Cardiac Arrhythmia (Dysrhythmia)

Question 1

→ Definition of Cardiac Arrhythmia (Dysrhythmia)

Answer 1

Disturbance of normal cardiac rhythm

Question 2

Transmission of Cardiac Rhythm

Answer 2

From Sinoatrial node (SA node)
to Atrium
to Atrioventricular
node
(AV node)
to Purkinje fibre
to Ventricle

Question 3

Causes of Cardiac Arrhythmias

Answer 3

Ischaemia [shortage of blood supply]

Hypoxia [shortage of blood supply]
which ischemia and hypoxia lead to → Myocardial Infarction (damage/death of heart tissue)

Electrolyte Abnormalities e g hyperkalemia

Autonomic Influences

Drug Toxicity e g digoxin

Infection

Question 4

Therapeutic Goals of Antiarrhythmic Drugs

Answer 4

Termination of an Ongoing Arrhythmia
Prevention of an Arrhythmia

→ Acute Therapy: Intravenous administration

→ Chronic Therapy: Long term oral use

Question 5

Approaches of Anti

Arrhythmic Drugs

Answer 5

Alter Autonomic Function

Decreased Ectopic Pacemaker Activity

Decreased Impulse Conduction Rate

Increased Effective Refractory Period ( ERP)[the longest interval at which a premature stimulus
fails to generate a propagated response]

Question 6

Classification of Anti

Arrhythmic Drugs

Answer 6

Class I Drugs
-sodium channel blockers

Class II Drugs
- β adrenoceptor antagonists

Class III Drugs
- potassium channel blockers

Class IV Drugs
- calcium channel blockers

Question 7

Characteristics of Class I Anti

Arrhythmic Drugs Sodium Channel Blockers

Answer 7

•
Use Dependence
- binds preferentially to sodium channels which are in the open or inactivated state
→the more frequently the channels are activated, the greater is the degree of block

Question 8

Name and effect of Subtypes

of Class I Drugs

Answer 8

sodium channel blockers
→ decreased conduction velocity →block tachycardias

Class Ia ::(oldest group)
eg quinidine procainamide disopyramide

Class Ib rapid kinetics
-preferentially block premature beats
e g lidocaine mexiletine

Class Ic slow kinetics
-markedly decreased conduction
eg flecainide encainide propafenone

Question 9

Name Property and Adverse effect of Class Ib Drugs

Answer 9

e.g. lidocaine , mexiletine

Rapid Kinetics
- dissociate rapidly from sodium channels within the time frame of NORMAL heartbeat
→preferentially block premature beats

Selective for Refractory Channels
→preferentially suppress depolarized cells
(eg in ischaemia)

Adverse Effects
- central nervous system disturbances
(eg nausea, tremor, drowsiness, convulsions)

Question 10

Name Property and Adverse effect of Class Ic Drugs

Answer 10

flecainide , propafenone

Slow Kinetics
- dissociate slowly from sodium channels
→markedly decreases conduction even at normal heart rates

Adverse Effects
- pro-arrhythmia
→ increases the incidence of sudden death especially in presence of severe heart failure

Propafenone
- structural similarities to propranolol
→weak b adrenergic blocker activity (-ve inotropic)
→→worsen heart failure

Question 11

Name Property and Adverse effect of Class

Ia Drugs

Answer 11

e.g. quinidine , procainamide , disopyramide

Intermediate Rate of Dissociation from Sodium Channels
→ inhibit increased automaticity
→ moderately decreased conduction

Block Potassium Channels
→ decreased rate of repolarization of cardiac cells
→ increased duration of action potential
→ → increased effective refractory period (ERP)

Adverse Effects of Class
Ia Drugs
Pro-Arrhythmia

→ ectopic beats due to inhibition of potassium channels [→→ polymorphic ventricular

→tachycardia torsades de pointes arrhythmia)]→

Other Adverse Effects

• gastrointestinal disturbances e.g diarrhoea (or constipation), nausea and vomiting
• -less likely with disopyramide
• lupus-related symptoms e g arthralgia and arthritis
• -due to long term use of procainamide
• decreased force of contraction of heart
• disopyramide quinidine procainamide

Question 12

Effect, class, and Adverseeffect of Class II Anti
Arrhythmic Drugs
Adrenoceptor Antagonists

Answer 12

Oppose b Adrenergic Stimulation
→decreased heart rate
→ increased AV nodal conduction time
→ decreased intracellular calcium overload

Different Subclasses
selective b 1 adrenoceptor antagonists e g metoprolol esmolol [esmolol short half-life because rapidly metabolized by erythrocyte esterases
→intravenous administration primarily used for intraoperative and for acute arrhythmias]

non-selective β adrenoceptor antagonists e g propranolol
-antagonize both b-1 and b-2 adrenergic receptors

Adverse effect
Bronchospasm
→contraindicated in patients with asthma or other forms of obstructive airways
disease

Decreased Force and Rate of Contraction of Heart
→cautious in patients with heart failure

Hypoglycaemia
→contraindicated in patients with diabetes

Question 13

Name, effect of Class III Anti
arrhythmic Drugs
Potassium Channel Blockers

Answer 13

amiodarone, dofetilide ibutilide sotalol

Decrease Rate of Repolarization of Cardiac Cells
→increased action potential duration
→→ increased effective refractory period
→→→→decreased automaticity

Question 14

Characteristics and adverse effect of Dofetilide

Answer 14

Potent and “ Potassium Channel Blocker

Risk of Developing Ectopic Beats
[→ polymorphic ventricular tachycardia]
- due to increased action potential duration
- cautious with hypokalemia
- avoided in patients with advanced renal failure or with inhibitors of renal cation transport (e g cimetidine)

Question 15

Effect and Adverse effect Amiodarone

Answer 15

Highly Effective Anti Arrhythmic Drug

Additional Effects to Potassium Channel Blockade
-block inactivated sodium channels

-weak adrenergic blocking activity

-weak calcium channel blocking activity
→broad spectrum of actions

Low Incidence of Developing Ectopic Beats
[Ie low risk for polymorphic ventricular tachycardia]

Adverser effect

• Pulmonary Fibrosis
• Hypersensitivity hepatitis

-Photosensitivity
→skin rashes and grey blue -skin discoloration following sun exposure

-Corneal Deposits → visual problems

-Thyroid Abnormalities
→hypo or hyper thyroidism due to high iodine content

• Pro Arrhythmia (Bradycardia and Heart Block)
• Drug Interaction [metabolized by liver cytochrome P 450 enzymes]

Question 16

Effect and Adverse effect Dronedarone

Answer 16

-Same Mechanisms of Actions as Amiodarone
- possesses the properties of all 4 classes of antiarrhythmic drugs Vaughan Williams
classification)

Lower Incidence of Adverse Effects than Amiodarone
- BUT risk of liver toxicity
-“black box” warning against use in acute decompensated or advanced (class
IV) heart failure

Question 17

Effect and Adverse effect

Sotalol

Answer 17

Class III Anti Arrhythmic Drug with Class II Action

Racemic Mixture of d and l Sotalol
-only l isomer contains b adrenoceptor blocking activity

Adverse Effects
-pro arrhythmia
→risk of developing ectopic beats →polymorphic ventricular tachycardia]
-depression of left ventricular function
→caution in patients with heart failure

Question 18

name, effect and adverse effect of Class IV Anti
Arrhythmic Drugs
Calcium Channel Blockers

Answer 18

verapamil, diltiazem

Inhibit Voltage Operated L type Calcium Channels in Cardiac Cells
→ Decreased heart rate
→ Decreased AV nodal conduction velocity
→ Decreased intracellular calcium overload

Adverse Effects
- decreased force of contraction of heart

• atrioventricular block

-hypotension
→ lead to heart failure

Question 19

Name, effect, and adverse effect of Miscellaneous Anti
arrhythmic Drugs (I)

Answer 19

Adenosine

mechanisms of action
-activate presynaptic purinergic receptors on sympathetic nerve terminal
→decrease release of noradrenaline

activate A 1 receptors on SA and AV nodes
→inhibit activity of adenylyl cyclase (AC)
→→decreased cAMP production
→→→decreased calcium overload

• activate potassium channels in SA and AV Nodes
  →diastolic potential more hyperpolarized
  →→prolong the phase 4 depolarization
  →→→decreased conduction velocity

Adverse effects
- flushing, hypotension
[due
to activation of A 2 receptors in vascular smooth muscle cells
→increased cAMP production → vasodilatation]

-chest pain, shortness of breath [perhaps
related to bronchospasm]

Characteristics
-rapid uptake into cells for metabolism
→short half life in blood
→→short duration of action
→→→adverse effects rapidly resolved

Effects of adenosine
-potentiated by dipyridamole, which inhibit its uptake mechanism
-inhibited by theophylline and caffeine, which antagonize its binding to
receptors

Question 20

Name, effect, and adverse effect of Miscellaneous Anti
arrhythmic Drugs (II)

Answer 20

Magnesium

mechanisms of action

• affect ion channel activity
• normalize plasma magnesium level hypomagnesium plasma Mg <1.5 mg/dl arrhythmia]

Potassium
-normalize potassium pools in the body [hypokalemia plasma K <2.5 mg/dl arrhythmia]

Digoxin

mechanism of action
-parasympathomimetic effects
→decreased heart rate
→decreased conduction velocity (especially at AV node)
-adverse effects

-pro arrhythmia due to inhibition of sodium potassium ATPase
→ectopic beats

-gastrointestinal and central nervous system disturbances

Question 21

Name, effect, and adverse effect of Miscellaneous Anti
arrhythmic Drugs (III)

Answer 21

Atropine

Mechanism of action
- antagonize muscarinic receptors
→reduce vagal influence
→→ increased heart rate

→→increased conduction velocity (especially at AV node)
→→→For management of bradycardia

Adverse effects
-tachycardia, dry mouth, dilation of pupils, constipation
[mainly with overdose or repeated dosing]

Question 22

Considerations with Anti

Arrhythmic Drugs

Answer 22

Causes of Arrhythmia
- elimination of “ causes
eg ischemia, acute cardiac dilation, drug toxicity

-appropriate therapy (pharmacological vs non -pharmacological)

Route of Administration
- intravenous preparations preferred for emergency

Therapy Regimen
- combination therapy→ prevent adverse effects

Justification

• decreased symptoms e g palpitations, syncope or cardiac arrest
• decreased long term mortality in asymptomatic patients