New-onset atrial fibrillation after percutaneous patent foramen ovale closure: a meta-analysis

We performed an electronic search of the bibliographic databases (MEDLINE, EMBASE, and Cochrane Database of Systematic Reviews) and hand-searching of reference lists. We used the following search terms “patent foramen ovale”, “PFO”, “atrial fibrillation” and “AF”, and connected these terms with Boolean operators. The first search was conducted on April 1, 2022. The last search update was carried out on November 21, 2022. No restrictions on publication date or study size were applied.

The study selection was independently performed by two reviewers (DJ, ER). In case of any disagreement, this was resolved by consensus with the senior authors (TS, CF). We included all publications fitting the following inclusion criteria: retrospective, prospective and randomised controlled trials reporting on AF after PFO closure, type of device and AF screening method. Articles published in either German or English were eligible for analysis. Main study reports as well as any supplementary appendices were reviewed.

AF incidence after percutaneous PFO closure was defined as primary outcome of this meta-analysis.

We extracted data on AF incidence from randomised and non-randomised trials and, if available, device-related AF incidence according to AF screening method and subsequent AF management strategies.

Random effects meta-analyses were performed using the Mantel–Haenszel method for dichotomous data to estimate pooled odds ratios (ORs) and confidence intervals (CI). Weights were calculated using Mantel–Haenszel methods. Furthermore, the I² statistics to quantify possible heterogeneity was calculated (I² < 30%: low heterogeneity; 30% < I² < 75%: moderate heterogeneity; I² > 75%: considerable heterogeneity; Review Manager 5.4, Nordic Cochrane Centre, Cochrane Collaboration). We defined P < 0.05 as a statistically significant difference. The level of evidence of the original trials was evaluated according to the criteria of the Oxford University [16]. To assess the studies’ quality, we judged the individual and overall risk of bias. The risk of bias was assessed by RoB2 tool provided by the Cochrane Collaboration in randomised trials [17]. We used the ROBINS-IAQ8 (Risk of Bias in Non-randomised Studies of Interventions) tool to evaluate non-randomised trials [18]. Two reviewers independently judged the risk of bias according to the given criteria (E. R. and D. J.)

First, we decided to take 45 days as a distinctive cut-off for early or late onset of atrial fibrillation because it was chosen in in the EAPCI position paper [2]. During the study selection and data extraction process, it turned out that most studies chose the first ECG follow-up after one month. Therefore, it was changed for the analysis in the second step to one month. The AF screening method was divided into high quality and low quality. The first included only Holter-ECG and/or external loop recorders (ELR). The latter was at least a structured 12-lead ECG follow-up. Additional symptom-led Holter-ECGs defined an intermediate group of opportunistic AF screening created post hoc.

We did not obtain ethical approval for this meta-analysis because we did not collect data from individual human subjects. The study was registered on PROSPERO (CRD42022359945).

Six randomised controlled (RCT) and two non-randomised controlled trials were eligible for quantitative analysis of AF incidence after percutaneous PFO closure [3, 4, 7, 10, 19‐22]. These eight studies reporting on 3745 patients included exclusively patients after cryptogenic stroke and TIA with proven PFO. Patients undergoing percutaneous PFO closure were compared to conservative comparator treatment. Medication strategies included either antiplatelet therapy [10, 19, 22] or oral anticoagulants (OAC) in a minority of cases. The results were published from 2008 to 2021. The mean age of the patients within each trial was 42.9–51.8 years and 45–65% were male. Only the two oldest trials had a systematic approach in AF detection using event loop recorders, but a limited follow-up period of 6 and 12 months [7, 19]. The others had structured ECGs and rarely Holter-ECG for symptomatic patients, though, for a long mean follow-up duration of 2.0 to 5.9 years. Burow et al., PC, RESPECT and DEFENSE-PFO used the Amplatzer PFO device [4, 19‐21], CLOSURE I the Starflex (NMT) [3], REDUCE the Gore Helex and Cardioform [10]. In CLOSE [22] and Bonvini et al., the operators chose different devices that were most suitable.

Pooled data analyses of these eight studies showed 99 AF events within the PFO closure group consisting of 1,953 patients in comparison to 28 events within in the placebo-controlled group consisting of 1,792 patients. The AF incidence was 5.1% vs. 1.6% in favour for conservative treatment (N = 8 trials, OR 3.17, 95% CI 1.46–6.86, P = 0.03, I² = 55%, Fig. 3).

Bild vergrößern

According to the study designs, different approaches in detection of AF after percutaneous PFO closure were chosen. Amongst the 24 studies, the screening of AF was conducted in distinctive levels of quality.

Throughout the 24 studies, the Amplatzer PFO Device (Abbott) was mostly used in 49.5% of all cases. Helex (Gore), CardioSEAL (NMT), Starflex (NMT) and Premere (St. Jude Medical) were second, third, fourth and fifth with 15.4%, 11.2%, 9.4% and 7.2%, respectively. Further devices Cardioform Septal (3.8%, Gore), Ultrasept (2.0%, Cardia), Figulla (0.9%, Occlutech), BioSTAR (0.4%, NMT), Sideris and Solysafe (each 0.1%, the latter Swissimplant AG) were not compared due to low implantation numbers (n = 565, 7.4%). Additional information is available in the supplementary table 1. Due to the varying study designs, a direct head-to-head comparison was not feasible. Ranges of AF incidence and total events are also divided in early and late onset. Not all studies reported AF events for the used devices (n = 16).

The average AF incidence can be compared amongst the frequently used devices (Table 4). Early-onset AF was reported in 0.9% of cases for Amplatzer, 0.7% for Helex, 4.2% for CardioSEAL, 4.5% for Starflex and 2.1% for Premere. Late-onset AF incidence was reported in 1.5% of cases for Amplatzer, 1.3% for Helex, 2.0% for CardioSEAL, 2.5% for Starflex and 0.7% for Premere.

Overall, 307 patients had documented AF episodes during follow-up (Table 5). Of these, 172 had detailed information of AF management. Spontaneous conversion was documented in 44 patients. Rhythm control strategy by either medical or electrical cardioversion was chosen in 111 patients. Two patients underwent catheter ablation, and two other patients were treated with surgical LA ablation. Rate control strategy was preferred in 17 patients. In 72 individuals were data on treatment with OAC after detection of AF available, 56 patients on long-term therapy.

For the whole study cohort of 7643 patients, the cumulative incidence of TIA and stroke was 1.9%, summarising all events since implantation. Only four studies [3, 10, 30, 32] reported six patients with ischaemic events after detected AF episodes.

Consistently, the separate tables of AF screening quality showed similar results. The high-quality studies [7, 19]had the highest AF incidences in the entire study cohort with 6.5–15%. The latter was detected in the Amplatzer device, which was in contrary associated with almost lowest AF incidence in all other trials. A recent study in patients with higher cardiovascular risk factors and age older than 55 years showed an overall high incidence of 20.9% (AF, atrial flutter and supraventricular arrhythmia) within the first month after implantation, using high-quality loop recorder screening [35]. Wagdi et al. demonstrated a presuming high rate of 25% with Occlutech device [6]. No AF was detected in two other trials [11, 30]. The device type made up 1% of all 24 studies. Despite the methodological limitations of the comparison, new onset AF is obviously more likely detected by high-quality screening method regardless of onset.

Device association of peri-interventional AF has been previously investigated [6‐8, 10, 11, 35]. Potential mechanisms are local irritation of atrial myocardium, implantation itself or device size and configuration. Higher AF risk following interventional PFO occlusion in patients with larger PFO or presence of atrial septal aneurysm was postulated by some authors [6‐8, 35]. Device size, age or sex was associated with heterogeneous effects on AF incidence [8, 10, 11, 35]. To date, evaluation of predictors for AF following PFO closure is limited to few studies. Given the observed high incidence in the occlusion group, future studies should systematically investigate these risk factors for individual decision making or risk factor modification in each patient.

Most frequently implanted devices were compared. 16 studies that documented AF events for implanted devices showed presumingly higher AF rates for CardioSeal and Starflex devices regardless of onset compared to the Premere, Helex and Amplatzer. Previous meta-analysis by Vukadinovic et al. showed lower AF incidence in Amplatzer vs. two Gore Devices in REDUCE [14]. However, Amplatzer had the highest rate in Burow et al. with 15% in ELR screening, other studies reached up to 3.6% in late onset. This rather supports a high-quality screening strategy and underlying mechanisms of AF development [36].

Occult AF might play a major role, former screening strategies were less continuous. 25% of patients with cryptogenic stroke have undetected AF [37]. However, a temporal relationship between stroke and AF onset is difficult as shown by device-monitored patients suffering from strokes and recording AF. In ASSERT, subclinical AF was detected in 8% preceding their stroke, 16% after the event [38]. Therefore, thorough screening according to the guidelines before, during and after percutaneous PFO closure is recommended. Due to the results of the highest AF incidence within one month after implantation, the hypothesis of temporary inflammation seems to be more likely to explain the new onset of AF than a chronic condition. Current guidelines recommend at least 24 h of short-term ECG followed by 72 h of continuous ECG in patients with acute stroke or TIA and previously unknown AF. In this population of cryptogenic strokes, a more extensive AF rule-out must be performed, and a PFO might appear as an innocent bystander. In these 24 trials, only 15 gave details about their rule-out strategy and 12 fulfilled the guideline recommendations. In conclusion, we propose a standardised AF rule-out protocol (Fig. 4). Based on the results, we would recommend a basic screening of 72 h Holter-ECG and, if available, a wearable to detect AF before, during and after the procedure. In the presence of additional cardiovascular risk factors or symptoms, an advanced AF screening with 7 days Holter-ECG or Loop Recorder should be performed before the implantation.

Bild vergrößern

Stroke and Prevention.

The incidence of recurrent neurological events was 1.9% in this study group over the whole duration. OAC can be administered as an alternative. Several studies were performed in the field of embolic stroke of undetermined source. Four studies showed neutral results in recurrent stroke reduction comparing ASS to OAC, including Warfarin [39], Rivaroxaban [40], Dabigatran [41] and Apixaban [42]. Systematic AF screening with consequent OAC in prevention of stroke was lately studied in STROKESTOP [43] and LOOP [44], where no clinical benefit in primary prevention was found. However, the patients were older, and had higher cardiovascular risk profiles compared to the PFO cohort. An algorithm for post-PFO closure AF was proposed by Elgendy et al., led by differentiation in primary and secondary AF. Long-term OAC was recommended for primary AF, short-term in secondary AF [12].

Both, AF rule out before PFO closure and AF follow-up strategies are performed heterogeneously due to a lack of standardised protocols. In one-third of the trials, the AF rule-out strategy was not documented in detail. Moreover, large RCTs on differentiation of AF surveillance strategies are missing. Device comparisons were statistically not possible according to different study designs.