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Journal of Arrhythmia logoLink to Journal of Arrhythmia
. 2017 Sep 15;33(5):369–409. doi: 10.1016/j.joa.2017.08.001

2017 HRS/EHRA/ECAS/APHRS/SOLAECE expert consensus statement on catheter and surgical ablation of atrial fibrillation: Executive summary

Hugh Calkins 1, Gerhard Hindricks 2,, Riccardo Cappato 3,61,62,, Young-Hoon Kim 4,§, Eduardo B Saad 5,, Luis Aguinaga 6,, Joseph G Akar 7, Vinay Badhwar 8,#, Josep Brugada 9,, John Camm 10,, Peng-Sheng Chen 11, Shih-Ann Chen 12,§, Mina K Chung 13, Jens Cosedis Nielsen 14,, Anne B Curtis 15,, D Wyn Davies 16,, John D Day 17, André d’Avila 18,‡‡, NMS (Natasja) de Groot 19,, Luigi Di Biase 20,, Mattias Duytschaever 21,, James R Edgerton 22,#, Kenneth A Ellenbogen 23, Patrick T Ellinor 24, Sabine Ernst 25,, Guilherme Fenelon 26,, Edward P Gerstenfeld 27, David E Haines 28, Michel Haissaguerre 29,, Robert H Helm 30, Elaine Hylek 31, Warren M Jackman 32, Jose Jalife 33, Jonathan M Kalman 34,§, Josef Kautzner 35,, Hans Kottkamp 36,, Karl Heinz Kuck 37,, Koichiro Kumagai 38,§, Richard Lee 39,#, Thorsten Lewalter 40,, Bruce D Lindsay 41, Laurent Macle 42,⁎⁎, Moussa Mansour 43, Francis E Marchlinski 44, Gregory F Michaud 45,, Hiroshi Nakagawa 46, Andrea Natale 47, Stanley Nattel 48, Ken Okumura 49,††, Douglas Packer 50, Evgeny Pokushalov 51,, Matthew R Reynolds 52, Prashanthan Sanders 53, Mauricio Scanavacca 54,, Richard Schilling 55,, Claudio Tondo 56,, Hsuan-Ming Tsao 57,§, Atul Verma 58, David J Wilber 59, Teiichi Yamane 60,††
PMCID: PMC5634725  PMID: 29021841

Document Reviewers: Carina Blomström-Lundqvist, MD, PhD; Angelo A.V. De Paola, MD, PhD; Peter M. Kistler, MBBS, PhD; Gregory Y.H. Lip, MD; Nicholas S. Peters, MD; Cristiano F. Pisani, MD; Antonio Raviele, MD; Eduardo B. Saad, MD, PhD; Kazuhiro Satomi, MD, PhD; Martin K. Stiles, MB ChB, PhD; Stephan Willems, MD, PhD

Section 1: Introduction

During the past three decades, catheter and surgical ablation of atrial fibrillation (AF) have evolved from investigational procedures to their current role as effective treatment options for patients with AF. Surgical ablation of AF, using either standard, minimally invasive, or hybrid techniques, is available in most major hospitals throughout the world. Catheter ablation of AF is even more widely available, and is now the most commonly performed catheter ablation procedure.

In 2007, an initial Consensus Statement on Catheter and Surgical AF Ablation was developed as a joint effort of the Heart Rhythm Society (HRS), the European Heart Rhythm Association (EHRA), and the European Cardiac Arrhythmia Society (ECAS).1 The 2007 document was also developed in collaboration with the Society of Thoracic Surgeons (STS) and the American College of Cardiology (ACC). This Consensus Statement on Catheter and Surgical AF Ablation was rewritten in 2012 to reflect the many advances in AF ablation that had occurred in the interim.2 The rate of advancement in the tools, techniques, and outcomes of AF ablation continue to increase as enormous research efforts are focused on the mechanisms, outcomes, and treatment of AF. For this reason, the HRS initiated an effort to rewrite and update this Consensus Statement. Reflecting both the worldwide importance of AF, as well as the worldwide performance of AF ablation, this document is the result of a joint partnership between the HRS, EHRA, ECAS, the Asia Pacific Heart Rhythm Society (APHRS), and the Latin American Society of Cardiac Stimulation and Electrophysiology (Sociedad Latinoamericana de Estimulación Cardíaca y Electrofisiología [SOLAECE]). The purpose of this 2017 Consensus Statement is to provide a state-of-the-art review of the field of catheter and surgical ablation of AF and to report the findings of a writing group, convened by these five international societies. The writing group is charged with defining the indications, techniques, and outcomes of AF ablation procedures. Included within this document are recommendations pertinent to the design of clinical trials in the field of AF ablation and the reporting of outcomes, including definitions relevant to this topic.

The writing group is composed of 60 experts representing 11 organizations: HRS, EHRA, ECAS, APHRS, SOLAECE, STS, ACC, American Heart Association (AHA), Canadian Heart Rhythm Society (CHRS), Japanese Heart Rhythm Society (JHRS), and Brazilian Society of Cardiac Arrhythmias (Sociedade Brasileira de Arritmias Cardíacas [SOBRAC]). All the members of the writing group, as well as peer reviewers of the document, have provided disclosure statements for all relationships that might be perceived as real or potential conflicts of interest. All author and peer reviewer disclosure information is provided in Table A1 and Table B1.

In writing a consensus document, it is recognized that consensus does not mean that there was complete agreement among all the writing group members. Surveys of the entire writing group were used to identify areas of consensus concerning performance of AF ablation procedures and to develop recommendations concerning the indications for catheter and surgical AF ablation. These recommendations were systematically balloted by the 60 writing group members and were approved by a minimum of 80% of these members. The recommendations were also subject to a 1-month public comment period. Each partnering and collaborating organization then officially reviewed, commented on, edited, and endorsed the final document and recommendations.

The grading system for indication of class of evidence level was adapted based on that used by the ACC and the AHA.3, 4 It is important to state, however, that this document is not a guideline. The indications for catheter and surgical ablation of AF, as well as recommendations for procedure performance, are presented with a Class and Level of Evidence (LOE) to be consistent with what the reader is familiar with seeing in guideline statements. A Class I recommendation means that the benefits of the AF ablation procedure markedly exceed the risks, and that AF ablation should be performed; a Class IIa recommendation means that the benefits of an AF ablation procedure exceed the risks, and that it is reasonable to perform AF ablation; a Class IIb recommendation means that the benefit of AF ablation is greater or equal to the risks, and that AF ablation may be considered; and a Class III recommendation means that AF ablation is of no proven benefit and is not recommended.

The writing group reviewed and ranked evidence supporting current recommendations with the weight of evidence ranked as Level A if the data were derived from high-quality evidence from more than one randomized clinical trial, meta-analyses of high-quality randomized clinical trials, or one or more randomized clinical trials corroborated by high-quality registry studies. The writing group ranked available evidence as Level B-R when there was moderate-quality evidence from one or more randomized clinical trials, or meta-analyses of moderate-quality randomized clinical trials. Level B-NR was used to denote moderate-quality evidence from one or more well-designed, well-executed nonrandomized studies, observational studies, or registry studies. This designation was also used to denote moderate-quality evidence from meta-analyses of such studies. Evidence was ranked as Level C-LD when the primary source of the recommendation was randomized or nonrandomized observational or registry studies with limitations of design or execution, meta-analyses of such studies, or physiological or mechanistic studies of human subjects. Level C-EO was defined as expert opinion based on the clinical experience of the writing group.

Despite a large number of authors, the participation of several societies and professional organizations, and the attempts of the group to reflect the current knowledge in the field adequately, this document is not intended as a guideline. Rather, the group would like to refer to the current guidelines on AF management for the purpose of guiding overall AF management strategies.5, 6 This consensus document is specifically focused on catheter and surgical ablation of AF, and summarizes the opinion of the writing group members based on an extensive literature review as well as their own experience. It is directed to all health care professionals who are involved in the care of patients with AF, particularly those who are caring for patients who are undergoing, or are being considered for, catheter or surgical ablation procedures for AF, and those involved in research in the field of AF ablation. This statement is not intended to recommend or promote catheter or surgical ablation of AF. Rather, the ultimate judgment regarding care of a particular patient must be made by the health care provider and the patient in light of all the circumstances presented by that patient.

The main objective of this document is to improve patient care by providing a foundation of knowledge for those involved with catheter ablation of AF. A second major objective is to provide recommendations for designing clinical trials and reporting outcomes of clinical trials of AF ablation. It is recognized that this field continues to evolve rapidly. As this document was being prepared, further clinical trials of catheter and surgical ablation of AF were under way.

Section 2: Definitions, Mechanisms, and Rationale for AF Ablation

This section of the document provides definitions for use in the diagnosis of AF. This section also provides an in-depth review of the mechanisms of AF and rationale for catheter and surgical AF ablation (Table 1, Figure1, Figure 2, Figure 3, Figure 4, Figure 5, Figure 6).

Table 1.

Atrial fibrillation definitions

AF episode An AF episode is defined as AF that is documented by ECG monitoring or intracardiac electrogram monitoring and has a duration of at least 30 seconds, or if less than 30 seconds, is present throughout the ECG monitoring tracing. The presence of subsequent episodes of AF requires that sinus rhythm be documented by ECG monitoring between AF episodes.
Chronic AF Chronic AF has variable definitions and should not be used to describe populations of AF patients undergoing AF ablation.
Early persistent AF Early persistent AF is defined as AF that is sustained beyond 7 days but is less than 3 months in duration.
Lone AF Lone AF is a historical descriptor that is potentially confusing and should not be used to describe populations of patients with AF undergoing AF ablation.
Long-standing persistent AF Long-standing persistent AF is defined as continuous AF of greater than 12 months’ duration.
Paroxysmal AF Paroxysmal AF is defined as AF that terminates spontaneously or with intervention within 7 days of onset.
Permanent AF Permanent AF is defined as the presence of AF that is accepted by the patient and physician, and for which no further attempts to restore or maintain sinus rhythm will be undertaken. The term permanent AF represents a therapeutic attitude on the part of the patient and physician rather than an inherent pathophysiological attribute of AF. The term permanent AF should not be used within the context of a rhythm control strategy with antiarrhythmic drug therapy or AF ablation.
Persistent AF Persistent AF is defined as continuous AF that is sustained beyond 7 days.
Silent AF Silent AF is defined as asymptomatic AF diagnosed with an opportune ECG or rhythm strip.

AF = atrial fibrillation; ECG = electrocardiogram.

Figure1.

Figure1

Anatomical drawings of the heart relevant to AF ablation. This series of drawings shows the heart and associated relevant structures from four different perspectives relevant to AF ablation. This drawing includes the phrenic nerves and the esophagus. A: The heart viewed from the anterior perspective. B: The heart viewed from the right lateral perspective. C: The heart viewed from the left lateral perspective. D: The heart viewed from the posterior perspective. E: The left atrium viewed from the posterior perspective.Illustration: Tim Phelps © 2017 Johns Hopkins University, AAM.

Figure 2.

Figure 2

This figure includes six CT or MR images of the left atrium and pulmonary veins viewed from the posterior perspective. Common and uncommon variations in PV anatomy are shown. A: Standard PV anatomy with 4 distinct PV ostia. B: Variant PV anatomy with a right common and a left common PV. C: Variant PV anatomy with a left common PV with a short trunk and an anomolous PV arising from the right posterior left atrial wall. D and E: Variant PV anatomy with a common left PV with a long trunk. F: Variant PV anatomy with a massive left common PV.

Figure 3.

Figure 3

Schematic drawing showing various hypotheses and proposals concerning the mechanisms of atrial fibrillation. A: Multiple wavelets hypothesis. B: Rapidly discharging automatic foci. C: Single reentrant circuit with fibrillatory conduction. D: Functional reentry resulting from rotors or spiral waves. E: AF maintenance resulting from dissociation between epicardial and endocardial layers, with mutual interaction producing multiplying activity that maintains the arrhythmia.

Figure 4.

Figure 4

Structure and mechanisms of atrial fibrillation. A: Schematic drawing of the left and right atria as viewed from the posterior perspective. The extension of muscular fibers onto the PVs can be appreciated. Shown in yellow are the five major left atrial autonomic ganglionic plexi (GP) and axons (superior left GP, inferior left GP, anterior right GP, inferior right GP, and ligament of Marshall). Shown in blue is the coronary sinus, which is enveloped by muscular fibers that have connections to the atria. Also shown in blue is the vein and ligament of Marshall, which travels from the coronary sinus to the region between the left superior PV and the left atrial appendage. B: The large and small reentrant wavelets that play a role in initiating and sustaining AF. C: The common locations of PV (red) and also the common sites of origin of non-PV triggers (shown in green). D: Composite of the anatomic and arrhythmic mechanisms of AF.Adapted with permission from Calkins et al. Heart Rhythm 2012; 9:632--696.e21.2

Figure 5.

Figure 5

Schematic drawing showing mechanisms of atrial flutter and atrial tachycardia. A: Isthmus-dependent reverse common (clockwise) atrial flutter. B: Isthmus-dependent common (counter clockwise) atrial flutter. C: Focal atrial tachycardia with circumferential spread of activation of the atria (can arise from multiple sites within the left and right atrium). D: Microreentrant atrial tachycardia with circumferential spread of activation of the atria. E: Perimitral atrial flutter. F: Roof-dependent atrial flutter.

Figure 6.

Figure 6

Schematic of common lesion sets employed in AF ablation. A: The circumferential ablation lesions that are created in a circumferential fashion around the right and the left PVs. The primary endpoint of this ablation strategy is the electrical isolation of the PV musculature. B: Some of the most common sites of linear ablation lesions. These include a "roof line" connecting the lesions encircling the left and/or right PVs, a "mitral isthmus" line connecting the mitral valve and the lesion encircling the left PVs at the end of the left inferior PV, and an anterior linear lesion connecting either the "roof line" or the left or right circumferential lesion to the mitral annulus anteriorly. A linear lesion created at the cavotricuspid isthmus is also shown. This lesion is generally placed in patients who have experienced cavotricuspid isthmus-dependent atrial flutter clinically or have it induced during EP testing. C: Similar to 6B, but also shows additional linear ablation lesions between the superior and inferior PVs resulting in a figure of eight lesion sets as well as a posterior inferior line allowing for electrical isolation of the posterior left atrial wall. An encircling lesion of the superior vena cava (SVC) directed at electrical isolation of the SVC is also shown. SVC isolation is performed if focal firing from the SVC can be demonstrated. A subset of operators empirically isolates the SVC. D: Representative sites for ablation when targeting rotational activity or CFAEs are targeted.Modified with permission from Calkins et al. Heart Rhythm 2012; 9:632--696.e21.2

Section 3: Modifiable Risk Factors for AF and Impact on Ablation

Management of patients with AF has traditionally consisted of three main components: (1) anticoagulation for stroke prevention; (2) rate control; and (3) rhythm control. With the emergence of large amounts of data, which have both defined and called attention to the interaction between modifiable risk factors and the development of AF and outcomes of AF management, we believe it is time to include risk factor modification as the fourth pillar of AF management. This section of the document reviews the link between modifiable risk factors and both the development of AF and their impacts on the outcomes of AF ablation.

Section 4: Indications

Shown in Table 2, and summarized in Figures 7 and 8 of this document, are the Consensus Indications for Catheter and Surgical Ablation of AF. As outlined in the introduction section of this document, these indications are stratified as Class I, Class IIa, Class IIb, and Class III indications. The evidence supporting these indications is provided, as well as a selection of the key references supporting these levels of evidence. In making these recommendations, the writing group considered the body of published literature that has defined the safety and efficacy of catheter and surgical ablation of AF. Also considered in these recommendations is the personal lifetime experience in the field of each of the writing group members. Both the number of clinical trials and the quality of these trials were considered. In considering the class of indications recommended by this writing group, it is important to keep several points in mind. First, these classes of indications only define the indications for catheter and surgical ablation of AF when performed by an electrophysiologist or a surgeon who has received appropriate training and/or who has a certain level of experience and is performing the procedure in an experienced center (Section 11). Catheter and surgical ablation of AF are highly complex procedures, and a careful assessment of the benefit and risk must be considered for each patient. Second, these indications stratify patients based only on the type of AF and whether the procedure is being performed prior to or following a trial of one or more Class I or III antiarrhythmic medications. This document for the first time includes indications for catheter ablation of select asymptomatic patients. As detailed in Section 9, there are many other additional clinical and imaging-based variables that can be used to further define the efficacy and risk of ablation in a given patient. Some of the variables that can be used to define patients in whom a lower success rate or a higher complication rate can be expected include the presence of concomitant heart disease, obesity, sleep apnea, left atrial (LA) size, patient age and frailty, as well as the duration of time the patient has been in continuous AF. Each of these variables needs to be considered when discussing the risks and benefits of AF ablation with a particular patient. In the presence of substantial risk or anticipated difficulty of ablation, it could be more appropriate to use additional antiarrhythmic drug (AAD) options, even if the patient on face value might present with a Class I or IIa indication for ablation. Third, it is important to consider patient preference and values. Some patients are reluctant to consider a major procedure or surgery and have a strong preference for a pharmacological approach. In these patients, trials of antiarrhythmic agents including amiodarone might be preferred to catheter ablation. On the other hand, some patients prefer a nonpharmacological approach. Fourth, it is important to recognize that some patients early in the course of their AF journey might have only infrequent episodes for many years and/or could have AF that is responsive to well-tolerated AAD therapy. And finally, it is important to bear in mind that a decision to perform catheter or surgical AF ablation should only be made after a patient carefully considers the risks, benefits, and alternatives to the procedure.

Table 2.

Indications for catheter (A and B) and surgical (C, D, and E) ablation of atrial fibrillation

Recommendation Class LOE References
Indications for catheter ablation of atrial fibrillation
A. Indications for catheter ablation of atrial fibrillation
Symptomatic AF refractory or intolerant to at least one Class I or III antiarrhythmic medication Paroxysmal: Catheter ablation is recommended. I A 7, 8, 9, 10, 11, 12, 13, 14, 15, 16, 17, 18
Persistent: Catheter ablation is reasonable. IIa B-NR 8, 16, 17, 18, 19, 20, 21, 22, 23, 24, 25, 26
Long-standing persistent: Catheter ablation may be considered. IIb C-LD 8, 16, 17, 18, 19, 20, 21, 22, 23, 24, 25, 26
Symptomatic AF prior to initiation of antiarrhythmic therapy with a Class I or III antiarrhythmic medication Paroxysmal: Catheter ablation is reasonable. IIa B-R 27, 28, 29, 30, 31, 32, 33, 34, 35
Persistent: Catheter ablation is reasonable. IIa C-EO
Long-standing persistent: Catheter ablation may be considered. IIb C-EO
B. Indications for catheter atrial fibrillation ablation in populations of patients not well represented in clinical trials
Congestive heart failure It is reasonable to use similar indications for AF ablation in selected patients with heart failure as in patients without heart failure. IIa B-R 36, 37, 38, 39, 40, 41, 42, 43, 44, 45, 46, 47, 48, 49, 50, 51, 52
Older patients (>75 years of age) It is reasonable to use similar indications for AF ablation in selected older patients with AF as in younger patients. IIa B-NR 53, 54, 55, 56, 57, 58, 59
Hypertrophic cardiomyopathy It is reasonable to use similar indications for AF ablation in selected patients with HCM as in patients without HCM. IIa B-NR 60, 61, 62
Young patients (<45 years of age) It is reasonable to use similar indications for AF ablation in young patients with AF (<45 years of age) as in older patients. IIa B-NR 63, 64
Tachy-brady syndrome It is reasonable to offer AF ablation as an alternative to pacemaker implantation in patients with tachy-brady syndrome. IIa B-NR 33, 34, 35
Athletes with AF It is reasonable to offer high-level athletes AF as first-line therapy due to the negative effects of medications on athletic performance. IIa C-LD 27, 28, 65
Asymptomatic AF⁎⁎ Paroxysmal: Catheter ablation may be considered in select patients.⁎⁎ IIb C-EO 66, 67
Persistent: Catheter ablation may be considered in select patients. IIb C-EO 68
Indications for surgical ablation of atrial fibrillation
C. Indications for concomitant open (such as mitral valve) surgical ablation of atrial fibrillation
Symptomatic AF refractory or intolerant to at least one Class I or III antiarrhythmic medication Paroxysmal: Surgical ablation is recommended. I B-NR 69, 70, 71, 72, 73, 74, 75, 76, 77, 78, 79, 80, 81, 82
Persistent: Surgical ablation is recommended. I B-NR 69, 70, 71, 72, 73, 74, 75, 76, 77, 78, 79, 80, 81, 82
Long-standing persistent: Surgical ablation is recommended. I B-NR 69, 70, 71, 72, 73, 74, 75, 76, 77, 78, 79, 80, 81, 82
Symptomatic AF prior to initiation of antiarrhythmic therapy with a Class I or III antiarrhythmic medication Paroxysmal: Surgical ablation is recommended. I B-NR 69, 70, 71, 72, 73, 74, 75, 76, 77, 78, 79, 80, 81, 82
Persistent: Surgical ablation is recommended. I B-NR 69, 70, 71, 72, 73, 74, 75, 76, 77, 78, 79, 80, 81, 82
Long-standing persistent: Surgical ablation is recommended. I B-NR 69, 70, 71, 72, 73, 74, 75, 76, 77, 78, 79, 80, 81, 82
D. Indications for concomitant closed (such as CABG and AVR) surgical ablation of atrial fibrillation
Symptomatic AF refractory or intolerant to at least one Class I or III antiarrhythmic medication Paroxysmal: Surgical ablation is recommended. I B-NR 83, 84, 85, 86, 87, 88
Persistent: Surgical ablation is recommended. I B-NR 83, 84, 85, 86, 87, 88
Long-standing persistent: Surgical ablation is recommended. I B-NR 83, 84, 85, 86, 87, 88
Symptomatic AF prior to initiation of antiarrhythmic therapy with a Class I or III antiarrhythmic medication Paroxysmal: Surgical ablation is reasonable. IIa B-NR 83, 84, 85, 86, 87, 88
Persistent: Surgical ablation is reasonable. IIa B-NR 83, 84, 85, 86, 87, 88
Long-standing persistent: Surgical ablation is reasonable. IIa B-NR 83, 84, 85, 86, 87, 88
E. Indications for stand-alone and hybrid surgical ablation of atrial fibrillation
Symptomatic AF refractory or intolerant to at least one Class I or III antiarrhythmic medication Paroxysmal: Stand-alone surgical ablation can be considered for patients who have failed one or more attempts at catheter ablation and also for those who are intolerant or refractory to antiarrhythmic drug therapy and prefer a surgical approach, after review of the relative safety and efficacy of catheter ablation versus a stand-alone surgical approach. IIb B-NR 83, 84, 85, 89, 90, 91, 92, 93, 94, 95, 96, 97, 98, 99, 100, 101, 102, 103
Persistent: Stand-alone surgical ablation is reasonable for patients who have failed one or more attempts at catheter ablation and also for those patients who prefer a surgical approach after review of the relative safety and efficacy of catheter ablation versus a stand-alone surgical approach. IIa B-NR 83, 84, 85, 89, 90, 91, 92, 93, 94, 95, 96, 97, 98, 99, 100, 101, 102, 103
Long-standing persistent: Stand-alone surgical ablation is reasonable for patients who have failed one or more attempts at catheter ablation and also for those patients who prefer a surgical approach after review of the relative safety and efficacy of catheter ablation versus a stand-alone surgical approach. IIa B-NR 83, 84, 85, 89, 90, 91, 92, 93, 94, 95, 96, 97, 98, 99, 100, 101, 102, 103
It might be reasonable to apply the indications for stand-alone surgical ablation described above to patients being considered for hybrid surgical AF ablation. IIb C-EO 103, 104, 105, 106, 107, 108

AF = atrial fibrillation; LOE = Level of Evidence; HCM = hypertrophic cardiomyopathy.

⁎⁎

A decision to perform AF ablation in an asymptomatic patient requires additional discussion with the patient because the potential benefits of the procedure for the patient without symptoms are uncertain.

Figure 7.

Figure 7

Indications for catheter ablation of symptomatic atrial fibrillation. Shown in this figure are the indications for catheter ablation of symptomatic paroxysmal, persistent, and long-standing persistent AF. The Class for each indication based on whether ablation is performed after failure of antiarrhythmic drug therapy or as first-line therapy is shown. Please refer to Table 2B and the text for the indications for catheter ablation of asymptomatic AF.

Figure 8.

Figure 8

Indications for surgical ablation of atrial fibrillation. Shown in this figure are the indications for surgical ablation of paroxysmal, persistent, and long-standing persistent AF. The Class for each indication based on whether ablation is performed after failure of antiarrhythmic drug therapy or as first-line therapy is shown. The indications for surgical AF ablation are divided into whether the AF ablation procedure is performed concomitantly with an open surgical procedure (such as mitral valve replacement), a closed surgical procedure (such as coronary artery bypass graft surgery), or as a stand-alone surgical AF ablation procedure performed solely for treatment of atrial fibrillation.

Section 5: Strategies, Techniques, and Endpoints

The writing group recommendations for techniques to be used for ablation of persistent and long-standing persistent AF (Table 3), adjunctive ablation strategies, nonablative strategies to improve outcomes of AF ablation, and endpoints for ablation of paroxysmal, persistent, and long-standing persistent AF are covered in this section. A schematic overview of common lesion sets created during an AF ablation procedure is shown in Figure 6.

Table 3.

Atrial fibrillation ablation: strategies, techniques, and endpoints

Recommendation Class LOE References
PV isolation by catheter ablation Electrical isolation of the PVs is recommended during all AF ablation procedures. I A 7, 8, 9, 10, 11, 12, 13, 14, 15, 16, 19, 20, 21, 22, 23, 24, 25, 26, 109
Achievement of electrical isolation requires, at a minimum, assessment and demonstration of entrance block into the PV. I B-R 7, 8, 9, 10, 11, 12, 13, 14, 15, 16, 19, 20, 21, 22, 23, 24, 25, 26, 109
Monitoring for PV reconnection for 20 minutes following initial PV isolation is reasonable. IIa B-R 9, 110, 111, 112, 113, 114, 115, 116, 117, 118, 119, 120
Administration of adenosine 20 minutes following initial PV isolation using RF energy with reablation if PV reconnection might be considered. IIb B-R 109, 111, 112, 113, 114, 120, 121, 122, 123, 124, 125, 126, 127, 128
Use of a pace-capture (pacing along the ablation line) ablation strategy may be considered. IIb B-R 129, 130, 131, 132, 133
Demonstration of exit block may be considered. IIb B-NR 134, 135, 136, 137, 138, 139
Ablation strategies to be considered for use in conjunction with PV isolation If a patient has a history of typical atrial flutter or typical atrial flutter is induced at the time of AF ablation, delivery of a cavotricuspid isthmus linear lesion is recommended. I B-R 140, 141, 142, 143
If linear ablation lesions are applied, operators should use mapping and pacing maneuvers to assess for line completeness. I C-LD 19, 141, 142, 143, 144, 145, 146, 147, 148, 149
If a reproducible focal trigger that initiates AF is identified outside the PV ostia at the time of an AF ablation procedure, ablation of the focal trigger should be considered. IIa C-LD 150, 151, 152, 153, 154, 155, 156, 157, 158, 159, 160, 161
When performing AF ablation with a force-sensing RF ablation catheter, a minimal targeted contact force of 5 to 10 grams is reasonable. IIa C-LD 13, 14, 128, 162, 163, 164, 165, 166, 167, 168, 169, 170, 171, 172, 173, 174, 175, 176, 177, 178
Posterior wall isolation might be considered for initial or repeat ablation of persistent or long-standing persistent AF. IIb C-LD 21, 179, 180, 181, 182, 183, 184, 185
Administration of high-dose isoproterenol to screen for and then ablate non-PV triggers may be considered during initial or repeat AF ablation procedures in patients with paroxysmal, persistent, or long-standing persistent AF. IIb C-LD 150, 151, 152, 153, 154, 155, 156, 157, 158, 159, 160, 161
DF-based ablation strategy is of unknown usefulness for AF ablation. IIb C-LD 186, 187, 188, 189, 190, 191, 192, 193
The usefulness of creating linear ablation lesions in the right or left atrium as an initial or repeat ablation strategy for persistent or long-standing persistent AF is not well established. IIb B-NR 19, 20, 142, 145, 146, 147, 148, 149, 194, 195, 196, 197, 198, 199, 200, 201
The usefulness of linear ablation lesions in the absence of macroreentrant atrial flutter is not well established. IIb C-LD 19, 20, 142, 145, 146, 147, 148, 149, 194, 195, 196, 197, 198, 199, 200, 201
The usefulness of mapping and ablation of areas of abnormal myocardial tissue identified with voltage mapping or MRI as an initial or repeat ablation strategy for persistent or long-standing persistent AF is not well established. IIb B-R 179, 202, 203, 204, 205, 206, 207, 208, 209, 210, 211
The usefulness of ablation of complex fractionated atrial electrograms as an initial or repeat ablation strategy for persistent and long-standing persistent AF is not well established. IIb B-R 19, 20, 195, 196, 197, 212, 213, 214, 215, 216, 217, 218, 219, 220
The usefulness of ablation of rotational activity as an initial or repeat ablation strategy for persistent and long-standing persistent AF is not well established. IIb B-NR 221, 222, 223, 224, 225, 226, 227, 228, 229, 230, 231, 232, 233, 234, 235, 236, 237, 238, 239, 240, 241
The usefulness of ablation of autonomic ganglia as an initial or repeat ablation strategy for paroxysmal, persistent, and long-standing persistent AF is not well established. IIb B-NR 19, 89, 242, 243, 244, 245, 246, 247, 248, 249, 250, 251, 252, 253, 254, 255, 256, 257, 258, 259
Nonablation strategies to improve outcomes Weight loss can be useful for patients with AF, including those who are being evaluated to undergo an AF ablation procedure, as part of a comprehensive risk factor management strategy. IIa B-R 260, 261, 262, 263, 264, 265, 266, 267, 268, 269, 270, 271, 272, 273, 274, 275, 276, 277, 278, 279, 280, 281, 282, 283, 284, 285, 286, 287, 288
It is reasonable to consider a patient׳s BMI when discussing the risks, benefits, and outcomes of AF ablation with a patient being evaluated for an AF ablation procedure. IIa B-R 260, 261, 262, 263, 264, 265, 266, 267, 268, 269, 270, 271, 272, 273, 274, 275, 276, 277, 278, 279, 280, 281, 282, 283, 284, 285, 286, 287, 288
It is reasonable to screen for signs and symptoms of sleep apnea when evaluating a patient for an AF ablation procedure and to recommend a sleep evaluation if sleep apnea is suspected. IIa B-R 270, 276, 277, 278, 289, 290, 291, 292, 293, 294, 295, 296, 297, 298, 299, 300, 301, 302, 303, 304, 305, 306, 307
Treatment of sleep apnea can be useful for patients with AF, including those who are being evaluated to undergo an AF ablation procedure. IIa B-R 270, 276, 277, 278, 289, 290, 291, 292, 293, 294, 295, 296, 297, 298, 299, 300, 301, 302, 303, 304, 305, 306, 307
The usefulness of discontinuation of antiarrhythmic drug therapy prior to AF ablation in an effort to improve long-term outcomes is unclear. IIb C-LD 308, 309, 310, 311, 312
The usefulness of initiation or continuation of antiarrhythmic drug therapy during the postablation healing phase in an effort to improve long-term outcomes is unclear. IIb C-LD 308, 309, 310, 311, 312
Strategies to reduce the risks of AF ablation Careful identification of the PV ostia is mandatory to avoid ablation within the PVs. I B-NR 313, 314, 315, 316, 317, 318, 319, 320, 321, 322, 323, 324, 325, 326, 327, 328, 329, 330, 331, 332, 333, 334, 335
It is recommended that RF power be reduced when creating lesions along the posterior wall near the esophagus. I C-LD 68, 336, 337, 338, 339, 340, 341, 342, 343, 344, 345, 346, 347, 348, 349, 350, 351, 352, 353, 354, 355, 356, 357, 358, 359, 360, 361, 362, 363, 364, 365
It is reasonable to use an esophageal temperature probe during AF ablation procedures to monitor esophageal temperature and help guide energy delivery. IIa C-EO 68, 336, 345, 365

AF = atrial fibrillation; LOE = Level of Evidence; PV = pulmonary vein; RF = radiofrequency; MRI = magnetic resonance imaging; BMI = body mass index.

Section 6: Technology and Tools

This section of the consensus statement provides an update on many of the technologies and tools that are employed for AF ablation procedures. It is important to recognize that this is not a comprehensive listing and that new technologies, tools, and approaches are being developed. It is also important to recognize that radiofrequency (RF) energy is the dominant energy source available for ablation of typical and atypical atrial flutter (AFL). Although cryoablation is a commonly employed tool for AF ablation, it is not well suited for ablation of typical or atypical AFL. Other energy sources and tools are available in some parts of the world and/or are in various stages of development and/or clinical investigation. Shown in Figure 9 are schematic drawings of AF ablation using point-by-point RF energy (Figure 9A) and AF ablation using the cryoballoon (CB) system (Figure 9B).

Figure 9.

Figure 9

Schematic drawing showing catheter ablation of atrial fibrillation using either RF energy or cryoballoon AF ablation. A: Shows a typical wide area lesion set created using RF energy. Ablation lesions are delivered in a figure of eight pattern around the left and right PV veins. Also shown is a linear cavotricuspid isthmus lesion created for ablation of typical atrial flutter in a patient with a prior history of typical atrial flutter or inducible isthmus-dependent typical atrial flutter at the time of ablation. A multielectrode circular mapping catheter is positioned in the left inferior PV. B: Shows an ablation procedure using the cryoballoon system. Ablation lesions have been created surrounding the right PVs, and the cryoballoon ablation catheter is positioned in the left superior PV. A through the lumen multielectrode circular mapping catheter is positioned in the left superior PV.Illustration: Tim Phelps © 2017 Johns Hopkins University, AAM.

Section 7: Technical Aspects of Ablation to Maximize Safety and Anticoagulation

Anticoagulation strategies pre-, during, and postcatheter ablation of AF (Table 4); signs and symptoms of complications that can occur within the first several months following ablation (Table 5); anesthesia or sedation during ablation; and approaches to minimize risk of an atrial esophageal fistula are discussed in this section.

Table 4.

Anticoagulation strategies: pre-, during, and postcatheter ablation of AF

Recommendation Class LOE References
Preablation For patients undergoing AF catheter ablation who have been therapeutically anticoagulated with warfarin or dabigatran, performance of the ablation procedure without interruption of warfarin or dabigatran is recommended. I A 366, 367, 368, 369, 370, 371, 372, 373
For patients undergoing AF catheter ablation who have been therapeutically anticoagulated with rivaroxaban, performance of the ablation procedure without interruption of rivaroxaban is recommended. I B-R 374
For patients undergoing AF catheter ablation who have been therapeutically anticoagulated with a NOAC other than dabigatran or rivaroxaban, performance of the ablation procedure without withholding a NOAC dose is reasonable. IIa B-NR 375
Anticoagulation guidelines that pertain to cardioversion of AF should be adhered to in patients who present for an AF catheter ablation procedure. I B-NR 5, 6
For patients anticoagulated with a NOAC prior to AF catheter ablation, it is reasonable to hold one to two doses of the NOAC prior to AF ablation with reinitiation postablation. IIa B-NR 372, 376, 377, 378, 379, 380
Performance of a TEE in patients who are in AF on presentation for AF catheter ablation and who have been receiving anticoagulation therapeutically for 3 weeks or longer is reasonable. IIa C-EO 5, 6
Performance of a TEE in patients who present for ablation in sinus rhythm and who have not been anticoagulated prior to catheter ablation is reasonable. IIa C-EO 5, 6
Use of intracardiac echocardiography to screen for atrial thrombi in patients who cannot undergo TEE may be considered. IIb C-EO 381, 382, 383, 384, 385, 386
During ablation Heparin should be administered prior to or immediately following transseptal puncture during AF catheter ablation procedures and adjusted to achieve and maintain an ACT of at least 300 seconds. I B-NR 369, 380, 381, 382, 387, 388, 389, 390, 391, 392, 393
Administration of protamine following AF catheter ablation to reverse heparin is reasonable. IIa B-NR 394
Postablation In patients who are not therapeutically anticoagulated prior to catheter ablation of AF and in whom warfarin will be used for anticoagulation postablation, low molecular weight heparin or intravenous heparin should be used as a bridge for initiation of systemic anticoagulation with warfarin following AF ablation. I C-EO
Systemic anticoagulation with warfarin or a NOAC is recommended for at least 2 months postcatheter ablation of AF. I C-EO 1, 2
Adherence to AF anticoagulation guidelines is recommended for patients who have undergone an AF ablation procedure, regardless of the apparent success or failure of the procedure. I C-EO 5, 6
Decisions regarding continuation of systemic anticoagulation more than 2 months post ablation should be based on the patient׳s stroke risk profile and not on the perceived success or failure of the ablation procedure. I C-EO 5, 6
In patients who have not been anticoagulated prior to catheter ablation of AF or in whom anticoagulation with a NOAC or warfarin has been interrupted prior to ablation, administration of a NOAC 3 to 5 hours after achievement of hemostasis is reasonable postablation. IIa C-EO 372, 376, 377, 378, 379, 380
Patients in whom discontinuation of anticoagulation is being considered based on patient values and preferences should consider undergoing continuous or frequent ECG monitoring to screen for AF recurrence. IIb C-EO

AF = atrial fibrillation; LOE = Level of Evidence; NOAC = novel oral anticoagulant; TEE = transesophageal electrocardiogram; ACT = activated clotting time.

Time in therapeutic range (TTR) should be > 65% -- 70% on warfarin.

Table 5.

Signs and symptoms following AF ablation

Differential Suggested evaluation
Signs and symptoms of complications within a month postablation
 Back pain Musculoskeletal, retroperitoneal hematoma Physical exam, CT imaging
 Chest pain Pericarditis, pericardial effusion, coronary stenosis (ablation related), pulmonary vein stenosis, musculoskeletal (after cardioversion), worsening reflux Physical exam, chest X-ray, ECG, echocardiogram, stress test, cardiac catheterization, chest CT
 Cough Infectious process, bronchial irritation (mechanical, cryoballoon), pulmonary vein stenosis Physical exam, chest X-ray, chest CT
 Dysphagia Esophageal irritation (related to transesophageal echocardiography), atrioesophageal fistula Physical exam, chest CT or MRI
 Early satiety, nausea Gastric denervation Physical exam, gastric emptying study
 Fever Infectious process, pericarditis, atrioesophageal fistula Physical exam, chest X-ray, chest CT, urinalysis, laboratory blood work
 Fever, dysphagia, neurological symptoms Atrial esophageal fistula Physical exam, laboratory blood work, chest CT or MRI; avoid endoscopy with air insufflation
 Groin pain at site of access Pseudoaneurysm, AV fistula, hematoma Ultrasound of the groin, laboratory blood work; consider CT scan if ultrasound negative
 Headache Migraine (related to anesthesia or transseptal access, hemorrhagic stroke), effect of general anesthetic Physical exam, brain imaging (MRI)
 Hypotension Pericardial effusion/tamponade, bleeding, sepsis, persistent vagal reaction Echocardiography, laboratory blood work
 Hemoptysis PV stenosis or occlusion, pneumonia Chest X-ray, chest CT or MR scan, VQ scan
 Neurological symptoms Cerebral embolic event, atrial esophageal fistula Physical exam, brain imaging, chest CT or MRI
 Shortness of breath Volume overload, pneumonia, pulmonary vein stenosis, phrenic nerve injury Physical exam, chest X-ray, chest CT, laboratory blood work
Signs and symptoms of complications more than a month postablation
 Fever, dysphagia, neurological symptoms Atrial esophageal fistula Physical exam, laboratory blood work, chest CT or MRI; avoid endoscopy with air insufflation
 Persistent cough, atypical chest pain Infectious process, pulmonary vein stenosis Physical exam, laboratory blood work, chest X-ray, chest CT or MRI
 Neurological symptoms Cerebral embolic event, atrial esophageal fistula Physical exam, brain imaging, chest CT or MRI
 Hemoptysis PV stenosis or occlusion, pneumonia CT scan, VQ scan

AF = atrial fibrillation; ECG = electrocardiogram; CT = computed tomography; MRI = magnetic resonance imaging; VQ = ventilation-perfusion.

Section 8: Follow-up Considerations

AF ablation is an invasive procedure that entails risks, most of which are present during the acute procedural period. However, complications can also occur in the weeks or months following ablation. Recognizing common symptoms after AF ablation and distinguishing those that require urgent evaluation and referral to an electrophysiologist is an important part of follow-up after AF ablation. The success of AF ablation is based in large part on freedom from AF recurrence based on ECG monitoring. Arrhythmia monitoring can be performed with the use of noncontinuous or continuous ECG monitoring tools (Table 6). This section also discusses the important topics of AAD and non-AAD use prior to and following AF ablation, the role of cardioversion, as well as the indications for and timing of repeat AF ablation procedures.

Table 6.

Types of ambulatory cardiac monitoring devices

Type of recorder Typical monitoring duration Continuous recording Event recording Auto trigger Unique features
Holter monitor 24--48 hours, approximately 7--30 days Yes Yes N/A Short term, provides quantitative data on arrhythmia burden
Patch monitor 1--3 weeks Yes Yes N/A Intermediate term, can provide continuous data for up to several weeks; improved patient compliance without lead wires
External loop recorder 1 month Yes Yes Variable Good correlation between symptoms and even brief arrhythmias
External nonloop recorder Months No Yes No May be used long term and intermittently; will not capture very brief episodes
Smartphone monitor Indefinite No Yes No Provides inexpensive long-term intermittent monitoring; dependent on patient compliance; requires a smartphone
Mobile cardiac telemetry 30 days Yes Yes Yes Real time central monitoring and alarms; relatively expensive
Implantable loop recorder Up to 3 years Yes Yes Yes Improved patient compliance for long-term use; not able to detect 30-second episodes of AF due to detection algorithm; presence of AF needs to be confirmed by EGM review because specificity of detection algorithm is imperfect; expensive
Pacemakers or ICDs with atrial leads Indefinite Yes Yes Yes Excellent AF documentation of burden and trends; presence of AF needs to be confirmed by electrogram tracing review because specificity of detection algorithms is imperfect; expensive
Wearable multisensor ECG monitors Indefinite Yes Yes Yes ECG 3 leads, temp, heart rate, HRV, activity tracking, respiratory rate, galvanic skin response

AF = atrial fibrillation; ICD = implantable cardioverter defibrillator; ECG = electrocardiogram; HRV = heart rate variability.

Section 9: Outcomes and Efficacy

This section provides a comprehensive review of the outcomes of catheter ablation of AF. Table 7 summarizes the main findings of the most important clinical trials in this field. Outcomes of AF ablation in subsets of patients not well represented in these trials are reviewed. Outcomes for specific ablation systems and strategies (CB ablation, rotational activity ablation, and laser balloon ablation) are also reviewed.

Table 7.

Selected clinical trials of catheter ablation of atrial fibrillation and/or for FDA approval

Trial Year Type N AF type Ablation strategy Initial time frame Effectiveness endpoint Ablation success Drug/ Control success P value for success Ablation complications Drug/Control complications Comments
Clinical Trials Performed for FDA Approval
 JAMA 2010; 303: 333-340 (ThermoCoolAF)14 2010 Randomized to RF ablation or AAD, multicenter 167 Paroxysmal PVI, optional CFAEs and lines 12 months Freedom from symptomatic paroxysmal atrial fibrillation, acute procedural failure, or changes in specified drug regimen 66% 16% <0.001 4.9% 8.8% FDA approval received
 JACC 2013; 61: 1713-1723 (STOP AF)9 2013 Randomized to cryoballoon ablation or AAD, multicenter 245 Paroxysmal PVI 12 months Freedom from any detectable AF, use of nonstudy AAD, or nonprotocol intervention for AF 70% 7% <0.001 3.1% NA FDA approval received
 Heart Rhythm 2014; 11: 202-209 (TTOP)22 2014 Randomized to phased RF ablation or AAD/cardioversion, multicenter 210 Persistent PVI + CFAEs 6 months Acute procedural success, ≥90% reduction in AF burden, off AAD 56% 26% <0.001 12.3% NA Not FDA approved
 JACC 2014; 64: 647-656 (SMART-AF)13 2014 Nonrandomzied multicenter study of contact force-sensing RF catheter, comparing to performance goals 172 Paroxysmal PVI, optional CFAEs and lines 12 months Freedom from symptomatic AF, flutter, tachycardia, acute procedural failure, or changes in AAD 72.5% N/A <0.0001 7.5% NA FDA approval received
 Circulation 2015; 132: 907-915 (TOCCASTAR)12 2015 Randomized to contact force sensing RF catheter or approved RF catheter, multicenter 300 Paroxysaml PVI, optional triggers, CAFEs and lines in both arms 12 months Acute procedural success + Freedom from Symptomatic AF/Flutter/Tachycardia off AAD 67.8% 69.4% 0.0073 for noninferiority 7.2% 9.1% FDA approval received
 JACC 2015; 66: 1350-1360 (HeartLight)11 2015 Randomized to laserballoon or approved RF catheter, multicenter 353 Paroxysmal PVI ± CTI ablation vs PVI, optional CFAEs, and Lines 12 months Freedom from Symptomatic AF/Flutter/Tachycardia, acute procedural failure, AAD, or non-prototocol intervention 61.1% 61.7% 0.003 for noninferiority 5.3% 6.4% FDA approval received
First-Line Therapy Trials
 JAMA 2005; 293: 2634-2640 (RAAFT)29 2005 Randomized to drug, multicenter 70 Paroxysmal (N=67), persistent (N= 3) PVI 12 months Freedom from detectable AF 84% 37% <0.01 9% 11%
 NEJM 2012; 367:1587-1595 (MANTRA-PAF)30 2012 Randomized to drug, multicenter 294 Paroxysmal AF PVI, roof line, optional mitral and tricuspid line 24 months Cumulative AF burden 13% AF burden 19% AF burden NS 17% 15%
 JAMA 2014; 311: 692-700 (RAAFT-2)31 2014 Randomized to drug multicenter 127 Paroxysmal AF PVI plus optional non-PVI targets 24 months Freedom from detectable AF, flutter, tachycardia 45% 28% 0.02 9% 4.9%
Other Paroxysmal AF Ablation Trials
 JACC 2006; 48: 2340-2347 (APAF)16 2006 Randomized to drug single center 198 Paroxysmal AF PVI, mitral line and tricuspid line 12 months Freedom from detectable AF, flutter, tachycardia 86% 22% <0.001 1% 23%
 Circulation 2008; 118: 2498-2505 (A4)7 2008 Randomized to drug 112 Paroxysmal PVI (optional LA lines, CTI, focal) 12 months Freedom from AF 89% 23% <0.0001 5.7% 1.7%
 NEJM 2016; 374: 2235-2245 (FIRE AND ICE)10 2016 Randomized RF vs Cryo, multicenter 762 Paroxysmal AF PVI 12 months Freedom from detectable AF, flutter, tachycardia 64.1% (RF) 65.4% (cryo) NS 12.8% 10.2%
 JACC 2016; 68: 2747-275715 2016 Randomized to hot balloon or drug, multicenter 100 Paroxysmal AF PVI 12 months Freedom from AF 59% 5% <0.001 10.4% 4.7%
Other Persistent AF Ablation Trials
 NEJM 2006; 354: 934-94125 2006 Randomized to RF ablation or to CV and short term amio 146 Persistent PVI, roof, mitral line 12 months No AF or flutter month 12 74% 58% 0.05 1.3% 1.4%
 EHJ 2014; 35: 501-507 (SARA)26 2014 Randomized to drug (2:1 ablation to drug), multicenter 146 Persistent PVI (optional LA lines, CFAEs) 12 months Freedom from AF/flutter lasting >24h 70% 44% 0.002 6.1% 4.20%
 NEJM 2015; 372: 1812-182219 2015 Randomized ablation strategies, multicenter 589 Persistent PVI alone versus PVI & CFAEs or PVI & lines 18 months Freedom from afib with or without drugs 59% (PVI alone) 49% & 46% NS 6% 4.3% & 7.6%
Other Mixed Paroxysmal and Persistent AF Ablation Trials
 J Med Assoc Thai 2003; 86 (Suppl 1): S8-S1624 2003 Randomized to RF ablation or amiodarone 30 Paroxysmal (70%), Persistent (30%) PVI, mitral line, CTI, SVC to IVC 12 months Freedom from AF 79% 40% 0.018 6.70% 47%
 EHJ 2006; 27: 216-22117 2006 Randomized to RF ablation or drug, multicenter 137 Paroxysmal (67%), Persistent (33%) PVI, mitral line, CTI 12 months Freedom from AF, flutter, tachycardia 66% 9% <0.001 4.40% 2.90%
 JCVEP 2009, 20: 22-2818 2009 Randomized to RF ablation or drug, multicenter 70 Paroxysmal (41%), Persistent (59%) & type 2 DM PVI, CTI, optional mitral line and roof line 12 months Freedom from AF and atypical atrial flutter 80% 43% 0.001 2.90% 17%
Randomized Trials of AF Ablation in Patients with Heart Failure
 NEJM 2008; 359: 1778-1785 (PABA-HF)38 2008 Randomized to RF ablation of AVJ abl and BiV pacing 81 Persistent (50%), Paroxysmal (50%), EF 27% abl, 29% AVJ PVI, optional linear abl and CFAEs 6 months Composite EF, 6 min walk, MLWHF score; freedom from AF (secondary, mult proc, +/- AA drugs) 88% AF free, EF 35% abl, 28% AVJ (P <.001), > QOL and 6 min walk increase with abl <0.001 14.60% 17.50%
 Heart 2011; 97: 740-74739 2011 Randomized to RF ablation or pharmacological rate control 41 Persistent , EF 20% abl, 16% rate control PVI, roof line, CFAEs 6 months Change in LVEF, sinus rhythm at 6 months (secondary) 50% in NSR, LVEF increase 4.5% 0% in NSR, LVEF increase 2.8% 0.6 (for EF increase) 15% Not reported
 JACC 2013; 61: 1894-190346 2013 Randomized to RF ablation or pharmacological rate control 52 Persistent AF (100%), EF 22% abl, 25% rate control PVI, optional linear abl and CFAEs 12 months Change in peak O2 consumption (also reported single procedure off drug ablation success) Peak O2 consumption increase greater with abl, 72% abl success 0.018 15% Not reported
 Circ A and E 2014; 7:31-3840 2014 Randomized to RF ablation or pharmacological rate control 50 Persistent AF (100%), EF 32% abl, 34% rate control PVI, optional linear abl and CFAEs 6 months Change in LVEF at 6 months, multiple procedure freedom from AF also reported LVEF 40% with abl, 31% rate control, 81% AF free with abl 0.015 7.70%

AF = atrial fibrillation; RF = radiofrequency; AVJ = atrioventricular junction; abl = ablation; BiV = biventricular; EF = ejection fraction; PVI = pulmonary vein isolation; CFAEs = complex fractionated atrial electrograms; MLWHF = Minnesota Living with Heart Failure; LVEF = left ventricular ejection fraction; QOL = quality of life; NSR = normal sinus rhythm.

Section 10: Complications

Catheter ablation of AF is one of the most complex interventional electrophysiological procedures. AF ablation by its nature involves catheter manipulation and ablation in the delicate thin-walled atria, which are in close proximity to other important organs and structures that can be impacted through collateral damage. It is therefore not surprising that AF ablation is associated with a significant risk of complications, some of which might result in life-long disability and/or death. This section reviews the complications associated with catheter ablation procedures performed to treat AF. The types and incidence of complications are presented, their mechanisms are explored, and the optimal approach to prevention and treatment is discussed (Tables 8 and 9).

Table 8.

Definitions of complications associated with AF ablation

Asymptomatic cerebral embolism Asymptomatic cerebral embolism is defined as an occlusion of a blood vessel in the brain due to an embolus that does not result in any acute clinical symptoms. Silent cerebral embolism is generally detected using a diffusion weighted MRI.
Atrioesophageal fistula An atrioesophageal fistula is defined as a connection between the atrium and the lumen of the esophagus. Evidence supporting this diagnosis includes documentation of esophageal erosion combined with evidence of a fistulous connection to the atrium, such as air emboli, an embolic event, or direct observation at the time of surgical repair. A CT scan or MRI scan is the most common method of documentation of an atrioesophageal fistula.
Bleeding Bleeding is defined as a major complication of AF ablation if it requires and/or is treated with transfusion or results in a 20% or greater fall in hematocrit.
Bleeding following cardiac surgery Excessive bleeding following a surgical AF ablation procedure is defined as bleeding requiring reoperation or ≥2 units of PRBC transfusion within any 24 hours of the first 7 days following the index procedure.
Cardiac perforation We recommend that cardiac perforation be defined together with cardiac tamponade. See "Cardiac tamponade/perforation."
Cardiac tamponade We recommend that cardiac tamponade be defined together with cardiac perforation. See "Cardiac tamponade/perforation."
Cardiac tamponade/perforation Cardiac tamponade/perforation is defined as the development of a significant pericardial effusion during or within 30 days of undergoing an AF ablation procedure. A significant pericardial effusion is one that results in hemodynamic compromise, requires elective or urgent pericardiocentesis, or results in a 1-cm or more pericardial effusion as documented by echocardiography. Cardiac tamponade/perforation should also be classified as "early" or "late" depending on whether it is diagnosed during or following initial discharge from the hospital.
Deep sternal wound infection/mediastinitis following cardiac surgery Deep sternal wound infection/mediastinitis following cardiac surgery requires one of the following: (1) an organism isolated from culture of mediastinal tissue or fluid; (2) evidence of mediastinitis observed during surgery; (3) one of the following conditions: chest pain, sternal instability, or fever (>38°C), in combination with either purulent discharge from the mediastinum or an organism isolated from blood culture or culture of mediastinal drainage.
Esophageal injury Esophageal injury is defined as an erosion, ulceration, or perforation of the esophagus. The method of screening for esophageal injury should be specified. Esophageal injury can be a mild complication (erosion or ulceration) or a major complication (perforation).
Gastric motility/pyloric spasm disorders Gastric motility/pyloric spasm disorder should be considered a major complication of AF ablation when it prolongs or requires hospitalization, requires intervention, or results in late disability, such as weight loss, early satiety, diarrhea, or GI disturbance.
Major complication A major complication is a complication that results in permanent injury or death, requires intervention for treatment, or prolongs or requires hospitalization for more than 48 hours. Because early recurrences of AF/AFL/AT are to be expected following AF ablation, recurrent AF/AFL/AT within 3 months that requires or prolongs a patient׳s hospitalization should not be considered to be a major complication of AF ablation.
Mediastinitis Mediastinitis is defined as inflammation of the mediastinum. Diagnosis requires one of the following: (1) an organism isolated from culture of mediastinal tissue or fluid; (2) evidence of mediastinitis observed during surgery; (3) one of the following conditions: chest pain, sternal instability, or fever (>38°C), in combination with either purulent discharge from the mediastinum or an organism isolated from blood culture or culture of mediastinal drainage.
Myocardial infarction in the context of AF ablation The universal definition of myocardial infarction395 cannot be applied in the context of catheter or surgical AF ablation procedures because it relies heavily on cardiac biomarkers (troponin and CPK), which are anticipated to increase in all patients who undergo AF ablation as a result of the ablation of myocardial tissue. Similarly, chest pain and other cardiac symptoms are difficult to interpret in the context of AF ablation both because of the required sedation and anesthesia and also because most patients experience chest pain following the procedure as a result of the associated pericarditis that occurs following catheter ablation. We therefore propose that a myocardial infarction, in the context of catheter or surgical ablation, be defined as the presence of any one of the following criteria: (1) detection of ECG changes indicative of new ischemia (new ST-T wave changes or new LBBB) that persist for more than 1 hour; (2) development of new pathological Q waves on an ECG; (3) imaging evidence of new loss of viable myocardium or new regional wall motion abnormality.
Pericarditis Pericarditis should be considered a major complication following ablation if it results in an effusion that leads to hemodynamic compromise or requires pericardiocentesis, prolongs hospitalization by more than 48 hours, requires hospitalization, or persists for more than 30 days following the ablation procedure.
Phrenic nerve paralysis Phrenic nerve paralysis is defined as absent phrenic nerve function as assessed by a sniff test. A phrenic nerve paralysis is considered to be permanent when it is documented to be present 12 months or longer following ablation.
Pulmonary vein stenosis Pulmonary vein stenosis is defined as a reduction of the diameter of a PV or PV branch. PV stenosis can be categorized as mild <50%, moderate 50%–70%, and severe ≥70% reduction in the diameter of the PV or PV branch. A severe PV stenosis should be considered a major complication of AF ablation.
Serious adverse device effect A serious adverse device effect is defined as a serious adverse event that is attributed to use of a particular device.
Stiff left atrial syndrome Stiff left atrial syndrome is a clinical syndrome defined by the presence of signs of right heart failure in the presence of preserved LV function, pulmonary hypertension (mean PA pressure >25 mm Hg or during exercise >30 mm Hg), and large V waves ≥10 mm Hg or higher) on PCWP or left atrial pressure tracings in the absence of significant mitral valve disease or PV stenosis.
Stroke or TIA postablation
  • Stroke diagnostic criteria
    • Rapid onset of a focal or global neurological deficit with at least one of the following: change in level of consciousness, hemiplegia, hemiparesis, numbness or sensory loss affecting one side of the body, dysphasia or aphasia, hemianopia, amaurosis fugax, or other neurological signs or symptoms consistent with stroke
    • Duration of a focal or global neurological deficit ≥24 hours; OR <24 hours if therapeutic intervention(s) were performed (e.g., thrombolytic therapy or intracranial angioplasty); OR available neuroimaging documents a new hemorrhage or infarct; OR the neurological deficit results in death.
    • No other readily identifiable nonstroke cause for the clinical presentation (e.g., brain tumor, trauma, infection, hypoglycemia, peripheral lesion, pharmacological influences).
    • Confirmation of the diagnosis by at least one of the following: neurology or neurosurgical specialist; neuroimaging procedure (MRI or CT scan or cerebral angiography); lumbar puncture (i.e., spinal fluid analysis diagnostic of intracranial hemorrhage)
  • Stroke definitions
    • Transient ischemic attack: new focal neurological deficit with rapid symptom resolution (usually 1 to 2 hours), always within 24 hours; neuroimaging without tissue injury
    • Stroke: (diagnosis as above, preferably with positive neuroimaging study);
  • Minor–Modified Rankin score <2 at 30 and 90 days

  • Major–Modified Rankin score ≥2 at 30 and 90 days

Unanticipated adverse device effect Unanticipated adverse device effect is defined as complication of an ablation procedure that has not been previously known to be associated with catheter or surgical ablation procedures.
Vagal nerve injury Vagal nerve injury is defined as injury to the vagal nerve that results in esophageal dysmotility or gastroparesis. Vagal nerve injury is considered to be a major complication if it prolongs hospitalization, requires hospitalization, or results in ongoing symptoms for more than 30 days following an ablation procedure.
Vascular access complication Vascular access complications include development of a hematoma, an AV fistula, or a pseudoaneurysm. A major vascular complication is defined as one that requires intervention, such as surgical repair or transfusion, prolongs the hospital stay, or requires hospital admission.

AF = atrial fibrillation; CT = computed tomography; MRI = magnetic resonance imaging; PRBC = packed red blood cell; AFL = atrial flutter; AT = atrial tachycardia; CPK = creatine phosphokinase; ECG = electrocardiogram; LBBB = left bundle branch block.

Patients with nonfocal global encephalopathy will not be reported as a stroke without unequivocal evidence based on neuroimaging studies.

Modified Rankin score assessments should be made by qualified individuals according to a certification process. If there is discordance between the 30- and 90-day modified Rankin scores, a final determination of major versus minor stroke will be adjudicated by the neurology members of the clinical events committee.

Table 9.

Incidence, prevention, diagnosis, and treatment of selected complications of AF ablation

Complication Incidence Selected prevention techniques Diagnostic testing Selected treatment options References
Air embolism <1% Sheath management Nothing or cardiac catheterization Supportive care with fluid, oxygen, head down tilt, hyperbaric oxygen 388, 396, 397, 398, 399, 400, 401
Asymptomatic cerebral emboli (ACE) 2% to 15% Anticoagulation, catheter and sheath management, TEE Brain MRI None 402, 403, 404, 405, 406, 407, 408, 409, 410, 411, 412, 413, 414, 415, 416, 417, 418, 419
Atrial esophageal fistula 0.02% to 0.11% Reduce power, force, and RF time on posterior wall, monitor esophageal temp, use proton pump inhibitors; avoid energy delivery over esophagus CT scan of chest, MRI; avoid endoscopy with air insufflation Surgical repair 337, 338, 339, 340, 341, 342, 343, 344, 345, 346, 347, 348, 349, 350, 351, 352, 353, 354, 355, 356, 357, 358, 359, 360, 361, 362, 363, 364, 365, 420, 421, 422, 423, 424, 425, 426, 427, 428, 429, 430, 431, 432, 433, 434, 435, 436, 437, 438, 439, 440, 441, 442, 443, 444, 445, 446, 447, 448, 449, 450, 451, 452, 453, 454, 455, 456
Cardiac tamponade 0.2% to 5% Cather manipulation, transseptal technique, reduce power, force, and RF time Echocardiography Pericardiocentesis or surgical drainage 338, 343, 347, 457, 458, 459, 460, 461, 462, 463, 464, 465, 466, 467
Coronary artery stenosis/occlusion <0.1% Avoid high-power energy delivery near coronary arteries Cardiac catheterization PTCA 468, 469, 470, 471, 472, 473, 474, 475, 476
Death <0.1% to 0.4% Meticulous performance of procedure, attentive postprocedure care NA NA 338, 343, 347, 458, 477
Gastric hypomotility 0% to 17% Reduce power, force, and RF time on posterior wall Endoscopy, barium swallow, gastric emptying study Metoclopramide, possibly intravenous erythromycin 478, 479, 480, 481, 482, 483, 484, 485, 486, 487, 488, 489, 490
Mitral valve entrapment <0.1% Avoid circular catheter placement near or across mitral valve; clockwise torque on catheter Echocardiography Gentle catheter manipulation, surgical extraction 491, 492, 493, 494, 495, 496, 497, 498
Pericarditis 0% to 50% None proven Clinical history, ECG, sedimentation rate, echocardiogram NSAID, colchicine, steroids 499, 500, 501, 502, 503, 504, 505, 506
Permanent phrenic nerve paralysis 0% to 0.4% Monitor diaphragm during phrenic pacing, CMAP monitoring, phrenic pacing to identify location and adjust lesion location CXR, sniff test Supportive care 9, 11, 156, 347, 367, 446, 457, 478, 479, 487, 488, 489, 490, 507, 508, 509, 510, 511, 512, 513, 514, 515, 516, 517, 518, 519, 520, 521, 522, 523, 524, 525, 526, 527, 528
Pulmonary vein stenosis <1% Avoid energy delivery within PV CT or MRI, V/Q wave scan Angioplasty, stent, surgery 9, 11, 313, 316, 317, 318, 319, 320, 321, 322, 323, 324, 325, 326, 327, 328, 329, 330, 331, 332, 333, 334, 335, 457, 529, 530, 531
Radiation injury <0.1% Minimize fluoroscopy exposure, especially in obese and repeat ablation patients, X-ray equipment None Supportive care, rarely skin graft 513, 532, 533, 534, 535, 536, 537, 538, 539, 540, 541, 542, 543, 544, 545, 546, 547, 548, 549, 550
Stiff left atrial syndrome <1.5% Limit extent of left atrial ablation Echocardiography, cardiac catheterization Diuretics 551, 552, 553, 554, 555, 556, 557, 558
Stroke and TIA 0% to 2% Pre-, post-, and intraprocedure anticoagulation, catheter and sheath management, TEE Head CT or MRI, cerebral angiography Thrombolytic therapy, angioplasty 10, 11, 12, 13, 338, 347, 367, 458, 559, 560, 561, 562, 563, 564, 565
Vascular complications 0.2% to 1.5% Vascular access techniques, ultrasound-guided access, anticoagulation management Vascular ultrasound, CT scan Conservative treatment, surgical repair, transfusion 338, 347, 371, 373, 374, 380, 458, 511, 566, 567, 568, 569, 570, 571, 572, 573, 574, 575

AF = atrial fibrillation; CT = computed tomography; MRI = magnetic resonance imaging; TEE = transesophageal electrocardiogram; RF = radiofrequency; PTCA = percutaneous transluminal coronary angioplasty; NA = not applicable; ECG = electrocardiogram; NSAID = nonsteroidal anti-inflammatory drug; CMAP = compound motor action potentials; CXR = chest X-ray; TIA = transient ischemic attack.

Section 11: Training Requirements

This section of the document outlines the training requirements for those who wish to perform catheter ablation of AF.

Section 12: Surgical and Hybrid AF Ablation

Please refer to Table 2 and Figure 8 presented earlier in this Executive Summary.

Section 13: Clinical Trial Design

Although there have been many advances made in the field of catheter and surgical ablation of AF, there is still much to be learned about the mechanisms of initiation and maintenance of AF and how to apply this knowledge to the still-evolving techniques of AF ablation. Although single-center, observational reports have dominated the early days of this field, we are quickly moving into an era in which hypotheses are put through the rigor of testing in well-designed, randomized, multicenter clinical trials. It is as a result of these trials that conventional thinking about the best techniques, success rates, complication rates, and long-term outcomes beyond AF recurrence–such as thromboembolism and mortality–is being put to the test. The ablation literature has also seen a proliferation of meta-analyses and other aggregate analyses, which reinforce the need for consistency in the approach to reporting the results of clinical trials. This section reviews the minimum requirements for reporting on AF ablation trials. It also acknowledges the potential limitations of using specific primary outcomes and emphasizes the need for broad and consistent reporting of secondary outcomes to assist the end-user in determining not only the scientific, but also the clinical relevance of the results (Table 10, Table 11, Table 12, Table 13).

Table 10.

Definitions for use when reporting outcomes of AF ablation and in designing clinical trials of catheter or surgical ablation of AF

Acute procedural success (pulmonary vein isolation) Acute procedural success is defined as electrical isolation of all pulmonary veins. A minimal assessment of electrical isolation of the PVs should consist of an assessment of entrance block. If other methods are used to assess PVI, including exit block and/or the use of provocative agents such as adenosine or isoproterenol, they should be prespecified. Furthermore, it is recommended that the wait time used to screen for early recurrence of PV conduction once initial electrical isolation is documented be specified in all prospective clinical trials.
Acute procedural success (not related by pulmonary vein isolation) Typically, this would apply to substrate ablation performed in addition to PVI for persistent AF. Although some have proposed AF termination as a surrogate for acute procedural success, its relationship to long-term success is controversial. Complete elimination of the additional substrate (localized rotational activation, scar region, non-PV trigger, or other target) and/or demonstration of bidirectional conduction block across a linear ablation lesion would typically be considered the appropriate endpoint.
One-year success One-year success is defined as freedom from AF/AFL/AT after removal from antiarrhythmic drug therapy as assessed from the end of the 3month blanking period to 12 months following the ablation procedure. Because cavotricuspid isthmus-dependent atrial flutter is easily treated with cavotricuspid isthmus ablation and is not an iatrogenic arrhythmia following a left atrial ablation procedure for AF, it is reasonable for clinical trials to choose to prespecify that occurrence of isthmus-dependent atrial flutter, if confirmed by entrainment maneuvers during electrophysiology testing, should not be considered an ablation failure or primary effectiveness endpoint.
Alternative one-year success Although the one-year success definition provided above remains the recommended end point that should be reported in all AF ablation trials, and the endpoint for which the objective performance criteria listed below were developed, the Task Force recognizes that alternative definitions for success can be used if the main goal of therapy in the study is to relieve AF-related symptoms and to improve patient QOL. In particular, it is appropriate for clinical trials to define success as freedom from only symptomatic AF/AFL/AT after removal from antiarrhythmic drug therapy as assessed from the end of the 3-month blanking period to 12 months following the ablation procedure if the main goal of therapy in the study is to relieve AF-related symptoms and to improve patient QOL. However, because symptoms of AF can resolve over time, and because studies have shown that asymptomatic AF represents a greater proportion of all AF postablation than prior to ablation, clinical trials need to continue to report freedom from both symptomatic and asymptomatic AF even if this alternative one year success definition is used as the primary trial endpoint.
Clinical/partial success It is reasonable for clinical trials to define and incorporate one or more secondary definitions of success that can be referred to as "clinical success" or "partial success." If these alternative definitions of success are included, they should be defined prospectively. In prior Consensus Documents the Task Force has proposed that clinical/partial success be defined as a "75% or greater reduction in the number of AF episodes, the duration of AF episodes, or the % time a patient is in AF as assessed with a device capable of measuring AF burden in the presence or absence of previously ineffective antiarrhythmic drug therapy." Because there is no firm scientific basis for selecting the cutoff of 75% rather than a different cutoff, this prior recommendation is provided only as an example of what future clinical trials may choose to use as a definition of clinical/partial success.
Long-term success Long-term success is defined as freedom from AF/AFL/AT recurrences following the 3-month blanking period through a minimum of 36-month follow-up from the date of the ablation procedure in the absence of Class I and III antiarrhythmic drug therapy.
Recurrent AF/AFL/AT Recurrent AF/AFL/AT is defined as AF/AFL/AT of at least 30 seconds׳ duration that is documented by an ECG or device recording system and occurs following catheter ablation. Recurrent AF/AFL/AT may occur within or following the post ablation blanking period. Recurrent AF/AFL/AT that occurs within the postablation blanking period is not considered a failure of AF ablation.
Early recurrence of AF/AFL/AT Early recurrence of AF/AFL/AT is defined as a recurrence of atrial fibrillation within three months of ablation. Episodes of atrial tachycardia or atrial flutter should also be classified as a "recurrence." These are not counted toward the success rate if a blanking period is specified.
Recurrence of AF/AFL/AT Recurrence of AF/AFL/AT postablation is defined as a recurrence of atrial fibrillation more than 3 months following AF ablation. Episodes of atrial tachycardia or atrial flutter should also be classified as a "recurrence."
Late recurrence of AF/AFL/AT Late recurrence of AF/AFL/AT is defined as a recurrence of atrial fibrillation 12 months or more after AF ablation. Episodes of atrial tachycardia or atrial flutter should also be classified as a "recurrence."
Blanking period A blanking period of three months should be employed after ablation when reporting efficacy outcomes. Thus, early recurrences of AF/AFL/AT within the first 3 months should not be classified as treatment failure. If a blanking period of less than 3 months is chosen, it should be prespecified and included in the Methods section.
Stroke screening A risk-based approach to determine the level of postablation stroke screening in clinical trials is recommended by the Task Force. For ablation devices with a lower risk of stroke and for which a stroke signal has not been reported, a minimum standardized neurological assessment of stroke should be conducted by a physician at baseline and at hospital discharge or 24 hours after the procedure, whichever is later. If this neurological assessment demonstrates new abnormal findings, the patient should have a formal neurological consult and examination with appropriate imaging (i.e., DW-MRI), used to confirm any suspected diagnosis of stroke. For devices in which a higher risk of stroke is suspected or revealed in prior trials, a formal neurological examination by a neurologist at discharge or 24 hours after the procedure, whichever is later, is recommended. Appropriate imaging should be obtained if this evaluation reveals a new neurological finding. In some studies in which delayed stroke is a concern, repeat neurological screening at 30 days postablation might be appropriate.
Detectable AF/AFL/AT Detectable AF is defined as AF/AFL/AT of at least 30 seconds׳ duration when assessed with ECG monitoring. If other monitoring systems are used, including implantable pacemakers, implantable defibrillators, and subcutaneous ECG monitoring devices, the definition of detectable AF needs to be prespecified in the clinical trial based on the sensitivity and specificity of AF detection with the particular device. We recommend that episodes of atrial flutter and atrial tachycardia be included within the broader definition of a detectable AF/AFL/AT episode.
AF/AFL/AT burden It is reasonable for clinical trials to incorporate AF/AFL/AT burden as a secondary endpoint in a clinical trial of AF ablation. In stating this it is recognized that there are no conclusive data that have validated a rate of AF burden reduction as a predictor of patient benefit (i.e. reduction in mortality and major morbidities such as stroke, CHF, QOL, or hospitalization). If AF burden is included, it is important to predefine and standardize the monitoring technique that will be used to measure AF burden. Available monitoring techniques have been discussed in this document. Should AF burden be selected as an endpoint in a clinical trial, the chosen monitoring technique should be employed at least a month prior to ablation to establish a baseline burden of AF.
Entrance block Entrance block is defined as the absence, or if present, the dissociation, of electrical activity within the PV antrum. Entrance block is most commonly evaluated using a circular multielectrode mapping catheter positioned at the PV antrum. Entrance block can also be assessed using detailed point-by-point mapping of the PV antrum guided by an electroanatomical mapping system. The particular method used to assess entrance block should be specified in all clinical trials. Entrance block of the left PVs should be assessed during distal coronary sinus or left atrial appendage pacing in order to distinguish far-field atrial potentials from PV potentials. It is recommended that reassessment of entrance block be performed a minimum of 20 minutes after initial establishment of PV isolation.
Procedural endpoints for AF ablation strategies not targeting the PVs Procedural endpoints for AF ablation strategies not targeting the PVs: The acute procedural endpoints for ablation strategies not targeting the PVs vary depending on the specific ablation strategy and tool. It is important that they be prespecified in all clinical trials. For example, if a linear ablation strategy is used, documentation of bidirectional block across the ablation line must be shown. For ablation of CFAEs, rotational activity, or non-PV triggers, the acute endpoint should at a minimum be elimination of CFAEs, rotational activity, or non-PV triggers. Demonstration of AF slowing or termination is an appropriate procedural endpoint, but it is not required as a procedural endpoint for AF ablation strategies not targeting the PVs.
Esophageal temperature monitoring Esophageal temperature monitoring should be performed in all clinical trials of AF ablation. At a minimum, a single thermocouple should be used. The location of the probe should be adjusted during the procedure to reflect the location of energy delivery. Although this document does not provide formal recommendations regarding the specific temperature or temperature change at which energy delivery should be terminated, the Task Force does recommend that all trials prespecify temperature guidelines for termination of energy delivery.
Enrolled subject An enrolled subject is defined as a subject who has signed written informed consent to participate in the trial in question.
Exit block Exit block is defined as the inability to capture the atrium during pacing at multiple sites within the PV antrum. Local capture of musculature within the pulmonary veins and/or antrum must be documented to be present to make this assessment. Exit block is demonstrated by a dissociated spontaneous pulmonary vein rhythm.
Nonablative strategies The optimal nonablative therapy for patients with persistent and long-standing persistent AF who are randomized to the control arm of an AF ablation trial is a trial of a new Class I or III antiarrhythmic agent or a higher dose of a previously failed antiarrhythmic agent. For patients with persistent or long-standing persistent AF, performance of a direct-current cardioversion while taking the new or dose adjusted antiarrhythmic agent should be performed, if restoration of sinus rhythm is not achieved following initiation and/or dose adjustment of antiarrhythmic drug therapy. Failure of pharmacological cardioversion alone is not adequate to declare this pharmacological strategy unsuccessful.
Noninducibility of atrial fibrillation Noninducibility of atrial fibrillation is defined as the inability to induce atrial fibrillation with a standardized prespecified pharmacological or electrical stimulation protocol. The stimulation protocol should be prespecified in the specific clinical trial. Common stimulation approaches include a high-dose isoproterenol infusion protocol or repeated atrial burst pacing at progressively more rapid rates.
Patient populations for inclusion in clinical trials It is considered optimal for clinical trials to enroll patients with only one type of AF: paroxysmal, persistent, or long-standing persistent. If more than one type of AF patient is enrolled, the results of the trial should also be reported separately for each of the AF types. It is recognized that "early persistent" AF responds to AF ablation to a similar degree as patients with paroxysmal AF and that the response of patients with "late persistent AF" is more similar to that in those with long-standing persistent AF.
Therapy consolidation period Following a 3-month blanking period, it is reasonable for clinical trials to incorporate an additional 1- to 3-month therapy consolidation period. During this time, adjustment of antiarrhythmic medications and/or cardioversion can be performed. Should a consolidation period be incorporated into a clinical trial design, the minimum follow-up duration should be 9 months following the therapy consolidation period. Performance of a repeat ablation procedure during the blanking or therapy consolidation period would "reset" the endpoint of the study and trigger a new 3-month blanking period. Incorporation of a therapy consolidation period can be especially appropriate for clinical trials evaluating the efficacy of AF ablation for persistent or long-standing persistent AF. The challenge of this approach is that it prolongs the overall study duration. Because of this concern regarding overall study duration, we suggest that the therapy consolidation period be no more than 3 months in duration following the 3-month blanking period.
Recommendations regarding repeat ablation procedures It is recommended that all clinical trials report the single procedure efficacy of catheter ablation. Success is defined as freedom from symptomatic or asymptomatic AF/AFL/AT of 30 seconds or longer at 12 months postablation. Recurrences of AF/AFL/AT during the first 3-month blanking period post-AF ablation are not considered a failure. Performance of a repeat ablation procedure at any point after the initial ablation procedure should be considered a failure of a single procedure strategy. It is acceptable for a clinical trial to choose to prespecify and use a multiprocedure success rate as the primary endpoint of a clinical trial. When a multiprocedure success is selected as the primary endpoint, efficacy should be defined as freedom from AF/flutter or tachycardia at 12 months after the final ablation procedure. In the case of multiple procedures, repeat ablation procedures can be performed at any time following the initial ablation procedure. All ablation procedures are subject to a 3-month post blanking window, and all ablation trials should report efficacy at 12 months after the final ablation procedure.
Cardioversion definitions
 Failed electrical cardioversion Failed electrical cardioversion is defined as the inability to restore sinus rhythm for 30 seconds or longer following electrical cardioversion.
 Successful electrical cardioversion Successful electrical cardioversion is defined as the ability to restore sinus rhythm for at least 30 seconds following cardioversion.
 Immediate AF recurrence postcardioversion Immediate AF recurrence postcardioversion is defined as a recurrence of AF within 24 hours following cardioversion. The most common time for an immediate recurrence is within 30–60 minutes postcardioversion.
 Early AF recurrence postcardioversion Early AF recurrence postcardioversion is defined as a recurrence of AF within 30 days of a successful cardioversion.
 Late AF recurrence postcardioversion Late AF recurrence postcardioversion is defined as recurrence of AF more than 30 days following a successful cardioversion.
Surgical ablation definitions
 Hybrid AF surgical ablation procedure Hybrid AF surgical ablation procedure is defined as a joint AF ablation procedure performed by electrophysiologists and cardiac surgeons either as part of a single "joint" procedure or performed as two preplanned separate ablation procedures separated by no more than 6 months.
 Surgical Maze ablation procedure Surgical Maze ablation procedure is defined as a surgical ablation procedure for AF that includes, at a minimum, the following components: (1) line from SVC to IVC; (2) line from IVC to the tricuspid valve; (3) isolation of the PVs; (4) isolation of the posterior left atrium; (5) line from MV to the PVs; (6) management of the LA appendage.
 Stand-alone surgical AF ablation A surgical AF ablation procedure during which other cardiac surgical procedures are not performed such as CABG, valve replacement, or valve repair.
 Nomenclature for types of surgical AF ablation procedures We recommend that the term "Maze" procedure is appropriately used only to refer to the biatrial lesion set of the Cox-Maze operation. It requires ablation of the RA and LA isthmuses. Less extensive lesion sets should not be referred to as a "Maze" procedure, but rather as a surgical AF ablation procedure. In general, surgical ablation procedures for AF can be grouped into three different groups: (1) a full biatrial Cox-Maze procedure; (2) PVI alone; and (3) PVI combined with left atrial lesion sets.
 Hybrid epicardial and endocardial AF ablation This term refers to a combined AF ablation procedure involving an off-pump minimally invasive surgical AF ablation as well as a catheter-based AF ablation procedure designed to complement the surgical lesion set. Hybrid ablation procedures may be performed in a single-procedure setting in a hybrid operating room or a cardiac catheterization laboratory environment, or it can be staged. When staged, it is most typical to have the patient undergo the minimally invasive surgical ablation procedure first following by a catheter ablation procedure 1 to 3 months later. This latter approach is referred to as a "staged Hybrid AF ablation procedure."
Minimum AF documentation, endpoints, TEE performance, and success rates in clinical trials
 Minimum documentation for paroxysmal AF The minimum AF documentation requirement for paroxysmal AF is (1) physician׳s note indicating recurrent self-terminating AF and (2) one electrocardiographically documented AF episode within 6 months prior to the ablation procedure.
 Minimum documentation for persistent AF The minimum AF documentation requirement for persistent AF is (1) physician׳s note indicating continuous AF >7 days but no more than 1 year and (2) a 24-hour Holter within 90 days of the ablation procedure showing continuous AF.
 Minimum documentation for early persistent AF The minimum AF documentation requirement for persistent AF is (1) physician׳s note indicating continuous AF >7 days but no more than 3 months and (2) a 24-hour Holter showing continuous AF within 90 days of the ablation procedure.
 Minimum documentation for long-standing persistent AF The minimum AF documentation requirement for long-standing persistent AF is as follows: physician׳s note indicating at least 1 year of continuous AF plus a 24-hour Holter within 90 days of the ablation procedure showing continuous AF. The performance of a successful cardioversion (sinus rhythm >30 seconds) within 12 months of an ablation procedure with documented early recurrence of AF within 30 days should not alter the classification of AF as long-standing persistent.
 Symptomatic AF/AFL/AT AF/AFL/AT that results in symptoms that are experienced by the patient. These symptoms can include but are not limited to palpitations, presyncope, syncope, fatigue, and shortness of breath. For patients in continuous AF, reassessment of symptoms after restoration of sinus rhythm is recommended to establish the relationship between symptoms and AF.
 Documentation of AF-related symptoms Documentation by a physician evaluating the patient that the patient experiences symptoms that could be attributable to AF. This does not require a time-stamped ECG, Holter, or event monitor at the precise time of symptoms. For patients with persistent AF who initially report no symptoms, it is reasonable to reassess symptom status after restoration of sinus rhythm with cardioversion.
 Minimum effectiveness endpoint for patients with symptomatic and asymptomatic AF The minimum effectiveness endpoint is freedom from symptomatic and asymptomatic episodes of AF/AFL/AT recurrences at 12 months following ablation, free from antiarrhythmic drug therapy, and including a prespecified blanking period.
 Minimum chronic acceptable success rate: paroxysmal AF at 12-month follow-up If a minimum chronic success rate is selected as an objective effectiveness endpoint for a clinical trial, we recommend that the minimum chronic acceptable success rate for paroxysmal AF at 12-month follow-up is 50%.
 Minimum chronic acceptable success rate: persistent AF at 12-month follow-up If a minimum chronic success rate is selected as an objective effectiveness endpoint for a clinical trial, we recommend that the minimum chronic acceptable success rate for persistent AF at 12-month follow-up is 40%.
 Minimum chronic acceptable success rate: long-standing persistent AF at 12-month follow-up If a minimum chronic success rate is selected as an objective effectiveness endpoint for a clinical trial, we recommend that the minimum chronic acceptable success rate for long-standing persistent AF at 12-month follow-up is 30%.
 Minimum follow-up screening for paroxysmal AF recurrence For paroxysmal AF, the minimum follow-up screening should include (1) 12-lead ECG at each follow-up visit; (2) 24-hour Holter at the end of the follow-up period (e.g., 12 months); and (3) event recording with an event monitor regularly and when symptoms occur from the end of the 3-month blanking period to the end of follow-up (e.g., 12 months).
 Minimum follow-up screening for persistent or long-standing AF recurrence For persistent and long-standing persistent AF, the minimum follow-up screening should include (1) 12-lead ECG at each follow-up visit; (2) 24-hour Holter every 6 months; and (3) symptom-driven event monitoring.
 Requirements for transesophageal echocardiogram It is recommended that the minimum requirement for performance of a TEE in a clinical trial should be those requirements set forth in ACC/AHA/HRS 2014 Guidelines for AF Management pertaining to anticoagulation at the time of cardioversion. Prior to undergoing an AF ablation procedure a TEE should be performed in all patients with AF of >48 hours׳ duration or of unknown duration if adequate systemic anticoagulation has not been maintained for at least 3 weeks prior to AF ablation. If a TEE is performed for this indication, it should be performed within 24 hours of the ablation procedure.

AF = atrial fibrillation; DW-MRI = diffusion-weighted magnetic resonance imaging; CHF = congestive heart failure; QOL = quality of life; ECG = electrocardiogram; CABG = coronary artery bypass grafting; PV = pulmonary vein; SVC = superior vena cava; IVC = inferior vena cava; CFAE = complex fractionated atrial electrogram; PVI = pulmonary vein isolation; AFL = atrial flutter; AT = atrial tachycardia; ACC = American College of Cardiology; AHA = American Heart Association; HRS = Heart Rhythm Society.

When reporting outcomes of AF ablation, the development of atrial tachycardia or atrial flutter should be included in the broad definition of recurrence following AF ablation. All studies should report freedom from AF, atrial tachycardia, and atrial flutter. These endpoints can also be reported separately. All studies should also clearly specify the type and frequency of ECG monitoring as well as the degree of compliance with the prespecified monitoring protocol.

Table 11.

Quality-of-life scales, definitions, and strengths

Scale Definition/Details Strengths/Weaknesses
Short Form (36) Health Survey (SF36)38
(General)
Consists of 8 equally weighted, scaled scores in the following sections: vitality, physical functioning, bodily pain, general health perceptions, physical role functioning, emotional role functioning, social role functioning, mental health. Each section receives a scale score from 0 to 100.
Physical component summary (PCS) and mental component summary (MCS) is an average of all the physically and mentally relevant questions, respectively.
The Short Form (12) Health Survey (SF12) is a shorter version of the SF-36, which uses just 12 questions and still provides scores that can be compared with SF-36 norms, especially for summary physical and mental functioning.
Gives more precision in measuring QOL than EQ-5D but can be harder to transform into cost utility analysis.
Advantages: extensively validated in a number of disease and health states. Might have more resolution than EQ-50 for AF QOL.
Disadvantages: not specific for AF, so might not have resolution to detect AF-specific changes in QOL.
EuroQol Five Dimensions Questionnaire (EQ-5D)39
(General)
Two components: Health state description is measured in five dimensions: mobility, self-care, usual activities, pain/discomfort, anxiety/depression. Answers may be provided on a three-level (3L) or five-level (5L) scale. In the Evaluation section, respondents evaluate their overall health status using a visual analogue scale (EQ-VAS). Results can easily be converted to quality-adjusted life years for cost utility analysis. Advantages: extensively validated in a number of disease and health states. Can easily be converted into quality-adjusted life years for cost-effectiveness analysis.
Disadvantages: might not be specific enough to detect AF-specific changes in QOL. Might be less specific than SF-36.
AF effect on Quality of Life Survey (AFEQT)40 (AF specific) 20 questions: 4 targeting AF-related symptoms, 8 evaluating daily function, and 6 assessing AF treatment concerns. Each item scored on a 7-point Likert scale. Advantages: brief, simple, very responsive to AF interventions. Good internal validity and well validated against a number of other global and AF-specific QOL scales. Used in CABANA.
Disadvantages: validation in only two published studies (approximately 219 patients).
Quality of Life Questionnaire for Patients with AF
(AF-QoL)41
(AF specific)
18-item self-administered questionnaire with three domains: psychological, physical, and sexual activity. Each item scores on a 5-point Likert scale. Advantages: brief, simple, responsive to AF interventions; good internal validity; used in SARA trial.
Disadvantages: external validity compared only to SF-36; formal validation in 1 study (approximately 400 patients).
Arrhythmia-Related Symptom Checklist (SCL)42 (AF specific) 16 items covering AF symptom frequency and symptom severity. Advantages: most extensively validated in a number of arrhythmia cohorts and clinical trials.
Disadvantages: time-consuming and uncertain generalizability.
Mayo AF Specific Symptom Inventory (MAFSI)43 (AF specific) 10 items covering AF symptom frequency and severity. Combination of 5- point and 3-point Likert scale responses.
Used in CABANA trial.
Advantages: validated in an AF ablation population and responsive to ablation outcome; used in CABANA trial.
Disadvantages: external validity compared only to SF-36; 1 validation study (approximately 300 patients).
University of Toronto Atrial Fibrillation Severity Scale (AFSS) (AF specific)44 10 items covering frequency, duration, and severity. 7-point Likert scale responses. Advantages: validated and reproducible; used in CTAF trial.
Disadvantages: time-consuming and uncertain generalizability.
Arrhythmia Specific Questionnaire in Tachycardia and Arrhythmia (ASTA)45 (AF specific) Records number of AF episodes and average episode duration during last 3 months. 8 symptoms and 2 disabling symptoms are recorded with scores from 1--4 for each. Advantages: validated in various arrhythmia groups; external validity compared with SCL, EQ5D, and SF-36; used in MANTRA-PAF; brief; simple.
Disadvantages: one validation study (approximately 300 patients).
European Heart Rhythm Association (EHRA)46 (AF specific) Like NYHA scale. I = no symptoms, II = mild symptoms not affecting daily activity, III = severe symptoms affecting daily activity, and IV = disabling symptoms terminating daily activities. Advantage: very simple, like NYHA.
Disadvantages: not used in studies and not well validated; not very specific; unknown generalizability.
Canadian Cardiovascular Society Severity of Atrial Fibrillation Scale (CCS-SAF)47 (AF specific) Like NYHA scale. O = asymptomatic, I = AF symptoms have minimal effect on patient׳s QOL, II = AF symptoms have minor effect on patient QOL, III = symptoms have moderate effect on patient QOL, IV= AF symptoms have severe effect on patient QOL. Advantages: very simple, like NYHA; validated against SF-36 and University of Toronto AFSS.
Disadvantages: poor correlation with subjective
AF burden; not very specific.

AF = atrial fibrillation; QOL = quality of life; CABANA = Catheter Ablation vs Anti-arrhythmic Drug Therapy for Atrial Fibrillation; SARA = Study of Ablation Versus antiaRrhythmic Drugs in Persistent Atrial Fibrillation; CTAF = Canadian Trial of Atrial Fibrillation; MANTRA-PAF = Medical ANtiarrhythmic Treatment or Radiofrequency Ablation in Paroxysmal Atrial Fibrillation; NYHA = New York Heart Association; AFSS = atrial fibrillation severity scale.

Table 12.

Non-AF recurrence--related endpoints for reporting in AF ablation trials

Stroke and bleeding endpoints Definitions/Details
Stroke (2014 ACC/AHA Key Data Elements) An acute episode of focal or global neurological dysfunction caused by brain, spinal cord, or retinal vascular injury as a result of hemorrhage or infarction. Symptoms or signs must persist ≥24 hours, or if documented by CT, MRI or autopsy, the duration of symptoms/signs may be less than 24 hours. Stroke may be classified as ischemic (including hemorrhagic transformation of ischemic stroke), hemorrhagic, or undetermined. Stroke disability measurement is typically performed using the modified Rankin Scale (mRS).
Transient ischemic attack (2014 ACC/AHA Key Data Elements) Transient episode of focal neurological dysfunction caused by brain, spinal cord, or retinal ischemia without acute infarction and with signs and symptoms lasting less than 24 hours.
Major bleeding (ISTH definition) Fatal bleeding AND/OR symptomatic bleeding in a critical area or organ, such as intracranial, intraspinal, intraocular, retroperitoneal, intraarticular, pericardial, or intramuscular with compartment syndrome AND/OR bleeding causing a fall in hemoglobin level of 2 g/dL (1.24 mmol/L) or more, or leading to transfusion of two or more units of blood.
Clinically relevant nonmajor bleed (ISTH definition) An acute or subacute clinically overt bleed that does not meet the criteria for a major bleed but prompts a clinical response such that it leads to one of the following: hospital admission for bleeding; physician-guided medical or surgical treatment for bleeding; change in antithrombotic therapy (including interruption or discontinuation).
Minor bleeding (ISTH definition) All nonmajor bleeds. Minor bleeds are further divided into clinically relevant and not.
Incidence and discontinuation of oral anticoagulation The number of patients receiving oral anticoagulation and the type of oral anticoagulation should be documented at the end of follow-up. If patients have their oral anticoagulation discontinued, the number of patients discontinuing, the timing of discontinuation, and the reasons for discontinuation of oral anticoagulation, as well as the clinical characteristics and stroke risk profile of the patients should be reported.

AF = atrial fibrillation; CT = computed tomography; MRI = magnetic resonance imaging.

Table 13.

Advantages and disadvantages of AF-related endpoints in AF ablation trials

Endpoint Advantages Disadvantages Relevance and Comments
Freedom from AF/AFL/AT recurrence "gold standard" is 30 seconds
  • -

    Has been in use for many years

  • -

    Can be used to compare results of new trials with historical trials

  • -

    Sets a high bar for AF elimination

  • -

    Can systematically underestimate the efficacy of AF ablation, particularly for persistent AF, if 30-second cutoff is used

  • -

    Particularly well suited for paroxysmal AF outcomes

  • -

    Reporting of cutoffs other than 30 seconds encouraged as secondary endpoints to better contextualize results

  • -

    May be reported as proportion of patients free from arrhythmia or time to recurrence

Freedom from stroke-relevant AF/AFL/AT-duration cutoff of 1 hour
  • -

    Useful for trials in which interest is more for prognostic change conferred by ablation rather than elimination of all arrhythmias

  • -

    No consistent definition of what a stroke-relevant duration of AF is: ranges from 6 minutes to 24 hours in literature

  • -

    More than 1 hour could be a useful cutoff based on results of 505 trial

  • -

    May be reported as proportion of patients free from arrhythmia or time to recurrence

Freedom from AF/AFL/AT requiring intervention (emergency visits, cardioversion, urgent care visit, reablation, etc.)
  • -

    Can provide an endpoint more relevant to systemic costs of AF recurrence

  • -

    Clinically relevant

  • -

    Will overestimate efficacy of ablation by ignoring shorter episodes not requiring intervention that still might be important to quality of life or stroke

  • -

    Determination of what is an "intervention" must be prespecified in protocol and biases mitigated to avoid over- or underintervention in the trial

Freedom from persistent AF/AFL/AT-duration cutoff of 7 days
  • -

    Useful for trials assessing additional substrate modification in persistent AF

  • -

    Can systematically overestimate the efficacy of AF ablation, particularly for persistent AF

  • -

    Can require continuous monitoring to definitively assess if episode is >7 days

Freedom from AF/AFL/AT on previously ineffective antiarrhythmic therapy
  • -

    If patient maintains sinus rhythm on previously ineffective drug therapy, this may be considered a clinically relevant, successful outcome

  • -

    Will increase the success rate compared with off-drug success

  • -

    May not be relevant to patients hoping to discontinue drug therapy

  • -

    Postablation drug and dosage of drug should be identical to preablation drug and dosage

Significant reduction in AF burden: >75% reduction from pre- to postablation and/or total postablation burden <12%
  • -

    Can be useful in persistent AF studies, but might not be suited for early, paroxysmal AF studies

  • -

    Ideally requires continuous monitoring using an implantable device

  • -

    No scientific basic exists showing that a 75% reduction in AF burden impacts hard endpoints, including heart failure, stroke, and mortality

  • -

    AF burden can be estimated by intermittent monitoring and reporting of patient symptoms and recurrences like a "time in therapeutic range" report for oral anticoagulation; see text

  • -

    Could also see 75% reduction in number and duration of AF episodes

  • -

    Because there is no firm scientific basis for selecting the cutoff of 75%, this prior recommendation is provided only as an example of what future clinical trials may choose to use as a definition of clinical/partial success

Prevention in AF progression: time to first episode of persistent AF (>7 days)
  • -

    Does not assume that total elimination of AF is required

  • -

    Well suited for paroxysmal or "early" AF studies in which goal is to prevent progression to persistent AF

  • -

    Prevention in progression might be irrelevant for stroke or thromboembolic outcomes

  • -

    Long follow-up time might be required unless population is "enriched"

  • -

    Can ideally require continuous implantable monitoring

  • -

    Might be useful for specific populations such as heart failure or hypertrophic cardiomyopathy, in which progression to persistent AF can lead to increased hospitalization

Regression of AF: reduction in burden to a given threshold or conversion of persistent to paroxysmal AF
  • -

    Does not assume that total elimination of AF is required

  • -

    Well suited for persistent "late" AF studies in which goal is to regress to paroxysmal AF, which might be easier to control with drug therapy

  • -

    Regression endpoint will overestimate efficacy of AF ablation

  • -

    Might ideally require continuous implantable monitoring

  • -

    Patients will require ongoing drug therapy

  • -

    Could be particularly useful for long-standing persistent AF populations with structural heart disease, heart failure, etc.

Acute AF termination during ablation procedure
  • -

    Could provide indication of successful modification of substrate responsible for maintaining AF, most relevant to persistent or long-standing persistent AF

  • -

    Limited studies have linked acute AF termination to long-term success

  • -

    Relevance of acute AF termination has not consistently been shown to correlate to long-term success

  • -

    Endpoint might not be relevant to paroxysmal AF patients in whom AF might terminate spontaneously

  • -

    Some studies employ administration of intravenous or oral antiarrhythmics during ablation that could cause spontaneous termination

  • -

    Studies consider termination as reversion to sinus rhythm, whereas others consider reversion to any regular tachycardia as termination

  • -

    Intraprocedural administration of preprocedural oral antiarrhythmics or intraprocedural intravenous antiarrhythmics are discouraged

  • -

    If antiarrhythmics are used, their use and dosage before and during the ablation should be clearly documented

  • -

    Termination to sinus rhythm and termination to another regular tachycardia (AT or AFL) should be separately reported

AF = atrial fibrillation; AFL = atrial flutter; AT = atrial tachycardia.

Unanswered Questions in AF Ablation

There is still much to be learned about the mechanisms of AF, techniques of AF ablation, and long-term outcomes. The following are unanswered questions for future investigation:

  • 1.

    AF ablation and modification of stroke risk and need for ongoing oral anticoagulation (OAC): The CHA2DS2-VASc score was developed for patients with clinical AF. If a patient has received a successful ablation such that he/she no longer has clinical AF (subclinical, or no AF), then what is the need for ongoing OAC? Are there any patients in whom successful ablation could lead to discontinuation of OAC?

  • 2.

    Substrate modification in catheter-based management of AF–particularly for persistent AF: What is the proper lesion set required beyond pulmonary vein isolation? Do lines and complex fractionated atrial electrogram (CFAE) have any remaining role? Are these approaches ill-advised or simply discouraged?

  • What is the role of targeting localized rotational activations? How do we ablate a localized rotational activation? How can scar be characterized and targeted for ablation? Do we need to replicate the MAZE procedure? Does the right atrium need to be targeted as well as the left atrium?

  • 3.

    Autonomic influence in AF: Is clinical AF really an autonomic mediated arrhythmia? Is elimination of ganglionated plexi required? Is there a role for autonomic modulation, for example, spinal cord or vagal stimulation?

  • 4.

    Contribution and modulation of risk factors on outcomes of AF ablation: Obesity reduction has been shown to reduce AF burden and recurrence in patients undergoing ablation. What is the role of bariatric surgery? Does the modulation of other risk factors influence outcome such as hypertension, sleep apnea, and diabetes?

  • 5.

    Outcomes in ablation of high-risk populations: Do high-risk populations benefit from AF ablation? Congestive heart failure has been assessed in smaller trials, but larger trials are required. Outcome data are needed in patients with very enlarged LAs, hypertrophic cardiomyopathy, patients with renal failure on dialysis, and the very elderly.

  • 6.

    Surgical vs catheter-based vs hybrid ablation: There should be more comparative work between percutaneous and minimally invasive surgical approaches. Both report similar outcomes, but there is a dearth of comparative data. Is there any patient benefit to hybrid procedures?

  • 7.

    How do we characterize patients who are optimal candidates for ablation? Preablation late gadolinium-enhanced (LGE)-magnetic resonance imaging (MRI) might identify patients with heavy burdens of scar who are unlikely to respond to ablation. These techniques must become reproducible and reliable and must be assessed in multicenter trials. Other markers need to be investigated, including genetic markers, biochemical markers, and clinical markers based on aggregated risk scores.

  • 8.

    The incremental role of new technologies: As newer and often more expensive technologies are produced for AF ablation, their definitive incremental value must be determined in order to justify change in practice or case cost. These technologies include global (basket) mapping techniques, newer ablation indices for assessing lesion durability, advanced imaging for viewing lesions in the myocardium, etc. New energy sources, including laser, low-intensity ultrasound, photonic particle therapy, external beam ablation, and MRI-guided ablation, must be assessed in comparative fashion.

  • 9.

    Outcomes of AF ablation: We need to better understand the clinical relevance of ablation outcomes. What is the significance of time to recurrence of 30 seconds of arrhythmia? How do we best quantify AF burden? How do these outcomes relate to quality of life and stroke risk?

  • 10.

    What is the role of surgical LA reduction? Does left atrial appendage (LAA) occlusion or obliteration improve outcome of persistent AF ablation with an accompanying reduction in stroke? Does ablation work through atrial size reduction? What is the incidence of "stiff atrial" syndrome and does this mitigate the clinical impact of ablation?

  • 11.

    Working in teams: What is the role of the entire heart team in AF ablation? Does a team approach achieve better outcomes than a "silo" approach?

  • 12.

    Improving the safety of catheter ablation: As ablation extends to more operators and less experienced operators, the statistical occurrence of complications will increase. We need newer techniques to minimize complications and institute standards for operators to improve the reproducibility of ablation results and safety profiles at a variety of centers worldwide.

  • 13.

    How does catheter ablation affect mortality, stroke, and hospitalization in broad and selected patient populations receiving catheter ablation for AF?

  • 14.

    Management of patients who fail initial attempts at catheter ablation: Should there be specific criteria for repeat ablations (e.g., atrial size, body mass index)? Should patients be referred for surgery for repeat ablation?

In order to address these and other important questions in the field of catheter and surgical AF ablation, we urge investigators to create and participate in multisite collaborations and electrophysiology research networks with involvement of senior and junior investigators on the steering committees to push forward the next phase of AF research. We also urge funding bodies to support these important initiatives.

Section 14: Conclusion

Catheter ablation of AF is a very commonly performed procedure in hospitals throughout the world. This document provides an up-to-date review of the indications, techniques, and outcomes of catheter and surgical ablation of AF. Areas for which a consensus can be reached concerning AF ablation are identified, and a series of consensus definitions have been developed for use in future clinical trials of AF ablation. Also included within this document are recommendations concerning indications for AF ablation, technical performance of this procedure, and training. It is our hope to improve patient care by providing a foundation for those involved with care of patients with AF as well as those who perform AF ablation. It is recognized that this field continues to evolve rapidly and that this document will need to be updated. Successful AF ablation programs optimally should consist of a cooperative team of cardiologists, electrophysiologists, and surgeons to ensure appropriate indications, procedure selection, and follow-up.

Acknowledgments

The authors acknowledge the support of Jun Dong, MD, PhD; Kan Fang, MD; and Mark Fellman at the Division of Cardiovascular Devices, Center for Devices and Radiological Health, U.S. Food and Drug Administration (FDA) during the preparation of this document. This document does not necessarily represent the opinions, policies, or recommendations of the FDA.

Footnotes

Developed in partnership with and endorsed by the European Heart Rhythm Association (EHRA), the European Cardiac Arrhythmia Society (ECAS), the Asia Pacific Heart Rhythm Society (APHRS), and the Latin American Society of Cardiac Stimulation and Electrophysiology (Sociedad Latinoamericana de Estimulación Cardíaca y Electrofisiología [SOLAECE]).

Developed in collaboration with and endorsed by the Society of Thoracic Surgeons (STS), the American College of Cardiology (ACC), the American Heart Association (AHA), the Canadian Heart Rhythm Society (CHRS), the Japanese Heart Rhythm Society (JHRS), and the Brazilian Society of Cardiac Arrhythmias (Sociedade Brasileira de Arritmias Cardíacas [SOBRAC]).

Chair: Hugh Calkins, MD, Johns Hopkins Medical Institutions, Baltimore, MD, USA.

Section Chairs:

Definitions, Mechanisms, and Rationale for AF Ablation: Shih-Ann Chen, MD, National Yang-Ming University, Taipei, Taiwan.

Modifiable Risk Factors for AF and Impact on Ablation: Jonathan M. Kalman, MBBS, PhD, Royal Melbourne Hospital and University of Melbourne, Melbourne, Australia.

Indications: Claudio Tondo, MD, PhD, Cardiac Arrhythmia Research Center, Centro Cardiologico Monzino, IRCCS, Department of Cardiovascular Sciences, University of Milan, Milan, Italy.

Strategies, Techniques, and Endpoints: Karl Heinz Kuck, MD, PhD, Asklepios Klinik St. Georg, Hamburg, Germany.

Technology and Tools: Andrea Natale, MD, Texas Cardiac Arrhythmia Institute, St. David׳s Medical Center, Austin, TX, USA.

Technical Aspects of Ablation to Maximize Safety and Anticoagulation: David E. Haines, MD, Beaumont Health System, Royal Oak, MI, USA.

Follow-up Considerations: Francis E. Marchlinski, MD, Hospital of the University of Pennsylvania, University of Pennsylvania School of Medicine, Philadelphia, PA, USA.

Outcomes and Efficacy: Matthew R. Reynolds, MD, MSc, Lahey Hospital and Medical Center, Burlington, MA, USA.

Complications: D. Wyn Davies, MD, Imperial College Healthcare NHS Trust, London, United Kingdom.

Training Requirements: Bruce D. Lindsay, MD, Cleveland Clinic, Cleveland, OH, USA.

Surgical and Hybrid AF Ablation: James R. Edgerton, MD, The Heart Hospital, Baylor Plano, Plano, TX, USA.

Clinical Trial Design: Atul Verma, MD, Southlake Regional Health Centre, University of Toronto, Toronto, Canada.

Correspondence: Heart Rhythm Society, 1325 G Street NW, Suite 400, Washington, DC 20005. E-mail address: clinicaldocs@hrsonline.org.

Appendix A

Supplementary data associated with this article can be found in the online version at 10.1016/j.joa.2017.08.001.

Appendix A. Supplementary material

Supplementary material

mmc1.doc (20.7MB, doc)

Table A1.

Author disclosure table

Writing group member Institution Consultant/Advisory board/Honoraria Speakers׳ bureau Research grant Fellowship support Stock options/Partner Board Mbs/Other
Hugh Calkins, MD (Chair) Johns Hopkins Medical Institutions, Baltimore, MD 1: Abbott Laboratories, 1: AtriCure, Inc., 1: Boston Scientific Corp., 1: Pfizer Inc., 1: St. Jude Medical, 1: Toray Industries Inc., 2: iRhythm, 3: Boehringer Ingelheim, 3: Medtronic, Inc. None 2: Medtronic, Inc., 2: Boston Scientific Corp. None None None
Gerhard Hindricks, MD (Vice-Chair) Heart Center Leipzig, Leipzig, Germany None None 1: SIEMENS, 3: Biosense Webster, Inc., 3: Stereotaxis, Inc., 4: BIOTRONIK,
5: Boston Scientific Corp., 5: St. Jude Medical
None None None
Riccardo Cappato, MD (Vice-Chair) Humanitas Research Hospital, Arrhythmias and Electrophysiology Research Center, Milan, Italy None None None None None None
Young-Hoon Kim, MD, PhD (Vice-Chair) Korea University, Seoul, South Korea None 1: St. Jude Medical 2: St. Jude Medical None None None
Eduardo B. Saad, MD, PhD (Vice-Chair) Hospital Pro-Cardiaco and Hospital Samaritano, Botafogo, Rio de Janeiro, Brazil None None None None None None
Luis Aguinaga, MD, PhD Centro Privado de Cardiología, Tucuman, Argentina None None None None None None
Joseph G. Akar, MD, PhD Yale University School of Medicine, New Haven, CT 1: Biosense Webster None None None None None
Vinay Badhwar, MD West Virginia University School of Medicine, Morgantown, WV None None None None None None
Josep Brugada, MD, PhD Cardiovascular Institute, Hospital Clínic, University of Barcelona, Catalonia, Spain None None None None None None
John Camm, MD St. George׳s University of London, London, United Kingdom 1: Actelion Pharmaceuticals, 1: Daiichi-Sankyo, 1: Eli Lilly, 1: Gilead Sciences, Inc., 1: Heart Metabolics, 1: InCarda Therapeutics, 1: InfoBionic, 1: Johnson and Johnson, 1: Medtronic, Inc., 1: Milestone, 1: Pfizer, Inc., 2: Boehringer Ingelheim, 2: Boston Scientific Corp., 2: Novartis 3: Bayer HealthCare, LLC 1: Daiichi-Sankyo, 1: Servier, 2: Bayer/Schering Pharma, 2: Boehringer Ingelheim 3: Boehringer Ingelheim, 3: Daiichi-Sankyo, 3: Pfizer, Inc. None None 0: European Heart Rhythm Association, 1: Oxford
Peng-Sheng Chen, MD Indiana University School of Medicine, Indianapolis, IN None None 5: National Institutes of Health None 5: Arrhythmotech None
Shih-Ann Chen, MD National Yang-Ming University, Taipei, Taiwan 1: Bayer/Schering Pharma, 1: Biosense Webster, 1: Boehringer Ingelheim, 1: Boston Scientific Corp., 1: Daiichi-Sankyo, 1: Medtronic Inc., 1: Pfizer Inc., 1: St. Jude Medical 1: St. Jude Medical 2: Biosense Webster, 2: St. Jude Medical None None None
Mina K. Chung, MD Cleveland Clinic, Cleveland, OH 0: Amarin, 0: BIOTRONIK, 0: Boston Scientific Corp., 0: Medtronic, Inc., 0: St. Jude Medical, 0: Zoll Medical Corporation 1: American College of Cardiology None None None 1: Up to Date
Jens Cosedis Nielsen, DMSc, PhD Aarhus University Hospital, Skejby, Denmark None None 5. Novo Nordisk Foundation None None None
Anne B. Curtis, MD University at Buffalo, Buffalo, NY 1: Daiichi-Sankyo, 1: Medtronic, Inc., 1: Projects in Knowledge, 2: St. Jude Medical None None None None None
D. Wyn Davies, MD Imperial College Healthcare NHS Trust, London, United Kingdom 1: Boston Scientific Corp., 1: Janssen Pharmaceuticals, 1: Medtronic, Inc., 1: Rhythmia Medical None None None 3: Rhythmia Medical None
John D. Day, MD Intermountain Medical Center Heart Institute, Salt Lake City, UT 1: BIOTRONIK, 1: Boston Scientific Corp., 3: St. Jude Medical None None None None None
André d’Avila, MD, PhD Hospital SOS Cardio, Florianopolis, SC, Brazil None 0: BIOTRONIK, 0: St. Jude Medical 0: BIOTRONIK, 0: St. Jude Medical None None None
N.M.S. (Natasja) de Groot, MD, PhD Erasmus Medical Center, Rotterdam, the Netherlands None None None None None None
Luigi Di Biase, MD, PhD Albert Einstein College of Medicine, Montefiore-Einstein Center for Heart & Vascular Care, Bronx, NY 1: Atricure, 1: Biosense Webster, Inc., 1: BIOTRONIK, 1: Boston Scientific Corp., 1: EpiEP, 1: Medtronic, Inc., 1: St. Jude Medical, 1: Stereotaxis, Inc. None None None None None
Mattias Duytschaever, MD, PhD Universitair Ziekenhuis Gent (Ghent University Hospital), Ghent, Belgium None None None None None None
James R. Edgerton, MD The Heart Hospital, Baylor Plano, Plano, TX 2: AtriCure, Inc. 1: AtriCure, Inc. 2: AtriCure, Inc. None None None
Kenneth A. Ellenbogen, MD Virginia Commonwealth University School of Medicine, Richmond, VA 1: American Heart Association, 1: Heart Rhythm Society, 2: Boston Scientific Corp. 1: AtriCure, Inc., 1: Biosense Webster, Inc., 1: BIOTRONIK, 1: St. Jude Medical, 2: Boston Scientific Corp., 2: Medtronic, Inc. 2: Biosense Webster, Inc., 2: Daiichi-Sankyo, 2: National Institutes of Health, 4: Boston Scientific Corp., 4: Medtronic, Inc. None None 1: Elsevier, 1: Wiley-Blackwell
Patrick T. Ellinor, MD, PhD Massachusetts General Hospital, Boston, MA 1: Bayer HealthCare, LLC, 1: Quest Diagnostics None 1: Leducq Foundation, 3: American Heart Association, 3: National Institutes of Health, 5: Bayer HealthCare, LLC None None None
Sabine Ernst, MD, PhD Royal Brompton and Harefield NHS Foundation Trust, National Heart and Lung Institute, Imperial College London, London, United Kingdom 2: Biosense Webster, Inc. None 4: Spectrum Dynamics None None None
Guilherme Fenelon, MD, PhD Albert Einstein Jewish Hospital, Federal University of São Paulo, São Paulo, Brazil 1: Biosense Webster, Inc., 1: BIOTRONIK, 1: St. Jude Medical None None None None None
Edward P. Gerstenfeld, MS, MD University of California, San Francisco, San Francisco, CA 1: Boehringer Ingelheim, 1: Boston Scientific Corp., 1: Medtronic, Inc., 1: St. Jude Medical None 4: Biosense Webster, Inc., 4: St. Jude Medical 2: Biosense Webster, Inc., 2: BIOTRONIK, 2: Boston Scientific Corp., 2: Medtronic, Inc. 1: Rhythm Diagnostic Systems Inc. None
David E. Haines, MD Beaumont Health System, Royal Oak, MI 1: Lake Region Medical, 1: Terumo Medical Corp None None None None 1: Biosense Webster, Inc., 1: Boston Scientific Corp., 1: Medtronic, Inc., 1: St. Jude Medical
Michel Haissaguerre, MD Hôpital Cardiologique du Haut-Lévêque, Pessac, France None None None None None None
Robert H. Helm, MD Boston University Medical Center, Boston, MA None None None None None 1: Boston Scientific Corp.
Elaine Hylek, MD, MPH Boston University School of Medicine, Boston, MA 1: Bayer, 1: Boehringer Ingelheim, 1: Bristol-Myers Squibb, 1: Daiichi-Sankyo, 1: Medtronic, 1: Portola, 1: Pfizer None 2: Janssen Pharmaceuticals None None None
Warren M. Jackman, MD Heart Rhythm Institute, University of Oklahoma Health Sciences Center, Oklahoma City, OK 1: ACT, 1: VytronUS, Inc., 2: Biosense Webster, Inc., 2: Boston Scientific Corp., 2: Spectrum Dynamics 1: BIOTRONIK, 1: St. Jude Medical, 2: Biosense Webster, Inc., 2: Boston Scientific Corp. None None None None
Jose Jalife, MD University of Michigan, Ann Arbor, MI, the National Center for Cardiovascular Research Carlos III (CNIC) and CIBERCV, Madrid, Spain 1: Topera Medical None 1: Medtronic, Inc. None None None
Jonathan M. Kalman, MBBS, PhD Royal Melbourne Hospital and University of Melbourne, Melbourne, Australia None 1: Boston Scientific Corp., 1: Medtronic, Inc. 4: Medtronic, Inc. 3: St. Jude Medical, 4: Biosense Webster, Inc., 4: Medtronic, Inc. None 2: Biosense Webster, Inc., 4: Boston Scientific Corp.
Josef Kautzner, MD, PhD Institute for Clinical and Experimental Medicine, Prague, Czech Republic 1: Bayer/Schering Pharma, 1: Boehringer Ingelheim, 1: Boston Scientific Corp., 1: Daiichi-Sankyo, 1: Sorin Group, 1: St. Jude Medical, 1: Biosense Webster, Inc., 2: Medtronic, Inc. 1: BIOTRONIK
1: Medtronic, Inc.
1: St. Jude Medical
None None None None
Hans Kottkamp, MD Hirslanden Hospital, Dept. of Electrophysiology, Zurich, Switzerland 1: Biosense Webster, Inc., 1: Kardium None None None 1: Kardium None
Karl Heinz Kuck, MD, PhD Asklepios Klinik St. Georg, Hamburg, Germany 1: Biosense Webster, Inc., 1: BIOTRONIK, 1: St. Jude Medical, 1: Stereotaxis, Inc. None 1: Biosense Webster, Inc., 1: BIOTRONIK, 1: St. Jude Medical, 1: Stereotaxis, Inc. None 1: Endosense None
Koichiro Kumagai, MD, PhD Heart Rhythm Center, Fukuoka Sanno Hospital, Fukuoka, Japan None None None None None None
Richard Lee, MD, MBA Saint Louis University Medical School, St. Louis, MO None None None None None None
Thorsten Lewalter, MD, PhD Dept. of Cardiology and Intensive Care, Hospital Munich-Thalkirchen, Munich, Germany 1: BIOTRONIK, 1: Medtronic, Inc., 1: St. Jude Medical 1: Abbott Vascular, 1: BIOTRONIK, 1: Medtronic, Inc., 1: St. Jude Medical None None None None
Bruce D. Lindsay, MD Cleveland Clinic, Cleveland, OH 0: Medtronic, Inc., 1: Abbott Vascular, 1: Biosense Webster, Inc. None None 3: Boston Scientific Corp., 3: Medtronic, Inc., 3: St. Jude Medical None None
Laurent Macle, MD Montreal Heart Institute, Department of Medicine, Université de Montréal, Montréal, Canada 1: Bayer HealthCare, LLC, 1: Biosense Webster, Inc., 1: Boehringer Ingelheim, 1: Bristol-Myers Squibb, 1: Medtronic, Inc., 1: Pfizer, Inc., 1: Servier, 1: St. Jude Medical None 4: Biosense Webster, Inc., 5: St. Jude Medical None None None
Moussa Mansour, MD Massachusetts General Hospital, Boston, MA 1: Biosense Webster, Inc., 1: St. Jude Medical None 4: Biosense Webster, Inc., 4: St. Jude Medical,
5: Pfizer,
5: Boehringer Ingelheim
None 4: NewPace Ltd. None
Francis E. Marchlinski, MD Hospital of the University of Pennsylvania, University of Pennsylvania School of Medicine, Philadelphia, PA 1: Abbot Medical; 1: Biosense Webster, Inc., 2: BIOTRONIK, 1: Medtronic, Inc., 1: Boston Scientific Corp., 1: St. Jude Medical None 3: Medtronic, Inc., 4: Biosense Webster, Inc. 1: BIOTRONIK, 3: Boston Scientific Corp., 3: Medtronic, Inc., 4: Biosense Webster, Inc., 5: St. Jude Medical None None
Gregory F. Michaud, MD Brigham and Women׳s Hospital, Boston, MA 1: Biosense Webster, Inc., 1: Boston Scientific Corp., 1: Medtronic, Inc., 1: St. Jude Medical None 4: Biosense Webster, Inc., 4: Boston Scientific Corp. None None None
Hiroshi Nakagawa, MD, PhD Heart Rhythm Institute, University of Oklahoma Health Sciences Center, Oklahoma City, OK 2: Biosense Webster, Inc 1: Boston Scientific Corp., 2: Stereotaxis, Inc., 3: Japan Lifeline, 3: Fukuda Denshi 1: Medtronic, Inc, 2: Boston Scientific Corp., 1: Spectrum Dynamics 4: Biosense Webster, Inc.,
2: Japan Lifeline,
2: Affera
None None None
Andrea Natale, MD Texas Cardiac Arrhythmia Institute, St. David׳s Medical Center, Austin, TX 1: Boston Scientific Corp., 1: Janssen Pharmaceuticals, 1: Medtronic, Inc., 1: St. Jude Medical, 2: Biosense Webster, Inc. None None None None None
Stanley Nattel, MD Montreal Heart Institute and Université de Montréal, Montreal, Canada, McGill University, Montreal, Canada, and University Duisburg-Essen, Essen, Germany 1: Merck Pharmaceuticals, 1: Xention Discovery None 3: OMEICOS Therapeutics None None 0: Montreal Heart Institute/Inventor Patents
Ken Okumura, MD, PhD Division of Cardiology, Saiseikai Kumamoto Hospital, Kumamoto, Japan 1: Biosense Webster, Inc., 1: Boehringer Ingelheim, 1: Bristol-Myers Squibb, 1: Medtronic, Inc., 2: Bayer/Schering Pharma, 3: Daiichi-Sankyo None 2: Biosense Webster, Inc., 2: Medtronic, Inc. None None None
Douglas Packer, MD Mayo Clinic, Rochester, MN 0: Abbott Laboratories, 0: Abiomed, 0: Aperture Diagnostics, 0: Biosense Webster, Inc., 0: Boston Scientific Corp., 0: CardioFocus, Inc., 0: CardioInsight Technologies, 0: Johnson and Johnson, 0: Johnson and Johnson Healthcare Systems, 0: MediaSphere Medical, LLC, 0: Medtronic CryoCath, 0: SIEMENS, 0: St. Jude Medical None 0: American Heart Association, 0: Boston Scientific/EPT, 0: CardioInsight, 0: Endosense, 0: SIEMENS Acuson, 0: SIEMENS Acunav, 1: CardioFocus, 1: Hansen Medical, 1: Medtronic, Inc. 2: National Institutes of Health, 3: Thermedical (EP Limited), 5: Biosense Webster, 5: St. Jude Medical None None 1: Medtronic, 1: Oxford Press (Royalty), 1: SIEMENS, 1: WebMD, 1: Wiley-Blackwell (Royalty), 2: Biosense Webster, 4: St. Jude Medical (Royalty)
Evgeny Pokushalov, MD, PhD State Research Institute of Circulation Pathology, Novosibirsk, Russia 1: Biosense Webster, Inc., 1: Boston Scientific Corp., 1: Medtronic, Inc. None None None None None
Matthew R. Reynolds, MD, MSc Lahey Hospital and Medical Center, Burlington, MA 1: Biosense Webster, Inc., 1: Medtronic, Inc., 1: St. Jude Medical None None None None None
Prashanthan Sanders, MBBS, PhD Centre for Heart Rhythm Disorders, South Australian Health and Medical Research Institute, University of Adelaide and Royal Adelaide Hospital, Adelaide, Australia 1: Biosense Webster, Inc., 1: Boston Scientific Corp., 1: CathRx, 1: Medtronic, Inc., 1: St. Jude Medical 1: Biosense Webster, Inc., 1: Boston Scientific Corp., 1: Medtronic, Inc., 1: St. Jude Medical 4: Sorin Group, 5: BIOTRONIK, 5: Boston Scientific Corp., 5: Medtronic, Inc., 5: St. Jude Medical None None None
Mauricio Scanavacca, MD, PhD Instituto do Coração (InCor), São Paulo, Brazil 1: Biosense Webster, Inc., 1: St. Jude Medical 1: Bayer/Schering Pharma, 1: Bristol-Myers Squibb, 1: Johnson and Johnson, 1: Daiichi-Sankyo 2: Johnson and Johnson 2: Johnson and Johnson None None
Richard Schilling, MD Barts Heart Centre, London, United Kingdom 1: Biosense Webster, Inc., 1: Boehringer Ingelheim, 1: Daiichi-Sankyo, 1: Hansen Medical, 1: Medtronic, Inc., 1: St. Jude Medical None 1: Boston Scientific Corp., 1: Hansen Medical, 1: Medtronic, Inc., 1: St. Jude Medical, 4: Boston Scientific Corp., 4: Medtronic, Inc., 4: St. Jude Medical None None None
Claudio Tondo, MD, PhD Cardiac Arrhythmia Research Center, Centro Cardiologico Monzino, IRCCS, Department of Cardiovascular Sciences, University of Milan, Milan, Italy None None None None None None
Hsuan-Ming Tsao, MD National Yang-Ming University Hospital, Yilan City, Taiwan None None None None None None
Atul Verma, MD Southlake Regional Health Centre, University of Toronto, Toronto, Canada 1: Bayer HealthCare, LLC, 1: Boehringer Ingelheim None 5: Bayer HealthCare, LLC, 5: Biosense Webster, Inc., 5: BIOTRONIK, 5: Medtronic, Inc. None None None
David J. Wilber, MD Loyola University of Chicago, Chicago, IL 1: Biosense Webster, Inc., 1: Janssen Pharmaceuticals, 1: Medtronic, Inc., 1: St. Jude Medical, 1: Thermedical None 1: Abbott Vascular, 1: Medtronic, Inc., 1: St. Jude Medical, 1: Thermedical, 3: Biosense Webster, Inc. 3: Biosense Webster, Inc., 3: Medtronic, Inc., 3: St. Jude Medical None 1: Elsevier, 1: Wiley-Blackwell, 4: American College of Cardiology Foundation
Teiichi Yamane, MD, PhD Jikei University School of Medicine, Tokyo, Japan 1: Bayer HealthCare, 1: Medtronic, 2: Abott Japan, 2: Daiichi-Sankyo, 2: Boehringer Ingelheim, 2: Bristol-Myers Squibb None 1: Boehringer Ingelheim, 1: Bayer HealthCare None None None

Number Value: 0 = $0; 1 = ≤ $10,000; 2 = > $10,000 to ≤ $25,000; 3 = > $25,000 to ≤ $50,000; 4 = > $50,000 to ≤ $100,000; 5 = > $100,000.

Dr. Cappato is now with the Department of Biomedical Sciences, Humanitas University, Milan, Italy, and IRCCS, Humanitas Clinical and Research Center, Milan, Italy

Table B1.

Reviewer disclosure table

Peer reviewer Institution Consultant/Advisory board/Honoraria Speakers׳ bureau Research grant Fellowship support Stock options/Partner Board Mbs/Other
Carina Blomström-Lundqvist, MD, PhD Department of Cardiology and Medical Science, Uppsala University, Uppsala, Sweden 1: Bayer/Schering Pharma, 1: Boston Scientific Corp., 1: Medtronic, Inc., 1: Sanofi, 1: Pfizer, MSD, Bristol-Myers Squibb, Biosense Webster, Inc. None 1: Cardiome Pharma/Astellas, 1: Medtronic, Inc. None None None
Angelo A.V. De Paola, MD, PhD Hospital São Paulo -- Federal University of São Paulo, São Paulo, Brazil None None None None None None
Peter M. Kistler, MBBS, PhD The Alfred Hospital Heart Centre, Melbourne, Australia None 1: St. Jude Medical None None None None
Gregory Y.H. Lip, MD University of Birmingham, Birmingham, United Kingdom; Aalborg University, Aalborg, Denmark 1: Medtronic,
3: Bayer/Janssen, BMS/Pfizer, Boehringer Ingelheim, Daiichi-Sankyo
3: Bayer, BMS/Pfizer, Boehringer Ingelheim, Daiichi-Sankyo. No fees are received personally None None None None
Nicholas S. Peters, MD St Mary׳s Hospital, Imperial College London, London, United Kingdom 1: Boston Scientific Corp., 1: Cardialen, Inc., 1: Cardiologs, 1: Magnetecs, 1: Medtronic, Inc., 1: St. Jude Medical None None None None None
Cristiano F. Pisani, MD InCor, Heart Insitute, HCFMUSP, Arrhythmia Unit None None None None None None
Antonio Raviele, MD ALFA-Alliance to Fight Atrial Fibrillation, Rimini, Italy None None None None None None
Eduardo B. Saad, MD, PhD Hospital Pro-Cardiaco and Hospital Samaritano, Botafogo, Rio de Janeiro, Brazil None None None None None None
Kazuhiro Satomi, MD, PhD Tokyo Medical University, Tokyo, Japan 1: Bayer/Schering Pharma, 1: Boehringer Ingelheim, 1: Bristol-Myers Squibb, 1: Japan Lifeline, 1: Johnson and Johnson, 1: Medtronic, Inc., 1: Sankyo Pharmaceuticals, 1: St. Jude Medical None None None None None
Martin K. Stiles, MB ChB, PhD Waikato Hospital, Hamilton, New Zealand 1: Boston Scientific Corp., 1: Biosense Webster, Inc., 1: BIOTRONIK, 1: Medtronic, Inc. None None 1: Medtronic, Inc. None None
Stephan Willems, MD, PhD University Medical Center Hamburg-Eppendorf, Hamburg, Germany 1: Bayer HealthCare, LLC, 1: Biosense Webster, Inc., 1: Boehringer Ingelheim, 1: Bristol-Myers Squibb, 1: Sanofi, 1: St. Jude Medical, 1: Medtronic None None None None None

Number Value: 0 = $0; 1 = ≤ $10,000; 2 = > $10,000 to ≤ $25,000; 3 = > $25,000 to ≤ $50,000; 4 = > $50,000 to ≤ $100,000; 5 = > $100,000.

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