Cardiology 2

Question 1

Phases of the Action Potential

Answer 1

Phase 0: Depolarization

• Rapid Na entry
• Slow Ca entry

Phas 1: Repolarization
- K expulsion

Phase 2: Plateau

• Slow Ca entry
• Slow K expulsion

Phase 3: Resting potential
- K expulsion

Phase 4: Quiescence

• Na exits
• K reenters

Question 2

EKG P Wave (Length and Description)

Answer 2

Length: <0.1

Description: Atrial Depolarization

Question 3

QRS Complex (Length and Description)

Answer 3

Length: 0.05-0.1

Description: Ventricular Depolarization

Question 4

T Wave (Description)

Answer 4

Ventricular repolarization

Question 5

ST Segment (Description)

Answer 5

Ventricular repolarization

Question 6

QT Interval (Length and Description)

Answer 6

Length: <0.5

Description: Ventricular depolarization and repolarization

Question 7

Most common pediatric asymptomatic arrhythmias (3)

Answer 7

1. Sinus arrhythmia
2. Ventricular premature beats (VPBs)
3. Atrial premature beats (APBs)

Question 8

Sinus Arrhythmias (4)

Answer 8

1. Normal physiologic variant characterized by increased heart rate during inspiration and a decreased heart rate during expiration
2. Caused by changes in parasympathetic input to the heart
3. Usually a benign condition
4. Diagnosis confirmed by electrocardiogram

Question 9

Ventricular Premature beats (6)

Answer 9

1. Also known as ‘Premature Ventricular Contractions (PVCs)’
2. Premature depolarizations of the ventricles leading to early systolic contractions
3. Usually followed by a pause resulting in irregular heart rates and irregular patterns
4. Occur in isolation and are generally benign
5. MAY cause hemodynamic compromise
6. May present as bigemonys or trigemonys

Question 10

Atrial Premature Beats

Answer 10

1. Also known as ‘Premature Atrial Contractions (PACs)’
2. Early depolarizations of atrial myocardium leading to propagation of electrical impulses through the atrium
3. Results in early systolic ventricular contractions
4. Usually benign and rarely associated with sustained tachyarrhythmias

Question 11

Symptomatic Arrhythmias (3)

Answer 11

1. Underlying etiology may be due to a sustained tachyarrhythmia
2. Clinical symptoms often present as
   – Palpitations
   – Syncope
   – Chest pain
3. Supraventricular Arrhythmias
   – Atrial Fibrillation (AFib)
   – Paroxysmal Supraventricular Tachycardia

Question 12

Different Classifications of Atrial Fibrillation (5)

Answer 12

1. Acute: Onset within 48 hours
2. Paroxysmal: Abrupt start, converts spontaneously within 7 days
3. Persistent: Does not convert spontaneously, lasts longer than 7 days
   4: Permanent: Does not terminate with pharmacological conversion or electrical conversion
4. Recurrent: > 2 episodes

Question 13

Goal of therapy for atrial fibrillation

Answer 13

normalize ventricular rate

Question 14

Rate Control Therapies (4)

Answer 14

Everyone should receive rate control!!!

1. Beta Blockers
2. Non-DHP calcium channel blockers
3. Digoxin
4. Amiodarone*

Question 15

Rhythm Control Therapies (7)

Answer 15

Not everyone receives rhythm control!; incidence of rhythm control comes with more series side effects such as stroke/embolism and death

1. Amiodarone*
2. Sotalol (a rhythm control beta blocker)
3. Propafenone
4. Procainamide
5. Quinidine
6. Flecainide
7. Dofetilide

Question 16

Inotropes

Answer 16

Soft vs. Hard; strengthens or weakens the heartbeat

Ex: Digoxin is a positive inotrope

Question 17

Chronotope

Answer 17

Fast versus slow; alters the heart rate

Question 18

Dromotrope (2)

Answer 18

1. Speed of electrical conduction from either nerve or cardiac muscle
2. Usually has both inotropic and chronotropic effects as well (i.e. chronotrope)

Question 19

Beta blockers mechanism of action (5)

Answer 19

1. Blocks effect of sympathetic neurotransmitters (norepinephrine) on the heart and vasculature
2. Decreased ventricular arrhythmias
3. Decreased ventricular response rate
4. Decreased AV nodal conduction
5. Decreased impulse transmission

Question 20

Zabeta (Generic Name, Mechanism, Route)

Answer 20

Generic Name: Bisorolol

Mechanism: b1 selective

Route: PO

Question 21

Brevibloc (Generic Name, Mechanism, Route)

Answer 21

Generic Name: Esmolol

Mechanism: B1 selective

Route: IV

Question 22

Tenormin (Generic Name, Mechanism, Route)

Answer 22

Generic Name: Atenolol

Mechanism: B1 Selective

Route: PO

Question 23

Lopressor (Generic Name, Mechanism, Route)

Answer 23

Generic Name: Metoprolol IR

Mechanism: B1 Selective

Route: IV and PO

Question 24

Bystolic (Generic Name, Mechanism, Route)

Answer 24

Generic Name: Nebivolol

Mechanism: B1 selective

Route: PO

Question 25

Inderal (Generic Name, Mechanism, Route)

Answer 25

Generic Name: Propranolol

Mechanism: Non-selective

Route: IV and PO

Question 26

Cautions with Beta Blockers (4)

Answer 26

1. Severe bronchospastic disease (Asthma)
2. Bradycardia
3. Symptomatic hypotension
4. 2nd or 3rd degree heart block

Question 27

Beta Blocker Clinical Pearls (4)

Answer 27

1. Acute rate control in patients with normal left ventricular function
2. Chronic rate control in patients with normal or impaired left ventricular function
3. Higher doses needed for acute rate control compared to heart failure
4. IV route is preferred for acute rate control

Question 28

Non-Dihydropyridine CCBs Mechanism of Action (5)

Answer 28

1. Decreases influx of calcium on vascular smooth muscle and myocardium; slows conduction and automaticity through AV node
2. Decreased ventricular arrhythmias
3. Decrease ventricular response rate
4. Decrease AV nodal conduction
5. Decrease impulse transmission

Question 29

Types of CCBs (6)

Answer 29

1. Diltiazem
2. Cardizem
3. Tiazac
4. Verapamil
5. Calan
6. Verelan

Question 30

CCB Clinical Pearls (6)

Answer 30

1. Major CYP3A4 substrate
2. More constipation w. verapamil
3. With IV formulation have more pronounced side effects (Caution with IV use)
4. Agent of choice for acute rate control (but always use BB first with pediatric patients)
5. Avoid as chronic therapy for patients with impaired left ventricular function
6. IV CCBs should be used for LESS than 48 hours.

Question 31

CCB ADEs (6)

Answer 31

1. Hypotension
2. Decreased HR
3. Fluid retention
4. Dizziness
5. Flushing
6. Constipation (specifically verapamil)

Question 32

CCB Cautions (3)

Answer 32

1. Sick Sinus Syndrome
2. Wolff-Parkinson White Syndrome
3. 2nd or 3rd degree AV block

Question 33

Digoxin Mechanism of Action (2)

Answer 33

1. Direct inhibition of Na/K ATPase –> inhibition of Na/K ATP dependent pump
   - Indirect activation Na/Ca transport pump increased intracellular Ca = increased efficiency of excitationcontraction of cardiac muscle; “Positive Inotrope”
2. Indirect effect @ AV & SA nodes through vagal stimulation; “Negative chronotrope”

Question 34

Digoxin Dosing (2)

Answer 34

mcg/kg/day

1. Loading dose is based on: Age, Formulation, indication
   - May not be necessary
2. Maintenance dose: 2.5 – 10 mcg/kg q24
   – Requires renal dose adjustments***

Question 35

Digoxin Dose Monitoring

Answer 35

HF: 0.5-0.9

Toxicity: Over 2

Question 36

Digoxin ADEs (9)

Answer 36

MUST KNOW ALL

1. 3rd degree block, cardiac changes (PVC, VT/Vfib, etc)
2. Rash
3. N/V/D
4. Abdominal pain
5. anorexia
6. Visual disturbances
7. HA
8. dizziness
9. delerium

Question 37

Risk for Digoxin Toxicity (6)

Answer 37

MUST KNOW ALL

1. Hypokalemia
2. Hypomagneseia
3. Hypercalcemia
4. Decreased clearance
5. Low body weight (children)
6. *Digoxin has a very long half life

Question 38

Digibind (4)

Answer 38

1. Immune antigen-binding fragments for digoxin
2. Binds to digoxin to then be eliminated through kidneys
3. Onset: 20 – 90 min to resolution of symptoms
4. **Once administered lab values become irrelevant

Question 39

Normal Sinus Rhythm Conversion Therapies (5)

Answer 39

1. Dofetilide
2. Flecainide
3. Propafenone
4. Sotalol
5. Amiodarone*

Question 40

Vaughan Williams Classifications: Classification 1 (3 and what they block)

Answer 40

*Classifies different anti-arrhythmic drugs

1A: Quinidine, Procainamide, Disopyramide
Blocks - Na channel

1B: Lidocaine, Mexilitine
Blocks - Na channel

1C: Flecainide, Propafenone
Blocks - Na channel

Question 41

Vaughan Williams Classifications: Classification 2 (3 and what it blocks)

Answer 41

*Classifies different anti-arrhythmic drugs

1. Propranolol
2. Esmolol
3. Sotalol

Blocks beta adrenergics

Question 42

Vaughan Williams Classifications: Classification 3 (3 and what it blocks)

Answer 42

*Classifies different anti-arrhythmic drugs

1. Dofetilide
2. Sotalol
3. Amiodarone

Blocks potassium channels

Question 43

Vaughan Williams Classifications: Classification 4 (2 and what it blocks)

Answer 43

*Classifies different anti-arrhythmic drugs

1. Verapamil
2. Diltiazem

Blocks Ca channel

Question 44

Dofetilide Mechanism of action (3)

Answer 44

1. Classification: Class III antiarrhythmic
2. Blocks potassium channels to increase action potential due to delayed repolarization
3. NO effect on:
   - Sodium channels
   - Adrenergic alpha-receptors
   - Adrenergic beta-receptors

Question 45

Dofetilide ADEs (5)

Answer 45

1. Hypotension
2. Decreased HR
3. QTc prolongation
4. Syncope
5. Dizziness

Question 46

Dofetilide Cautions (3)

Answer 46

1. QTc > 440 msec
2. CrCl < 20 mL/minute
3. Concurrent use of verapamil

Question 47

Dofetilide Monitoring (6)

Answer 47

1. Vitals
2. BP
3. HR
4. EKG: Rhythm and QTc (delays action potential)
5. Basic metabolic panel (look at potassium; can affect rhythmic state)
6. Adverse effects

Question 48

Dofetilide Clinical Pearls (3)

Answer 48

1. Safe and effective in heart failure patients
2. Prolonged QTc requires 50% dose reduction
   * The starting dose should be reduced due to the baseline QTc prolongation.
3. Potential for proarrhythmic effects

Question 49

Sotalol Mechanism of Action (3)

Answer 49

1. Classification: Class II and III antiarrhythmic
2. Beta-Blocker (class II) effects
   - beta-adrenoreceptor-blocking properties
   - Cardiac action potential prolongation
3. Class III effects: Blocks K+ channels at higher doses

Question 50

Sotalol ADEs (7)

Answer 50

1. Hypotension
2. Decreased HR
3. AV block
4. QTc prolongation (dose reduce if > 450 QTc)
5. Bradyarrhythmia
6. Dizziness, headache
7. Fatigue

Question 51

Sotalol Cautions (4)

Answer 51

1. Severe bronchial asthma
2. 2nd or 3rd degree AV block
3. Uncontrolled heart failure
4. Renal failure

Question 52

Sotalol Clinical Pearls (4)

Answer 52

1. Potential for proarrhythmic effects
2. Titrate doses ONLY after 5-6 doses have been administered (titrate dose only after reaching steady state)
3. Decrease or discontinue if QTc exceeds 25% of baseline
4. May mask signs of hyperthyroidism (due to beta blocker effects)

Question 53

Flecainide Mechanism of Action (4)

Answer 53

1. Classification: Class Ic antiarrhythmic
2. Blocks sodium channels to prolong refractory periods and increases electrical thresholds
3. Moderate negative inotropic effects
4. Increases both anterograde & retrograde

Question 54

Flecainide Indications of Use (5)

Answer 54

1. Atrial flutter
2. Ectopic atrial and junctional tachycardia
3. Re-enterant atrial tachycardia
4. Wolf Parkinson White sundrome
5. Neonatal & Fetal tachycardia

Question 55

Flecainide ADEs (5)

Answer 55

1. Dizziness
2. Visual disturbances
3. Dyspnea
4. Ventricular arrhythmias
5. Worsening heart failure

Question 56

Flecainide Cautions and Contraindications (2,2)

Answer 56

Cautions:
1. 1st or 2nd degree
heart block
2. Renal disease

Contraindications:

1. Congestive heart failure
2. Post-myocardial infarction

Question 57

Flecainide Clinical Pearls (4)

Answer 57

1. Drug of choice for non-heart disease patients
2. Titrate dose by lowest effective dose not more often than once every week
3. Unique place in therapy – Used in neonates
4. Decrease dose by 50% in impaired renal function
   - Severely impaired renal function may require larger dose decreases

Question 58

Propafenone Mechanism of Action (3)

Answer 58

1. Classification: Class Ic antiarrhythmic
2. Blocks sodium channels to prolong refractory periods and increases electrical thresholds
3. Exhibits some beta-blockade activity

Question 59

Propafenone ADEs (7)

Answer 59

1. Decreased HR
2. QTc prolongation
3. Bronchospasms
4. Worsening heart failure, edema
5. Arrhythmias
6. Impaired taste sensations
7. Dizziness

Question 60

Propafenone Cautions (4)

Answer 60

1. Severe bronchial asthma
2. Congestive heart failure
3. Liver disease
4. Elevated ANA titers

Question 61

Propafenone monitoring (7)

Answer 61

1. BP
2. HR
3. EKG
4. LFTs
5. CBC
6. Lupus panel
7. Adverse effects

Question 62

Propafenone Clinical Pearls (3)

Answer 62

1. Titrate not more often than every 4-5 days
2. Reduce dose by 25-50% in patients with:
   – Liver disease
   – QRS widening
   – Heart block
3. Immediate release recommended for acute control, sustained release recommended for chronic control

Question 63

Amiodarone (4)

Answer 63

1. Fits in ALL Vaughan Williams Classifications
2. Has Most Class III effects

3. Place in therapy:
– Multiple arrhythmias
– Also helpful in retrograde eletrical disorders (i.e. WPW sundrome)
– Angina (due to vasodilatory effects)
– HF

Question 64

Amiodarone Mechanism of Action

Answer 64

Main effect works at the potassium channels to increase

the action potential (Class III)

Question 65

Amiodarone ADEs (14)

Answer 65

1. Decreased BP and HR; QTc prolongation; AV block
2. N/V
3. decreased appetite
4. constipation
5. Phlebitis
6. Optic neuropathy/neuritis (visual disturbances)
7. Dizziness
8. peripheral neuropathy
9. coordination
   disorders
10. Hepatitis
11. Hypo/hyperthyroidism
12. Blue-gray skin discolorations
13. photosensitivity
14. Pulmonary fibrosis (rare)

Question 66

Amiodarone Cautions (5)

Answer 66

1. Iodine allergies
2. 2nd or 3rd degree heart block
3. Hepatic disease
4. Drug interactions
5. QTc prolongation

Question 67

Amiodarone Monitoring (6)

Answer 67

1. Vitals (BP and HR)
2. EKG
3. Pulmonary testing
4. Thyroid testing
5. Ophthalmic testing
6. Adverse effects

Question 68

Amiodarone Pearls (

Answer 68

1. Intravenous route preferred in symptomatic patients
   – Quicker onset of action in correlation with long half-life
2. Safe and effective in patients with AFib and heart failure
3. The FDA REQUIRES that patients receive a drug information patient education leaflet

Question 69

QT Interval (3)

Answer 69

1. Duration from early ventricular depolarization to latest repolarization
2. QTc = corrected QT interval accounting for heart rate
   * Correction to take into account for HR
If greater than 450-470 be concerned 
Greater than 500 = definite prolongation; particularly concerning for medications
3. Standard values
   – Normal: < 430 (men) & < 450 (women)
   – Borderline: > 450 (men); > 470 (women)
   – Prolonged: > 450 (men) & > 470 (women)

Question 70

QTc Calculation

Answer 70

QTc= corrected QT interval

QTc = (QT Interval) / (RR interval in seconds)

*QT interval is from beginning of QRS complex (Q) to end of T wave; entire ventricular depolarization
and repolarization phase 
the longer it goes, the longer the ventricle is in limbo; higher risk for inducing a cardiac arrythmia

Question 71

Torsades De Pointes (3)

Answer 71

1. Life threatening; a specific form of polymorphic VT in patients with A PROLONGED QT INTERVAL. It is characterized by rapid, irregular QRS complexes, which appear to be twisting around the ECG baseline. This arrhythmia may cease spontaneously or degenerate into ventricular fibrillation.
2. Requires cardioversion

3. Use Class III anti-arrhythymic drugs
– Ondansetron (Zofran), Granisetron (Kytril)
– Methadone
– Fluoroquinolones
– Haloperidol

*Prolonged QT that turns into torsades de pointes is life threatening and requires cardioversion

Question 72

Prolonged QT Interval (3)

Answer 72

1. Congenital or Acquired
2. Risk factors for prolonged QT:
   – Multiple prolonging agents OR high doses of 1x agent; higher dose of any agent that prolonges QT can induce porsades
   – HypoK, hypoCa, HypoNa
3. So anything that can affect electrolyte balance can potentiate the risk (ie diuretics)
   - Lasix + QT prolonging agent + dehydration = higher risk of porsades
   – Female
   – Congenital prolonged QT