11. Anti-arrhythmic Drugs

Question 1

What are the 2 goals of treatment for arrhythmia?

What are the 4 classes of mechanisms?

Answer 1

2 goals:

1. Termination of an ongoing arrhythmia
2. Prevention of an arrhythmia

4 classes:
Class 1- Na channel blockers
Class 2- Beta blockers
Class 3- K channel blockers 
Class 4- Ca channel blockers

Question 2

Can anti-arrhythmic drugs cause arrhythmias too?

Answer 2

Yes with long term use

The function of the heart depends on its electrical activity- mediated by the action potential
The action potential depends on the activity of ion channels: Na ion channels, K ion channels, Ca ion channels
Anti-arrhythmic drugs alter activity of ion channels (if incorrectly used they can cause arrhythmias)

Question 3

Review the heart diagram slide 6-7 Anti-arrhythmic drugs

Answer 3

Okay

Question 4

What are the 2 types of cardiac tissue?

Answer 4

1. That with which action potentials occur automatically
   - SA node (60-100bpm)
   - AV node (50-60bpm)
   - bundle of His (50-60bpm)
   - purkinje system (30-40bpm)
2. That with which actions potentials do not occur automatically (received from automatic tissues and spread throughout)
   - atrial muscle
   - ventricular muscle

Question 5

What are the 3 phases of the pacemaker action potential?

SA node AP

Answer 5

Phase 4- spontaneous If current- non-selective action channels (If current)- mainly carry Na in

Phase 0- rapid depolarization - inward Ca L type channels

Phase 3- repolarization - outward K current

Slide 9 anti-arrhythmic drugs

Question 6

What are the 5 phases of action potential of cardiac myocytes?

Answer 6

Phase 0- rapid depolarization - inward Na - Ina current determines velocity if impulse conduction throughout ventricle

Phase 1- transient outward K current

Phase 2- (plateau) inward Ca current

Phase 3- repolarization - outward K current
(Phases 2/3 determine duration of AP and refractory period

Phase 4- resting phase, Na channels enter resting state from inactivated state

Slide 10 Anti-arrhythmic drugs

Question 7

What are the 3 differences between pacemaker cells (SA node, AV node) and myocitic cells (atrial and ventricular muscle cells)?

Answer 7

1. Pacemaker cells have automaticity (membrane starts to depolarizes slowly but spontaneously) while myocytes have no automaticity (membrane depolarizes when it receives AP from pacemakers)
2. Pacemaker action potential has 3 phases, myocytes has 5 phases
3. In pacemakers, Ca causes rapid depolarization in phase 0, in myocytes, Na causes rapid depolarization in phase 0

Slide 11 Anti-arrhythmic drugs

Question 8

What is the serum K+ physiologic range?
What values are hypokalemic?
What values are hyperkalemic?

Answer 8

Serum K+ physiological range: 3.5 to 5 mM

Hypokalemia (<3.5mM)
Hyperkalemia (>5mM)

Both arrhythmogenic

Question 9

What is hypokalemia?

How can they cause arrhythmias?

Answer 9

Serum K range of <3.5mM
Slows repolarization
Action potentials become wider (increased duration)

Cause arrhythmias by decreasing conductance of K channels, slow repolarization, K channel pores are blocked by Mg and polyamines, increase Na and Ca cause early and delayed after depolarizations, ectopic beats, ventricular tachycardia and fibrillation

Slides 12-14 anti-arrhythmic drugs

Question 10

How can diuretics cause arrhythmias?

Answer 10

Diuretics (thiazides and loop) can cause hypokalemia and predispose to arrhythmias

Question 11

What is hyperkalemia?

Answer 11

Serum K range of >5mM
Depolarizes membrane and slows conduction velocity
Renal failure can cause hyperkalemia and life threatening arrhythmias
Hyperkalemia decreases resting membrane potential (becomes more positive-depolarized)
Increases K channel conductance, faster repolarization

Decreases availability of Na channels responsible for phase 0 depolarization
At very high levels of K > 14mM conduction finals leading to cardiac arrest

Slides 15-16 anti-arrhythmic drugs

Question 12

What are the effects of class 1 anti-arrhythmic drugs?
Na channel blockers

Answer 12

Block Na channels in the open or inactive state
Decrease re entry and prevent arrhythmia

In atrial and ventricular muscle:
Decrease depolarization in phase 0, decrease conduction velocity

In SA node:
- decrease spontaneous Na channel opening in phase 4, decrease heart rate and automaticity

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Slide 27 AAD

Question 13

What is class IA of Na channel blockers?
Uses?
Adverse effects?

Answer 13

IA- procainamide: class IA sodium channel blocker that prefers binding to open state

Used to treat supraventricular and ventricular arrhythmias (ex: atrial fibrillation)

Adverse effects: chronic treatment may cause lupus like syndrome

Question 14

What is class IB of Na channel blockers?
Uses?
Adverse effects?

Answer 14

Lidocaine
Exhibits use dependant block (blocks Na channels in their open and inactive states)
Works best in depolarized or rapidly driven tissues (found in ischemic myocardium)
Also has local anesthetic action

Adverse effects: tremor, dysarthria, confusion, dizziness, seizures (due to block of CNS Na channels)

Used for acute IV treatment of ventricular arrhythmias. NOT useful in atrial arrhythmias
(Don’t think I have to know this use)

Slides 29-30 AAD

Question 15

What are the common therapeutic effects of Na channel blockers?
Who are class I drugs restricted to?

Answer 15

To treat supraventricular and ventricular arrhythmias (atrial flutter or fibrillation) and maintain sinus rhythm
To prevent ventricular tachycardia and fibrillation

Class I drugs restricted to patients with structurally normal hearts (can cause arrhythmias I’m not normal hearts)

Slide 31 AAD

Question 16

What are the effects of class 2 anti-arrhythmic drugs?
β blockers

Answer 16

Block β1 and β2 receptors in heart

In SA, AV nodes:

• decrease spontaneous Na channel opening in phase 4, decrease heart rate
• decrease Ca channel opening and depolarization in phase 0, decrease automaticity and conduction velocity at AV node

In ventricular muscle:
- decrease contractility (different mechanism)

Slide 19 AAD
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Question 17

What are the therapeutic uses of β blockers?
(4 of them)
Adverse effects?

Answer 17

Widely used, decrease mortality after myocardial infarction
Terminate re-entry arrhythmias involving AV node
Control the ventricular rate in atrial flutter and fibrillation
To suppress stress induced arrhythmias
Control arrhythmias induced by Na channel blockers

Adverse effects: can cause severe bradycardia and even AV block

Question 18

What are the effects of class 3 anti-arrhythmic drugs?
K channel blockers
Adverse effects?

Answer 18

Block K channels

In atrial and ventricular muscle:
- decrease repolarization in phases 2 and 3, increase action potential duration (wider), increase refractory period, decrease re entry, prolonged repolarization

No effect in SA node

Adverse effects: increased risk of early after hyperpolarizations and torsades de pointes

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Question 19

What is the K channel blocker Amiodarone?

Adverse effects?

Answer 19

Blocks K channels, inactivated Na channels, Ca channels, and β receptors
Increases action potential duration, decreases conduction velocity, increases refractoriness in all cardiac tissues
Used for recurrent ventricular tachycardia or fibrillation resistant to other drugs

Adverse effects: (with higher doses and long term therapy) pneumonitis, pulmonary fibrosis, hyper or hypothyroidism

Slide 35 AAD

Question 20

What is the K channel blocker sotalol?

Adverse effects?

Answer 20

Blocks K channels in all cardiac tissue (increases action potential duration)
Blocks β channels (decrease automaticity, decrease AV conduction, increase AV refractory period)
Used for ventricular tachyarrhythmias, atrial flutter and fibrillation

Adverse effects: fatigue, bradycardia, risk of torsades de pointes (with high dose and low plasma K)

Slide 36 AAD

Question 21

What are the effects of class 4 anti-arrhythmic drugs?
Ca channel blockers

Answer 21

Block L TYPE calcium channels in the heart

In AV node:
- decrease Ca channel opening and depolarization in phase 0, decrease automaticity and conduction velocity at AV node

In SA node:
- decrease depolarization in phase 0, decrease heart rate

Slide 21 AAD

Question 22

What are the uses and adverse effects of Ca channel blockers?

Answer 22

Uses: supraventricular tachyarrhythmias, AV re-entrant tachycardia, decrease ventricular rate in atrial flutter and fibrillation, parental verapamil and diltiazem for rapid conversion of PSVTs to sinus rhythm

Adverse effects: bradycardia or AV block, hypotension, constipation
Do not combine non-DHPs with β blocker (can precipitate heart failure)

Slide 40 AAD

Question 23

What are the 6 causes of arrhythmias?

Answer 23

1. Defects in impulse formation- increase sympathetic or parasympathetic activity
2. Electrolyte disturbances- hypo or hyperkalemia
3. Drugs that increase action potential duration (decrease K currents, EADs, and DADs)
4. Defects in impulse conduction- re entry, conduction block
5. Damage to myocytes- myocardial infraction (mostly ventricular tachycardia and fibrillation)
6. Structural defects

Question 24

What are the 5 types of arrhythmias?

Answer 24

1. Sinus tachycardia- SA node rate 100-180bpm
2. Paroxysmal supraventricular tachycardia (PSVT)- atrial rate 140-250bpm
3. Atrial flutter- atrial rate 280-300bpm
4. Atrial or ventricular fibrillation- rate >300bpm
   Atrial fibrillation can be fine for many years
   Ventricular fibrillation is emergency
5. Torsades de Pointes (twisting of points around the baseline in an ECG)- results from after depolarizations when action potential duration is increased (some have prolonged QT syndrome) - slide 37-38 AAD

Question 25

What do we do if something is wrong with pacemaker in an arrhythmia?
What do we do if something is wrong with conduction of action potential in an arrhythmia?

Answer 25

Something wrong with pacemaker- increase or decrease rate- use drugs that alter heart rate (pacemaker activity)

Something wrong with conduction of action potential:
In AV node, use drugs that alter conduction velocity in AV node
In atrial and ventricular smooth muscle, use drugs that alter conduction velocity (depolarization through Na channels) or refractory period (determines by K channel and APD)

Question 33

How do you pick anti-arrhythmic drugs if they’re from atrial myocytes and ventricular myocytes?

Answer 33

Atrial myocytes- drugs that decrease conduction velocity and increase action potential duration (refractory period):
Na channel blockers and K channel blockers

Ventricular myocytes- drugs that decrease conduction velocity and increase action potential duration (refractory period):
Na channel blockers and K channel blockers

Slide 25 AAD

Question 34

How do you pick anti-arrhythmic drugs from the SA node and AV node?

Answer 34

SA node- drugs that decrease automaticity:
β blockers, Ca channel blockers, and Na channel blockers

AV node- drugs that decrease automaticity (rate) and AV conduction velocity:
β blockers, Ca channel blockers, and Na channel blockers

Slide 25 AAD

Question 35

What is the problem with applying anti-arrhythmic drugs to atrial flutter?

Answer 35

At atrial rate of 300bpm ratio of impulses reaching ventricles 2:1 or 4:1 which makes ventricular rate 150bpm or 75bpm which means it can still pump blood efficiently
Adding anti-arrhythmic drug reduces flutter rate from 300 to 200bpm without ventricular protection
So atrial rate is at 200bpm with 1:1 ventricle impulse ratio so ventricle is at 200bpm which isn’t good to pump blood efficiently

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