BMS 204 Pharmacology: Drug Therapy of Dysrhythmia (Fall 2024) PDF

Summary

These lecture notes cover drug therapy of dysrhythmias. The document details the different types of heart rhythm disorders, along with risk factors and treatment strategies. It also includes a classification, adverse effects, and various drugs used in treatment.

Full Transcript

BMS 204
Pharmacology

Drug Therapy of Dyrrhythmia
Ahmed Nour Eldin Hassan
Professor of Clinical Pharmacology
Faculty of Medicine
Fall 2024
By the end of this lecture, you should be able to:
Classify antiarrhythmic drugs according to their electrophysiological effects.
Discuss the choices of different antiarrhythmic drugs in various types of
arrhythmias.
Discuss the different lines of treatment of atrial fibrillation
Explain why digoxin can be used in treatment of atrial fibrillation
Explain why lidocaine is used only in ventricular arrythmia
List the adverse effects of common antiarrhythmic drugs
 Dysrrhythmia
Definition: Abnormalities in heart rhythm and in severe case can impair
pumping ability of heart
Risk Factors:
1- Coronary Artery Diseases (CAD)
2- Myocardial Infarction (MI)
3- Hypoxia
4- Electrolyte imbalance: potassium
5-Drugs induced: theophylline, tricyclic antidepressants, overdose of
antiarrhythmic drugs
Bradyarrhythmia: < 60 beats/minute: Treatment: Conservative OR
1. Sinus bradycardia 1. Atropine
2-AV Block: with variable degrees 2. Cardiac pacing

Normal Heart rate: 60-90 Regular
Tachyarrhythmia:
1. Extra beat: atrial or ventricular
2. Supraventricular: Paroxysmal supraventricular tachycardia (PSVT), Atrial
Flutter and Atrial Fibrillation (AF)
3. Ventricular: tachycardia/Fibrillation & Prolonged Q-T
4. Accessory bundle
 Anti-arrhythmic Drugs: Vaughan Williams classification (1970)

Class I: Na+-channel blockers.
Class Ia: Procainamide, quinidine & disopyramide
Class Ib: Lidocaine (I.V.), phenytoin, mexiletine, tocainide,
Class Ic: Propafenone, flecainide, encainide
Class II: β-blockers.
Class III: K+-channel blockers: Amiodarone, sotalol, ibutilide, Dronedarone.
Class IV: Ca++ Channel Blockers (CCB): Verapamil &Diltiazem
Others (Non-classified): Adenosine, digoxin and Ivabradine.
 MODERNIZED SCHEME BASED ON THE
VAUGHAN WILLIAMS APPROACH (2018)
(Nice To Know)

https://www.ahajournals.org/doi/pdf/10.1161/CIRCULATIONAHA.
118.035455
Action Potential in Calcium-dependent Cells
SAN and AVN

K +

β1

If funny current
 Action Potential in Accessory Bundles, Abnormal Focus
and Cardiac Muscles

Na + Influx
*Rate of Maximum
Depolarization (Ѷ Max)
or Conduction Velocity K +
*Depends on number of β1
Na+ channels available Na+

APD and ERP
Correlation between action potential and ECG
AVN Ventricle

PR Interval QRS Interval
----------QT Interval------------
 Class I: Electrophysiology:
1. Na+ channel Blockade (fast fibers):  rate of maximum depolarization (Phase 0)
 Vmax & delay conduction.
 Slope of Phase 4 →↓automaticity genetrating electric current on their own

Class Ia Class Ib Class Ic
Procainamide Lidocaine Propafenone
Effect on Conduction Moderate Minimal Marked

2- Effect on K+ Channels and ERP/ ~APD
Block K+ channel → No effect on K+ But
AVN Block beta receptor
 APD/ERP → APD /ERP
Fast Fibers in Block K+ channel →  K+efflux → No effect on K+
Ventricles  APD/ERP  APD>↓ ERP → ~ APD /ERP
 Class Ia Agents:
Electrophysiology:
Other Cardiovascular Effects:
Effect Adverse Effects and Clinical implication
Antimuscarinic: Paradoxical ↑ AVN conduction →ventricular
tachycardia in AF.
Autonomic

(blocked by adding digoxin, β Bs or verapamil before)
Effects:

(Verapamil and β Bs (C.I. with Heart Failure)

Prolonged Q-T: "Torsade de Pointes" arrhythmia (↑ QT) →
Procainamide Procainamide >Amiodarone
Rational Professional
Prescription

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