Abstract
Introduction
Limited data exist on the outcomes after left atrial appendage closure (LAAC) with the Amplatzer™ Cardiac Plug (ACP; St. Jude Medical, Minneapolis, MN, USA) in patients with atrial fibrillation (AF) with very high stroke and bleeding risks, the subset expected to benefit most from this procedure. The objective of this study was to report clinical outcomes after LAAC with the ACP device in a very high stroke and bleeding risk cohort of patients with non-valvular AF and contraindications to oral anticoagulation (OAC).
Methods
LAAC using the ACP device was performed in 96 patients with AF who had median CHA2DS2-VASc and HAS-BLED scores of 5 and 3, respectively. Post-procedure, patients received dual antiplatelet therapy for 6 months. A transesophageal echocardiography (TEE) was scheduled at 6 months.
Results
Procedural success was 100%. Procedural-related complications occurred in 7.3% (pericardial effusion, 4.2%; thromboembolic events, 2.1%; device embolization, 1.0%). Additional thromboembolic events occurred in three patients during follow-up (92.7% follow-up). After 93.4 patient-years of follow-up, the annual rates of thromboembolic and major bleeding events were 3.2% and 1.1%, respectively. In those with TEE follow-up (70%), complete LAAC with no leaks was observed. Thrombus formation on the device was noted on TEE in two patients.
Conclusion
LAAC using the ACP device was associated with an acceptable low rate of embolic and bleeding events after a median follow-up of 9 months in a cohort of patients with AF who were amongst the highest stroke and bleeding risks reported so far in LAAC trials.
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Introduction
Embolic stroke is a serious complication in patients with atrial fibrillation (AF) [1]. Oral anticoagulation (OAC) is effective in reducing rates of thromboembolism, albeit with an increased bleeding risk [2, 3]. To identify patients with a significant risk of stroke and bleeding different risk stratification scores have been developed. Whereas the CHA2DS2-VASc score is recommended to evaluate the individual stroke risk in patients with AF, the HAS-BLED score was developed to assess the risk of bleeding during anticoagulation treatment [4]. Clinical trials have established the predictive value of these scores [5]. In day-to-day clinical practice, patients with the highest risk of stroke are those with a previous stroke, and patients with the highest risk of bleeding are those with a previous bleeding episode, especially the elderly. As risk factors for stroke and bleeding commonly overlap, management of patients with AF is still a clinical challenge and many patients at highest risk for stroke are not treated with OAC, even after the introduction of direct thrombin and factor Xa inhibitors.
New interventional therapies have been developed for stroke prevention in non-valvular AF. As about 90% of the thrombi originate from left atrial appendage (LAA) [6], LAA closure (LAAC) devices were developed to prevent thromboembolic events and to avoid long-term OAC.
Of these LAAC devices, the Watchman™ device (Boston Scientific, Marlborough, MA, USA) is the one that has been well studied. A recent meta-analysis has provided supportive data for the efficacy and safety of intervention with this device in patients with AF [7]. However, the observed effects were not uniformly in favor of the Watchman device: When compared with warfarin therapy at 2–3 years’ follow-up, LAAC was associated with a decreased likelihood of hemorrhagic stroke, cardiovascular death, and non-procedural bleeding, while the rates of ischemic stroke were higher [7]. The most commonly used device in Europe is the Amplatzer™ Cardiac Plug (ACP; St. Jude Medical, Minneapolis, MN, USA). A few studies that have been published with the ACP indicate a safe implantation with low rates of procedural-related complications [8–11]. Recent reports also suggest a reduction of stroke risk when compared to the expected stroke rate based on the CHA2DS2-VASc score [9–11].
Theoretically, the benefit of LAAC therapy should be more pronounced in patients with higher stroke and bleeding risks. The aim of the current analysis was to assess safety and efficacy of LAAC with the ACP device in a cohort of very high stroke and bleeding risk patients with contraindications for OAC.
Methods
This was a retrospective observational cohort analysis of a single German center database of LAAC with the ACP device. Patients with non-valvular-AF, a CHA2DS2-VASc score ≥2, and contraindications to OAC therapy including previous major bleeding, thromboembolic events while on OAC, high tendency to fall, intolerance and non-compliance to OAC, and labile international normalized ratio (INR) were included.
The study cohort comprised 96 consecutive patients, who underwent LAAC with the ACP between March 2009 and December 2014.
Procedure
Prior to the procedure, transthoracic and transesophageal echocardiography (TTE and TEE, respectively) were performed to exclude intracardiac thrombi, determine LAA anatomy, and record baseline parameters.
The procedure was performed under mild sedation (intravenous propofol and midazolam) with angiographic and TEE guidance. Access to the left atrium (LA) was gained by transseptal puncture using a Brockenbrough needle (Cook Medical, Bloomington, IN, USA) and a transseptal sheath (Cook Medical). Septum was imaged by TEE in a bicaval and a short axis view, and an inferior and posterior site was chosen for optimal LAA access. After puncture, heparin was administered at a dose of 70–100 U/kg to achieve an activated clotting time of at least 250 s. The sheath was then introduced into LAA and angiography performed by manual contrast injection. LAA measurements were obtained by TEE and angiography (Fig. 1a). In different projections, diameters of LAA ostium, landing zone, and length were taken. Sizing was based on the dimensions of the landing zone. The device was oversized by about 4 mm with respect to the LAA landing zone.
Then, the ACP device was introduced and placed in the LAA using a dedicated delivery system, the Amplatzer TorqVue™ 45° × 45° delivery sheath (AGA Medical Corp., Plymouth, MN, USA). Before releasing the device, stability was assessed (Minnesota wiggle maneuver, TEE, and angiographic evaluations; Fig. 1b, c). Assessments were made for any pericardial effusion during the procedure.
In all cases, intravenous ciprofloxacin (400 mg) was administered during the procedure. Dual antiplatelet therapy (DAPT) consisting of aspirin (100 mg) and clopidogrel (75 mg) were given for at least 6 months unless there was a contraindication. After 6 months, single antiplatelet therapy was recommended lifelong. Postprocedural TTE evaluation was done to rule out pericardial effusion and to confirm proper device position.
Follow-up
Clinical follow-up was carried out during hospital visit or through phone contact at 6 months and 1 year. Patients were scheduled a TEE at 6 months follow-up to assess the presence of a thrombus and a residual leak (mild <1 mm, moderate 1–3 mm, severe >3 mm).
Endpoints
Procedural success was defined as successful implantation of the ACP in LAA with no residual leak by angiographic and echocardiographic evaluation.
Complications that occurred during the procedure/hospitalization and during the clinical follow-up were documented. They were defined as: thromboembolic event (transient ischemic attack (TIA), stroke, and systemic embolism), major bleeding (Bleeding Academic Research Consortium [BARC] type ≥3b) [12], device embolization, myocardial infarction, and all-cause mortality.
Statistical Methods
Continuous variables were expressed as mean ± standard deviation and as median (interquartile range) depending on the data and its distribution. Categorical variables were reported as counts (percentages). Efficacy of the device to prevent thromboembolic events was tested by comparing the actual event rate at follow-up with the CHA2DS2-VASc score [4, 5] estimated event rates. The average annual risk for the whole study population was calculated. The total number of thromboembolic events during follow-up period was divided by the total patient-years of follow-up and was multiplied by 100 to get the actual annual rate of thromboembolism. Risk reduction of thromboembolism was calculated as follows: (estimated percent event rate−actual percent event rate)/estimated percent event rate.
Bleeding risk reduction was assessed analogous to stroke risk reduction. The annual event rate at follow-up was compared with the HAS-BLED score [13, 14] estimated event rates. Comparisons between observed and predicted thromboembolic and bleeding event rates were assessed using binomial tests. Rate ratios with 95% Poisson exact confidence intervals of observed and expected rates were also calculated. STATA® version 14 (StataCorp LP, College Station, TX, USA) and GraphPad Prism® 6 (GraphPad Software, Inc., La Jolla, CA, USA) were used for the statistical analysis.
Compliance with Ethics Guidelines
All procedures followed were in accordance with ethical standards of the responsible committee on human experimentation (institutional and national) and with the Helsinki Declaration of 1964, as revised in 2013. Informed written consent for the procedure was obtained from all patients.
Results
A total of 96 consecutive patients were included in this study. Patient’s baseline characteristics are summarized in Table 1. Mean age of the study population was 76 ± 7 years and 39.5% were female. AF was permanent in 52%, persistent in 25%, and paroxysmal in the remainder. Sixty-three patients (65.5%) had a previous stroke and 59 patients (61.4%) had a history of major bleeding. One-fifth of the patients had a concomitant history of stroke and bleeding. The median (interquartile range) CHA2DS2-VASc score was 5 (4.25–7) and the median (interquartile range) HAS-BLED score was 3 (3–4). A history of major bleeding was the principal contraindication for OAC and consequent LAAC. Other indications for LAAC were high tendency to fall (n = 12, 12.5%), and intolerance as well as non-compliance for OAC (n = 6, 6.2%). Notably in 16 (16.6%) patients, LAAC was performed because of thromboembolic events while on OAC.
Procedural Outcome
Successful device implantation was achieved in all patients (n = 96, 100%). The mean procedural time was 46 ± 5 min. The most commonly used device size was 24 mm (n = 34, 35.5%). LAAC was possible with the initial chosen device in 91 patients (95%). In five patients, device release criteria were not met and another device size was chosen (smaller sized device in four cases). LAAC was not combined with other procedures.
Procedural-related complications occurred in seven patients (7.3%) and are listed in Table 2. Pericardial effusion requiring pericardiocentesis was the most common complication and occurred in four patients (4.2%). None of the patients required surgical intervention. Device embolization occurred in one patient; the device embolized into the LA (Fig. 2), where it was snared out, reintroduced and successfully implanted.
There were two cases with a thromboembolic event (2.1%): One TIA (this was associated with device embolization) and one stroke that was attributed to hypotension. There were no procedural-related myocardial infarctions or deaths.
Follow-up Outcomes
Clinical follow-up was available in 89 patients (92.7%) with a median (interquartile range) follow-up duration of 9 months (6–18 months). Eighteen patients (20%) were followed up for more than 20 months, and for 35 patients (39.3%) at least 1-year follow-up was available.
After 93.4 patient-years of follow-up, a total of 13 events (14.6%) were recorded (Table 3). Three of them were thromboembolic events: One TIA and two strokes. One TIA occurred after 18 months in an 89-year-old male patient who had a previous ischemic stroke (CHA2DS2-VASc score = 6) as well as an intracranial bleeding event (HAS-BLED score = 5). TEE did not reveal thrombus on the device.
In a 76-year-old female patient with previous stroke (CHA2DS2-VASc score = 5), cranial computed tomography showed a sub-acute posterior inferior cerebellar arterial (PICA) and superior cerebellar artery (SCA) infarction on the left side 20 months after ACP implantation. This patient had no TEE follow-up. Cardioembolic stroke was the clinical diagnosis made by neurologists in both these cases.
Another patient, a 75-year-old with previous history of stroke (CHA2DS2-VASc score = 5), had a recurrent stroke 14 months after ACP implantation while on aspirin. Magnetic resonance imaging confirmed an acute right-sided thalamic infarct and showed microangiopathic disease. TEE did not reveal thrombus on the device in this patient as well.
Major bleeding occurred in one patient at follow-up. An 82-year-old male with a HAS-BLED score of 5 experienced an intracranial bleeding, caused by a fall 26 months after device implantation, while on aspirin. One patient experienced a clinically significant pericardial effusion 11 months after the procedure. A total of nine patients died during follow-up (Table 3).
TEE Outcomes
Sixty-two patients (70%) with clinical follow-up had a TEE evaluation after a mean duration of 8.6 months. None of the patients had a residual leak. Thrombus formation on the device was observed in two cases (3.2%), 5 and 6 months after LAAC. Both of them were on DAPT. The presence of thrombus did not correlate with a clinical event. In both of the patients, thrombus resolved after 5 and 6 weeks of OAC therapy.
Discussion
The prevention of thromboembolism is the most important therapeutic goal in patients with AF. Vitamin K antagonists (VKA) effectively reduce strokes rates [2], but as individual stroke and bleeding risks increase in parallel, physicians face a therapeutic dilemma concerning their use in very high stroke and bleeding risk patients.
One effective alternative to VKA are the novel oral anticoagulants (NOACs), i.e., dabigatran, rivaroxaban, apixaban, and edoxaban [15–17], whose main toted benefit in comparison to VKA is reduction of intracranial bleeding. But major bleedings still occur with these agents, especially in the elderly with renal impairment, and so far specific antidotes such as idarucizumab [18] are still in their investigational stage or undergoing phase three trials. In this context, the non-pharmacological treatment option of LAAC—which offers simultaneous advantages of stroke reduction as well as avoidance of long-term OAC—gains prominence.
The PLAATO System (ev3, Plymouth, MN, USA) was the first dedicated LAAC device [19]. This device was succeeded by the Watchman device, whose safety and efficacy were proved in two large randomized trials. The PROTECT AF (ClinicalTrials.gov identifier, NCT00129545) [20] and the PREVAIL (ClinicalTrials.gov identifier, NCT01182441) [21] trial were non-inferiority trials that evaluated the Watchman device compared with warfarin in patients with AF who were eligible to take OAC. As stroke prevention strategies are particularly challenging in patients who are ineligible to take OAC, the ASAP study (ClinicalTrials.gov identifier, NCT00851578) [22] was designed. This small, non-randomized trial documented a reasonable safety profile over short-term follow-up for the Watchman device.
Current available data with the ACP are derived from several small, observational studies [8–11]. In contrast to the Watchman trials, most of the patients enrolled in these studies were not suitable for long-term OAC and were treated with DAPT post-implantation. The largest conducted study so far on the ACP device was recently published in 2015 by Tzikas et al. [11], which was a multicenter trial of 1047 patients that established its safety and efficacy.
Because LAAC makes long-term OAC unnecessary, patients with very high stroke and bleeding risks should benefit most from this therapy. Nevertheless, LAAC carries inherent hazards especially in the periprocedural period and therefore a net clinical benefit of LAAC has to be established even in this particular subset of patients.
Our study population represents a very high-risk cohort of patients with AF with respect to stroke and bleeding, given the high median CHA2DS2-VASc score and HAS-BLED score of 5 (mean = 5.6) and 3 (mean = 3), respectively. The frequency of a previous stroke and bleeding episode were as high as 65.5% and 61.4%, respectively; 20% had a concomitant history of both events. Comparing stroke and bleeding risk with previous published studies, this study cohort is amongst the highest stroke and bleeding risks reported so far. In comparison, the mean CHA2DS2-VASc score of the study population in the PROTECT AF trial was 3.5; 18.5% had a previous stroke [7]. In the largest study reported so far with the ACP device, the mean CHA2DS2-VASc score was 4.4 with a history of previous stroke in 39% [11].
Procedural Outcomes
Our study confirms the results of previous studies: LAAC with the ACP has a high rate of procedural success and an acceptable rate of periprocedural complications. In recently reported studies, periprocedural complications were similar to those observed in our study, namely pericardial effusion, thromboembolic events, and device embolization. Postulated reasons for pericardial effusion are transseptal puncture related, extensive manipulation within the LAA, device recapture and repositioning, stiff wire exchange in the LAA, and extensive oversizing of the device [23, 24]. Pericardiocentesis alone seems to be sufficient enough to control this complication, its occurrence should decrease with more technical experience.
Device embolization is a well-known complication of LAAC with an average reported rate of less than 4% [25]. In our study, the device was successfully captured by a gooseneck snare. Our experience is in agreement with previous published cases of device embolization, which show that device embolizations into the LA can be successfully managed percutaneously. The reason for embolization in our case is unclear since this occurred despite ensuring a stable and safe device position. After retrieval, the same device was reintroduced and reimplanted successfully. Nonetheless, device embolization is a serious complication and more knowledge regarding its mechanisms is necessary.
Device Efficacy
Thromboembolic events during follow-up were observed at an annual rate of 3.2%. Comparing this observed rate with the estimated annual risk of 6.7–10.0% for patients without warfarin and with a CHA2DS2-VASc score of 5, a 52–68% reduction was calculated (Fig. 3). Rate ratio for incidence of thromboembolic events was 0.32 (95% CI 0.07–0.94), assuming estimated annual risk to be 10%. Reduction of thromboembolic events with ACP device in other case series varies from 59% to 80% [9–11]. Variabilities in risk reduction seem to be influenced by clinical characteristics of the patients including the CHA2DS2-VASc score. It must also be considered that when comparing risk reduction rates across different studies, the values of the expected stroke rate for a given CHA2DS2-VASc score used in the calculation of the relative risk reduction were not the same. Our results have confirmed that the reduction of thromboembolic events with the ACP device is significant even in very high stroke risk patients with AF, the derived magnitude of the benefit being large.
During the follow-up period, one patient had a fall-related intracranial bleeding and was classified as major bleeding event, but in reality was an event unrelated to the device. Apart from this patient, there were no overt bleeding events recorded during follow-up. Comparing an annual rate of 1.1% bleeding episodes during follow-up in our study with the estimated annual bleeding risk of 3.74–5.8% for patients on warfarin with a HAS-BLED score of 3, a 70–81% reduction of the bleeding risk was calculated (Fig. 3). Rate ratio for incidence of bleeding events was 0.18 (95% CI 0.00–1.03), assuming estimated annual risk to be 5.8%.
Of interest in our study was the presence of device-related thrombus, which was not associated with any thromboembolic events. The two patients who had thrombi on the device were on DAPT at the time of diagnosis (mean 5.5 months post-implant). Device-related thrombus was reported in other LAAC studies as well, although association with clinical stroke was rare. In the PROTECT AF study [25], device-associated thrombi were observed in 4.2%, and thrombus-associated annualized stroke rate was 0.3%. Interestingly, the rate of device-related thrombus in PROTECT AF was similar to that of ACP, despite the fact that patients were on OAC 45 days post-implant. In all cases reported so far, short-duration OAC therapy or low molecular weight heparin were effective in resolving thrombi.
Study Limitations
This study has all the limitations of a single-center retrospective observational study. The sample size of the study was small and no inference about comparative outcomes can be made due to lack of a control group. The annual stroke rate of our population was compared with the estimated events based on the CHA2DS2-VASc score. Because the expected events are based on historic controls and not validated in the current study population, the possibility of a type I error cannot be ruled out. For the above reasons, randomized controlled trials are needed for further validation of the results. It must be pointed out that patients of our study were on DAPT for 6 months after the procedure. DAPT has been reported to reduce stroke risk. This was not considered when comparing expected and observed stroke rates, and hence an inflated benefit cannot be ruled out. Finally, echocardiographic follow-up was incomplete and events such as minimal leaks or device thrombosis may have been missed.
Conclusions
LAAC with the ACP appears to be effective with acceptable rates of periprocedural complications and low rates of thromboembolic and bleeding events at follow-up in a cohort of very high stroke and bleeding risk patients with AF. With growing experience, this new technology of LAAC using ACP may become a valid alternative for high-risk patients with AF with contraindication for OAC.
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Acknowledgments
No funding or sponsorship was received for this study or publication of this article. All named authors meet the International Committee of Medical Journal Editors (ICMJE) criteria for authorship for this manuscript, take responsibility for the integrity of the work as a whole, and have given final approval for the version to be published.
Disclosures
M. Abdel-Wahab has received institutional research grants from St. Jude Medical and Biotronik, is a proctor for Boston Scientifc. G. Richardt has received institutional research Grants from St. Jude Medical and Biotronik, and receives lecture fees from Edwards Lifesciences and Boston Scientific. J. Jose is currently supported by an EAPCI Grant in Interventional Cardiology, which is partially sponsored by Medtronic. Julia Kebernik, Björn Stöcker, and Volker Geist have no conflicts of interest to disclose.
Compliance with Ethics Guidelines
All procedures followed were in accordance with ethical standards of the responsible committee on human experimentation (institutional and national) and with the Helsinki Declaration of 1964, as revised in 2013. Informed written consent for the procedure was obtained from all patients.
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Kebernik, J., Jose, J., Abdel-Wahab, M. et al. Safety and Efficacy of Left Atrial Appendage Closure with the Amplatzer Cardiac Plug in Very High Stroke and Bleeding Risk Patients with Non-Valvular Atrial Fibrillation. Cardiol Ther 4, 167–177 (2015). https://doi.org/10.1007/s40119-015-0053-z
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DOI: https://doi.org/10.1007/s40119-015-0053-z