Download Atrial Fibrillation

Atrial Fibrillation
(AF)
Disclaimer

2
All St. Jude Medical products should be used only according to
FDA approved indications. Discussion surrounding therapeutic
techniques in no way constitutes a recommendation of or
training toward the utilization of St. Jude Medical products
Objectives
3

To understand the Clinical Considerations of
the physician when dealing with AF

To understand the Mechanisms and Causes
of AF

To learn to visualize Significant Anatomy
relevant to AF

To discuss Tools and Techniques relevant to
treating AF
Clinical Considerations

Epidemiology

Atrial fibrillation is the
most common clinically
significant cardiac
arrhythmia in the world.

Approximately one third
of hospitalizations for
cardiac rhythm
disturbance

2.3 million people in the
United States and 4.5
million in the European
Union have paroxysmal or
persistent AF

Hospital admissions for AF
have increased by 66%
due to the aging
population
Issa, Z.F., Miller, J.M., & Zipes, D.P. (2009). Atrial Fibrillation. In Z.F. Issa,
J.M. Miller & D.P. Zipes, Clinical Arrhythmology and Electrophysiology
(208-284). Philadelphia: Saunders Elsevier
4
Clinical Considerations

Epidemiology

AF is associated with an
increased long-term risk of
stroke, heart failure, and allcause mortality, especially
in women

The mortality rate of patients
with AF is about double that
of patients in NSR and is
linked to the severity of
underlying heart disease

The most devastating
consequence of AF is stroke
as a result of
thromboembolism

1 out of every 6 strokes
occurs in patients with AF
ACCF/AHA Pocket Guideline. Management of Patients with Atrial
Fibrillation. Adapted from the 2006 ACC/AHA/ESC Guidline and the
2011 ACCF/AHA/HRS Focused Updates)
5
Clinical Considerations

Risk Stratification

CHADS2 Score

Prior Cerebrovascular
accident (CVA)

Prior transient ischemic
attack (TIA)

Age

History of hypertension
(HTN)

Diabetes

Heart failure (HF)
ACCF/AHA Pocket Guideline. Management of Patients with Atrial
Fibrillation. Adapted from the 2006 ACC/AHA/ESC Guidline and the
2011 ACCF/AHA/HRS Focused Updates)
6
7
O
nl
y
Clinical
Considerations
Clinical Presentation


Symptomatic or asymptomatic,
even in the same patient



up to 21% of newly diagnosed
patients with newly diagnosed
AF are asymptomatic
Symptoms associated with AF
vary with:

ventricular rate

underlying functional status

duration of AF

presence and degree of
structural heart disease

individual patient perception
Most patients with AF complain
of palpitations, angina, dyspnea,
fatigue, or dizziness
Issa, Z.F., Miller, J.M., & Zipes, D.P. (2009). Atrial Fibrillation. In Z.F. Issa,
J.M. Miller & D.P. Zipes, Clinical Arrhythmology and Electrophysiology
(208-284). Philadelphia: Saunders Elsevier
9
Clinical
Presentation
Initial Evaluation
10


Characterize the pattern of the arrhythmia

How long have they had it?

How long have they experienced symptoms?

Cardioversions in the past?

What drugs are they on?

Determine underlying causes (heart failure, pulmonary
problems, hypertension, or hyperthyroidism)

Define associated cardiac and extracardiac conditions
Issa, Z.F., Miller, J.M., & Zipes, D.P. (2009). Atrial Fibrillation. In Z.F. Issa,
J.M. Miller & D.P. Zipes, Clinical Arrhythmology and Electrophysiology
(208-284). Philadelphia: Saunders Elsevier
Classification of AF
11
First detected
episode
Permanent
(Cardioversion
failed)
Recurrent
(After 2
episodes)
AF
Persistent
7days – 1 year
ACCF/AHA Pocket Guideline. Management of Patients with Atrial
Fibrillation. Adapted from the 2006 ACC/AHA/ESC Guidline and the
2011 ACCF/AHA/HRS Focused Updates)
Paroxysmal
(selfterminates)
12
Clinical
Presentation
Patient Management
13




Four Main Issues that must be addressed
1.
Prevention of systemic embolization (clot)
2.
Rate control
3.
Rhythm control
4.
Choosing between rhythm and rate control
Choice of therapy is influenced by:

Patient preference

Associated structural heart disease

Severity of symptoms

Whether the AF is recurrent paroxysmal, recurrent persistent, or
permanent (chronic)
In addition, patient education is critical, given the potential
morbidity associated with AF and its treatment.
Issa, Z.F., Miller, J.M., & Zipes, D.P. (2009). Atrial Fibrillation. In Z.F. Issa,
J.M. Miller & D.P. Zipes, Clinical Arrhythmology and Electrophysiology
(208-284). Philadelphia: Saunders Elsevier
Electrocardiographic
Features
14
15
Electrocardiographic
Characterized by rapid and irregular atrial fibrillatory waves (f
waves) and lack of clearly defined P waves
Features
Best seen  Lead V1 and in the inferior leads (II, III, and AVF).



Rate of the fibrillatory waves -- between 350 and 600 beats/min


The atrium twitches “like bags of worms”
Ventricular response is typically irregularly irregular at a rate of
90-170 beats/min
Issa, Z.F., Miller, J.M., & Zipes, D.P. (2009). Atrial Fibrillation. In Z.F. Issa,
J.M. Miller & D.P. Zipes, Clinical Arrhythmology and Electrophysiology
(208-284). Philadelphia: Saunders Elsevier
Pathophysiology

Although useful, this classification does not account
for all presentations of AF and is not clearly related
to any specific pathophysiology or mechanism of
arrhythmogenesis

Pattern of AF may change in response to treatment


Paroxysmal often progresses to Persistent

Persistent can deteriorate into Permanent or Chronic

Persistent may become Paroxysmal with drug therapy
or catheter ablation
Distinction between classifications is not only a
function of the underlying arrhythmia, but also the
clinical pragmatism of the patient and physician
Issa, Z.F., Miller, J.M., & Zipes, D.P. (2009). Atrial Fibrillation. In Z.F. Issa,
J.M. Miller & D.P. Zipes, Clinical Arrhythmology and Electrophysiology
(208-284). Philadelphia: Saunders Elsevier
16
Mechanisms

Two concepts of the underlying mechanism of AF have
received considerable attention:
1.
Factors that trigger the onset of AF
2.
Factors that perpetuate AF

Patients with frequent, self-terminating episodes of AF are
likely to have a predominance of factors that trigger AF

Patients with AF that does not terminate spontaneously
are more likely to have a predominance of factors that
perpetuate AF

This generalization has clinical usefulness, but there is
considerable overlap of these mechanisms in the typical
AF patient
Issa, Z.F., Miller, J.M., & Zipes, D.P. (2009). Atrial Fibrillation. In Z.F. Issa,
J.M. Miller & D.P. Zipes, Clinical Arrhythmology and Electrophysiology
(208-284). Philadelphia: Saunders Elsevier
17
Mechanisms of Initiation

Stable focus (PAC) or
reentrant circuit with
activation arising from this
focus too rapid to be
conducted uniformly
throughout the atria

Rapid propagation of the
wave fronts breaks up into
irregular wavelets

Mechanism of initiation of AF
is not certain in most cases
and likely is multifactorial
18
Murgatroyd, F.D., Krahn, A.D., Klein, G.J., Yee, R.K, &
Skanes, A..C(2001). Atrial Arrhythmias. In Murgatroyd, F.D.,
Krahn, A.D., Klein, G.J., Yee, R.K, & Skanes, Handbook of
Cardiac Electrophysiology (55-71). London: ReMEDICA
Publishing Limited
Issa, Z.F., Miller, J.M., & Zipes, D.P. (2009). Atrial Fibrillation. In Z.F. Issa,
J.M. Miller & D.P. Zipes, Clinical Arrhythmology and Electrophysiology
(208-284). Philadelphia: Saunders Elsevier
Mechanisms of Initiation

AF Triggers

Premature Atrial Complexes (PACs) from the Pulmonary Veins (PVs),
Coronary Sinus (CS), Superior Vena Cava (SVC), Ligament of
Marshall, Left Atrial chamber, RA chamber (crista terminalis)

Sympathetic or Parasympathetic stimulation

Other Supraventricular Tachycardia (SVT)


19
AVRT, AFL, AVNRT
Identification and treatment of triggers may be curative
Issa, Z.F., Miller, J.M., & Zipes, D.P. (2009). Atrial Fibrillation. In Z.F. Issa,
J.M. Miller & D.P. Zipes, Clinical Arrhythmology and Electrophysiology
(208-284). Philadelphia: Saunders Elsevier
Mechanisms of Initiation

Triggering foci of rapidly
firing cells within the sleeves
of atrial myocytes extending
into the PVs have been
clearly shown to be the
underlying mechanism of
most paroxysmal AF

Thoracic veins are highly
arrhythmogenic

PV-LA Junction has
discontinuous myocardial
fibers separated by fibrotic
tissues and, therefore, is
highly anisotropic
More information can be found on page 210
20
Mechanisms of Perpetuation 21





Multiple wavelets of
depolarization propagate
within the atria.
These can divide, coalesce
extinguish each other as
they travel in an apparently
random fashion, seeking
tissue that is excitable.
Results in electrical and
structural remodeling

Atrial Dilation

Decreased Atrial
Refractoriness
Larger Hearts Fibrillate Easily
(Elephant and Whale)
Smaller Hearts Do Not
Fibrillate Easily (Mice)
Murgatroyd, F.D., Krahn, A.D., Klein, G.J., Yee, R.K, &
Skanes, A..C(2001). Atrial Arrhythmias. In Murgatroyd, F.D.,
Krahn, A.D., Klein, G.J., Yee, R.K, & Skanes, Handbook of
Cardiac Electrophysiology (55-71). London: ReMEDICA
Publishing Limited
Issa, Z.F., Miller, J.M., & Zipes, D.P. (2009). Atrial Fibrillation. In Z.F. Issa,
J.M. Miller & D.P. Zipes, Clinical Arrhythmology and Electrophysiology
(208-284). Philadelphia: Saunders Elsevier
Anatomy
Nathan, H., et al. “The Junction Between the Left Atrium and the Pulmonary
Veins: An Anatomic Study of Human Hearts.” Circ, Vol. 34, (1966): 412-422.
Print.
22
Anatomy
Nathan, H., et al. “The Junction Between the Left Atrium and the
Pulmonary Veins: An Anatomic Study of Human Hearts.” Circ, Vol. 34,
(1966): 412-422. Print.
23
Anatomy
Armour, J.A. ET AL. “Gross and Microscopic Anatomy of the Human Intrinsic
Cardiac Nervous System.”The Anatomical Record. Vol. 247.(1997):289–298.
Print.
24
Anatomy
Armour, J.A. ET AL. “Gross and Microscopic Anatomy of the Human Intrinsic
Cardiac Nervous System.”The Anatomical Record. Vol. 247.(1997):289–298.
Print.
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Electrophysiology Study

Pre-Procedure Considerations

Stop antiarrhythmic medications more than 5 days before

Anticoagulated with warfarin (INR, 2 to 3) for more than 4
to 6 weeks before the ablation procedure

Warfarin usually stopped 2 to 5 days before the procedure

TEE to screen for LA thrombus (mandatory in patients who
are in AF at the time of the procedure)

Optional magnetic resonance (MR) imaging or contrastenhanced, multi-slice CT scan of the LA with 3-D
reconstruction
Issa, Z.F., Miller, J.M., & Zipes, D.P. (2009). Atrial Fibrillation. In Z.F. Issa,
J.M. Miller & D.P. Zipes, Clinical Arrhythmology and Electrophysiology
(208-284). Philadelphia: Saunders Elsevier
41
Electrophysiology Study

Pre-Procedural Planning Considerations

Conscious sedation or general anesthesia?

Transseptal access tools and sheaths

Diagnostic catheters

HIS

CS

PV

TEE

Intracardiac Echo (ICE)
Item 100057675 Rev A
Issa, Z.F., Miller, J.M., & Zipes, D.P. (2009). Atrial Fibrillation. In Z.F. Issa,
J.M. Miller & D.P. Zipes, Clinical Arrhythmology and Electrophysiology
(208-284). Philadelphia: Saunders Elsevier
42
Spectrum of Techniques





Elimination of Triggers
 Pulmonary Vein Triggers
 Segmental Ostial
Pulmonary Vein Isolation
 Circumferential Antral
Pulmonary Vein Isolation
Substrate Modification
 Wide Area
Circumferential (WACA)
 Linear Atrial Method
Complex Fractionated Atrial
Electrogram (CFAE)
Central Nervous System
Denervation
Non-Pulmonary Vein Triggers
Issa, Z.F., Miller, J.M., & Zipes, D.P. (2009). Atrial Fibrillation. In Z.F. Issa,
J.M. Miller & D.P. Zipes, Clinical Arrhythmology and Electrophysiology
(208-284). Philadelphia: Saunders Elsevier
43
44
Focal
Pulmonary
Vein
1998  Haissaguerre demonstrated that PAF initiated by
spontaneous triggers (94% within the PVs)
Triggers
AF initiated with a burst of rapid firing from foci within 2 to 4 cm
of the ostium of the PV




Advantages
 Shorter procedure time, less fluoroscopy, potential cure
 Can be done without a 3D Mapping System
Limitations:
 High Rate of PV stenosis
 Probability of more than one culprit vein  Frequent
recurrences
 Difficult to elicit PV arrhythmia in the EP laboratory to allow
adequate mapping.
 Does not address reentry in the substrate (persistent or
chronic pts)
 Requires double or triple transseptal access
Issa, Z.F., Miller, J.M., & Zipes, D.P. (2009). Atrial Fibrillation. In Z.F. Issa,
J.M. Miller & D.P. Zipes, Clinical Arrhythmology and Electrophysiology
(208-284). Philadelphia: Saunders Elsevier
Focal Pulmonary Vein
Triggers
45
Pulmonary Vein Stenosis
Kato et al. “Pulmonary vein anatomy in patients
undergoing catheter ablation of atrial fibrillation: lessons
learned by use of magnetic resonance imaging.”
Circulation. Vol.107. (2003): 2004-10. Print.
Robbins, ER, et al, “Pulmonary vein stenosis after
catheter ablation of atrial fibrillation.” Circulation Vol. 98
(1998) :1769. Print
Focal Pulmonary Vein
Triggers
Issa, Z.F., Miller, J.M., & Zipes, D.P. (2009). Atrial Fibrillation. In Z.F. Issa,
J.M. Miller & D.P. Zipes, Clinical Arrhythmology and Electrophysiology
(208-284). Philadelphia: Saunders Elsevier
46
Segmental Ostial
Pulmonary Vein Isolation



Map segments of the ostium at which muscle fibers
extending from the LA into the PV are present (PV muscle
potentials)
Advantages:
 No risk of PV stenosis
 Easy to identify PV potentials
 Short case times, less fluoroscopy
 Eliminates the need for detailed mapping of
spontaneous ectopy
Limitations
 1-4 PVs (Time vs. Recurrence)
 Anatomical variance between PVs can add to
difficulty and time
 Does not account for reentry in the substrate
 Requires double or triple transseptal access
Issa, Z.F., Miller, J.M., & Zipes, D.P. (2009). Atrial Fibrillation. In Z.F. Issa,
J.M. Miller & D.P. Zipes, Clinical Arrhythmology and Electrophysiology
(208-284). Philadelphia: Saunders Elsevier
47
Segmental Ostial
Pulmonary Vein Isolation
Kato et al. “Pulmonary vein anatomy in patients undergoing catheter ablation
of atrial fibrillation: lessons learned by use of magnetic resonance imaging.”
Circulation. Vol.107. (2003): 2004-10. Print.
More information can be found on page 232-33
48
Segmental Ostial Pulmonary
Vein Isolation
Issa, Z.F., Miller, J.M., & Zipes, D.P. (2009). Atrial Fibrillation. In Z.F. Issa,
J.M. Miller & D.P. Zipes, Clinical Arrhythmology and Electrophysiology
(208-284). Philadelphia: Saunders Elsevier
49
Segmental Ostial Pulmonary Vein Isolation
Issa, Z.F., Miller, J.M., & Zipes, D.P. (2009). Atrial Fibrillation. In Z.F. Issa,
J.M. Miller & D.P. Zipes, Clinical Arrhythmology and Electrophysiology
(208-284). Philadelphia: Saunders Elsevier
50
Segmental Ostial Pulmonary
Vein Isolation
Issa, Z.F., Miller, J.M., & Zipes, D.P. (2009). Atrial Fibrillation. In Z.F. Issa,
J.M. Miller & D.P. Zipes, Clinical Arrhythmology and Electrophysiology
(208-284). Philadelphia: Saunders Elsevier
51
Circumferential Antral
Pulmonary Vein Isolation



Focusing on the outermost atrial side of the antral-LA
junction rather than at the ostium.
Advantages:

Isolates PVs and accounts for foci in the antrum

Does does not rely on localizing the sites of electrical
breakthroughs into the PV  easier to perform during AF

Easier to account for variation in PV anatomy (e.g. common
antrum)

Begins to account for reentry in the substrate

Less chance for PV stenosis

Modifies posterior wall and areas of CNS innervation
Limitations

Longer cases and more potential for complications (other
than stenosis)

Can create AT/AFL post procedure

Relies upon a good 3D reconstruction/registration of anatomy
Issa, Z.F., Miller, J.M., & Zipes, D.P. (2009). Atrial Fibrillation. In Z.F. Issa,
J.M. Miller & D.P. Zipes, Clinical Arrhythmology and Electrophysiology
(208-284). Philadelphia: Saunders Elsevier
52
Circumferential Antral
Pulmonary Vein Isolation
Kato et al. “Pulmonary vein anatomy in patients undergoing catheter ablation
of atrial fibrillation: lessons learned by use of magnetic resonance imaging.”
Circulation. Vol.107. (2003): 2004-10. Print.
53
Circumferential Antral
ICE Guided Positioning at the PV
Pulmonary
Vein Isolation
antrum


The anatomical region within the
ablation circles typically
encompasses the entire posterior
wall, LA roof, and anteroseptal
extension of the right PVs

ICE can help visualize evolving
microbubble formation during
tissue heating.

Microbubble formation,
however, is not a straightforward
surrogate for tissue heating
Issa, Z.F., Miller, J.M., & Zipes, D.P. (2009). Atrial Fibrillation. In Z.F. Issa,
J.M. Miller & D.P. Zipes, Clinical Arrhythmology and Electrophysiology
(208-284). Philadelphia: Saunders Elsevier
54
Circumferential Antral
Pulmonary Vein Isolation

Endpoint  electrical isolation of all four PVs (just like
segmental ostial PVI)

Reconfirmation of isolation after 60 min has been
suggested to detect early recurrence of PV conduction

Studies using ICE-guided circumferential PV isolation have
reported a success rate after the first procedure of about
80%, with higher success rates seen in younger patients
with paroxysmal AF

One study compared segmental ostial PV isolation and
circumferential extraostial PV isolation. At 11 ± 3 months’
follow-up, 60% of patients in the segmental group were
free of AF, compared with 75% of patients in the
circumferential group
Issa, Z.F., Miller, J.M., & Zipes, D.P. (2009). Atrial Fibrillation. In Z.F. Issa,
J.M. Miller & D.P. Zipes, Clinical Arrhythmology and Electrophysiology
(208-284). Philadelphia: Saunders Elsevier
55
Wide Area Circumferential
(WACA)


Advantages
 Efficacy is not dependent upon complete and lasting
PV disconnection from the LA
 Can be done with a single transseptal access
 Eliminates AF by addressing other mechanisms 
Substrate reentry, CNS denervation, Ligament of
Marshall, Bachmann’s Bundle
 Tailored lesion sets to accommodate unusual anatomy
 Does not require identification of PV potentials
 Risk of PV stenosis is decreased
Limitations
 More lesions = longer cases and more potential for
complications (other than stenosis)
 Can create AT/AFL post procedure
 Relies upon a good 3D reconstruction/registration of
anatomy
Issa, Z.F., Miller, J.M., & Zipes, D.P. (2009). Atrial Fibrillation. In Z.F. Issa,
J.M. Miller & D.P. Zipes, Clinical Arrhythmology and Electrophysiology
(208-284). Philadelphia: Saunders Elsevier
56
Wide Area Circumferential
(WACA)







Can use activation mapping in correlation with
voltage mapping to assess lesion sets
PVI Isolation is not required
Termination of AF occurs in about one third of pts
If AF does not terminate, cardioversion is performed
at the end of the procedure
If AF recurs immediately, the completeness of the
lines is reassessed and additional lines should be
considered
WACA ablation may create macroreentrant circuits
in the LA, mediating conversion of AF into AFL
Inducibility of AF after ablation was found to be a
significant independent predictor of recurrent AF
Issa, Z.F., Miller, J.M., & Zipes, D.P. (2009). Atrial Fibrillation. In Z.F. Issa,
J.M. Miller & D.P. Zipes, Clinical Arrhythmology and Electrophysiology
(208-284). Philadelphia: Saunders Elsevier
57
Linear Left Atrial

Success of surgical linear lesions has led to the
development of the catheter-based approach

Address the substrate

Preevent reentry

Eliminate non-PV foci

Roof line, mitral isthmus line, cavotricuspid isthmus
line

Used to do posterior and anterior lines  deemed
proarrhythmic or dangerous
Issa, Z.F., Miller, J.M., & Zipes, D.P. (2009). Atrial Fibrillation. In Z.F. Issa,
J.M. Miller & D.P. Zipes, Clinical Arrhythmology and Electrophysiology
(208-284). Philadelphia: Saunders Elsevier
58
Complex Fractionated
Atrial Electrograms (CFAE)






Map sites with complex fractionated atrial electrograms
(CFAEs) during AF
May represent continuous reentry of the fibrillation waves
into the same area or overlap of different wavelets
entering the same area at different times
May indicate the presence of a driver or a rotor
What defines a CFAE?
“CFAEs are defined as (1) atrial electrograms that are
fractionated and composed of two deflections or more,
and/or have a perturbation of the baseline with
continuous deflection of a prolonged activation complex
over a 10-second recording period, or (2) atrial
electrograms with a very short CL (120 milliseconds or less)
averaged over a 10-second recording period”
An important limitation of this approach is that the visual
appearance of CFAEs is variable and they are often of
very low amplitude
Issa, Z.F., Miller, J.M., & Zipes, D.P. (2009). Atrial Fibrillation. In Z.F. Issa,
J.M. Miller & D.P. Zipes, Clinical Arrhythmology and Electrophysiology
(208-284). Philadelphia: Saunders Elsevier
59
Complex Fractionated
Atrial Electrograms (CFAE)
Issa, Z.F., Miller, J.M., & Zipes, D.P. (2009). Atrial Fibrillation. In Z.F. Issa,
J.M. Miller & D.P. Zipes, Clinical Arrhythmology and Electrophysiology
(208-284). Philadelphia: Saunders Elsevier
60
Autonomic Nervous
System Denervation
Hyperactivity of the intrinsic autonomic nervous
system constitutes a dysautonomia that can lead to
a greater propensity for AF
 Denervation of the autonomic nerves at a few
specific sites on that heart that are directly related
to arrhythmia formation
 Ganglionated plexuses are located predominantly
in six regions of the atria. In the LA, they are located
around the antral regions of the PVs and in the crux.
In the RA, they are localized at the junction of the
RA and SVC
 How do you know where they are?



Anatomy or vagal response using high-frequency
electrical nerve stimulation
Endpoint, Outcome, and Repeatability?
Issa, Z.F., Miller, J.M., & Zipes, D.P. (2009). Atrial Fibrillation. In Z.F. Issa,
J.M. Miller & D.P. Zipes, Clinical Arrhythmology and Electrophysiology
(208-284). Philadelphia: Saunders Elsevier
61
Superior Vena Cava Isolation62

Proximal SVC contains cardiac muscles connected to the RA, and
atrial excitation can propagate into the SVC

The SVC myocardial extension harbors most (up to 55%) non-PV
triggers of AF (especially in females), and elimination of SVC triggers is
associated with improved long-term maintenance of sinus rhythm
post–AF ablation.
Issa, Z.F., Miller, J.M., & Zipes, D.P. (2009). Atrial Fibrillation. In Z.F. Issa,
J.M. Miller & D.P. Zipes, Clinical Arrhythmology and Electrophysiology
(208-284). Philadelphia: Saunders Elsevier
Cryothermy

Biomechanics

Biophysics
63

Pressurized cryorefrigerant
Nitrous Oxide (N20)

3 Phases of lesion formation
1. Freeze/thaw phase
2. Hemorrhagic-inflammatory
phase
3. Replacement-fibrosis phase
Andrade, J, et al. “The Biophysics and Biomechanics of Cryoballoon Ablation.”
Pacing and Clinical Electrophysiology.Vol. 35:9, (2012): 1162–1168.
DOI: 10.1111/j.1540-8159.2012.03436.x
Challenges
64
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Phrenic Nerve Palsy (PNP)
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Pulmonary Vein Stenosis
Andrade, J, et al. “The Biophysics and Biomechanics of Cryoballoon Ablation.”
Pacing and Clinical Electrophysiology.Vol. 35:9, (2012): 1162–1168.
DOI: 10.1111/j.1540-8159.2012.03436.x
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