendations [
9]. The following echocardiographic parameters were acquired: LV end-diastolic septal (LVSd) and posterior wall thickness (LVPWd), and LV end-diastolic (LVEDD) and end-systolic dimension (LVESD). LV mass was calculated with the Devereux formula [
10]. Body surface area (BSA) was calculated according to the Mosteller formula [
11]. LV mass was indexed by BSA as recommended in the guidelines [
12].
From the mitral inflow pattern, peak early (E-wave velocity) and late (A-wave velocity) filling velocities, E/A ratio and E-wave velocity deceleration time were measured. Tissue Doppler was applied end-expiratory in the pulsed-wave Doppler mode at the level of the inferoseptal side of the mitral annulus from an apical four-chamber view, to obtain Em septal (peak early diastolic wave velocity of the mitral annulus) and E/Em ratio.
To acquire the highest wall tissue velocities, the angle between the Doppler beam and the longitudinal motion of the investigated structure was adjusted to a minimal level. The spectral pulsed-wave Doppler velocity range was adjusted to obtain appropriate scale.
To optimise STE, the settings were adjusted to obtain a frame rate of 50–70 frames/s. The echo images were transformed to a QLAB Advanced Quantification Software workstation (version 10.0, Philips, Best, The Netherlands) for offline analysis.
Speckle tracking analysis
STE is an approved echocardiographic modality that provides information on regional and global ventricular function [
13]. In order to obtain this information, apical long-axis views (four-, three- and two-chamber views) and parasternal short-axis views (at the apical, mid-ventricular and basal LV levels) were assessed. The aortic valve closure was assessed in a parasternal long-axis view and added manually. After selecting the appropriate view, the endocardial border was automatically recognised and the tracking points were positioned. When this auto-trace function was not optimal, the tracking points were re-positioned manually on an end-diastolic frame. Next, the software automatically tracked these points using speckle tracking. LV ejection fraction was assessed using this automated endocardial border detection. Most components of LV systolic function [rotation (clockwise rotation as viewed from the apical level has a positive value and counterclockwise rotation from the basal level has a negative value), twist, global circumferential strain (GCS) and GCS rate (GCSR)] and diastolic function (peak untwisting velocity, time to peak untwisting velocity, peak early and late circumferential diastolic strain rate) were abstracted from parasternal short-axis views, whereas others were derived from the apical views [systolic function: global longitudinal strain (GLS) and GLS rate (GLSR); diastolic function: peak early and late longitudinal diastolic strain rate]. Data were exported to a spreadsheet program (Excel, Microsoft Corporation, Redmond, WA) to determine these parameters. In a previous study, we have demonstrated the reproducibility and variability of the parameters investigated in the current study in our centre [
14].
RDN procedure
Procedures were performed using four different systems: Paradise™ (ReCor Medical, Palo Alto, CA) (
n = 13), OneShot™ (Covidien, Campbell, CA) (
n = 3), Vessix V2™ (Boston Scientific, Natick, MA) (
n = 5) and Symplicity™ (Medtronic, Minneapolis, MN) (
n = 10). Procedures were performed according to the device-specific instructions for use [
7,
15]. All procedures were performed under conscious sedation with midazolam and fentanyl.
Statistical analysis
All continuous variables are expressed as mean ± standard deviation (SD). Continuous variables were compared using Student’s t test. Simple linear regression of peak untwisting velocity against heart rate was performed. Categorical variables were compared with the Chi square test or Fisher’s exact test when appropriate. A p-value <0.05 was considered statistically significant. The statistical analysis was performed with SPSS software (version 21.0).
Discussion
The aim of this study was to assess if RDN resulted in functional and structural cardiac changes as assessed using both conventional 2D echocardiography and 2D STE. A secondary objective was to assess any differences in these parameters between responders and non-responders. We observed a significant difference in blood pressure and heart rate at 6 months post procedure. Echocardiographically, at 6 months, a significant difference was noted in LVPWd and A-wave velocity. Additionally, STE demonstrated a significant difference in peak untwisting velocity.
Persistent sympathetic nervous system hyperactivity plays a critical role in hypertension and is associated with significant structural and functional cardiac changes [
16]. In this study, we found that RDN significantly reduced office blood pressure by 18.9 ± 26.8/8.5 ± 13.5 mmHg (
p < 0.001) and heart rate by 4.5 ± 9.9 beats/min (
p = 0.016). In line with these findings, we observed a significant decrease in LVPWd (0.47 ± 1.0 mm), along with a reduction in LVMI of 3.2 ± 11.6 g/m
2 in the total cohort. The fact that this reduction did not reach statistical significance could be due to a lack of power.
Looking further into diastolic function, which is strongly related to hypertension and blood pressure control, revealed a pseudonormal diastolic dysfunction, based on normal E/A ratio, but increased left atrial (LA) dimension and E/Em ratio in the overall study population. We observed a significant decrease in the A-wave velocity by 5.3 ± 13.2 cm/s (
p = 0.044) in the total population. In the responders, the difference in the A-wave velocity even decreased to 8.5 ± 13.8 cm/s (
p = 0.027). The decrease in A-wave velocity after renal denervation could implicate an improvement in the LV relaxation and a subsequent better diastolic function [
17]. Additionally, a pseudonormal diastolic function may reflect a decrease in LV compliance and a moderate increase in LA pressure in our population, with impaired relaxation and prolonged A-wave velocity before treatment. The link between peak untwisting velocity and A-wave velocity may be explained by the rate of uncoiling. In other words, it is likely that less force is needed for the active atrial contraction during late diastolic filling after blood pressure lowering. The relation between LV untwisting and the conventional parameters was also described in previous work, in which a positive correlation between untwisting rate and A-wave velocity was found, while there was no correlation between E-wave velocity and untwisting rate [
8]. However, these findings should be interpreted with caution, as no differences were noted in other echocardiographic parameters determining diastolic function, such as the E/Em ratio and LA dimensions.
Hypertensive patients have a greater risk of developing cardiac fibrosis, myocyte hypertrophy and diastolic dysfunction [
18]. These changes may influence the LV twist and rotation [
19]. LV twist is a wringing motion of the heart as the apex rotates with respect to the base around the LV long axis, which is a key element for regulating LV systolic and diastolic mechanics [
20]. LV twist is derived from the dynamic interaction between subendocardial and subepicardial myocardial fibres, the latter defining the direction of the LV twist. It is known that, in myocardial fibrosis and LV hypertrophy, which is related to pressure overload, impairment appears frequently in the subendocardial layer, leading to a dominance of the subepicardial fibres [
21]. This might explain the increased LV twist in patients with LV hypertrophy. LV untwisting starts after the peak LV twist. In a healthy population, the peak systolic twist is supposed to store potential energy and is thought to contribute towards diastolic suction and facilitate early LV diastolic filling. Previous work from our group demonstrated that peak untwisting velocity is increased in hypertrophic cardiomyopathy patients with mild diastolic dysfunction, as well as in aortic stenosis patients [
8,
22]. Our study is the first to demonstrate a significant decrease in peak untwisting velocity of 14.5 ± 28.9°/s (
p = 0.025) in patients undergoing RDN. This change was mainly driven by a change in peak untwisting velocity by 24.1 ± 28.7°/s (
p = 0.006) in the responders. In non-responders, no difference following RDN was observed. The decrease in untwisting velocity after renal denervation could implicate an improvement in the LV relaxation and a subsequent better diastolic function, similar to A-wave velocity. One may hypothesise that, in hypertension patients, like in hypertrophic cardiomyopathy and aortic stenosis patients, increased peak untwisting velocity serves as a compensatory mechanism for abnormal relaxation and prevents the need to increase LA pressure [
22,
23]. RDN probably leads to an improvement of these specific changes in LV rotational and de-rotational mechanics, especially in responders. However, no significant change was seen in twist and twist velocity. Finally, we observed a significant decrease in heart rate following RDN in our population. This is in line with several randomised controlled studies which also demonstrated a decrease in heart rate following RDN [
24,
25]. Interestingly, a similar decrease in heart rate was observed in the (sham) control arm of both studies, suggesting that RDN by itself has no significant effect on heart rate. Additional exploratory analyses in our study ruled out a correlation between heart rate and untwisting velocity (
R
2 = 0.1%).
Future studies, comparing hypertensive patients with a healthy control group, may be warranted in order to investigate myocardial geometry changes in hypertensive subjects in the context of diastolic LV twisting and untwisting, blood pressure or heart rate independently.