16.3 Dysrhythmia for dentists

Question 1

What is a dysrhythmia?

Answer 1

An abnormality in the rate, rhythm, conduction or site of origin of the cardiac action potential.

A dysrhythmia can involve more than one of these e.g. 3rd degree heart block causes an abnormality of the heart rate, rhythm, conduction and site of origin.

Question 2

Describe the polarity of cardaic mycoytes.

Answer 2

-Cardiac tissue is excitable tissue
- Cells can alter their polarity from -80/-90mV to+30mV
- Changes in voltage are mediated by voltage-gated ion channels

Question 3

Explain the phases of cardiac action potential.

Answer 3

Phase 0 = initiation of cardiac AP, voltage gated Na channels open, sodium influx causes rapid depolarisation

Phase 1 = Na channels close, voltage gated K channels open, efflux of potassium ions, rapid repolarisation

Phase 2 = voltage gated Ca channels open and Ca influx into cells, slows the rate of repolarisation

Phase 3 = excess potassium release, calcium channels close, rapid repolarisation

Phase 4 = return to resting potential

Question 4

Describe the electrophysiology of the heart.

Answer 4

• Myocardium has its own intrinsic myogenic acitvity
• Sinoatrial node is where the primary pacemaker cells of the heart are found
• SA node causes atria to depolarise (right then left)
• The intrinsic rate of the SA node is approx. 70bpm
• Wave of excitation spreads across the atria causing them to contract, and reaches the AV node
• Atrioventricular node beats approx. 50bpm
• AV node contraction travels through the Bundle of His (typically beats at 40bpm) and into the Purkinje fibres (can beat at 30-40bpm )which causes the ventricles to contract

Question 5

What does an ECG measure?

Answer 5

ECG measures resultant changes in electric potential over time (dmV/dt) at the skin surface.

• A positive voltage (AP) moving towards the electrode = upstroke on ECG trace
• An ECG shows the pattern of a resultant net effect of all the different action potentials recorded in that lead, e.g. 100mV travelling towards electrode, and 30mV moving away = overall change by 70mV

Question 6

How is an ECG recorded?

Answer 6

• Electrodes are placed on the chest and limbs
• An ECG lead is a graphical representation of the heart’s electrical activity which is calculated by analysing data from several ECG electrodes
• Different leads provide different views of the heart

Question 7

Describe the ECG wave form.

Answer 7

• P wave: atrial depolarisation in response to SA node triggering (atria contract)
• PR interval: delay of AV node to allow filling of ventricles
• QRS complex: ventricular depolarisation (ventricles contract) shape of wave depends on where the dominant block of muscle is relating to the positive lead of the ECG
• ST segment: should be flat, beginning of ventricle repolarisation
• T wave: ventricular repolarisation

Question 8

What is sinus rhythm?

Answer 8

Normal/healthy rhythm of the heart.
Each P wave is followed by a QRS complex, and each PR interval is 120-200ms.

Question 9

What are the clinical features of dysrhythmias/arrythmias?

Answer 9

• Palpitations
• Dyspnoea (breathlessness)
• Angina, caused by excessive workload for tachydysrhythmias, or by a relatively reduced perfusion of the coronary arteries for bradycardic individuals
• Syncope, fainting episode
• Sudden adult death

Question 10

How are dysrhythmias classified?

Answer 10

By rate:
- Greater than 100bpm = tachydysrhythmia
- Less than 50bpm = bradydysrhythmia

By rhythm:
- Ectopic: abnormal site of pacemaker activity
- Atrial fibrillation
- Atrial flutter
- Asytole/ventricular fibrillation = flatline, death

Question 11

How are tachydysrhythmias classified?

Answer 11

Classified accoridng to QRS complex width:
- Narrow complex tachycardia = 3 small squares or less (<120ms). Could be sinus tachycardia, atrial tachycardia, atrial fibrillation, atrial flutter
- Broad complex tachycardia = wider than 3 small squares (>120ms)

Question 12

Name the aetiologies of arrhythmias.

Answer 12

• Conduction system abnormalities: conduction system block, accessory pathways
• Abnormal pacemaker activity: electrophysiology abnormalities

Question 13

What is a conduction system block?

Answer 13

Issue with the conduction of the heart causing an arrhythmia.
- Can be congenital
- Can be due to cariac myopathies
- Valvular heart disease: stretches and damages conduction system
- Myocardial fibrosis

Question 14

What are accessory pathways?

Answer 14

• People can be born with abnormal or excessive accessory pathways which cause excessive short circuits in the conduction system
• E.g. Wolf-Parkinson-White syndrome, bundle of Kent, micro short-circuits

Question 15

What are electrophysiological abnormalities?

Answer 15

Conditions where the cardiac myocytes depolarise at the wrong time of the cardiac cycle, variety of causes:
- Electrolyte disturbances e.g. sodium, potassium, calcium, magnesium
- Ion channel abnormalities
- Acid/base disturbances
- Endocrine conditions e.g. thyroid disorders

Question 16

What system is used to classify anti-arryhthmic drugs?

Answer 16

Vaughan Williams Classification
- Class I
- Class II
- Class III
- Class IV

Question 17

What are class I drugs?

Answer 17

• Act on phase 0 of the cardiac cycle
• Block voltage gated sodium channels
• Use-dependent drug, meaning it is more likely to act on a channel in an active state (open) than an inactive channel

Question 18

How are class I drugs sub-classified?

Answer 18

• Type 1a: drugs dissociate at an intermediate rate, historic
• Type 1b: fast dissociation, used to treatment ventricular tachycardias and ventricular fibrillation e.g. Lidocaine binds to voltage gated sodium channels, risk of causing dysrhythmia
• Type1c: slow dissociation, main drug used in practice. E.g. flecainide to treat atrial fibrillation and Wolf-Parkinson-White syndrome

Question 18

What are class II drugs?

Answer 18

• Beta blockers
• Act on phases 2 and 4
• Mainly used to reduce tachydysrhythmias
• E.g. propanolol, bisoprolol, atenolol
• Side effects: bronchospasm, peripheral vasoconstriction, erectile dysfunciton

Question 19

What are class III drugs?

Answer 19

• Potassium channel blockers
• Delay repolarisation
• Act on phase 3
• Amiodarone and Sotalol

Question 20

What are the side effects of potassium channel blockers/Amiodarone?

Answer 20

• Thyroid abnormalities
• Skin discolouration
• Pulmonary fibrosis
• Prolonged QT interval

Question 21

What is QT prolongation?

Answer 21

• QT interval is very long, poses a risk of a long repolarisation period
• Creates risk of developing polymorphic ventricular tachycardia

Question 22

Which 2 drugs pose a risk of QT prolongation?

Answer 22

• Amiodarone
• Sotalol

Both pose risk of dysrhythmia as a result

Question 23

What are class IV drugs?

Answer 23

• Calcium channel blockers
• Slow the heart and weaken the strength of the heart’s contraction
• Can exacerbate heart failure
• E.g. diltiazem and verapamil
• Adverse effects: gingival hypertrophy, flushing, constipation, perivenual oedema

Question 24

Provide examples of antidysrhythmic drugs outside of the Vaughan Williams classification system.

Answer 24

• Atropine
• Catecholamines: adrenaline, isoprenaline, noradrenaline
• Adenosine
• Calcium chloride
• Magnesium chloride
• Digoxin

Question 25

What is digoxin?

Answer 25

• A cardiac glycoside
• Strutu
• Derived from digitalis plant
• Used to treat atrial fibrillation and heart failure with atrial fibrillation

Question 26

What is a chronotrope?

Answer 26

• Positive chronotropes increase heart rate
• Negative chronotropes decrease heart rate

Question 27

Explain the positive chronotropic action of digoxin.

Answer 27

• Inhibits sodium/potassium ATPase pump of cardiac myocytes
• Increases intracellular sodium
• Increased intracellular calcium

Increases strength of contraction of the heart

Question 28

Explain the negative chronotropic action of digoxin.

Answer 28

• Increases vagus nerve stimulation
• Increases atrioventricular node block

Decreases heart rate

Question 29

What are the side effects of digoxin?

Answer 29

• Nausea and vomiting
• Yellow tinged vision
• Dysrhythmia: usually bradydysrhythmia, ventricular dysrhythmia, AV block