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. 2022 Jan 29;36(10):887–897. doi: 10.1038/s41371-022-00658-0

Renal denervation for atrial fibrillation: a comprehensive updated systematic review and meta-analysis

Khaled Nawar 1,#, Ahmed Mohammad 1,#, Edward J Johns 2, Mohammed H Abdulla 2,
PMCID: PMC9553644  PMID: 35094013

Abstract

The study aims to compare clinical outcomes following renal denervation (RDN) in hypertensive patients with atrial fibrillation (AF). Three online databases were searched (MEDLINE, EMBASE and PubMed) for literature related to outcomes of RDN on hypertension and AF, between January 1, 2010, and June 1, 2021. Where possible, risk ratios (RR) and mean differences (MD) were combined using a random effects model. Significance was set at p ≤ 0.05. Seven trials were included that assessed the effect of adding RDN to pulmonary vein isolation (PVI) in patients with hypertension and AF. A total of 711 patients (329 undergoing PVI + RDN and 382 undergoing PVI alone), with an age range of 56 ± 6 to 68 ± 9 years, were included. Pooled analysis showed a significant lowering of AF recurrence in the PVI + RDN (31.3%) group compared to the PVI-only (52.9%) group (p < 0.00001). Pooled analysis of patients with resistant hypertension showed a significant mean reduction of systolic blood pressure (SBP) (−9.42 mm Hg, p = 0.05), but not diastolic blood pressure (DBP) (−4.11 mm Hg, p = 0.16) in favor of PVI + RDN. Additionally, the pooled analysis showed that PVI + RDN significantly improved estimated glomerular filtration rate (eGFR) (+10.2 mL/min per 1.73 m2, p < 0.001) compared to PVI alone. RDN procedures in these trials have proven to be both safe and efficacious with an overall complication rate of 6.32%. Combined PVI and RDN is beneficial for patients with hypertension and AF. Combined therapy showed improvement in SBP and eGFR, reducing the risk of AF recurrence. RDN may serve as an innovative intervention in the treatment of AF.

Subject terms: Atrial fibrillation, Clinical trials

Introduction

Atrial fibrillation (AF) is the most common type of heart arrhythmia currently affecting 0.51% of the population globally [1]. The prevalence of AF has increased by 33% over the last 20 years particularly due to the increase in the ageing population [1, 2]. In addition to the high prevalence of AF, the spectrum and severity of the condition varies tremendously. However, a common underpinning in AF patients is that hypertension (HTN) is associated with one in five cases of AF [3].

Despite the availability of a variety of pharmacological and lifestyle interventions, around 50% of patient with HTN remain resistant to such strategies [4]. This highlights the existence of a more complex pathophysiological mechanism that defies current therapeutic regimens [5]. More recently, the development of endovascular catheters has allowed for easy access to the renal artery lumen to specifically ablate renal nerves and hence multiple trials were executed over the last decade to carefully examine the effect on renal sympathetic outflow and the downstream effect on blood pressure [6]. The benefits as such of renal denervation (RDN) were further reiterated in multiple trials and a recent network meta-analysis of 20 trials (n = 2152) showed that RDN of main renal artery branches in addition to antihypertensive therapy is most effective in reducing office blood pressure and that RDN using this approach was superior in reducing ambulatory blood pressure compared to sham or antihypertensive therapy alone [6].

Catheter ablation through pulmonary vein isolation (PVI) in patients who fail to demonstrate a reduction in AF recurrence following pharmacological agents is currently a highly effective intervention [7]. Despite PVI being superior to drug therapy, the intervention shows a failure rate of 20–50%, which warrants further investigation of alternative strategies for treating AF [8, 9]. The pathophysiological association between an elevated sympathetic tone, AF and HTN, in addition to the significant failure rate of PVI, prompted the investigation of the effect of RDN on AF and hence, a pilot trial was executed [10]. The trial demonstrated the superiority of combining RDN and PVI and their additive effect in reducing both blood pressure and AF recurrence [10]. Subsequently, multiple clinical trials investigated the efficacy of RDN in addition to PVI to lower AF recurrence. To this end, this analysis aimed to analyse the published literature to compare the effect of RDN and PVI on AF recurrence, blood pressure and estimated glomerular filtration rate (eGFR) in hypertensive patients. Secondarily, the study aimed to examine the overall safety of the combined techniques.

Materials and methods

This study utilised the Preferred Reporting Items for Systematic Reviews and Meta-Analyses (PRISMA) guidelines and Revised Assessment of Multiple Systematic Reviews guidelines to perform and design the review [11, 12]. This included using an a priori study design; exhaustive literature search; duplication of study screening, selection and data extraction; scientific quality and bias assessment of included studies; reporting of study characteristics and utilising appropriate statistical methods for assessment of study findings [11, 12].

Literature search and inclusion criteria

Two authors searched three online databases (MEDLINE, PubMed, and Embase) for papers published from January 1, 2009, to June 1, 2021, using the following combination of keywords: RDN, renal sympathetic denervation, catheter-based RDN, kidney denervation, renal artery denervation. Studies that were retrieved from the initial database search were published in English and from human trials. Additionally, any missed studies were included into screening following a full reference screen of relevant studies. The inclusion criteria were as follows: (1) Original research articles, (2) published after January 1, 2009, in English language, (3) Level I or Level II prospective comparative studies that (4) assessed the effect of RDN on AF in patients with essential HTN that are undergoing PVI. The exclusion criteria were as follows: (1) Studies that assessed patients with secondary HTN, (2) type I diabetes mellitus, (3) late-stage kidney disease/failure (mean eGFR <45 mL/min per 1.73 m2), (4) congestive heart failure, (5) left-ventricular ejection fraction (LVEF) < 35% (6) studies published in non-English language.

Literature screening

The studies were screened during the three stages (title, abstract and full-text screen) independently and in duplicates by two authors (KN and AM). Disagreements were internally discussed before moving to the subsequent stage of screening. A PRISMA flow chart of the literature screening is shown in Fig. 1 [12].

Fig. 1. PRISMA chart.

Fig. 1

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Flow chart outlining the screening process for the included/excluded studies and detailing the results following each screening stage.

Quality assessment of included studies

The Cochrane risk of bias (ROB) tool was used to assess quality and publication bias of the individual studies that were randomized (The Cochrane Collaboration, Copenhagen, Denmark) (Supplementary Fig. 1). Studies that were non-randomized but prospective were assessed for quality and publication bias using The Methodological Index for Non-Randomized Studies (MINORS) [13] (Supplementary Table 1).

Interviewer agreement

The Kappa (k) scores were used at each stage of the screening process in order to determine inter-rater reliability as well as agreement [14]. The k scores were all above the 0.6 threshold which indicates strong inter-rater reliability [14].

Data extraction

Two authors (KN and AM) independently collected and extracted data into a standardized form, in Excel 2019 (Microsoft, Redmond, WA, USA). The following information, if available, was extracted from the studies: primary author and year, study design and purpose, sample size, age and gender information, country of study, follow-up time frame, baseline study sample characteristics (number of HTN medications, eGFR, presence of type II diabetes, coronary artery disease (CAD), LVEF, and left-atrial diameter (LAD), AF type, and systolic and diastolic blood pressure), follow-up data on AF recurrence and blood pressure, and safety complications.

Data analysis

This analysis primarily aimed to compare the effects of RDN on AF recurrence in hypertensive patients that were undergoing PVI for treatment of AF. The main outcomes were AF recurrence, the blood pressure lowering effect of RDN as well as the effect of RDN of eGFR. AF recurrence was defined as episodes of atrial tachyarrhythmias lasting >30 s during the follow-up period. Secondarily, the analysis aimed to assess the safety, efficacy, and sustainability of RDN.

The pooled analysis of quantitative results was synthesized using RevMan 5.3 (The Cochrane Collaboration, Copenhagen, Denmark). Pooling of data was conducted using a random effects model and study weighing was based on inverse variance. A minimum of three studies was required for outcome pooling. To assess for heterogeneity due to differences in study methods and populations, the I2 values were used [15]. Moreover, a sensitivity analysis was performed in analyses showing a high heterogeneity of I2 > 65% by removing each study separately and examining the effect on the I2 value [16].

Treatment effects for dichotomous variables were compared using risk ratios (RR) and 95% confidence intervals (CI), and those for continuous variables were compared using mean difference (MD) and 95% CI. For studies that did not report standard deviations (SD), the values were estimated according to the guidelines outlined in the Cochrane Handbook for Systematic Reviews [16].

Results

Literature screen and baseline study characteristics

Figure 1 is a PRISMA chart demonstrating the results of the literature search. Table 1 outlines the characteristics of the six included studies [1722]. Table 2 summarizes the inclusion criteria, as well as the procedural methods employed by the studies.

Table 1.

Baseline characteristics of included studies.

Study Author (Year) Turagam-HFIB 2 (2021) [22] Turagam-HFIB 1 (2021) [22] Steinberg et al., (2020) [21] Kiuchi et al.,(2018) [20] Kiuchi et al., (2017) [19] Kiuchi et al., (2016) [18] Pokushalov et al., (2014) [17]
Study design RCT RCT RCT RCT Prospective Non-randomized RCT RCT
Country USA USA Germany, Poland, and Russia Brazil Brazil Brazil USA, Russia
F/U period (months) 24 24 12 12 22.4 ± 4.10 12 12
Study groups PVI + RDN PVI PVI + RDN PVI PVI + RDN PVI PVI + RDN PVI + Spironolactone PVI + RDN PVI PVI + RDN PVI PVI + RDN PVI
Number of patients 28 22 13 17 154 148 33 36 39 96 21 24 41 39
Age 64.0 ± 7.00 65.0 ± 8.00 59.0 ± 10.0 68.0 ± 9.00 59 (IQR 54–65)a 60 (IQR 58–65)a 56.8 ± 6.50 58.4 ± 5.10 60.0 ± 14 59.0 ± 15.0 68.0 ± 9.0 66.0 ± 9.0 56.0 ± 6.00 56.0 ± 6.00
Number of females 12 8 5 8 63 57 8 6 15 31 8 8 10 15
Number anti-HTN drugs 2.80 ± 0.95 2.50 ± 1.00 2.80 ± 1.20 2.80 ± 1.30 2.10b 2.10b 3.50 ± 0.50 3.74 ± 0.40 2.20 ± 0.40 2.40 ± 0.50 3.41 ± 0.60 3.30 ± 0.50 3.40 ± 0.70 3.40 ± 0.80
% Patients with T2D 17.9 36.4 0.00 17.6 10.4 12.2 24.2 27.8 35.9 37.5 76.2 54.2 12.2 22.5
% Patients with CAD NR NR NR NR 9.10 6.80 15.2 25.0 NR NR 57.1 58.3 12.2 10.3
LAD (mm) 54.0 ± 0.90 47.0 ± 1.30 51.0 ± 0.90 46.0 ± 0.70 48.00 (CI 47.0,49.0)c 48.0 (CI 46.0,49.0)c NR NR NR NR 54.1 ± 3.20 44.9 ± 3.90 47.0 ± 5.00 47.0 ± 4.00
LVEF (%) 62.0 ± 6.00 64.0 ± 5.00 60.0 ± 6.00 61.0 ± 5.00 62.0 ± 5.00 62.0 ± 5.00 62.2 ± 7.20 61.2 ± 5.70 65.8 ± 12.8 66.5 ± 10.0 62.7 ± 6.60 63.5 ± 6.80 60.0 ± 4.00 61.0 ± 5.00
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Data for age, antihypertensive medications, left-atrial diameter, and left-ventricular ejection fraction are displayed as means and standard deviation (SD).

RCT randomized control trial, F/U follow-up, PVI pulmonary vein isolation, RDN renal denervation, IQR interquartile range, CI confidence interval, HTN hypertension, T2D type II diabetes, CAD coronary artery disease, LAD left-atrial diameter, NR not reported, LVEF left-ventricular ejection fraction.

aThis study reported data as median and interquartile range.

bStandard deviation could not be estimated for this study.

cThis study reported data as mean and confidence interval.

Table 2.

Criteria and intervention method of included studies.

Study Author (Year) Turagam-HFIB 2 (2021) [22] Turagam-HFIB 1 (2021) [22] Steinberg et al., (2020) [21] Kiuchi et al., (2018) [20] Kiuchi et al., (2017) [19] Kiuchi et al., (2016) [18] Pokushalov et al., (2014) [17]
Study population

• Paroxysmal and persistent AF

• Drug-resistant HTN (Office SBP ≥ 160 or DBP ≥ 100)

• At least 1 antihypertensive

• eGFR>45

• Paroxysmal and persistent AF

• Drug-resistant HTN (Office SBP ≥ 160 or DBP ≥ 100)

• At least 1 antihypertensive

• eGFR>45

• Paroxysmal AF

• Drug-resistant HTN (Office SBP ≥ 130 or DBP ≥ 80)

• At least 1 antihypertensive

• Paroxysmal AF or symptomatic refractory AF

• Drug-resistant HTN (ASBP ≥ 130, ADBP ≥ 80)

• At least 3 antihypertensive

• eGFR ≥60 and microalbuminuria

• Paroxysmal AF

• Drug-controlled HTN (130>ASBP ≥ 100)

• eGFR >15 (if eGFR>60 have microalbuminuria)

• Refractory paroxysmal or persistent AF

• Drug-controlled HTN (130>ASBP ≥ 100)

• eGFR between 30–89 and if >60 microalbuminuria

• Refractory paroxysmal or persistent AF

• Moderate drug-resistant HTN (Office BP ≥ 140/90) or severe drug-resistant HTN (Office BP ≥ 160/100)

• At least 3 antihypertensive (including 1 diuretic)

• eGFR ≥ 45
AF definition Persistent AF = AF ≥ 7 Days Persistent AF = AF ≥ 7 Days PAF = AF up to 7 days PAF = AF up to 7 days PAF = AF up to 7 days

PAF = AF up to 7 days

Persistent AF = AF ≥ 7 Days

PAF = AF up to 7 days

Persistent AF = AF ≥ 7 Days
% PAF 70.0 66.7 100.0 100.0 100.0 60.0 43.8
% Persistent AF 30.0 33.3 0.00 0.00 0.00 40.0 56.2
PVI method Radiofrequency ablation Radiofrequency ablation Cryoballoon catheter Radiofrequency ablation Radiofrequency ablation Radiofrequency ablation Radiofrequency ablation
RDN method Vessix ThermoCool Irrigated tip and RDN catheter EngligHTN Irrigated tip Irrigated tip ThermoCool (n = 20), Symplicity (n = 21)
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HTN hypertension, AF atrial fibrillation, SBP systolic blood pressure, DBP diastolic blood pressure, ASBP ambulatory systolic blood pressure, ADBP ambulatory diastolic blood pressure, eGFR estimated glomerular filtration rate, BP blood pressure, PAF paroxysmal atrial fibrillation, PVI pulmonary vein isolation, RDN renal denervation.

Units for blood pressure and eGFR are in mm Hg and mL/min per 1.73 m2 respectively.

The seven trials included a total of 711 patients, with 329 patients in the PVI + RDN group and 382 patients in the PVI-only group (Table 1). The mean age ranged between 56 ± 6 and 68 ± 9 years and a follow-up time ranging from 12 to 24 months (Table 1). There was a total of 623 patients with paroxysmal AF and 88 patients with persistent AF (Table 2).

Effect of RDN on AF recurrence

All the included studies reported the rate of AF recurrence throughout the follow-up period (Table 3). The rate of AF recurrence was significantly lower across five trials in the RDN + PVI group [1721]. Although the rates of AF recurrence were lower in the PVI + RDN groups of HFIB-1 and HFIB-2 trials, they failed to show a significant difference [22]. The overall pooled results of the recurrence of AF demonstrated a significantly lower rate of AF recurrence in the PVI + RDN (31.3%) group compared to the PVI-only (52.9%) group (p < 0.00001) (Fig. 2).

Table 3.

Atrial Fibrillation recurrence following interventions and baseline and 12-month follow-up blood pressure.

Study Author (Year) Study group % AF recurrence at follow-up Baseline SBP (mm Hg) SBP at follow-up (mm Hg) Mean difference (mm Hg) Baseline DBP (mm Hg) DBP at follow-up (mm Hg) Mean difference (mm Hg)
Turagam-HFIB 2 (2021)a [22] PVI + RDN 25.0 146.6 ± 20.6 138.2 −8.40 ± 25.1 81.4 ± 13.4 82.6 1.20 ± 12.4
PVI 27.3 143.4 ± 18.4 142.8 −0.60 ± 27.2 79.1 ± 12.4 80.8 1.70 ± 11.1
P-value NS NS ___ NS NS ___ NS
Turagam-HFIB 1 (2021)a [22] PVI + RDN 38.5 147.0 ± 31.0 152.3 5.30 ± 25.8 84.1 ± 25.0 84.7 0.630 ± 14.7
PVI 52.9 153.0 ± 20.0 144.4 −8.60 ± 24.1 88.0 ± 12.0 82.5 −5.50 ± 12.9
P-value NS NS ___ NS NS ___ NS
Steinberg et al., (2020) [21] PVI + RDN 27.9 150.0 ± 9.50 135.0 ± 9.50 −16.0 ± 12.663 90.0 ± 6.33 79.0 ± 9.50 −11.0 ± 9.50
PVI 43.2 151.0 ± 9.31 147.0 ± 9.31 −3.00 ± 15.5 90.0 ± 9.31 88.0 ± 9.31 −2.00 ± 15.5
P-value 0.006 NS ___ <0.0001 NS ___ <0.0001
Kiuchi et al., (2018)b [20] PVI + RDN 39.4 142.0 ± 6.00 123.0 ± 4.00 −19.0 ± 6.83 103.0 ± 8.00 82.0 ± 4 −21.0 ± 8.54
PVI 63.9 140.0 ± 6.00 130.0 ± 6.00 −10.0 ± -8.76 103.0 ± 7.00 89.0 ± 5.00 −14.0 ± 10.1
P-value 0.043 NS ___ <0.0001 NS ___ NS
Kiuchi et al., (2017)b [19] PVI + RDN 38.5 Controlled HTN Controlled HTN ___ Controlled HTN Controlled HTN ___
PVI 61.5 Controlled HTN Controlled HTN ___ Controlled HTN Controlled HTN ___
P-value 0.015 ___ ___ ___ ___ ___ ___
Kiuchi et al., (2016)b [18] PVI + RDN 23.8 Controlled HTN Controlled HTN ___ Controlled HTN Controlled HTN ___
PVI 75.0 Controlled HTN Controlled HTN ___ Controlled HTN Controlled HTN ___
P-value 0.001 ___ ___ ___ ___ ___ ___
Pokushalov et al., (2014) [17] PVI + RDN 36.6 163.0 ± 18.0 142.0 ± 11.0 −21.0 ± 20.0 89.0 ± 11.0 79.0 ± 5.00 −10.0 ± 11.6
PVI 59.0 164.0 ± 17.0 162.0 ± 10.0 −2.00 ± 22.8 88.0 ± 11.0 86.0 ± 5.00 −2.00 ± 13.7
P-value 0.046 NS ___ 0.0002 NS ___ 0.006
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Data for blood pressures are displayed as means and standard deviation (SD).

PVI pulmonary vein isolation, RDN renal denervation, AF atrial fibrillation, SBP systolic blood pressure, DBP diastolic blood pressure, NS not significant.

aBlood pressure data from these studies was at 12-month follow-up for comparison purposes.

bThese studies reported ambulatory blood pressure data.

Fig. 2. Effects of renal denervation on atrial fibrillation.

Fig. 2

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Forest plot of the pooled comparison between PVI + RDN and PVI alone in the rate of AF recurrence of all included studies. IV inverse variance, df degrees of freedom.

Effects of RDN on blood pressure

All included studies reported follow-up data on blood pressure following the procedure (Table 3). Two of the studies included patients with drug-controlled HTN and one reported blood pressure as ambulatory rather than office and thus were excluded from the meta-analysis [1820]. For the pooled analysis, 12-month follow-up data was used to compare changes in blood pressure. Two studies reported a significant reduction in both office systolic blood pressure (SBP) and diastolic blood pressure (DBP) in the PVI + RDN group vs. the PVI alone group [17, 21]. One study reported a significant reduction in ambulatory SBP in the PVI + RDN group vs. the PVI alone group [20]. When pooled, the overall results showed a significant MD in SBP of −9.42 mm Hg in the PVI + RDN group vs. the PVI alone group (p = 0.05) (Fig. 3A). The pooled DBP analysis failed to show a significant difference between the groups (p = 0.16) (Fig. 3C). The pooled analysis for both SBP and DBP showed a high heterogeneity of I2 value = 71% and 76% respectively.

Fig. 3. Effects of renal denervation on blood pressure.

Fig. 3

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Forest plot of pooled comparison of office BP between PVI + RDN and PVI (A) SBP (B) SBP sensitivity analysis after HFIB-1 removal (C) DBP (D) DBP sensitivity analysis after HFIB-1 removal. IV inverse variance, df degrees of freedom.

A sensitivity analysis was conducted by removing each study consecutively and assessing its effect on the SBP and DBP pooled analyses (Fig. 3B,D). Following the removal of HFIB-1, the results indicated a more strongly significant difference of p < 0.00001 for SBP and a significant difference of p = 0.006 for DBP demonstrating the superiority of the blood pressure lowering effect of the PVI + RDN group and the heterogeneity for both SBP and DBP decreased to I2 to 0% and 63% respectively (Fig. 3B, D).

Effect of RDN on eGFR

All studies reported eGFR at baseline, however, only four studies reported eGFR during the follow-up period (Table 4) [1720]. One of these studies only reported eGFR changes for the PVI + RDN group and was therefore excluded from the meta-analysis [17]. For the purposes of the pooled analysis, the eGFR was compared at the 6-month follow-up period (Fig. 4). The pooled analysis showed a significant MD of +10.22 mL/min/1.73 m2 significantly favouring the PVI + RDN group (p = 0.0007) (Fig. 4A). Sensitivity analysis was conducted due to the high heterogeneity, and the removal of Kiuchi 2017, led to a decrease in I2 from 96% to 0 and a stronger significant increase in eGFR following PVI + RDN compared to PVI alone (P < 0.00001) (Fig. 4B).

Table 4.

eGFR at baseline, 6-month, and 12-month of included studies.

Study Author (Year) Study group eGFR baseline (mL/min per 1.73 m2) eGFR 6-month (mL/min per 1.73 m2) Mean difference at 6-month (mL/min per 1.73 m2) eGFR 12-month (mL/min per 1.73 m2) Mean difference at 12-month (mL/min per 1.73 m2)
Turagam-HFIB 2 (2021)a [22] PVI + RDN >45a NR __ NR __
PVI >45a NR __ NR __
P-value NS __ __ __ __
Turagam-HFIB 1 (2021)a [22] PVI + RDN >45a NR __ NR __
PVI >45a NR __ NR __
P-value NS __ __ __ __
Steinberg et al., (2020) [21] PVI + RDN 79.0 ± 11.0 NR __ NR __
PVI 76.0 ± 11.0 NR __ NR __
P-value NS __ __ __ __
Kiuchi et al., (2018)b [20] PVI + RDN 69.2 ± 6.70 76.2 ± 7.20 7.00 ± 4.96 81.8 ± 6.8 12.6 ± 4.80
PVI 66.7 ± 7.70 66.4 ± 8.60 −0.300 ± 5.60 64.8 ± 9.9 −1.90 ± 6.33
P-value NS __ <0.0001 __ <0.0001
Kiuchi et al., (2017)b [19] PVI + RDN 47.9 ± 6.80 59.0 ± 5.00 11.1 ± 4.52 NR __
PVI 50.0 ± 5.40 46.0 ± 5.00 −4.00 ± 3.55 NR __
P-value NS __ __ __ __
Kiuchi et al., (2016)b [18] PVI + RDN 59.3 ± 13.3 64.9 ± 13.4 5.60 ± 9.49 65.7 ± 14.0 6.40 ± 9.73
PVI 60.5 ± 15.9 58.3 ± 14.0 −2.20 ± 10.3 56.6 ± 14.7 −3.90 ± 10.5
P-value NS __ NS __ <0.05
Pokushalov et al., (2014) [17] PVI + RDN 75.5 ± 9.2 80.9 ± 4.3 5.40 ± 6.63 NR __
PVI 77.0 ± 8.50 NR __ __ __
P-value NS __ __ __ __
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Data are displayed as means and standard deviation (SD).

PVI pulmonary vein isolation, RDN renal denervation, eGFR estimated glomerular filtration rate, NR not reported, NS not significant.

aThis study did not report baseline eGFR data but as per the inclusion criteria eGFR of all patients were greater than 45 mL/min per 1.73 m2.

Fig. 4. Effects of renal denervation on eGFR.

Fig. 4

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Forest plot of A pooled comparison of eGFR between PVI + RDN and PVI and B sensitivity analysis after removal of Kiuchi 2017. IV inverse variance, df degrees of freedom.

Complications

Five trials reported data on complications following the procedure and during the follow-up period in both the PVI + RDN group and the PVI alone groups [17, 2022], one reported complications only in the PVI + RDN group [18], and one study failed to specify the group in which the complications occurred and hence the rate could not be estimated for the PVI-alone group [19] (Table 5). HFIB-1 was excluded from the overall rates in both the RDN + PVI and PVI alone groups due to the early termination of study recruitment owing to a high rate of post-RDN renal vascular complications that might be attributed to the use of a non-FDA approved catheter [22]. The overall complication rate between the RDN + PVI and PVI alone group was 6.32% (n = 316) and 11.8% (n = 245) respectively.

Table 5.

Complications post-procedures during follow-up period.

Study Author (Year) Turagam-HFIB 2 (2021) [22] Turagam-HFIB 1 (2021) [22]a Steinberg et al., (2020) [21] Kiuchi et al., (2018) [20] Kiuchi et al., (2017) [19] Kiuchi et al., (2016) [18] Pokushalov et al., (2014) [17]
Study groups PVI + RDN PVI PVI + RDN PVI PVI + RDN PVI PVI + RDN PVI + Spironolactone PVI + RDN PVI PVI + RDN PVI PVI + RDN PVI
Femoral venous vascular events 2/28 0/22 0 1/17 6/154 4/148 0 0 0 0 0 NR 0 0
Transient phrenic nerve plasty 0 0 0 0 1/154 1/148 0 0 0 0 0 NR 0 0
Cardiac tamponade 0 0 0 0 0/154 1/148 0 0 0 4/?b 0 NR 1/41 0
Pneumothorax 0 0 0 0 0/154 1/148 0 0 0 0 0 NR 0 0
Hospitalization 0 0 0 0 8/154 18/148 0 0 0 0 0 NR 0 0
Death 0 0 0 0 2/154 2/148 0 0 0 0 0 NR 0 0
Stroke 0 0 0 1/17 0 0 0 0 0 0 0 NR 0 0
Renal artery stenosis 0 0 3/13 0 0 0 0 0 0 0 0 NR 0 0
Renal artery dissection in procedure 0 0 3/13 0 0 0 0 0 0 0 0 NR 0 0
Total 2/28 0/22 6/13 2/17 17/154 27/148 0 0 0 - 0 NR 1/41 0
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Data reported as number of events over sample size.

PVI pulmonary vein isolation, RDN renal denervation, NR not reported.

aThis study was terminated early due to a high rate of renovascular complications.

bFour cardiac tamponade events were reported in this study, but it was not clear which PVI group this occurred in.

Discussion

We examined the findings from six studies investigating the use of RDN in addition to PVI in the treatment of paroxysmal and/or persistent AF in 711 patients with HTN and AF. The pooled results from these studies showed the following in favor of the RDN and PVI treated group in comparison to PVI alone: (1) A significant reduction in the risk of AF recurrence at follow-up; (2) a significant reduction in SBP at 12-month follow-up; (3) a significant increase in eGFR at 6-month follow-up; (4) a low overall rate of complications in both groups both during the procedures and during the follow-up period.

Currently, the main treatment for HTN is often a combination of lifestyle and drug therapy. First-line agents according to the latest American College of Cardiology and American Heart Association guidelines include angiotensin-converting enzyme inhibitors (ACE-I), thiazide diuretics, and calcium channel blockers [23]. While various drug combinations, doses, and additional agents can be used to reach blood pressure targets, HTN remains the main risk factor for cardiovascular disease including AF and premature death worldwide [24]. Thus, there is a complex pathophysiological mechanism underlying chronic HTN that goes beyond first-line agents addressing the sodium/volume components of the renin-angiotensin-aldosterone system (RAAS).

Studies suggest that HTN can also have neurogenic roots as sympathetic nervous system (SNS) tone is higher in hypertensive patients as opposed to non-hypertensive patients [25]. Increased activity, particularly in the efferent renal nerves, leads to increased stimulation in both renal alpha and beta-adrenoceptors [26]. Stimulation of beta-adrenoreceptors of the juxtaglomerular apparatus increases renin secretion, which ultimately leads to increased systemic vascular resistance and thus arterial pressure [26]. Likewise, increased SNS tone has also been shown to reduce eGFR through the effects of alpha-adrenoceptors on the afferent arterioles [26]. Kidney damage such as due to chronic kidney disease (CKD) or drug-resistant/uncontrolled HTN has been shown to be a driver of increased SNS tone seen in neurogenic HTN [27].

RDN proposes ablation of the renal efferent and afferent nerves to interrupt the communication between the kidney and the autonomic nervous system and thus reduce blood pressure. SYMPLICITY HTN-3, the first of its kind, was a prospective, blinded, sham-controlled trial that included 367 patients and aimed to investigate the effect of RDN on HTN [28]. The trial failed to show any significant blood pressure lowering effects after ablation of the renal nerves [28]. However, it was found that there were many confounders that led to the null effect of SYMPLICITY HTN-3 such as adherence, antihypertensive medications, improper procedural methods, and a lack of operator experience [29]. These among others were addressed in recent trials, leading to significant blood pressure lowering effects of RDN seen in the SPYRAL HTN-ON/OFF MED and RADIANCE-HTN SOLO trials [3032]. These benefits of RDN were reiterated in a recent meta-analysis of 12 trials (n = 1539) and showed that catheter-based RDN is not only effective in the reduction of office blood pressure compared to sham or antihypertensive therapy alone but is also safe for patients [33]. Initially it was thought that RDN would be most efficacious in patients with drug-resistant HTN, but the lessons learned from SYMPLICITY HTN-3 and later trials suggested superior responses of RDN in patient with moderate and neurogenic HTN. Therefore, the ideal candidate for RDN is yet to be identified.

With recent trials supporting the revival of RDN, further findings have also emphasised the potential of its therapeutic uses beyond blood pressure lowering in HTN into AF treatment where HTN is an established risk factor. One of which is seen in a recent post-hoc study of 226 patients from SPYRAL HTN-OFF MED where RDN lowered renin and aldosterone during the follow-up period [34]. For the first time in a human model, the findings of this study established the interaction between RDN, renal sympathetic tone, and HTN [34]. Indeed the improved catheter technology as well as the increase in the sites and frequency of ablation within the renal vasculature has facilitated the utility of RDN beyond just treating HTN [29]. The use of RDN to treat AF can be further supported by various epidemiological studies, one of which (n = 1332) significantly showed that a reduction in SBP into lower hypertensive categories reduced the odds of AF recurrence [35]. The present study demonstrated, through a pooled analysis of literature, that in hypertensive patients with AF, when treated with either PVI alone or a combination of PVI and RDN, that the combined treatment group showed a significant mean reduction of SBP by 9.42 mm Hg (p = 0.05) and a reduction of DBP by 4.11 mm Hg (p = 0.16) at follow-up.

The pathophysiological link between HTN and AF is unclear. However, a review proposed that the link mainly stems from the structural changes associated with HTN, such as LV hypertrophy and LV systolic/diastolic dysfunction which subsequently lead to an increase in left-atrial pressure and fibrosis [36]. Simultaneously, the activation of RAAS further exacerbates those structural modifications and hence leads to electrical remodeling and AF [36]. This hypothesis was evident in our review, where the ablation of the renal nerves, and hence the reduction in sympathetic activation and consequently in RAAS activity, significantly reduced the recurrence of AF by more than 20% (compared to PVI and drug therapy alone), which outlines the involvement of RAAS and HTN in AF development and/or recurrence. Additionally, in one of the studies included in this review, subgroup-analysis of AF recurrence in moderate vs severe resistant hypertensive patients was conducted [17]. Results revealed that in moderate resistant HTN the average blood pressure reduction was −12.5/7.8 mm Hg following RDN and that the rate of AF recurrence was not significantly different between the groups [17]. However, in the severe resistant HTN group, average blood pressure reduction was −29.1/12.2 mm Hg and AF recurrence was significantly lower in the RDN group [17]. In a study by Grassi et al., it was demonstrated that there was a strong positive correlation between sympathetic activity and blood pressure [37]. The study revealed that control subjects had the lowest muscle sympathetic nerve activity compared to those with severe HTN [37]. This suggests that the greater reduction in blood pressure shown in the study by Pokushalov et al. might lead to either a stronger decrease in sympathetic activity or a decrease in sympathetic vascular tone or both, which might have therefore led to the superiority of the decrease in the rate of AF in the severe resistant HTN group [17].

Uncontrolled HTN has been implicated in the development of kidney disease with an average yearly decrease in eGFR of 0.5–2.7 mL/min/1.73 m2 [3840]. The activation of the SNS and RAAS have been identified as the main contributors in the development and progression of renal disease [41]. Therefore, it is clear that AF, HTN and CKD are interlinked and share multiple underlying pathophysiological processes. Interestingly, in one of the included studies in this review, it was noted that patients with CKD had an increased left-atrial volume compared to those without CKD, which therefore contributes strongly to the development of AF [19]. Owing to the hyperactivation of renal sympathetics and RAAS in patients with CKD, the addition of RDN to PVI yielded a stronger decrease in AF recurrence as well as an improvement of multiple structural cardiac parameters including left-atrial volume, LVEF, left-ventricular mass index and left-ventricular end-diastolic diameter [19].

The treatment efforts to dampen RAAS clinically, such as with pharmacological therapy, have failed to yield significant improvements in eGFR and CKD [41]. The progression demonstrated by RDN has led to multiple investigations on the topic and a recent meta-analysis of 11 non-randomized studies was conducted, looking at the effect of RDN in hypertensive patients with CKD [42]. The study mainly concluded that RDN was superior in reducing blood pressure and had no increase in the rate of decline in renal function in patients with CKD. Drawing upon the connection between AF, HTN and CKD, three of the included trials in this review sought to explore the effect of RDN on eGFR and CKD, in an attempt to elucidate the interplay between the outlined mechanisms [1820]. The pooled analysis showed that RDN significantly improved eGFR compared to PVI alone (MD = 10.2; p < 0.001). This may be explained in part by the reduction in sympathetic overdrive following RDN. Kiuchi et al. further noted that more rigorous methods of assessment of renal function should be used in future studies to clearly elucidate the effect of RDN on renal function and CKD [19].

Regarding the safety of RDN, a recent meta-analysis assessing renal function as a safety parameter included 52 quantitative and 14 qualitative studies and concluded that no adverse effects were present following treatment with RDN deeming it as a safe method for use in treatment of HTN [43].

Clinical implications

The present study, in addition to the aforementioned evidence outlines the critical interplay between HTN, AF and kidney disease, and given the high rate of AF recurrence following PVI alone, the development and consideration of incorporating RDN in addition to current therapeutic strategies to treat both HTN and AF is clinically justified. The pooled analysis further revealed that the use of RDN led to a significant increase in eGFR and hence supported the clinical application of this technology in the context of kidney disease.

Our study supplemented the extensive body of literature on the topic that proved that both procedural and follow-up complications of RDN are low and that the technology has proven to be safe and efficacious with an overall complication rate of 6.32%.

Limitations

Although multiple reviews have been published on the topic, they failed to account for patients that were concurrently included in multiple studies within the analysis, and have therefore duplicated patients [22, 4447]. In the 2014 trial by Pokushalov et al., it was stated that the cohort included the 27 patients from the 2012 trial (pilot study) [10, 17]. Furthermore, a trial published in 2017 by Romanov et al. involved the same cohort of patients from the previous 2014 trial by Pokushalov et al., but isolated patients that had cardiac monitor implantation [48]. Indeed, all previously published reviews contain either Pokushalov et al. 2012 and/or 2014 and/or Romanov et al. 2017 and thus incorporate duplicated patients and run the risk of misrepresentation of the data and lack robustness in the true assessment of the impact of RDN on AF and HTN. To this end, this is the first review reporting on the topic with a total of 711 patients as well as including the most recent data following the incorporation of the trials by Turagam et al., [22]. Moreover, our review was the first review on the topic to pool and meta-analyze the effect of RDN on eGFR in patients with HTN and AF.

This review has common limitations to all reviews/analyses as well as specific limitations pertaining to the included studies. Hence, the findings presented are based on the quality of the included studies. Although all studies were prospective, two of those were non-randomized [18, 19]. Furthermore, the reliability of the reported results depends on the consistency in inclusion criteria and the methods employed by the studies, including baseline characteristics, underlying comorbidities, definition of HTN (i.e., HTN cut-off values) and AF, number of antihypertensive and anti-arrhythmic drugs, catheterization and ablation methods, differences in follow-up times as well as methods to assess the outcomes during follow-up; all of which may have varied between the studies and hence might have affected the reliability and introduced heterogeneity in our results. The heterogeneity was combatted by conducting a sensitivity analysis. Finally, it is also worth noting that one of the included trials (HFIB-1) was terminated early due to an increase in renovascular complications, which may be owing to the use of a non-FDA approved catheter and hence caution should be exercised when assessing pooled outcomes that included the mentioned study [22].

Conclusion and future directions

This review demonstrated that the introduction of RDN to PVI in hypertensive patients with AF is more efficacious and superior to using PVI alone in treating AF. RDN + PVI was also shown to reduce SBP more significantly in patients with resistant HTN as well improve eGFR outcomes. Moreover, analysis of the safety of the technique proved it to be safe and hence the introduction of RDN to PVI should be considered clinically in patients with AF. Larger and longer-term trials are required to substantiate these findings including those that utilise sham-controls to improve robustness of the assessed outcomes. Future trials should also assess the effect of the autonomic reduction of blood pressure on AF and hence examine whether the effect of RDN on AF is dependent solely on autonomic reduction or if there is a mechanism independent of blood pressure that contributes to the improvement in AF.

Summary

What is known about topic?

  • There is an established interaction between renal denervation, renal sympathetic tone, and hypertension. The recent introduction of endovascular catchers to lower moderate/resistant hypertension has yielded promising results due to its ability to dampen the renin-angiotensin-aldosterone axis.

  • The success rate of pulmonary vein isolation in reducing atrial fibrillation is limited (20–50%). The significant morbidity associated with atrial fibrillation and the complex interaction of atrial fibrillation and hypertension has prompted the investigation of the additive benefit of renal denervation, with preliminary results of multiple trials demonstrating the superiority of such method in improving outcomes compared to conventional therapy.

What this study adds?

  • The pooled analysis demonstrates that combined renal denervation and pulmonary vein isolation reduces atrial fibrillation recurrence compared to pulmonary vein isolation alone. This supports the inclusion of renal denervation in the management of atrial fibrillation. The overall safety of the technique has proven it to be safe and efficacious.

  • The analysis outlines the critical interplay between atrial fibrillation, hypertension, and kidney function, and demonstrates the significant blood pressure lowering effect of renal denervation.

  • Renal denervation was also shown to have a significant effect on kidney function via an improvement in estimated glomerular filtration rate, which is hypothesized to be due to the dampening effects on the renin-angiotensin-aldosterone axis.

Supplementary information

Supplementary Table S1 and Figure S1 (34.9KB, pdf)

Author contributions

KN and AM equally conducted the literature search and determined studies for inclusion and exclusion. KN and AM equally extracted data from the studies included, performed the meta-analysis, and drafted the manuscript. MA, EJJ, KN, and AM conceived the idea of the study, designed the study, and critically revised the manuscript for important intellectual content. All authors gave final approval of the version to be published and agreed to be accountable for all aspects of the work.

Funding

Open Access funding provided by the IReL Consortium.

Competing interests

The authors declare no competing interests.

Footnotes

Publisher’s note Springer Nature remains neutral with regard to jurisdictional claims in published maps and institutional affiliations.

These authors contributed equally: Khaled Nawar, Ahmed Mohammad.

Supplementary information

The online version contains supplementary material available at 10.1038/s41371-022-00658-0.

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Supplementary Materials

Supplementary Table S1 and Figure S1 (34.9KB, pdf)

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