Rx- Antiarrhythmics

Question 1

This plateau in cardiac depolarization causes
ventricular contraction to last as much as ____
times longer than skeletal muscle
contractions from a single action potential

Answer 1

15

Question 2

Phase 4

Answer 2

Resting membrane potential

Question 3

Phase 0

Answer 3

Depolarization
■ When the cell is stimulated, voltage-gated
sodium channels open quickly and permit
sodium to rush in, depolarizing the cell
membrane extremely quickly.

Question 4

Phase 1

Answer 4

• Initial Repolarization
  ■ The voltage-gated sodium channels rapidly
  close. By this time, voltage-gated potassium
  channels are open, allowing potassium to rush
  out of the cell, causing some repolarization.

Question 5

Phase 2

Answer 5

The Plateau
■ L-Type Calcium Channels that open slowly
during Phases 0 and 1 allow calcium to rush in. This influx of calcium balances the efflux of
potassium from early potassium channels,
thereby extending depolarization (plateau)

Question 6

Phase 3

Answer 6

• Rapid Repolarization
  ■ L-Type Calcium Channels close and additional potassium channels open, permitting potassium to exit the cell at a faster rate, causing rapid repolarization of the membrane.

Question 7

Some genetic mutations can result in abnormalities in channel proteins
in the heart, further resulting in arrhythmogenic syndromes
■ An example is_____

Answer 7

familial prolonged QT syndrome

Question 8

The most commonly used classification system for the antiarrhythmic drugs

Answer 8

Vaughan-Williams classification

Question 9

Modified Vaughan-Williams Classification of Antiarrhythmic Medications:

Answer 9

○ Class 1 - Sodium Channel Blockers (split up into three subclasses)
○ Class 2 - Beta Blockers
○ Class 3 - Potassium Channel Blockers
○ Class 4 - Calcium Channel Blockers
○ (Class 5 - Variable mechanisms; miscellaneous group)

Question 10

Class 1 Agents & subcategories

Answer 10

Class 1 antiarrhythmic medications act by modulating or
blocking the sodium channels that are responsible for rapid depolarization.
○ Class 1A - Increase duration of PR, QRS, and QT
○ Class 1B - Increase QRS duration, shorten AP duration
○ Class 1C - Increase duration of PR and QRS, not AP

Question 11

Class 1A Agents

Answer 11

● Procainamide, Quinidine, and Disopyramide

Question 12

Class 1A Agents MOA

Answer 12

○ Sodium Channel Blocker - Presumably interact with specific amino acids
in the internal pore of the sodium channel.
○ These depress Phase 0, thereby slowing QRS depolarization.
○ These also have moderate Potassium channel blocking activity, which
tends to slow the rate of the repolarization and prolongs the overall
action potential duration (Increases duration of PR, QRS, and QT)
○ These also seem to have a little anticholinergic activity and tend to
depress myocardial contractility

Question 13

Indications for Class 1A agents

Answer 13

○ Supraventricular Tachycardias
○ Ventricular Tachycardia
○ Quinidine only- Severe Malaria

Question 14

Contraindications for Class 1A agents

Answer 14

○ Systemic Lupus Erythematosus (Procain.)
○ 2nd or 3rd Degree AV Block
○ Congenital QT prolongation

Question 15

BBWs of Class 1A agents

Answer 15

○ Procainamide: Proarrhythmic effects can
occur; advised to restrict use
to life-threatening ventricular
arrhythmias.
■ Can cause positive ANA tests,
w/ or w/o Sxs of SLE.
■ Can cause blood dyscrasias;
check CBC qwk x 3 months.
○ Quinidine and Disopyramide: Increased mortality in Tx of non-life-threatening arrhyth.

Question 16

Class 1A Agents SA

Answer 16

○ Urinary retention, dry mouth, constipation (especially with Disopyramide)
○ Hypotension
○ Reversible Lupus Syndrome (with long-term Procainamide; 30%)
■ Increased ANA (50%)

Question 17

Major Adverse Reactions of Class 1A agents

Answer 17

○ At slower heart rates, potassium channel blockade may predominate, leading to
even longer action potential duration and the QT interval, resulting in increased
automaticity. Widened QT can result in Torsades.
○ Ventricular fibrillation and Asystole.
○ Severe blood dyscrasias can occur with Procainamide and Disopyramide.
○ Complete AV blocks can occur with Quinidine

Question 18

Follow Up for Class 1A agents

Answer 18

○ Dose adjustments needed if renal and/or hepatic impairment.
○ Check electrolytes, CBC, and ANA at baseline.
■ Repeat CBC weekly for 3 months with Procainamide
○ Lots and lots of drug interactions - Always run through checker.
○ Pregnancy/Lactation: Caution advised, but no harm expected

Question 19

a treatment of choice for AVRT (SVT in WPW)

Answer 19

Class 1A agents

Question 20

Class 1B Agents

Answer 20

Lidocaine and Mexiletine

Question 21

Class 1B Agents MOA

Answer 21

○ Sodium Channel Blocker - Presumably interact with specific amino acids
in the internal pore of the sodium channel.
○ These have less prominent sodium channel blocking activity at rest, but
effectively block the sodium channel in depolarized tissues.
■ For this reason, they seem to be more effective with
tachyarrhythmias than with slow arrhythmias
○ They also seem to shorten repolarization to some extent.
■ Shortens the action potential duration and the QT interval

Question 22

Class 1B Agents Indications

Answer 22

○ Ventricular Tachycardia and Fibrillation (Lidocaine used in ACLS)
○ Lidocaine: Local anesthesia
○ Mexiletine: *Off-label use of diabetic neuropathic pain

Question 23

Class 1B Agents Contraindications

Answer 23

○ Cardiogenic shock
○ AV Blocks
○ Lidocaine: Wolff-Parkinson-White syndrome

Question 24

BBWs of Class 1B agents

Answer 24

Mexiletine: Excessive mortality or nonfatal cardiac arrest rate in nonlife-threatening arrhythmias. Restrict use to life-threatening vent. arrhythmias.

Question 25

Class 1B Agents SAs

Answer 25

○ GI upset
○ Nausea
○ Anxiety
○ Lightheadedness
○ Tremor
○ Palpitations
○ Headache
○ Tinnitus

Question 26

Major Adverse Reactions of Class 1B agents

Answer 26

○ Ventricular arrhythmias
○ Lidocaine:
■ CNS depression or seizures
■ Coma
■ Heart block
■ Respiratory depression or arrest
■ Bradycardia and hypotension

Question 27

Follow Up for Class 1B agents

Answer 27

○ EKG should be monitored continually during Lidocaine infusion.
○ Monitor vital signs closely.
○ Check electrolytes at baseline.
○ Lidocaine may be used during pregnancy and lactation.
■ Mexiletine, however, should be used with caution

Question 28

Pearl for Class 1B agents

Answer 28

When injecting lidocaine for local anesthesia purposes, it’s important to not inject into a major vessel because it’s an antiarrhythmic drug

Question 29

Class 1C Agents

Answer 29

Flecainide and Propafenone

Question 30

Class 1C Agents MOA

Answer 30

○ Sodium Channel Blocker - Presumably interact with specific amino acids
in the internal pore of the sodium channel.
○ These primarily block open sodium channels, depressing Phase 0
depolarization and slowing conduction (QRS prolongation).
○ They dissociate slowly during diastole, resulting in increased effect at
more rapid rates. This is the basis of their antiarrhythmic efficacy,
especially against supraventricular arrhythmias
○ These both have mild potassium channel blocking activity as well, but
do not significantly change the action potential duration.

Question 31

Class 1C Agents indications

Answer 31

○ Ventricular Arrhythmias (VT and VF) prevention
○ Supraventricular Tachycardia prevention (A-Fib and PSVT)

Question 32

Class 1C Agents contraindications

Answer 32

○ Ischemic conditions (CAD, post-MI, etc.)
○ Cardiomyopathy
○ Heart blocks
○ Cardiogenic Shock
○ Severe hypotension
○ Long QT syndrome
○ Strong caution if structural heart disease

Question 33

Class 1C Agents SAs

Answer 33

○ Dizziness
○ Dyspnea
○ Headache
○ Nausea
○ Fatigue
○ Palpitations
○ Chest pain
○ Constipation
○ Abdominal pain

Question 34

Major Adverse Reactions of Class 1C Agents

Answer 34

○ Ventricular arrhythmias
■ Especially in diseased myocardium
(CAD, cardiomyopathy)
○ Congestive Heart Failure
○ Heart block
○ QT prolongation / Torsades
○ Cholestasis with hepatic failure
○ Blood dyscrasias

Question 35

BBW of Class 1C agents

Answer 35

○ Both drugs: Excessive mortality or nonfatal cardiac arrest rate in non-lifethreatening ventricular arrhythmias. Avoid use in non-life-threatening
ventricular arrhythmias.
○ Flecainide: Due to proarrhythmic effects, restrict use to life-threatening
ventricular arrhythmias; not recommended chronic A-Fib treatment.

Question 36

Follow up for Class 1C agents

Answer 36

○ Check renal and hepatic function at baseline, as well as CBC and CMP.
○ Check EKG frequently. Check CBC periodically.
○ Possible risk of fetal harm, so caution strongly advised during pregnancy. May
use during lactation, however

Question 37

Class 2 Agents

Answer 37

● Esmolol, Metoprolol, Atenolol, and Propranolol

Question 38

Class 2 Agents MOA

Answer 38

○ Beta Blockers - These act by inhibiting sympathetic activity by blocking
beta adrenergic receptors.
○ Because increased sympathetic stimulation is proarrhythmic, beta
blockade has moderate antiarrhythmic effects.
○ This blockade slows the rate of discharge from the SA node and ectopic
pacers, and increases the effective refractory period of the AV node.
■ Slows conduction through the AV node (increases PR Interval)
○ These decrease the upslope during Phase 4 (RMP), thereby slowing the
overall heart rate

Question 39

Class 2 Agents Indications

Answer 39

○ Sinus Tachycardia (rate control)
○ Supraventricular Tachycardia (such as A-Fib, rate control)
○ *Off-label: Premature Atrial Contractions (PACs)
○ Hypertension, Compensated heart failure, post-MI event prevention, tremor

Question 40

Class 2 Agents contraindications

Answer 40

○ Sinus bradycardia
○ 2nd or 3rd degree AV block and Sick Sinus Syndrome
○ Cardiogenic shock
○ Uncompensated heart failure
○ Pulmonary Hypertension
○ Significant asthma and/or COPD (Propranolol)

Question 41

Class 2 Agents Adverse reactions

Answer 41

○ Severe bradycardia
○ Severe hypotension
○ Congestive heart failure
○ MI if abrupt D/C
○ Ventricular arrhythmia
○ Sick Sinus Syndrome
○ New AV Block
○ Bronchospasm (especially with
Propranolol)

Question 42

Class 2 Agents BBW

Answer 42

Avoid abrupt cessation; can trigger angina, MI, and ventricular
arrhythmias is discontinued abruptly.

Question 43

Pearl for Class 2 agents

Answer 43

Propranolol is non-cardioselective, meaning it has more of an affect on
the pulmonary system than do the others.

Question 44

Class 3 Agents

Answer 44

Amiodarone, Sotalol, Ibutilide, Dofetilide, Dronedarone

Question 45

Class 3 Agents MOA

Answer 45

○ Potassium Channel Blockers - By blocking the movement of potassium out of the cell, meaning repolarization is prolonged and the duration of the action potential is significantly prolonged.
■ This also means there is prolongation of the refractory period and the QT
interval
○ Sotalol also has some beta blocking activity.
○ Amiodarone and it’s cousin Dronedarone also block sodium and calcium
channels to some extent, as well as adrenergic receptors.

Question 46

Class 3 Agents Indications

Answer 46

○ Sotalol: Life-threatening Ventricular Rhythms
○ Amiodarone: Ventricular Tachycardia and Ventricular Fibrillation (also used in
ACLS), as well as *off-label for Atrial Fibrillation
○ Dofetilide and Ibutilide: Atrial Fibrillation and Flutter Conversion
○ Dronedarone: Atrial Fibrillation and Flutter Prevention

Question 47

Class 3 Agents contraindications

Answer 47

○ Cardiogenic shock or decompensated heart failure
○ Severe SA node dysfunction and/or 2nd-3rd degree AV Blocks
○ Congenital Long QT syndrome
○ Significant electrolyte abnormalities
○ Dronedarone: Contraindicated in permanent Atrial Fibrillation

Question 48

BBW for Class 3 Agents

Answer 48

○ All Class 3 Drugs: Appropriate use- Restrict use to indicated life-threatening arrhythmias, and initiate treatment in a facility that can provide CrCl, continuous EKG, and ACLS abilities.

○ Amiodarone, Sotalol, and Ibutilide: Proarrhythmic Effects- Arrhythmias worsen, significant heart block develops, or
ventricular tachycardia. Beware of baseline QT prolongation. Monitor closely.
○ Amiodarone: Pulmonary Toxicity- Severe pneumonitis occurs in 10-17% of patients, fatal in 10% of
patients. Monitor CXR.
■ Hepatotoxicity- Common but usually mild bump in LFTs.
○ Dronedarone: Risk of death, stroke, and heart failure increased if the patient has decompensated congestive heart failure or permanent Atrial Fibrillation.

Question 49

Class 3 Agents SA

Answer 49

○ Amiodarone: Thyroid Disease (hypo or hyper), photosensitivity, corneal
deposits (long-term use), tremor, LFT elevation
○ Ibutilide: Extrasystoles, non-sustained V-Tach

Question 50

Major Adverse Reactions of Class 3 Agents

Answer 50

○ All Class 3 drugs: QT prolongation, Torsades de Pointes, heart failure, severe
bradycardia, heart blocks, cardiac arrest
○ Amiodarone (and to a lesser extent Dronedarone): Pulmonary Fibrosis,
hepatitis, pulmonary toxicity, ARDS

Question 51

Class 3 Agents follow up

Answer 51

○ Check CBC, BP, EKG, and electrolytes periodically.
○ Check QT interval for more than 3 days after dose start or increase.
○ Amiodarone (and Dronedarone): Check LFTs and CXR at baseline and
periodically. LFTs, PFTs, TSH/fT4 every 3-6 months while on the drug.
○ Dofetilide: Monitor Creatinine periodically, discontinue if elevation.
○ Pregnancy/lactation: Caution advised, risk unknown.
■ Dronedarone contraindicated in pregnancy- animal studies show risk.

Question 52

Class 4 Agents

Answer 52

Verapamil and Diltiazem (non-dihydropyridines)

Question 53

Class 4 Agents MOA

Answer 53

○ Calcium Channel Blockers - These slow the overall depolarization
conduction and prolong Phase 2 duration.
○ Slows the SA rate (decreased HR), and increases the refractoriness of
and prolongs conduction through the AV node (increased PR interval).

Question 54

Class 4 Agents indications

Answer 54

○ Supraventricular Tachycardias (A-Fib, A-Flutter, PSVT)
○ Other uses for both: Angina and Hypertension
○ Verapamil only: *Off-label for Migraine prophylaxis

Question 55

Class 4 Agents Contraindications

Answer 55

○ Severe left ventricular dysfunction
○ 2nd or 3rd degree AV block
○ Atrial fibrillation/flutter with bypass
tract (such as WPW Syndrome)
○ Sick Sinus Syndrome
○ Severe hypotension / Cardiogenic shock
○ Caution if CHF or bradycardia

Question 56

Class 4 Agents SAs

Answer 56

○ Hypotension
○ Decreased LV
contractility
○ Constipation
○ Flushing
○ Headache
○ Dizziness
○ Nausea
○ Peripheral edema

Question 57

Class 4 Agents Adverse reactions

Answer 57

○ Congestive Heart Failure
○ Severe hypotension
○ Severe bradycardia
○ Sick Sinus Syndrome (in
diseased hearts)
○ New AV heart block
○ Hepatotoxicity
○ Paralytic ileus

Question 58

Class 4 Agents follow up

Answer 58

○ Caution advised during pregnancy
and lactation.
■ If needed, Verapamil seems to
be safe in pregnancy based on
limited data

Question 59

Class 5 Agents

Answer 59

● Class 5 is a miscellaneous group of antiarrhythmic medications that do not fit
into the other 4 Classes
○ Adenosine
○ Digoxin
○ Magnesium Sulfate

Question 60

Adenosine MOA

Answer 60

○ Aggressively blocks the AV nodal conduction.
■ Causes a very brief and usually complete AV blockage
○ This terminates supraventricular tachycardias and allows for a reset of
normal conduction (allows the SA node to resume pacing).

Question 61

Adenosine Indications

Answer 61

○ Conversion of Paroxysmal Supraventricular Tachycardia (PSVT)
■ Prompt cardioversion in 90-95% of cases
○ ACLS Tachycardia (used in protocol)
○ Cardiac Stress Testing (at small dose, causes coronary dilation)

Question 62

Adenosine contraindications

Answer 62

○ 2nd or 3rd degree AV block
○ Sinus node dysfunction
○ Signs/symptoms of acute
myocardial ischemia

Question 63

Adenosine SAs

Answer 63

○ Flushing (18%)
○ Dyspnea (12%)
○ Chest discomfort
○ Headache
○ Nausea

Question 64

Major Adverse
Reactions of Adenosine

Answer 64

○ Cardiac arrest
○ Ventricular arrhythmias
○ Severe bradycardia
○ Myocardial infarction
○ Atrial Fibrillation

Question 65

Follow Up for Adenosine

Answer 65

○ Minimal drug interactions; half-life in the body is less than 10 seconds.
○ No adjustment needed for renal or hepatic impairment.
○ Monitor EKG throughout administration of the drug.
○ May use during pregnancy and lactation.

Question 66

Pearl for Adenosine

Answer 66

○ Essentially stops the heart for a few seconds and allows it to reset
normal conduction.
○ Conscious patient feels their heart stop and experiences chest pressure,
dyspnea, and sometimes panic

Question 67

Digoxin MOA

Answer 67

○ Inhibits the Sodium-Potassium Pump in myocardium.
○ Prolongs the AV nodal conduction and AV nodal refractory period.
○ Because of its positive inotropic effects, Digoxin can strengthen the
contractility of even failing hearts (useful in later heart failure).

Question 68

Indications of Digoxin

Answer 68

○ Atrial Fibrillation (not first line)
○ Congestive heart failure (not first line)
○ *Off-label use of PSVT conversion (not commonly used)

Question 69

Digoxin Contraindications

Answer 69

○ Ventricular fibrillation
○ Myocarditis
○ Acute Myocardial Infarction

Question 70

Digoxin SA

Answer 70

○ Dizziness
○ Headache
○ GI upset
○ Bradycardia
○ Palpitations
○ Anxiety
○ Depression

Question 71

Major Adverse Reactions of Digoxin

Answer 71

○ AV block
○ Severe bradycardia
○ Ventricular arrhythmias
○ Delirium/hallucinations

Question 72

Digoxin plant origin

Answer 72

● Digoxin is derived from the leaves of Digitalis, a
flowering plant commonly called foxglove digitalis.

Question 73

Digoxin follow up

Answer 73

○ Digoxin has a narrow therapeutic window and toxicity is common.

Question 74

Digoxin pearls

Answer 74

○ Losing favor due to its toxicity and the availability of other options.
○ First symptoms of toxicity include blurred vision, GI upset, fatigue, weakness.
○ The most common cardiac manifestations of toxicity include a new junctional
rhythm, Premature Ventricular Contractions (PVCs), and/or a new Second
Degree AV Block

Question 75

The treatment of choice for significant digoxin toxicity is ____

Answer 75

prompt insertion of a temporary cardiac pacemaker catheter and administration of digitalis antibodies (Digoxin Immune Fab, AKA DigiFab or DigiBind).
■ These antibodies bind to and reverse digitalis (and other glycosides)

Question 76

Magnesium Sulfate MOA

Answer 76

○ Poorly understood. Specific mechanism is largely unknown.
○ Is believed to interact with Sodium-Potassium pump, as well as
potassium and calcium channels.
○ Normalizes or increases plasma magnesium levels as well.

Question 77

Magnesium Sulfate Indications

Answer 77

○ Hypomagnesemia
○ Seizures in Preeclampsia/Eclampsia
○ *Off-label uses: Tocolysis, Ventricular arrhythmias (stable), Torsades de
Pointes (stable), and Severe asthma exacerbation

Question 78

Magnesium Sulfate contraindications

Answer 78

○ Myocardial damage
○ Diabetic coma
○ Heart Blocks
○ Caution if renal impairment

Question 79

Magnesium Sulfate adverse reactions

Answer 79

○ Cardiovascular collapse
○ Respiratory paralysis
○ Hypothermia
○ Depressed cardiac function
○ Pulmonary edema
○ Severe electrolyte disturbances