Pathophysiology of Arrhythmias

Question 1

Learning outcomes

Answer 1

• know why dysrhythmias may arise and how they are classified
• know how heart block arises and its classification
• know how circus re-entry may arise
• know the differences in the electrical activity of the different parts of the heart and between normal and abnormal pacemaker cells which allow antidysrhythmic drug treatment
• understand the importance of correct identification of location and nature of the dysrhythmia for proper choice of antidysrhythmic drug
• Understand genetic basis of VT and ionchannelopathies
• Understand the management of atrial fibrillation

Question 2

1st degree AV block?

Answer 2

lengthening of the PR interval

Question 3

2nd degree AV block?

Answer 3

Mobitz TYPE 1
- progresive lengthening of PR internal until P wave blocked and then PR short again

Mobitz Type 2
- block after 2 or 3 conducted beats in regular pattern

Question 4

3rd degree AV block?

Answer 4

complete AV dissociation

Question 5

What are the 2 main types of arrhythmias?

Answer 5

• The 2 main types of arrhythmias are tachycardias and bradycardias

Question 6

bradycardia?
tachycardia?

Answer 6

bradycardia = <50 bpm
tachycardia = >100bpm

Question 7

What is decremental conduction?
What does this prevent?

Answer 7

• Decremental conduction references the fact that the more frequently the AV node is stimulated, the slower it will conduct
• This prevents rapid conduction to the ventricle in cases of rapid atrial rhythms, such as atrial fibrillation or atrial flutter.

Question 8

Where is fast conduction found in the heart?

What is fast conduction?

Answer 8

• Fast conduction is found in the His Purkinje system
• Fast conduction is where the His Purkinje System will conduct faster and faster until it stops conducting and enters its absolute refractory period where no more action potentials can be generated

Question 9

What are the 5 phases of cardiomyocyte action potential?

Answer 9

• 5 phases of cardiomyocyte action potential:
  1) Phase 0 = rapid depolarisation
  2) Phase 1 = partial repolarisation
  3) Phase 2 = plateau
  4) Phase 3 = repolarisation
  5) Phase 4 = resting potential

Question 10

What is pacemaker potential?

Answer 10

• The pacemaker potential is the slow, positive increase in voltage across the cell’s membrane that occurs between the end of one action potential and the beginning of the next action potential

Question 11

How does pacemaker cell action potential compare with cardiomyocyte action potential?

Answer 11

• Pacemaker cells do not have phases 1 or 2, but have an additional phase (partial repolarisation or plateau phase) (phase 4 on the diagram) known as the pacemaker potential

Question 12

What are the 2 main type of bradycardia?

How do they each occur?

Answer 12

• 2 main types of bradycardia:

1) Sinus bradycardias
* Happens when your SA node generates a heartbeat less than 60 times a minute (60bpm)

2) AV blocks
* An AV heart block happens when the electrical impulses are delayed or blocked as they travel between your atria (the top chambers of your heart) and your ventricles (the bottom chambers of your heart)
* Occurs below the SA Node

Question 13

What are the 5 causes of Sinus Bradycardia?

Answer 13

• 5 Causes of sinus bradycardia:
• Sinus Bradycardia is always a secondary event to:
  1) Drugs (e.g. Beta Blockers, Diltazem(CCB))
  2) Vagal activity
  3) Hypothyroidism
  4) Sinus Node disease
  5) Electrolyte abnormalities

Question 14

What are the 4 causes of AV heart block?

Answer 14

• 4 Causes of AV heart block:
  1) Vagal activity
  2) Myocardial infarction
  3) Electrolyte abnormalities
  4) Degenerative diseases

Question 15

What are the 3 types of AV block based on ECG abnormality?

How do they appear on an ECG?

Answer 15

• 3 types of AV block based on ECG abnormality:

1) 1st degree
* Lengthening of the PR interval

2) 2nd degree
* Has 2 types:
* Mobitz Type 1 (Wenckebach block) - Progressive lengthening of PR interval until P wave is blocked and then PR is short again
* Mobitz Type 2 - Block after 2 or 3 conducted beats in regular pattern

3) 3rd degree
* Complete AV dissociation
* Atrial activation (usually from the sinus node) is independent from ventricular activation (originating from the AV junction, His-Purkinje system, or ventricles)

Question 16

What is the main type of treatment for bradycardia?

What 3 other treatments might be offered if needed?

Answer 16

• The main treatment for bradycardia is pacemaker (temporary or permanent)
• Only if needed, treatment for:
  1) Symptoms of syncope dizziness
  2) Prophylactic at time of operations
  3) Post AMI (acute MI)

Question 17

Based on ECG, what are the 2 main types of tachycardia?

How do they appear on an ECG?

Where do they each originate?

Answer 17

• 2 main types of tachcyardia based on ECG:

1) Narrow Complex / Supraventricular Tachycardias
* Whatever is causing it originates above AV node and sending it below AV node, rises above the purkinje fibres.

1) Broad Complex Tachycardias
* Origin is below AV node and therefore arising from ventricle)
* QRS complex is longer than 0.12ms

Question 18

what are the 5 main types of narrow complex/supraventricular tachycardias?

Answer 18

• atrial tachycardias
• junctional tachycardias
• AVNRT + AVRT (atrialventricular nodal re-entry tachycardia and atrial re-entry tachycardia)
• atrial flutter
• atrial fibrillation

Question 19

What are the 5 main types of narrow complex / supraventricular tachycardias?

How do they each appear on ECGs?

Answer 19

• 5 main types of narrow complex / supraventricular tachycardias:

1) Atrial Tachycardias
* Focus in the atria
* There is a narrow complex tachycardia at 95 bpm.
* Each QRS complex is preceded by an abnormal P wave
* P wave morphology is consistent throughout.

2) Junctional Tachycardias
* Junctional mean associated with the AV node
* Arise at junction of the heart
* Retrograde P waves — inverted in II, III and aVF; upright in V1 and aVR.

3) AVNRT + AVRT
* Atrioventricular nodal re-entry tachycardia (AVNRT)
* AV re-entrant (or reciprocating) tachycardia (AVRT)
* Involves the AV node intrinsically or AV node and accessory pathway
* IN AVNRT, Regular, narrow complex tachycardia without P waves activity (p waves merge into QRS complex), or P-wave occurs after QRS complex in retrograde with a short RP interval (70ms)
* IN AVRT P-wave is visible in most cases.
* It is retrograde (inverted) in leads II, III and aVF and it occurs after the QRS complex (somewhere on the ST segment or early on the T-wave)
* Typically longer RP interval in AVRT (>70ms)

4) Atrial Flutter
* Narrow and regular
* Flutter waves are present, best seen in leads II, III, and aVF (*)
* The atrium can beat 300 times, making 3 p waves per QRS complex, which creates a saw tooth pattern

5) Atrial Fibrillation
* Narrow but irregularly irregular.
* Could still be AF is broad and irregular

Question 20

What are the 3 main types of broad complex tachycardia?

How do they appear on an ECG?

How does bundle branch block appear on an ECG?

What is aberration?

Answer 20

• 3 main types of broad complex tachycardia:

1) Ventricular Tachycardia
* Can be monomorphic (every complex is the same) and polymorphic (complexes are different) VT

2) SVT (supraventricular tachycardia) with aberration
* Aberration is acquired, rate- dependent bundle branch block

3) SVT with a pre-existing BBB morphology on ECG
* e.g. SVT of antidromic tachycardia in WPW

Question 21

what is broad complex tachycardia characterised by?

Answer 21

heart rate of more than 100 bpm and a QRS width of more then 120ms

Question 22

What are the 3 basic mechanisms of tachycardias?

Answer 22

• 3 basic mechanisms of tachycardias:

1) Ectopic Focus (aka ectopic pacemaker)
* An excitable group of cells that causes a premature heart beat outside the normally functioning SA node of the heart

2) Re-entry / circus movement

3) Fibrillation – independent wavelets of activity

Question 23

what are the 2 adjacent pathways in heart connective tissue?

Answer 23

In connective tissue of the heart, there are two adjacent pathways with different electrophysiological properties, which are connected proximally and distally.
1- One pathway has fast conduction and long refractory period
2- The other pathways has slow conduction and short refractory period

Absolute refractory period is a period when action potentials can not be generated, and cells can not be excited

Question 24

explain the mechanism of re-entry?

Answer 24

• impulses will split and go down the fast and slow pathways.
• fast pathway gets to the distal end first and will split to go down the distal portion or the to go down the distal portion of the slow pathway
• when these impulses meet here, both tissues on either side are in refectory.

Question 25

what happens if there is a premature beat in re-entry?

Answer 25

the impulse conducted down the fast pathway doesn’t have any effect, as this pathway is in the refectory period.
By the time the slow impulse gets around where it would normally meet the impulse coming from the fast pathway, the refectory period for the fast conduction pathway has ended, resulting in the impulse going back around the fast pathway around to the proximal connection.

Question 26

what happens when the impulse gets back around to the proximal connection in re-entry?

Answer 26

Once it reaches the proximal road, the action potential splits again, sending an action potential down the proximal route, and one down the slow conduction pathway

Question 27

how does the re-entry pathway constantly continue?

Answer 27

Once the action potential reaches the point at which it which it would meet the fast conduction action potential, the refractory period of the fast conduction pathway has ended, allowing it to continue

This cycle continues, resulting in a re-entry/circus movement, where action potentials are being send down the proximal and distal roads

Question 28

what happens when a normal AP is sent down if there is re-entry going on?

Answer 28

When a normal AP is sent by the SA node, it is likely not going to be able to move down the pathway due to refractory periods set off by the AP circling round the pathway, which results in unidirectional blockade

These re-entry circuits will lead to ventricular tachycardias and arrhythmias

Question 29

what drugs can we use to correct re-entry?

Answer 29

• To correct this pathway, we could use:
  1) Na+ channel blocker – slows conduction speed
  2) K+ channel blocker – extends the refractory period
• We could also use electrical cardioversion to shock the heart in order to return to Sinuous rhythm

Question 30

what are the tachycardias that are involving the AV node?

Answer 30

• narrow complex (usually no P waves, very fast and no history of cardiac disease)
• AVNRT
• AVRT

Question 31

what can be given to terminate any tachycardia involving the AV node?

Answer 31

IV adenosine

Question 32

What are AVNRT and AVRT?

What is the patient history associated with those diagnosed with AVNRT or AVRT?

How do AVNRT and AVRT re-entry circuits differ?

What is an accessory pathway?

Answer 32

• Those diagnosed with AVNRT or AVRT tend to have no history of cardiac diease
• AVNRT = AV nodal re-entrant tachycardia
• Tachycardia where re-entry circuit is through juxtanodal (nodal) material
• AVRT = AV re-entrant tachycardia where re-entry is through an accessory pathway
• An accessory pathway is His Purkinje material that has breached the AV ring somewhere other than the AV node
• The accessory pathway through which re-entry occurs in AVRT may either be

Question 33

What 2 ways can the accessory pathway of AVRT be?

How does this effect ECG findings?

Answer 33

1) Revealed
* Means WPW (Wolff-Parkinson-White syndrome) on a 12-lead ECG

2) Concealed
* Means normal non-tachycardia on 12 lead ECG (i.e. the accessory pathway only conducts in a normal retrograde (backward moving) manner)

Question 34

What are the 3 different forms of AVRT?

Which one is associated with Wolff-Parkinson-White syndrome (WPW)

Answer 34

1) Orthodromic (most common)
2) Antidromic
* This type is associated with Wolff-Parkinson-White syndrome (WPW)
3) Duodromic

Question 35

What is Wolff-Parkinson-White syndrome (WPW)?

What is this due to?

What is the most common cause of WPW tachycardias?

What 3 ways characteristics does WPW have on an ECG?

Answer 35

• Wolff-Parkinson-White syndrome (WPW) is pre-excitation of the ventricles
• This is due to anatomical atrio-ventricular bypass tract with non-decremental conducting (conduction maintained) properties
• The most common cause of WPW tachycardias is antidromic revealed accessory pathway AVRT (narrow complex tachycardia)
• WPW appearance on an ECG:
  1) Shortened PR interval <0.12sec
  2) Slurred upstroke of QRS and
  3) Widened QRS complex >0.12sec

Question 36

when would you use the adenosine test?

Answer 36

in narrow complex/supraventricular tachycardias

Question 37

what does the adenosine test consist of?

Answer 37

• IV bolus of adenosine (3mg, then 6mg, then 12mg)
• half life of 4.5 secs

Question 38

what does the adenosine test cause?

Answer 38

it will cause transient and complete AV block

Question 39

what are the 3 responses to the adenosine test?

Answer 39

1) no effect = wrong diagnosis (sinus tachycardia in case of narrow complex or VT in case of broad complex)

2) transient slowing with atrial flutter or atrial tachycardia or without revealed P waves = AF

3) restoration of sinus rhythm

Question 40

How common if atrial fibrillation (AF)?

Describe the 3 features of AF appearance on an ECG? What are 3 signs of AF?

What are the associated symptoms?

Answer 40

• Atrial fibrillation (AF) is very common
• Appearance of AF on an ECG:
  1) Usually a narrow QRS complex
  2) Tachycardia
  3) No P waves
• 3 Signs of AF:
  1) Fast ventricular response rate (causes SOB, hypotension)
  2) Slow conduction (causes dizziness and syncope)
  3) Embolism of left atrial thrombus (can cause CVA (stroke))

Question 41

what are the 5 main causes of atrial fibrillation?

Answer 41

• ischaemic heart disease
• hypertensive heart disease
• mitral valve disease
• thyrotoxicosis
• alcohol

Question 42

what is the main atrial fibrillation cause?

Answer 42

size of the left atrium

Question 43

What are the 2 treatment objectives with AF?

Answer 43

• 2 treatment objectives with AF:
  1) Rate Control or Rhythm Control
• Rate control unless
• Symptomatic with high ventricular response rates to treatment
• Acute presentation with clear precipitating cause

2) Prevention of thrombo-embolism (esp. CVA)

Question 44

What 4 drugs can we use to slow AV conduction in AF?

What is another method to do this?

Answer 44

• 4 drugs we can use to slow AV conduction in AF:
  1) Diltiazem (non-dihydropyridine CBB)
  2) Verapamil (non-dihydropyridine CBB)
  3) Beta blocker
  4) (Digoxin)
• We can Ablate (remove) the AV node and put in a permanent pace maker to slow AV conduction

Question 45

What are the 2 types of treatments for rhythm control in AF?

What is cardioversion?

What are 2 methods of Cardioversion?

What are 3 methods for maintenance of sinus rhythm?

Answer 45

• Types of treatments for rhythm control in AF:

1) Cardioversion
* Process of restoring the heart’s normal rhythm by applying a controlled electric shock to the exterior of the chest
* Can be:
* Electrical DC cardioversion
* Chemical (e.g. Flecainide, Propafenone, Amiodarone)

2) Maintenance of Sinus Rhythm
* Can use:
* Class 3 Sotalol, Amiodarone
* Class 1c Flecainide
* Radiofrequency/cryo ablation (e.g. pulmonary vein ablation with or without atrial lines)

Question 46

What 2 drugs might we sued to prevent thrombo-embolisms in AF?

How does this differ between rheumatic and non-rheumatic AF?

Why do we prescribe them?

Why is aspirin not given?

What are the 2 main causes of stroke in AF?

What 3 methods do we use to decide between the 2 drugs that can be used in non-rheumatic AF?

What is a tool we can use for this?

Answer 46

• To prevent thrombo-embolisms in AF, we may prescribe:
  1) Warfarin (anticoagulant)
  2) NOAC (novel oral anti-coagulants)
• Warfarin is the only anticoagulant used in treatment of rheumatic AF
• These drugs are prescribed to reduce stroke risk attributable to AF
• Aspirin is not given as it has weak/no beneficial effect
• 2 main causes of stroke in AF:
  1) Non-rheumatic AF (less common type of AF)
  2) Mitral stenosis
• We decide between Warfarin and NOAC to treat non-rheumatic AF through:

1) Risk based
* Risk of stroke vs risk of anticoagulation

2) Risk of stroke (other than AF)
* Based on age, hypertension, previous stroke

3) Contraindications to anticoagulation
* Situations where drug should not be used e.g peptic ulcer disease, contact sports, alcoholism

• We can us CHA2DS2-VASc, which is a tool to measure risk of stroke in order to decide if the person gets warfarin/NOACs in non-rheumatic AF to prevent thromboembolisms.

Question 47

What are the 3 main types of broad complex tachycardia?

How do they appear on an ECG?

How does bundle branch block appear on an ECG?

What is aberration?

Answer 47

• 3 main types of broad complex tachycardia:

1) Ventricular Tachycardia
* Can be monomorphic (every complex is the same) and polymorphic (complexes are different) VT

2) SVT (supraventricular tachycardia) with aberration
* Aberration is acquired, rate- dependent bundle branch block
* Rate-dependent left bundle branch block refers to a transient left bundle branch block associated with an increase in heart rate
* If the QRS complex is widened and downwardly deflected in lead V1, a left bundle branch block is present.

3) SVT with a pre-existing BBB morphology on ECG
* e.g. SVT of antidromic tachycardia in WPW

Question 48

How do we differentiate between VT and SVT with aberration?

How serious and fast is VT?

What can it degenerate into?

Why is this deadly?

What is VT usually associated with in patients?

What does VT normally appear on an ECG?

What is the difference between monomorphic and polymorphic VT on ECGs?

What is Torsades do Pointes?

How does it present on an ECG?

Answer 48

• We differentiate between VT and SVT with aberration using an adenosine test, with there being no response for VT
• VT is very serious and often fast
• VT can degenerate into VF, which is an inherently unstable rhythm that can promote death through ischaemia in CAD
• VT is Usually associated with previous LV damage e.g MI
• On an ECG, VT has a broad complex, with no P waves associated with the QRS complex
• Monomorphic VT usually looks regular on an ECG
• Polymorphic VT is usually very irregular on an ECG (known as Torsades de Pointes – many morphologies)
• Torsades de Pointes is a type of polymorphic ventricular tachycardia characterized on electrocardiogram by oscillatory changes in amplitude of the QRS complexes around the isoelectric line.
• Torsades de Pointes is associated with QTc prolongation, which is the heart rate adjusted lengthening of the QT interval.

Question 49

What 3 questions must we ask when trying to see whether the broad complex tachycardia is VT or SVT with aberration?

Answer 49

• 3 questions must we ask when trying to see whether the broad complex tachycardia is VT or SVT with aberration:

1) Is the distinction important?
* If fast and the patient unwell the treatment is the same DC cardioversion

2) Is there a history of LV damage?
* If so, statistically a broad complex tachycardia will be VT whatever the ECG looks like

3) What is the AV relationship?
* Independent P waves, fusion or capture beats diagnose VT.
* Cannon waves in jugular vein pulse also diagnose VT.

Question 50

What are the 3 mechanisms/causes that lead to VT?

Answer 50

• 3 mechanisms/causes that lead to VT:

1) Acute LV damage
* Can be caused by ischaemia and trauma
* Specific mechanisms that interfere with cell membrane
* Electrophysiology

2) Chronic LV damage
* (micro) Re-entry around fibrotic areas of non-conduction

3) Abnormalities of the Na and K channels (Ion channelopathies) = Long QT interval syndrome
* Changes in intracellular K altering the cellular action potential
* Usually, polymorphic

Question 51

What are haemodynamic?

What is the Acute management of VT for compromised haemodynamics?

What 3 drugs can be used if haemoynamics are normal?

Answer 51

• Hemodynamics are the dynamics of blood flow.
• Acute treatment of VT:

1) If haemodynamically compromised
* DC synchronised cardioversion

2) Haemodynamics are normal
* i.v.Amiodarone
* i.v. lignocaine (only works in acute ischaemia VT)
* i.v.Class 1 agents (procainamide)

Question 52

What 2 phases are part of the management of VT in the long term?

What 3 things might we treat in phase 1?

What 4 things are we using as treatment in phase 2?

Answer 52

• 2 phases part of the management of VT in the long term:

1) Management for the underlying cause
* Treating:
* Active ischaemia in IHD – revascularize
* Pulmonary regurgitation post Fallot repair
* Heart Failure

2) Prevention of reoccurrence
* Implanted cardioverter defibrillator (ICD) – monitors heart and deliver shocks
* Beta blockers, Class 1 agents, Amiodarone
* Ablation
* Anti-tachycardia pacemaker (ATP)

Question 53

How fatal is VF?

How does it affect Cardiac output?

What is it often preceded by?

How does VF appear on an ECG?

Answer 53

• VF is Invariably fatal
• There is no detectable cardiac output in VF
• VF is Often (but not always) preceded by VT
• VF appears on an ECG as chaotic irregular deflections of varying amplitude

Question 54

What are 4 steps in the acute management of VF?

What treatment is used for VF in the long term?

Answer 54

• 4 steps in the acute management of VF:
  1) Defibrillation
  2) DC cardioversion
  3) IV adrenaline + DC cardioversion
  4) Treatment of any acute underlying cause
• In the long-term treatment of VF, we can use ICD implantation (Implantable cardioverter-defibrillator) if a patient survives

Question 55

What is the most likely cause of sudden death with normal heart at autopsy?

What is Torsades de Pointes?

How does it appear on an ECG?

Answer 55

• The most likely cause of sudden death with normal heart at autopsy is Polymorphic Ventricular Tachycardia
• Torsades de Pointes is a type of polymorphic ventricular tachycardia
• It is characterized on electrocardiogram by oscillatory changes in amplitude of the QRS complexes around the isoelectric line.
• Torsades de Pointes is associated with QTc prolongation, which is the heart rate adjusted lengthening of the QT interval.

Question 56

What are 4 congenital mechanisms associated with Torsades do Pointes?

What is also needed for Torsades do Pointes to occur?

Answer 56

• 4 congenital mechanisms associated with Torsades do Pointes:
  1) Ion channelopathy
  2) Brugarda syndrome – channelopathy that affects the way electrical signals pass through the heart
  3) Catacholaminergic Polymorphic VT
  4) ARVC - disorder of the myocardium,
• For Torsades do Pointes to occur, a provocation is needed, such as adrenalin, facial immersion, exercise, hypokalaemia

Question 57

What are 3 acquired mechanisms associated with Torsades do Pointes?

What are examples of each?

Answer 57

• 3 acquired mechanisms associated with Torsades do Pointes:

1) Drugs that inhibit inward rectifying K channel
* Erythromycin
* Antihistamines
* Nntifungal (conazoles)
* Some anti-malarials
* Some anti-psychotics

2) Drugs that lengthen QT interval
* Antiarrhythmics (such as Amiodarone, sotalol)

3) Slow AF with hypokalaemia and long-slow coupling interval

Question 58

What is another name for ion channelopathies?

What is the distinctive feature of ion channelopathies on an ECG?

Which phases of the AP change in a long QT interval syndrome?

Answer 58

• Another name for ion channelopathies is Long QT interval syndrome
• The distinctive feature of ion channelopathies on an ECG is a Long QT interval
• In long QT interval syndrome phases 2 and 3 are altered (determined by activity in sodium and potassium channels which is where mutations happen)

Question 59

What is Brugada syndrome?

How is it characterised on an ECG?

How is it associated with Torsades de Pointes?

Answer 59

• Brugada syndrome is A type of channelopathy in which people with no known heart problems or defects suffer sudden cardiac death or aborted sudden cardiac death.
• Characterised by Right bundle branch block, with persistent ST-segment elevation.
• One of the congenital causes of Torsades de Pointes.

Question 60

What are 9 risk factors for drug induced long QT syndrome (ion channelopathies)?

Answer 60

• 9 risk factors for drug induced long QT syndrome (ion channelopathies):
  1) Female gender
  2) Heart Failure
  3) LVH
  4) Hypokalaemia
  5) Hypomagnesaemia
  6) Digoxin
  7) Ca2+ Chan. Blockers
  8) Beta blockers
  9) Culprit drugs

Question 61

What are steps in Long QT Syndrome Management?

Answer 61

• Steps in Long QT Syndrome Management:
  1) Identify risk
  2) Avoid precipitating events
  3) Beta blockers
  4) Pacemaker
  5) Implantable cardioverter defibrillator (ICD)

Question 62

What is sudden cardiac death?

What are the 2 best tests to diagnose disturbance of the cardiac rhythm?

What is Holter monitoring?

Answer 62

• Sudden cardiac death is unexpected death due to heart problems, which occurs within one hour from the start of any cardiac-related symptoms
• 2 best tests to diagnose disturbance of the cardiac rhythm:

1) 12 lead ECG

2) Holter testing
* a technique for long-term, continuous usually ambulatory, recording of ECG signals on magnetic tape for scanning and selection of significant but fleeting changes that might otherwise escape notice.

Question 63

What type of AV block is this?

Answer 63

Type 1

Question 64

What type of AV block is this?

Answer 64

Type 2 mobritz 1

Question 65

What type of AV block is this?

Answer 65

Type 2 mobritz 2

Question 66

What type of AV block is this?

Answer 66

Type 3