Lecture 12: Anti-arrhythmic drugs

Question 1

What are the objectives of anti-arrhythmic drugs?

Answer 1

• Reduce morbidity
• Reduce mortality
• Ventricular arrhythmias lead to 70k deaths/year in the UK

Question 2

What are the phases of a cardiac cation potential in ventricular myocytes?

Answer 2

• Phase 0: rapid depolarisation, Na+ channels open, rapid influx into myocytes
• Phase 1: short depolarisation, K+ channels open, K+ efflux
• Phase 2: delay in repolarisation (Ca2+ entry via L-type channels) → small plateau
• Phase 3: rapid repolarisation, K+ channels open → K+ efflux → brings membrane potential back down
• Phase 4: automatically slow depolarisation → relatively flat as not peacemaker cells

Question 3

What are the phases of a cardiac action potential in SA nodes?

Answer 3

• Phase 4: slow depolarisation → causes pacemaker activity → mediated by if channels
• Phase 0: rapid influx of Ca via L type Ca channels
• Phase 3: repolarisation in channels → back to baseline

Question 4

What is the refractory period?

Answer 4

• Play crucial role in regulation of electrical impulses in heart, preventing arrhythmias
• Absolute refractory period → when there is an AP being fired, myocytes unresponsive to electrical stimulation
  → voltage-gated sodium channels inactivated
• Relative refractory period (vulnerable period) → followed ARP, could get an extra AP, could drive arrhythmias
• Supranormal period → excitable due to which channels are open - high chance of an extra beat

Question 5

What are afterdepolarisations?

Answer 5

• Extra depolarisations - not a full AP
• Early → during repolarisation
• Delayed → following complete repolarisation
• If they get big enough can cause arrhythmias
• Can occur if you don’t have enough K+ - cells → hyper excitable

Question 6

What are the major modes of action to block arrhythmias?

Answer 6

• Decrease phase 4 slope → slow rate
• Increase threshold potential → slow phase 0
• Increase refractory period → lengthen AP
• Aim: to prevent re-entrant circuits (loops)

Question 7

What is the Vaughan-Williams classification of anti-arrhythmic drugs?

Answer 7

• Class I: sodium channel blockade
• Class II: catecholamine blockade
• Class III: lengthening of refractoriness
• Class IV: calcium channel blockade

Question 8

What do sodium channel (class I) blockade anti-arrhythmic drugs do?

Answer 8

• Restrict rapid inflow of Na+ during phase 0
• Slows depolarization n conduction esp in damaged tissue
• Can also block K+ channels

Question 9

Explain the 3 subtypes of sodium channel (class I) blockade anti-arrhythmic drugs

Answer 9

• Sodium channel block w lengthened refractoriness
  
  • EFFECT: makes AP longer → slows repolarization
  • Blocks K+ channels
  • EXAMPLE: quinidine, disopyramide n procainamide
• Sodium channel block with reduced refractoriness
  
  • Doesn’t change rising phase
  • Stop premature beats by holding channel inactivated → block voltage gated Na+ channels→ local anaesthetics like lidocaine, supresses premature beats
  • Binds and unbinds quickly
• Sodium channel block with little effect on refractory period
  
  • Slows rising phase, slows QRS
  • Bind and unbinds slowly, general reduction in excitability, suppress re-rentrant rhythms
  • EXAMPLE: flecainide

Question 10

What do beta-andrenoceptor antagonist (class II) anti-arrhythmia drugs do?

Answer 10

• Used for ventricular dysrhythmias following MI often [the drug increases sympathetic activation]
• EFFECTS
  
  • Inhibits the effects of catecholamines like epinephrine and noradrenaline
  • Reduce delayed afterdpolarisations due to symptoms activity
  • Some ectopic pacemakers depend on adrenergic drive (useful for ectopic beats)
  • Increases refractory period of AV node → prevent re-entrant tachycardia
    
    • Useful if tachyarrhythmias are driven by overactive sympathetic system
  • Membrane stabilising activity → less excitable

Question 11

What do class III anti-arrhythmia drugs do?

Answer 11

• Long elimination half life (10-100 days) thus given as loading dose
• Block K+ channels (Phase 3) → lengthen refractory period
  
  • e.g. amiodarone - prolongs cardiac action potential
    → useful in re-entrant tachycardias, suppress ectopic activity
• ECG
  
  • Prolongs QT, widens QRS
• Sotalol → non-selective beta-adrenoceptor blocker, prolongs cardiac AP
  → delays slow outward K+ current
  → not as effective as amiodarone but less adverse effects
• SIDE EFFECTS
  
  • Photosensitive rash, thyroid abnormalities, pulmonary fibrosis

Question 12

How can class III anti-arrhythmia drugs be pro-arrhythmic?

Answer 12

• Can produce polymorphic ventricular tachycardia
• Dangerous when
  
  • Taken w other drugs that lengthen the QT interval (e.g. antipsychotic drugs)
  • Disturbed electrolyte balance (hypokalaemia)
  • Hereditary prolonged QT
• Occurs if amiodarone taken w other specific drugs

Question 13

What are class IV anti-arrhythmia drugs?

Answer 13

• Ca2+ channel antagonists → block L-type Ca2+ channels in the heart
• Half-life 6-8 hours
• Considerable first pass metabolism
• Slow release preparation available
• EXAMPLE: verapamil
  
  • Slow conduction in SA and AV nodes - as AP is carried by Ca2+ ions
  • Slow the heart and terminate supra ventricular tachycardia (partial AV block)
  • Shorten plateau of AP (phases 1 and 2) - less Ca2+ influx
  • Reduce force of contraction
  • Reduce after depolarisations
  • Suppress ectopic beats
• ECG
  
  • PR interval prolonged → slows conduction through AV node

Question 14

What does adenosine do?

Answer 14

• Receptors for adenosine in the heart at AV node → opens K+ channels → hyperpolarises AV node → slows conduction of beat → negative dromotropic effect
• Endogenous chemical mediator in the body (vasodilator)
• Acts via A1 receptors on AV node (hyper polarises cardiac tissue)
• Slows the rate of rise of pacemaker potential
• Slows conduction through AV node (negative dromotropic)
• Terminates paroxysmal supraventricular tachycardias
• Given as IV bolus (half life 8-10 seconds) - broken down very quickly

Question 15

What do digoxin and other cardiac glycosides do?

Answer 15

• Act directly in the heart → inhibit Na+/K+ ATPase pump
  → reduction in Na+ and Ca2+ exchange → less Na+ extrusion, reduces Ca2+ extrusion
• Increase in intracellular [Ca2+] increases excitability/contractility
• Decreases propagation and AP generation at SA and AV nodes
• Useful as slows conduction through AV node
• Enhances vagal activity by complex - indirect action bradycardia
• Useful in: atrial fibrillation, atrial flutter, heart failure

Question 16

What are the characteristics of digoxin?

Answer 16

• Eliminated 85% unchanged by the kidneys → renal failure digoxin accumulates
• Half life is 36horus - persists in body
• Given orally
• Low therapeutic index → small difference between therapeutic and toxic amount
• Treatment of overdose
  
  • Use FAB fragment of antibody (Digibind), collates digoxin,
  • No FC segment - no immune response

Question 17

What is electroconversion?

Answer 17

• Electric shock to reset rhythm of the heart → depolarises all heart muscle
• Direct current electric shock applied externally
• Successful shock: heart depolarised, ectopic focus extinguished, SA node resume dominant pacemaker
• Effects are immediate
• Supra/ventricular tachycardia, ventricular fibrillation, atrial fibrillation/flutter

Question 18

What drugs are used to help atrial fibrillation?

Answer 18

• Class II agents: β-blockers can help control ventricular rate via SA node
• Class IV agents: Ca2+ antagonists (e.g. Verapamil) slows conduction thru AV node

Question 19

What is used to help atrial flutter?

Answer 19

• Digoxin
• D.C. shock
• Class III agents: amiodarone/sotalol for maintenance
• Anticoagulants: if long standing condition to avoid emobli

Question 20

What is used to help ventricular tachycardia?

Answer 20

• Electrical conversion
• If patient is in good health
  
  • IV lidocaine (class I agent)
  • Failing that IV amiodarone
• Recurrent episodes
  
  • Amiodarone or sotalol

Question 22

What is the Maze procedure?

Answer 22

• Treatment of atrial fibrillation when drugs do not control the condition
• Create incisions in the atrium → disrupt re-entrant circuits
• Once incisions are made → sew together again
• Atrium can hold blood but electrical impulse can’t cross incisions
• RESULT: one path that electrical impulse takes from SA to AV node
• Atrium can no longer fibrillate n sinus rhythm is restored

Question 23

What is catheter ablation?

Answer 23

• Apply radiofrequency (RF) /electrical energy or freezing offending area (usually via catheter)
• Creates small scar that is electrically inactive → incapable of generating heart arrhythmias