1882 PART 6 Disorders of the Cardiovascular System
First-degree AV block
Fixed PR prolongation
Second-degree Mobitz I (Wenckebach) AV block
Progressive prolongation of PR interval followed by a nonconduct P wave
Second-degree Type II AV block
Fixed PR interval prior to a
nonconducted P wave
N N h h
v1
v
v3
v
v
Complete (third-degree) AV block
AV dissociation with ventricular rate slower than atrial rate
FIGURE 245-1 Types of atrioventricular (AV) block. The upper left figure displays fixed prolongation of the PR interval. The upper right figure demonstrates Mobitz I block
(Wenckebach AV block) manifested as progressive prolongation of the PR interval followed by a nonconducted P wave (“dropped beat”). The lower left figure displays AV
block with P wave with no QRS complex and no associated PR prolongation prior to the dropped beat (Mobitz type II AV block). The lower right figure demonstrates complete
heart block manifested as dissociation between P waves and QRS complexes (AV dissociation).
TABLE 245-2 Causes of AV Block
Fibrosis/sclerosis/calcification of the conduction system
Senile degeneration of the conduction system (Lev’s disease)
Lenègre’s disease
Calcification of the aortic valve annulus (mitral—less common)
Iatrogenic
After cardiac surgery (including valve surgery)
TAVR/alcohol septal ablation
Complication from catheter ablation
Medication (beta blockers, verapamil, diltiazem, digoxin)
Toxin/overdose/poisoning
Acute MI/coronary ischemia
Infectious causes
Lyme carditis
Bacterial endocarditis with perivalvular abscess
Viral myocarditis
Chagas’ disease
Toxoplasmosis
Infiltrative heart disease/inflammatory disease
Sarcoidosis
Amyloid
Rheumatologic disease: reactive arthritis (Reiter’s syndrome), SLE, RA,
systemic sclerosis
Congenital AV block
Maternal lupus
Idiopathic congenital AV block
Congenital heart defects
Genetic
Endocrine (e.g., thyroid disease, hypoadosteronism)
Autoimmune disease
Neuromuscular disease (e.g., myotonic dystrophy, Kearns-Sayre syndrome, Erb’s
dystrophy)
Lymphoma
Enhanced vagal tone/neurocardiogenic
Abbreviations: AV, atrioventricular; MI, myocardial infarction; RA, rheumatoid
arthritis; SLE, systemic lupus erythematosus; TAVR, transcatheter aortic valve
replacement.
unstable escape rhythms and a worse prognosis with high mortality
rates.
AV conduction abnormalities may be caused by either direct ischemia to the conduction system or enhanced autonomic tone (BezoldJarisch reflex). Conduction abnormalities can be considered based on
infarct location, and this may also predict which conduction abnormalities may be reversible. High-grade AV block associated with inferior
MI is often located proximal to the His bundle in 90% of patients.
Narrow junctional escape typically occurs with rates >40 beats/min,
and a temporary pacemaker is typically not required as the AV block
is often reversible and successfully managed with pharmacologic
therapy. High-grade AV block in the setting of anterior MI is typically
indicative of extensive infarction, is more often distal to the AV node,
and is associated with a high mortality rate. Temporary pacing in this
circumstance is typically indicated. CHB in the setting of anterior MI
may also be preceded by RBB block due to the arterial supply of the
proximal RBB.
■ INFECTIOUS CAUSES OF AV BLOCK
Infection can also cause AV block. AV block is a common manifestation of Lyme carditis due to infection with Borrelia burgdorferi. AV
block is typically at the level of the AV node with narrow junctional
escape rhythm >40 beats/min. Less commonly, conduction abnormalities can occur below the level of the AV node or in the sinus node. AV
block typically improves within 1 week of antibiotic therapy, although
a longer time frame can occur in some patients. AV block in the setting
of infective endocarditis should raise concern for perivalvular abscess,
which may necessitate surgical intervention. Viral myocarditis, Chagas’
disease, and toxoplasmosis are less common infectious causes of AV
block. Infiltrative heart disease such as cardiac sarcoid, amyloid, and
hemochromatosis can present as AV block. Autoimmune diseases,
including systemic lupus erythematosus (SLE), rheumatoid arthritis,
mixed connective tissue disease, and scleroderma, may cause AV block
due to infiltration of the conduction system. Rare malignancies also
may impair AV conduction.
■ AUTONOMIC AND FUNCTIONAL CAUSES OF AV
BLOCK
Functional causes of AV block (autonomic, metabolic/endocrine, and
drug-related) tend to be reversible. Most other etiologies produce
structural changes, typically fibrosis, in segments of the AV conduction
The Bradyarrhythmias: Disorders of the Atrioventricular Node
1883CHAPTER 245
400 ms
There is a slowing of the
sinus rate prior to AV block
AV block in the setting of
high vagal tone during sleep
30 s
17 mm/mV, 8 s
FIGURE 245-2 Evidence of atrioventricular (AV) block during sleep. During sleep, increased vagal tone leads to sinus bradycardia with associated Mobitz I (Wenckebach)
AV block. See Fig. 245-1 for an explanation of Mobitz I block.
axis that are generally permanent. Heightened vagal tone during sleep
or in well-conditioned individuals can be associated with all grades of
AV block (Fig. 245-2).
Carotid sinus hypersensitivity, vasovagal syncope, and cough and
micturition syncope may be associated with SA node slowing and
AV conduction block. Transient metabolic and endocrinologic disturbances and a number of pharmacologic agents also may produce
reversible AV conduction block.
■ ACQUIRED AV BLOCK FROM FIBROSIS AND
INFILTRATIVE CARDIOMYOPATHIES
Idiopathic progressive fibrosis of the conduction system is one of the
more common and degenerative causes of AV conduction block. Aging
is associated with degenerative changes in the summit of the ventricular septum, central fibrous body, and aortic and mitral annuli and has
been described as “sclerosis of the left cardiac skeleton.” The process
typically begins in the fourth decade of life and may be accelerated by
atherosclerosis, hypertension, and diabetes mellitus. Accelerated forms
of progressive familial heart block have been identified in families with
mutations in the cardiac sodium channel gene (SCN5A) and other loci
that have been mapped to chromosomes 1 and 19.
AV conduction block has been associated with heritable neuromuscular diseases, including the nucleotide repeat disease myotonic
dystrophy, the mitochondrial myopathy Kearns-Sayre syndrome, and
several of the monogenic muscular dystrophies.
■ CONGENITAL AV BLOCK
Congenital AV block may be observed in complex congenital cardiac
anomalies, such as transposition of the great arteries, ostium primum
ASDs, VSDs, endocardial cushion defects, and some single-ventricle
defects. Congenital AV block in the setting of a structurally normal
heart has been seen in children born to mothers with SLE and other
autoimmune diseases.
DIAGNOSTIC TESTING
Patients with conduction abnormalities should be evaluated for the
presence or absence of structural heart disease. Physical exam may
reveal valvular heart disease. ECG may suggest concomitant disease
that predisposes to conduction abnormalities. Echocardiography is
also indicated to evaluate for structural heart disease including valvular
abnormalities, ejection fraction, and ventricular wall motion. Because
age-dependent progressive fibrosis of the conduction system is the
most common cause, AV node block that develops at a younger age
(≤60 years) may warrant advanced imaging such as chest computed
tomography (CT), cardiac magnetic resonance imaging (MRI), or CT/
positron emission tomography (PET) scan to further evaluate for infiltrative heart disease such as sarcoidosis. Advanced imaging may also be
warranted based on other factors in the history and testing that suggest
the need for evaluation of infiltrative heart disease. Evaluation for cardiac ischemia should be driven by the clinical suspicion at presentation
(e.g., symptoms of ischemia, ECG abnormalities, etc.) (Fig. 245-3).
Diagnostic testing in the evaluation of AV block is aimed at determining the level of conduction block, particularly in asymptomatic
patients, since the prognosis and therapy depend on whether the block
is in or below the AV node. Vagal maneuvers, carotid sinus massage,
exercise, and administration of drugs such as atropine and isoproterenol may be diagnostically informative. Owing to the differences in the
innervation of the AV node and infranodal conduction system, vagal
stimulation and carotid sinus massage slow conduction in the AV node
but have less of an effect on infranodal tissue and may even appear to
improve conduction due to a reduced rate of activation of distal tissues.
Conversely, atropine, isoproterenol, and exercise improve conduction
through the AV node and may appear to impair infranodal conduction.
In patients with congenital CHB and a narrow QRS complex, exercise
typically increases heart rate; by contrast, those with acquired CHB,
particularly with wide QRS, do not respond to exercise with an increase
in heart rate.
Additional diagnostic evaluation, including electrophysiologic testing, may be indicated in patients with syncope and suspected highgrade AV block. This is particularly relevant if noninvasive testing
does not reveal the cause of syncope or if the patient has structural
heart disease with ventricular tachyarrhythmias as a cause of symptoms. Electrophysiologic testing provides more precise information
regarding the location of AV conduction block and permits studies of
AV conduction under conditions of pharmacologic stress and exercise.
Recording of the His bundle electrogram by a catheter positioned at the
superior margin of the tricuspid valve annulus provides information
about conduction at all levels of the AV conduction axis. A properly
recorded His bundle electrogram reveals local atrial activity, the His
electrogram, and local ventricular activation; when it is monitored
simultaneously with recorded body surface ECG traces, intra-atrial, AV
nodal, and infranodal conduction times can be assessed. The time from
the most rapid deflection of the atrial electrogram in the His bundle
recording to the His electrogram (AH interval) represents conduction
through the AV node and is normally <130 ms. The time from the His
electrogram to the earliest onset of the QRS on the surface ECG (HV
interval) represents the conduction time through the His-Purkinje
system and is normally ≤55 ms (Fig. 245-4).
Rate stress produced by pacing can unveil abnormal AV conduction.
Mobitz I second-degree AV block at short atrial paced cycle lengths is a
normal response. However, when it occurs at atrial cycle lengths >500 ms
(<120 beats/min) in the absence of high vagal tone, it is abnormal. Typically, type I second-degree AV block is associated with prolongation
of the AH interval, representing conduction slowing and block in the
AV node. AH prolongation occasionally is due to the effect of drugs
(beta blockers, calcium channel blockers, digitalis) or increased vagal
tone. Atropine can be used to reverse high vagal tone; however, if AH
prolongation and AV block at long pacing cycle lengths persist, intrinsic AV node disease is likely. Type II second-degree block is typically
infranodal, often in the His-Purkinje system. Block below the node
with prolongation of the HV interval or a His bundle electrogram with
no ventricular activation is abnormal unless it is elicited at fast pacing
rates or short coupling intervals with extra stimulation. It is often difficult to determine the type of second-degree AV block when 2:1 conduction is present; however, the finding of a His bundle electrogram
after every atrial electrogram indicates that block is occurring in the
distal conduction system.
Intracardiac recording at an electrophysiologic study that reveals
prolongation of conduction through the His-Purkinje system (i.e., long
1884 PART 6 Disorders of the Cardiovascular System
Evidence for AV
block
Reversible or
physiologic cause
Transthoracic
echocardiography
(Class I)
Transthoracic
echocardiography
(Class IIa)
Mobitz
type II 2nd AV block,
advanced AV block,
complete heart
block
Treatment
effective or not
necessary
Treat underlying cause as
needed, e.g., sleep apnea
(Class I)
Observe
Observe Observe
Symptoms Symptoms
Exercise testing
(Class IIa)
Electrophysiology
study
(Class IIb)
AV node
(Mobitz type I)
Determine
site of AV
block
Treat identified
abnormalities
Advanced
imaging*
(Class IIa)
Advanced
imaging*
(Class IIa)
AV node
Unclear
e.g., 2:1 AV block
Suspicion
for infiltrative CM,
endocarditis, ACHD,
etc. Suspicion
for infiltrative CM,
endocarditis, ACHD,
etc.
Suspicion
for structural heart
disease
AV block
treatment
algorithm
AV block
treatment
algorithm
AV block
treatment
algorithm
AV block
treatment
algorithm
AV block
treatment
algorithm
Yes
Yes
Yes
Yes
Yes
Yes Yes
Yes
No
No
No
No No
No No
No
Intranodal
Intranodal
Infranodal
FIGURE 245-3 Initial evaluation of suspected atrioventricular (AV) block algorithm. *Targeted advanced imaging—magnetic resonance imaging (MRI): amyloidosis,
myocarditis, hemochromatosis, sarcoidosis, congenital heart disease (CHD), sinus of Valsalva aneurysm, aortic dissection, arrhythmogenic right ventricular
cardiomyopathy; fluorodeoxyglucose-positron emission tomography (FDG-PET): sarcoidosis; technetium-99m pyrophosphate (Tc PYP) or 99m technetium 3,3-diphosphono1,2-propanodicarboxylic acid (TC-DPD): transthyretin (TTR) amyloidosis; cardiac computed tomography (CT): CHD, sinus of Valsalva. ACHD, adult CHD; CM, cardiomyopathy.
(Reproduced with permission from FM Kusumoto et al: 2018 ACC/AHA/HRS guideline on the evaluation and management of patients with bradycardia and cardiac conduction
delay. Heart Rhythm 16:e128, 2019.)
The Bradyarrhythmias: Disorders of the Atrioventricular Node
1885CHAPTER 245
I
II
III
V1
HI Sd
HI Sp
RVA
HRA
HA
H A
H A
H A
H A
H A
V
FIGURE 245-4 High-grade atrioventricular (AV) block below the His. The AH interval is normal and is not changing before the block. Atrial and His bundle electrograms
are recorded consistent with block below the distal AV junction. I, II, III, and V1
are surface ECG leads. HISp, HISd, and RVA are the proximal HIS, distal HIS, and right
ventricular apical electrical recordings, respectively. A, H, and V represent the atrial, His, and ventricular electrograms on the His bundle recording, respectively. (Courtesy
of Dr. Joseph Marine.)
HV interval) is associated with an increased risk of progression to
higher grades of block and is generally an indication for pacing. In the
setting of bundle branch block, the HV interval may reveal the condition of the unblocked bundle and the prognosis for developing more
advanced AV conduction block. Prolongation of the HV interval in
patients with asymptomatic bundle branch block is associated with an
increased risk of developing higher-grade AV block. The risk increases
with greater prolongation of the HV interval such that in patients with
an HV interval >100 ms, the annual incidence of complete AV block
approaches 10%, indicating a need for pacing. In patients with acquired
CHB, even if intermittent, there is little role for electrophysiologic testing, and pacemaker implantation is almost always indicated.
TREATMENT
Acute Management of AV Conduction Block
The first-line strategies for management of AV block should be
to eliminate reversible causes and to determine the immediate
safety and reliability of the heart rhythm (e.g., escape rhythm) and
whether or not temporary or permanent pacing is warranted. The
need for temporary pacing is determined by the symptoms of the
patient, hemodynamic status, and the estimate of the level at which
AV block is present. In a general sense, the lower in the conduction
system that an escape rhythm is occurring, the lower is the reliability of the escape rhythm. A narrow-complex junctional escape of
45 beats/min with no symptoms does not warrant urgent temporary
pacing, whereas a wide-complex (implying block lower in the conduction system) escape rhythm at 30 beats/min does. Elimination
of unnecessary medications known to slow AV conduction (e.g.,
beta blockers, diltiazem, verapamil, digoxin), correction of electrolyte abnormalities, ischemia, and inhibition of excessive vagal tone
may increase the heart rate. Adjunctive pharmacologic treatment
with atropine or isoproterenol may be useful if the block is in the
AV node. When pacing is indicated, the most expeditious technique
is the use of transcutaneous pacing, where pacing patches are placed
anteriorly over the cardiac apex (cathode) and posteriorly between
the spine and the scapula or above the right nipple (anode). Acutely,
transcutaneous pacing is highly effective, but its duration is limited
by patient discomfort and longer-term failure to capture the ventricle owing to changes in lead impedance. Transvenous temporary
pacing is more reliable, and a pacing wire can be placed from the
jugular, subclavian, or femoral venous system and advanced to the
right ventricle, permitting stable temporary pacing.
AV conduction abnormalities may be reversible in certain circumstances including removal of unnecessary medication or toxins,
correction of electrolyte abnormalities, relief of ischemia, treatment
of certain infiltrative heart disease (e.g., immunosuppression in
cardiac sarcoidosis), and treatment of sleep apnea in patients with
nocturnal vagally mediated AV block. When symptomatic or infranodal AV block is not reversible, which is often the case, permanent
pacing is warranted.
PERMANENT PACEMAKER IMPLANTATION
The indications for pacing in AV conduction block are shown in
Fig. 245-5. In patients with acquired Mobitz type II AV block,
high-grade AV block, or third-degree AV block that is not reversible
or physiologic, permanent pacing is recommended regardless of
symptoms. For all other types of AV block, in the absence of conditions associated with progressive AV conduction abnormalities,
permanent pacing should generally be considered only in the presence of symptoms that correlate with block. In patients with neuromuscular disease and other progressive cardiomyopathies affecting
the conduction system, permanent pacemaker implantation is recommended for marked first-degree AV block and Mobitz I AV
block. Pacemaker implantation should be performed in any patient
1886 PART 6 Disorders of the Cardiovascular System
with symptomatic bradycardia and irreversible second- or thirddegree AV block, regardless of the cause or level of block in the
conducting system. Symptoms may include those directly related to
bradycardia and low cardiac output or to worsening heart failure,
angina, or intolerance to an essential medication. Pacing in patients
with asymptomatic AV block should be individualized; situations in
which pacing should be considered are patients with acquired CHB,
particularly in the setting of cardiac enlargement; left ventricular
dysfunction; and waking heart rates ≤40 beats/min. Patients who
have asymptomatic second-degree AV block of either type should
be considered for pacing if the block is demonstrated to be intra- or
infra-His or is associated with a wide QRS complex. Pacing may
be indicated in asymptomatic patients in special circumstances, in
patients with profound first-degree AV block and left ventricular
dysfunction in whom a shorter AV interval produces hemodynamic
improvement, and in the setting of milder forms of AV conduction
delay (first-degree AV block, intraventricular conduction delay)
in patients with neuromuscular diseases that have a predilection
for the conduction system, such as myotonic dystrophy and other
muscular dystrophies and Kearns-Sayre syndrome.
AV block in acute MI is often transient, particularly in inferior
infarction. The circumstances in which pacing is indicated in acute
MI are persistent second- or third-degree AV block, particularly
if symptomatic, and transient second- or third-degree AV block
associated with bundle branch block. Pacing is generally not indicated in the setting of transient AV block in the absence of intraventricular conduction delays or in the presence of fascicular block
or first-degree AV block that develops in the setting of preexisting
bundle branch block. Fascicular blocks that develop in acute MI in
the absence of other forms of AV block also do not require pacing.
Distal forms of AV conduction block may require pacemaker
implantation in certain clinical settings. Patients with bifascicular
or trifascicular block and symptoms, particularly syncope that
is not attributable to other causes, should undergo pacemaker
implantation. Permanent pacemaker implantation is indicated in
asymptomatic patients with bifascicular or trifascicular block who
experience intermittent third-degree block, type II second-degree
AV block, or alternating bundle branch block. In patients with
fascicular block who are undergoing electrophysiologic study, a
markedly prolonged HV interval or block below the His at long
cycle lengths also may constitute an indication for permanent pacing. Patients with fascicular block and the neuromuscular diseases
previously described should also undergo pacemaker implantation.
SELECTION OF PACING MODE AND SYSTEM
In general, a pacing mode that maintains AV synchrony reduces
complications of pacing such as pacemaker syndrome and
pacemaker-mediated tachycardia. This is particularly true in
younger patients; the importance of dual-chamber pacing in the
elderly, however, is less well established, although AV synchrony in
patients with sinus rhythm and AV block is typically desired.
Physiologic Ventricular Pacing In patients with left ventricular
ejection fraction <50% and AV block who have an indication for
permanent pacing and are expected to require ventricular pacing
>40% of the time, techniques to provide more physiologic ventricular activation are preferred to right ventricular pacing to prevent
heart failure. Cardiac resynchronization therapy (CRT) involves
placement of an additional pacing lead in a lateral or anterolateral
branch of the coronary sinus to allow for simultaneous right ventricle and lateral left ventricle pacing leading to a more physiologic
left ventricular contraction. CRT pacing has been shown to improve
outcomes and mortality in appropriately selected patients. Physiologic ventricular pacing has also been achieved with placement
of a ventricular pacing lead in the region of the His bundle. His
bundle pacing recruits the specialized conduction system, leading
to a more physiologic cardiac contraction. In addition to His bundle pacing, left bundle branch area pacing in the proximal interventricular septal region has also been shown to achieve a more
Symptoms
Lamin A/C,
neuromuscular
disease
Neuromuscular
disease associated with
progressive conduction tissue
disorder
Complete heart
block (acquired),
advanced AV
block,
Mobitz Type II,
evidence for
infranodal block
Observation
Observation
Lamin
A/C
Neuromuscular
disease
Permanent
pacing
(Class IIa)
Permanent
pacing
(Class IIb)
Permanent
pacing
(Class IIa)
Permanent
pacing
(Class IIa)
Permanent
pacing
(Class I)
Permanent
pacing
(Class I)
Permanent
pacing
(Class III:
Harm)
Permanent
pacing
(Class III:
Harm)
Symptoms
Marked first degree AV Block Mobitz Type I Block
AV Block
Yes No Yes
Yes
No
No
Yes No
Yes Yes
No
FIGURE 245-5 Indications for pacing in patients with atrioventricular (AV) block. In patients presenting with AV block, the category of AV block should be determined
(first-degree, second-degree, or complete heart block). In first-degree AV block, permanent pacing may be indicated in the setting of symptoms or higher-risk systemic
disease such as neuromuscular disease or Lamin A/C cardiomyopathy. In Mobitz I AV block, pacing may be considered in the setting of symptoms or the additional
disease mentioned with first-degree AV block. In complete heart block or Mobitz II AV block, permanent pacing is generally indicated. Class I recommendations should be
performed or are indicated. Class IIa recommendations are considered reasonable to perform. Class IIb recommendations may be considered. Class III recommendations
are associated with harm more than benefit. (Reproduced with permission from FM Kusumoto et al: 2018 ACC/AHA/HRS guideline on the evaluation and management of
patients with bradycardia and cardiac conduction delay. Heart Rhythm 16:e128, 2019.)
The Bradyarrhythmias: Disorders of the Atrioventricular Node
1887CHAPTER 245
Pacing lead at
His position
FIGURE 245-6 His bundle pacing. The chest radiograph on the left shows a dual chamber pacemaker with a pacing lead in the right atrium (upper left) and a pacing lead
in the region of the tricuspid valve in the His position. The electrocardiograms demonstrated intrinsic conduction with complete heart block on the left and atrial sensed,
ventricular paced rhythm with a narrow QRS complex similar to the intrinsic QRS complex that results from pacing the His bundle and capturing the specialized conduction
system of the heart.
physiologic pacing response. The selection of pacing lead location
should be individualized (Fig. 245-6).
The availability of leadless miniaturized pacing systems may be
appropriate in selected patients. Leadless pacemakers are completely
self-contained devices that are implanted via the femoral vein into
the right ventricle. The technology for these devices continues to
evolve, and the most recent models are capable of detecting atrial
mechanical contraction to allow for the preservation of AV synchrony. The device can provide single-chamber ventricular pacing
in addition to containing technology that can sense atrial activity
(utilizing the accelerometer in the pacemaker) to coordinate an
atrial sensed, ventricular paced rhythm (AV synchrony). Leadless
pacemakers can be particularly useful in patients with vascular
access limitations. Because there is no intravascular pacing wire or
implanted subcutaneous pacemaker generator, the long-term infection rate is lower and there is no risk of lead fracture (Fig. 245-7).
Several studies have failed to demonstrate a difference in mortality rate in older patients with AV block treated with a single- (VVI)
compared with a dual- (DDD) chamber pacing mode. In some of
the studies that randomized pacing mode, the risk of chronic atrial
fibrillation and stroke risk decreased with physiologic pacing. In
patients with sinus rhythm and AV block, the very modest increase
in risk with dual-chamber pacemaker implantation appears to be
justified to avoid the possible complications of single-chamber
pacing.
Acknowledgment
David D. Spragg and Gordon F. Tomaselli contributed to this chapter in
the 20th edition, and some material from that chapter has been retained
here.
■ FURTHER READING
Ellenbogen K et al (eds): Clinical Cardiac Pacing, Defibrillation, and
Resynchronization Therapy, 5th ed. Philadelphia, Elsevier, 2016.
Jalife J, Stevenson W (eds): Zipes and Jalife’s Cardiac Electrophysiology: From Cell to Bedside, 8th ed. Philadelphia, Elsevier, 2021.
Kusumoto FM et al: 2018 ACC/AHA/HRS guideline on the evaluation and management of patients with bradycardia and cardiac
conduction delay: A report of the American College of Cardiology/
American Heart Association Task Force on Clinical Practice Guidelines and the Heart Rhythm Society. Heart Rhythm 16:e128, 2019.
Single chamber transvenous pacemaker Single chamber leadless pacemaker
FIGURE 245-7 Types of pacemakers. A single-chamber pacemaker with the pacing lead in the right ventricular outflow tract (arrow) is shown on the left. A single-chamber
leadless pacemaker (arrow) is shown on the right.
1888 PART 6 Disorders of the Cardiovascular System
The most common arrhythmias that patients present with are part of
a broad category defined by anatomic origin termed supraventricular
tachycardias (SVTs). SVTs originate from or are dependent on conduction through the atrium or atrioventricular (AV) node to the ventricles.
Most produce narrow QRS complex tachycardia (QRS duration <120 ms)
characteristic of ventricular activation over the Purkinje system and
thus are sometimes referred to as a narrow-complex tachycardias. The
QRS morphology of the SVT is usually identical to the sinus rhythm
QRS. Conduction block in the left or right bundle branch or activation
of the ventricles from an accessory pathway produces a wide QRS complex during SVT that must be distinguished from ventricular tachycardia (VT). Mechanisms of supraventricular tachyarrhythmia can be
divided into physiologic sinus tachycardia and pathologic tachycardia
(Table 246-1).
Pathologic tachycardia can be further subclassified by mechanism
as reentrant arrhythmias dependent on AV nodal conduction (e.g.,
AVNRT), large reentry circuits within the atrial tissue alone (e.g.,
atrial flutter), or focal atrial tachycardias that can be due to automaticity or small reentry circuits. The prognosis and treatment vary
considerably depending on the mechanism and underlying heart
disease. SVT can be of brief duration, termed nonsustained, or can
be sustained such that an intervention, such as cardioversion, catheter ablation, or drug administration, is required for termination and
maintenance of sinus rhythm. Episodes that occur with sudden onset
and termination are referred to as paroxysmal. Paroxysmal supraventricular tachycardia (PSVT) refers to a family of tachycardias including
AV node reentry, AV reciprocating tachycardia using an accessory
pathway, and atrial tachycardia described in subsequent chapters
(Fig. 246-1).
CLINICAL PRESENTATION
Symptoms of supraventricular arrhythmia vary depending on the rate,
duration, associated heart disease, and comorbidities and include palpitations, chest pain, dyspnea, diminished exertional capacity, and occasionally syncope. Rarely, a supraventricular arrhythmia precipitates
cardiac arrest in patients with Wolff-Parkinson-White (WPW) syndrome or severe heart disease, such as hypertrophic cardiomyopathy.
■ INITIAL EVALUATION
The diagnosis of SVT is most often entertained when evaluating a
patient for arrhythmia-related symptoms or when evidence of ventricular preexcitation is seen on an electrocardiogram (ECG) as an
outpatient. Diagnosis of SVT requires obtaining an ECG at the time of
symptoms (Fig. 246-2). Ventricular preexcitation on the resting ECG
suggests AV reciprocating tachycardia using an accessory pathway.
When the arrhythmia is ongoing at the time of recording, the ECG
usually establishes or suggests the diagnosis. In the urgent care or
inpatient setting, treatment of SVT will often involve vagal maneuvers
or carotid sinus massage (CSM) to achieve AV block (Table 246-2).
In the appropriate patient, CSM should be used cautiously, if at all,
if there is concern for carotid atherosclerosis that may be embolized
during manipulation. If this is unsuccessful, the administration of 6 or
12 mg of adenosine to cause transient AV block is usually successful
in terminating an AV nodal–dependent SVT or diagnosing a non-AV
nodal–dependent SVT such as atrial tachycardia or atrial flutter. There
are some atrial tachycardias that are adenosine sensitive, and thus,
246 Approach to
Supraventricular
Tachyarrhythmias
William H. Sauer, Paul C. Zei
TABLE 246-1 Mechanisms of Supraventricular Tachyarrhythmia
Physiologic Sinus Tachycardia
Defining feature: normal sinus mechanism precipitated by exertion, stress,
exogenous or endogenous stimulants, concurrent illness
Pathologic Supraventricular Tachycardia (SVT)
A. Tachycardias originating from the atrium
Defining feature: tachycardia may continue despite beats that fail to conduct to
the ventricles, indicating that the atrioventricular (AV) node is not participating in
the tachycardia circuit
1. Inappropriate sinus tachycardia
Defining feature: tachycardia from the normal sinus node area that occurs
without an identifiable precipitating factor as a result of dysfunctional autonomic
regulation
2. Focal atrial tachycardia (AT)
Defining feature: regular atrial tachycardia with defined P wave; may be
sustained, nonsustained, paroxysmal, or incessant; frequent sites of origin occur
along the valve annuli of left or right atrium, pulmonary veins, coronary sinus
musculature, superior vena cava
3. Atrial flutter and macroreentrant atrial tachycardia
Defining feature: macroreentry reflected as organized atrial activity on an
electrocardiogram (ECG), commonly seen as sawtooth flutter waves at rates
typically faster than 200 beats/min
4. Atrial fibrillation
Defining feature: chaotic rapid atrial electrical activity with variable ventricular
rate; the most common sustained cardiac arrhythmia in older adults
5. Multifocal atrial tachycardia
Defining feature: multiple discrete P waves often seen in patients with pulmonary
disease during acute exacerbations of pulmonary insufficiency
B. AV nodal reentry tachycardia (AVNRT)
Defining feature: paroxysmal regular tachycardia with P waves visible at the end
of the QRS complex or not visible at all; the most common paroxysmal sustained
tachycardia in healthy young adults; more common in women
C. Tachycardias associated with accessory atrioventricular pathways
1. Orthodromic AV reciprocating tachycardia (AVRT)
Defining feature: paroxysmal sustained tachycardia similar to AV nodal reentry;
during sinus rhythm, evidence of ventricular preexcitation may be present
(Wolff-Parkinson-White syndrome) or absent (concealed accessory
pathway)
2. Preexcited tachycardia
Defining feature: wide QRS tachycardia with QRS morphology similar to
ventricular tachycardia
a. Antidromic AV reciprocating tachycardia—regular paroxysmal
tachycardia
b. Atrial fibrillation with preexcitation—irregular wide-complex or
intermittently wide-complex tachycardia, some with dangerously rapid
rates faster than 250/min
c. Atrial tachycardia or flutter with preexcitation
termination of an SVT with adenosine does not exclude this potential
diagnosis.
For transient arrhythmias, ambulatory ECG recording is warranted.
Patients will often have access to ECG recording devices, such as a
watch or smartphone-enabled electrogram recording electrode pair.
Therefore, a patient may have the ECG diagnosis before seeing a physician (Fig. 246-3).
Exercise testing is useful for assessing exercise-related symptoms and potentially evoking the arrhythmia. Additional evaluation for underlying cardiac disease and to exclude potentially
dangerous arrhythmias should be performed based on the clinical scenario. Occasionally, an invasive electrophysiology study is
warranted to provoke the arrhythmia with pacing, confirm the
mechanism, and risk stratify the patient, but most commonly, this
is performed at the time of intended catheter ablation to treat the
arrhythmia.
Approach to Supraventricular Tachyarrhythmias
1889CHAPTER 246
NARROW-COMPLEX TACHYCARDIA – OBTAIN FULL
12-LEAD ECG WITH LONG RHYTHM STRIP
Regular
atrial rate
Irregular atrial
and ventricular
rates
Atrial fibrillation VA block: more
V’s than A’s
AV block: more
A’s than V’s
1:1 AV
response
• Junctional
tachycardia
• AVNRT
• ORT
• AT
• Rarely
atrial flutter
• Atrial
flutter
• Atrial
tachycardia
• Rarely
AVNRT with
2:1 block
below the
His bundle
Multifocal atrial
tachycardia
FIGURE 246-1 Diagnostic possibilities based on the appearance of the 12-lead electrocardiogram (ECG) recorded during an episode of supraventricular tachycardia
(SVT). AT, focal atrial tachycardia; AVNRT, atrioventricular (AV) nodal reentry tachycardia; ORT, orthodromic AV reentry tachycardia.
AV nodal blockade
(Adenosine or vagal reflex maneuver)
Atrial rate continues
with AV block No effect SVT slows SVT terminated
• AVNRT
• AVRT
• Adenosine sensitive
Focal AT
• Fascicular VT
• Inadequate dose/effect
• Sinus tachycardia
• Junctional tachycardia
• Atrial flutter
• Atrial tachycardia
FIGURE 246-2 Diagnostic effect of increasing atrioventricular (AV) node blockade with vagal maneuvers, carotid sinus massage, adenosine, verapamil, or beta blockers.
AT, focal atrial tachycardia; AVNRT, atrioventricular nodal reentry tachycardia; AVRT, atrioventricular reciprocating tachycardia; SVT, supraventricular tachycardia.
Paroxysmal SVT is most commonly encountered in patients who do
not have structural heart disease. Other supraventricular arrhythmias,
particularly atrial fibrillation, are often associated with a variety of
heart diseases. At initial evaluation, history and examination should
assess possible underlying heart disease. Any abnormal findings may
warrant further cardiac evaluation.
The most common SVT is sinus tachycardia in response to physiologic stress, such as exercise, but it can also be a manifestation
of acute illness. The first step in diagnosis of SVT is to consider
the possibility of sinus tachycardia. Therapy is then determined by
the clinical findings and probable diagnosis. If sinus tachycardia is
diagnosed, treatment of the underlying inciting cause is the primary
approach. If the arrhythmia is ongoing and is not due to sinus tachycardia, initial assessment determines whether immediate therapy is
needed to terminate the arrhythmia or slow the rate. Arrhythmias that
cause hypotension, impaired consciousness, angina, or heart failure
warrant immediate therapy, guided by the type of arrhythmia. Treatment options for specific types of SVT are discussed in more detail
in subsequent chapters and include pharmacologic and procedural
interventions.
1890 PART 6 Disorders of the Cardiovascular System
Heart Rate Over 120 — 200 BPM
Average
This ECG was not checked for AFib
because your heart rate was over 120 BPM.
If you repeatedly get this result or you’re
not feeling well, you should talk to your
doctor.
Reported Symptoms
• Rapid pounding, or fluttering heartbeat
• Chest tightness or pain
• Fainting
25 mm/s, 10 mm/mV, Lead I, 511Hz, iOS 12.1.4, watchOS 5.1.3, Watch4,2 — The waveform is similar to a Lead I ECG. For more information, see Instructions for Use.
20s 21s 22s 23s 24s 25s 26s 27s 28s 29s
10s 11s 12s 13s 14s 15s 16s 17s 18s 19s
0s 1s 2s 3s 4s 5s 6s 7s 8s 9s
FIGURE 246-3 Narrow-complex tachycardia recorded by a consumer wearable monitor (Apple watch). Afib, atrial fibrillation; ECG, electrocardiogram.
TABLE 246-2 Vagal Maneuvers
Diaphragm
Chest
muscles
Lungs
Larynx
Abdominal
cavity
Abdominal
muscles
Rectus muscles
Holding breath while bearing down to
increase intrathoracic pressure
15s
Breathing hard into a syringe against pressure
to increase intrathoracic pressure Raise legs abruptly to increase venous return
Submerge face into cold water (diver’s
reflex)
Carotid sinus
Vagus nerve
Right common
carotid artery
Sternocleidomastoid
muscle
Cardiac plexus
Carotid sinus massage
Adenosine
Adenosine
Physiologic and Nonphysiologic Sinus Tachycardia
1891CHAPTER 247
Acknowledgment
Gregory F. Michaud and William G. Stevenson contributed to this chapter in the 20th edition, and some material from that chapter has been
retained here.
■ FURTHER READING
Brugada J et al: 2019 ESC guidelines for the management of patients
with supraventricular tachycardia. The task force for the management
of patients with supraventricular tachycardia of the European Society
of Cardiology (ESC) developed in collaboration with the Association
for European Paediatric and Congenital Cardiology (AEPC). Eur
Heart J 41:655, 2020.
Callans DJ: Josephson’s Clinical Cardiac Electrophysiology: Techniques
and Interpretations, 6th ed. Philadelphia, Wolters Kluwer, 2021.
The sinus node is composed of a group of cells located in the lateral
superior aspect of the junction between the right atrium and superior
vena cava, within the superior aspect of the thick ridge of muscle
known as the crista terminalis where the posterior smooth atrial wall
derived from the sinus venosus meets the trabeculated anterior portion
of the right atrium. Patients with sinus tachycardia will often seek medical attention with the uncomfortable awareness of their heartbeat as
their chief complaint. Often, an arrhythmia is suspected because of the
similar constellation of symptoms that accompanies supraventricular
and ventricular tachycardia or atrial and ventricular ectopy. However,
a careful review of the 12-lead electrocardiogram (ECG) reveals a
characteristic P wave originating from the superior and lateral aspect
of the right atrium with a positive deflection in leads I, II, and III and
247 Physiologic and
Nonphysiologic Sinus
Tachycardia
William H. Sauer, Paul C. Zei
A B
II, III, aVF
V1
aVR
SVC
Compact
AVN
Sinus
node
IVC
Triangle of Koch
TVA
Pectinate
muscles
FO
Crista terminalis
CS Os
Eustachian
ridge
FIGURE 247-1 Right atrial anatomy pertinent to normal sinus rhythm and supraventricular tachycardia. A. Typical P-wave morphology during normal sinus rhythm based
on standard 12-lead electrocardiogram. There is a positive P wave in leads II, III, and aVF and a biphasic, initially positive P wave in aVR. B. Right atrial anatomy seen from
a right lateral perspective with lateral wall opened to view the septum. AVN, atrioventricular node; CS Os, coronary sinus ostium; FO, fossa ovalis; IVC, inferior vena cava;
TVA, tricuspid valve annulus.
a biphasic morphology in lead V1
. Sinus P waves are characterized
by a frontal plane axis directed inferiorly and leftward, with positive
P waves in leads II, III, and aVF; a negative P wave in aVR; and an initially positive biphasic P wave in V1
. Normal sinus rhythm has a range
of rates between 60 and 100 beats/min (Fig. 247-1).
PHYSIOLOGIC SINUS TACHYCARDIA
Sinus tachycardia (>100 beats/min) typically occurs in response to
sympathetic stimulation and vagal withdrawal, whereby the rate of
spontaneous depolarization of the sinus node increases and the focus
of earliest activation within the node typically shifts more leftward and
closer to the superior septal aspect of the crista terminalis, thus producing taller P waves in the inferior limb leads when compared to normal sinus rhythm. Sinus bradycardia is defined as rates <60 beats/min;
however, bradycardia can be normal during sleep and in fit individuals.
Sinus tachycardia is considered physiologic when it is an appropriate
response to exercise, stress, or illness. Sinus tachycardia can be difficult
to distinguish from focal atrial tachycardia (see below) that originates
near the sinus node. A causative factor (e.g., exertion) and a gradual
rate increase favor a diagnosis of sinus tachycardia, whereas abrupt
tachycardia onset and offset favor atrial tachycardia (Fig. 247-2).
The distinction can be difficult and occasionally requires extended
ECG monitoring or invasive electrophysiology study. Treatment for
physiologic sinus tachycardia is aimed at the underlying condition,
but frequently, no therapy is necessary. Consideration to abnormal
thyroid conditions and anemia should be given in patients with sinus
tachycardia as these represent reversible causes. In addition, structural
and functional cardiovascular abnormalities can present as sinus
tachycardia, especially pulmonary embolism, and thus must be ruled
out before considering sinus tachycardia as nonphysiologic. Finally, as
sinus rate varies widely between individuals, a relatively elevated sinus
rate (whether at rest or during exercise) without underlying cause,
particularly without symptoms, typical does not warrant treatment
(Table 247-1).
NONPHYSIOLOGIC SINUS TACHYCARDIA
Inappropriate sinus tachycardia is an uncommon condition in which
the sinus rate increases spontaneously at rest or out of proportion to
physiologic stress or exertion and is within a spectrum of ill-defined
conditions associated with autonomic dysregulation. The underlying
mechanism remains elusive, but it may be related to imbalance between
1892 PART 6 Disorders of the Cardiovascular System
sympathetic and parasympathetic inputs to the sinus node, altered
membrane automaticity of sinus node cells, or a combination of both.
Affected individuals are often women in the third or fourth decade of
life. Fatigue, dizziness, and even syncope may accompany palpitations,
which can be disabling. Additional symptoms of chest pain, headaches,
and gastrointestinal upset are common. Inappropriate sinus tachycardia must be distinguished from appropriate sinus tachycardia and from
focal atrial tachycardia arising from a region near the sinus node. The
distinction between physiologic sinus tachycardia due to an anxiety
disorder and inappropriate sinus tachycardia can be difficult. Therapy
is often ineffective or poorly tolerated. Careful titration of beta blockers
and/or calcium channel blockers may reduce symptoms. Clonidine
and serotonin reuptake inhibitors have also been used. Ivabradine,
a drug that blocks the If
current that causes spontaneous sinus node
depolarization, is approved in the United States for use in heart failure,
but it has also been effective in the treatment of inappropriate sinus
tachycardia. Catheter ablation of the sinus node to modify and thereby
decrease the sinus rate has been performed, but long-term control of
symptoms is usually poor and can result in a permanent pacemaker
requirement due to resultant symptomatic bradycardia or chronotropic
incompetence (Fig. 247-3).
Postural orthostatic tachycardia syndrome (POTS) is characterized
by symptomatic sinus tachycardia that occurs with postural change
12 am
200
150
100
50
0
6 am 12 pm 6 pm 12 am
12 am
A
B
200
150
100
50
0
6 am 12 pm 6 pm 12 am
FIGURE 247-2 Outpatient telemetry monitor in a patient with intermittent atrial
tachycardia (A) and normal physiologic sinus tachycardia (B).
Sinus tachycardia
Identify and treat
reversible causes
(See Table 247-1)
Evaluate for POTS Treatment of POTS
• Recumbent exercise and
conditioning regimen
• High-salt diet
• Compression stockings
• Fludrocortisone
• Midodrine
IST suspected
Beta blocker and/or
ivabradine
Consider catheter
ablation
FIGURE 247-3 Evaluation and treatment of sinus tachycardia. For the patient who
presents with sinus tachycardia, reversible causes of appropriate sinus tachycardia
must be excluded and treated as indicated. Otherwise, evaluation for a spectrum
of syndromes resulting in inappropriate sinus tachycardia should be undertaken.
Potential directed therapies are shown. IST, inappropriate sinus tachycardia; POTS,
postural orthostatic tachycardia syndrome.
TABLE 247-1 Common Causes of Sinus Tachycardia
Physiologic Causes
Emotion, physical exercise, sexual intercourse, pain, pregnancy
Pathologic Causes
Anxiety, panic attack, anemia, fever, dehydration, infection, malignancies,
hyperthyroidism, hypoglycemia, pheochromocytoma, Cushing’s disease,
diabetes mellitus with evidence of autonomic dysfunction, pulmonary embolus,
myocardial infarction, pericarditis, valve disease, decompensated heart failure,
shock, alcohol withdrawal
Drugs
Epinephrine, norepinephrine, dopamine, dobutamine, atropine, β2
-adrenergic
receptor agonists (salbutamol), methylxanthines, doxorubicin, daunorubicin, beta
blocker withdrawal, caffeine, alcohol
Illicit Drugs
Amphetamines, cocaine, lysergic acid diethylamide, psilocybin, ecstasy, cocaine
from a supine position to standing. The sinus rate increases by
30 beats/min or to >120 beats/min within 10 min of standing and in
the absence of hypotension. Symptoms are often similar to those in
patients with inappropriate sinus tachycardia. POTS is sometimes due
to autonomic dysfunction following a viral illness and may resolve
spontaneously over 3–12 months. Volume expansion with salt supplementation, oral fludrocortisone, compression stockings, and the
α-agonist midodrine, often in combination, can be helpful. Exercise
training has also been shown to improve symptoms and should be a
part of a treatment strategy to reduce symptoms. While it is sometimes
difficult to differentiate inappropriate sinus tachycardia from POTS,
recognition of these distinct clinical syndromes is critical for treatment.
Sinus node modification will be ineffective for the treatment of POTS.
Likewise, treatment strategies aimed at increasing blood pressure will
not be appropriate for inappropriate sinus tachycardia.
Acknowledgment
Gregory F. Michaud and William G. Stevenson contributed to this
chapter in the 20th edition, and some material from that chapter has
been retained here.
■ FURTHER READING
Brugada J et al: 2019 ESC guidelines for the management of patients
with supraventricular tachycardia. The task force for the management
of patients with supraventricular tachycardia of the European Society
of Cardiology (ESC) Developed in collaboration with the Association
for European Paediatric and Congenital Cardiology (AEPC). Eur
Heart J 41:655, 2020.
Mar PL, Raj SR: Postural orthostatic tachycardia syndrome: Mechanisms and new therapies. Ann Rev Med 71:235, 2020.
Olshansky B, Sullivan RM: Inappropriate sinus tachycardia. EP
Europace 21:194, 2019.
Sheldon RS et al: 2015 Heart Rhythm Society expert consensus
statement on the diagnosis and treatment of postural tachycardia
syndrome, inappropriate sinus tachycardia, and vasovagal syncope.
Heart Rhythm 12:e41, 2015.
Focal Atrial Tachycardia
1893CHAPTER 248
The underlying mechanisms of focal atrial tachycardia (AT) include
abnormal automaticity, triggered automaticity, or a small reentry
circuit in diseased atrial tissue. The term focal is used to differentiate
this form of atrial tachycardia from typical and atypical atrial flutter
but does not define a mechanism of the arrhythmia. ATs can originate
from most regions of the atria, including atrial tissue extending into a
pulmonary vein, the coronary sinus, or vena cava. It can be sustained,
nonsustained, paroxysmal, or incessant. Focal AT accounts for ~10% of
paroxysmal supraventricular tachycardia (PSVTs) in patients referred
for catheter ablation. Nonsustained focal AT is commonly observed on
ambulatory electrocardiogram (ECG) recordings, and the prevalence
increases with age. Treatment is not recommended for asymptomatic
nonsustained atrial tachycardia identified on ECG monitoring. However, frequent atrial ectopy and nonsustained AT are often precursors
to more significant arrhythmias such as atrial fibrillation and atrial
flutter. Nonsustained, frequent atrial ectopy or short bursts of AT may
be symptomatic and require therapy similar to that required for focal
AT (Fig. 248-1).
AT can occur in the absence of structural heart disease or may be
associated with any condition that causes atrial fibrosis, including prior
catheter ablation. Areas of fibrosis can act as a nidus for abnormal
automaticity from damaged cells or microreentry within zones of slow
conduction within and on the border of fibrotic areas. Sympathetic
stimulation is a promoting factor, and the emergence of AT can be a
sign of underlying illness. AT with atrioventricular (AV) block may
occur in digitalis toxicity. Symptoms from AT are highly variable but
similar to other supraventricular tachycardias (SVTs), and incessant
AT can cause tachycardia-induced cardiomyopathy.
AT typically presents with 1:1 AV conduction or with AV block
in a Wenckebach or fixed (e.g., 2:1 or 3:1) pattern. Because it is not
dependent on AV nodal conduction, AT will not terminate with AV
block, and the atrial rate will not be affected, which distinguishes
AT from most AV nodal–dependent SVTs, such as AV nodal reentry
and AV reentry using an accessory pathway (see below). A so-called
warm-up phase when the atrial activation rate increases after initiation
248 Focal Atrial Tachycardia
William H. Sauer, Paul C. Zei
or a cool-down phase when the rate slows prior to termination also
favors AT rather than AV nodal–dependent SVT, as this is a common
observation with triggered automaticity. P waves are often discrete,
with an intervening isoelectric segment, in contrast to atrial flutter and
macroreentrant AT because atrial activation from a focal source occurs
through a small portion of the tachycardia cycle (Fig. 248-2).
When 1:1 conduction to the ventricles is present, the arrhythmia can
resemble sinus tachycardia typically with a P-R interval shorter than
the R-P interval, particularly when sympathetic tone results in rapid AV
nodal conduction. It can be distinguished from sinus tachycardia by the
P-wave morphology, which usually differs from sinus P waves depending on the location of the focus. Focal AT tends to originate in areas
of complex atrial anatomy, such as the crista terminalis, valve annuli,
atrial septum, and atrial muscle extending along cardiac thoracic veins
(superior vena cava, coronary sinus, and pulmonary veins), and the
location can often be estimated by the P-wave morphology. AT from
the atrial septum will frequently have a narrower P-wave duration than
sinus rhythm. AT from the left atrium will usually have a monophasic,
positive P wave in lead V1
and negative P waves in I and aVL, indicating an activation wavefront away from the left atrial free wall. AT that
originates from superior atrial locations, such as the superior vena cava
or superior pulmonary veins, will be positive in the inferior limb leads
II, III, and aVF, whereas AT from a more inferior location, such as the
ostium of the coronary sinus, will inscribe negative P waves in these
same leads. When the focus is in the superior aspect of the crista terminalis, close to the sinus node, however, the P wave will resemble that
of sinus tachycardia. Abrupt onset and offset then favor AT rather than
sinus tachycardia. Depending on the atrial rate, the P wave may fall
on top of the T wave, or during 2:1 conduction, it may fall coincident
with the QRS. Maneuvers that increase AV block, such as carotid sinus
massage, Valsalva maneuver, or administration of AV nodal–blocking
agents, such as adenosine, are useful to create AV block that will expose
the P wave.
Acute management of sudden-onset, sustained AT is the same as
for other forms of PSVT, but the response to pharmacologic therapy is
variable, likely depending on the mechanism (Fig. 248-3).
For AT due to reentry, administration of adenosine or vagal
maneuvers may transiently increase AV block without terminating
tachycardia. Some ATs terminate with a sufficient dose of adenosine,
consistent with triggered activity as the mechanism. Cardioversion
can be effective in some but fails in others because of immediate
recurrence, suggesting automaticity as the mechanism in these cases.
AT
AVRT
AVNRT • Av node reentry
No P w-wave visible
RP < PR
RP< PR
RP < PR
RP < PR
• AV node reentry
• AV reentry using an
accessory pathway
• Focal atrial tachycardia
• AV reentry using an
accessory pathway
• AV node reentry
uncommon form
FIGURE 248-1 Common mechanisms underlying paroxysmal supraventricular tachycardia along with typical R-P relationships. A. Schematic showing a four-chamber
view of the heart with atrioventricular (AV) node and specialized conduction tissue (His-Purkinje) in yellow. Atrial tachycardia (AT; red circuit) is confined completely to atrial
tissue. Atrioventricular nodal reentry tachycardia (AVNRT; green circuit) uses AV nodal and perinodal atrial tissue. Atrioventricular reentry tachycardia (AVRT; blue circuit)
uses atrial and ventricular tissue, accessory pathway between the ventricle and atrium, AV node, and His-Purkinje tissue as part of the reentry circuit. B. Typical relation of
the P wave to QRS, commonly described as the R-P to P-R relationship, for the different tachycardia mechanisms.
1894 PART 6 Disorders of the Cardiovascular System
Adenosine Cardioversion
Hemodynamic
instability
No Yes
Focal atrial tachycardia
Non-DHP CCB
and/or beta blocker
Recurrent
or incessant
Ineffective
Ineffective
Ineffective
Recurrent
or incessant
Antiarrhythmic therapy
(see Table 243-2)
Catheter
ablation
FIGURE 248-3 Clinical approach and treatment algorithm for management of
focal atrial tachycardia. CCB, calcium channel blocker; DHP, dihydropyridine.
(Adapted from J Brugada et al: 2019 ESC Guidelines for the management
of patients with supraventricular tachycardia The Task Force for the
management of patients with supraventricular tachycardia of the European
Society of Cardiology (ESC) [published correction appears in Eur Heart J. 2020
Nov 21;41(44):4258]. Eur Heart J 41:655, 2020.)
I
II
III
aVR
aVL
aVF
V1
V2
V3
V4
V5
V6
VI
V5
III
I aVR
II
III
aVR
aVL
aVF
V1
V2
V3
V4
V5
V6
VI
V5
III
aVR
FIGURE 248-2 Focal atrial tachycardia. In the right panel, a surface 12-lead electrocardiogram shows focal intermittent atrial tachycardia. Note the discrete P waves, with
isoelectric segments between, as well as the sinus rhythm. The left panel shows an electroanatomic map of the same focal atrial tachycardia originating from the anterior
interatrial septum, as viewed in an anterior-posterior (AP) view of the left atrium obtained during electrophysiology study and ablation. The colors represent the timing of
local electrical activation during each tachycardia atrial activation, showing a focal early (red) site. Additional markers of white “flecks” represent conduction direction,
demonstrating activation of the atrium dispersing from this focal site. Of note, the pink and red dots represent ablation lesions, in this case, for pulmonary vein isolation.
(Adapted from J Brugada et al: 2019 ESC Guidelines for the management of patients with supraventricular tachycardiaThe Task Force for the management of patients with
supraventricular tachycardia of the European Society of Cardiology (ESC). Eur Heart J 41:655, 2020.)
In this chapter, sustained supraventricular tachycardias (SVTs) dependent on the atrioventricular (AV) node are discussed. These include
AV nodal reentry tachycardia (AVNRT), junctional tachycardia, AV
reciprocating tachycardia (AVRT) utilizing an accessory pathway, and
a group of additional various SVTs that involve an accessory pathway,
termed preexcited tachycardias. The term SVT encompasses a broad
group of tachyarrhythmias based on anatomic origin and technically
includes sinus tachycardia, atrial tachycardia (AT), atrial flutter, and
atrial fibrillation; however, for the purposes of describing an organized
approach to diagnosis and treatment of SVT, a separate discussion for
these non-AV nodal–dependent SVTs are discussed elsewhere.
249 Paroxysmal
Supraventricular
Tachycardias
William H. Sauer, Paul C. Zei
Beta blockers and calcium channel blockers may slow the ventricular rate
by increasing AV block, which can improve tolerance of the arrhythmias,
but large doses are sometimes required. Potential precipitating factors
and intercurrent illness should be sought and corrected. Underlying
heart disease should be considered and excluded.
For patients with recurrent episodes, beta blockers, calcium channel
blockers such as diltiazem or verapamil, and antiarrhythmic drugs
such as flecainide, propafenone, disopyramide, sotalol, and amiodarone can be effective, but potential toxicities and adverse effects often
warrant avoidance of long-term use.
Catheter ablation targeting the AT focus is effective in >80% of
patients and is recommended for recurrent symptomatic AT when
drugs fail or are not desired or for incessant AT causing tachycardiainduced cardiomyopathy. Although AT is often a precursor to atrial
fibrillation or atrial flutter, the associated risk for stroke and hence
indications for long-term anticoagulation are unclear but not considered equivalent.
Acknowledgment
Gregory F. Michaud and William G. Stevenson contributed to this chapter in the 20th edition and some material from that chapter has been
retained here.
■ FURTHER READING
Brugada J et al: 2019 ESC Guidelines for the management of patients
with supraventricular tachycardia. The Task Force for the Management
of Patients with Supraventricular Tachycardia of the European
Society of Cardiology (ESC) developed in collaboration with the
Association for European Paediatric and Congenital Cardiology
(AEPC). Eur Heart J 41:655, 2020.
Callans DJ: Josephson’s Clinical Cardiac Electrophysiology: Techniques
and Interpretations, 6th ed. Philadelphia, Wolters Kluwer, 2021.
No comments:
Post a Comment
اكتب تعليق حول الموضوع