1 / 41

Drugs used to treat cardiac arrhythmias

Drugs used to treat cardiac arrhythmias. Definition : a variation in either the site or rate of cardiac impulse formation, and/or a variation in the sequence of cardiac impulse propagation. Na +. K +. outside. R. -90 mV. Ligand-gated. Voltage-gated. Passive. inside. K +. Na +.

dexter-mcknight
Download Presentation

Drugs used to treat cardiac arrhythmias

An Image/Link below is provided (as is) to download presentation Download Policy: Content on the Website is provided to you AS IS for your information and personal use and may not be sold / licensed / shared on other websites without getting consent from its author. Content is provided to you AS IS for your information and personal use only. Download presentation by click this link. While downloading, if for some reason you are not able to download a presentation, the publisher may have deleted the file from their server. During download, if you can't get a presentation, the file might be deleted by the publisher.

E N D

Presentation Transcript

  1. Drugs used to treat cardiac arrhythmias

  2. Definition: a variation in either the site or rate of cardiac impulse formation, and/or a variation in the sequence of cardiac impulse propagation.

  3. Na+ K+ outside R -90 mV Ligand-gated Voltage-gated Passive inside K+ Na+

  4. The fast cardiac action potential Ca 2+ Ca 2+ 1 +55 mV 2 K + 3 K + Na + Na+ 0 4 4 K+ -90 mV Na/K ATPase

  5. Effect of local anesthetics on the fast cardiac action potential Refractory Period Na + Longer RP due to slower recovery from inactivation Slope phase 0 = conduction velocity Increased threshold

  6. Effect of drugs that block K channels 1 Refractory Period 2 K + 3 K + 0 4 4 Increase action potential duration (APD)

  7. Slow cardiac action potential Ca2+ 2 Ca2+ K+ 3 0 If 4 4 Na, K

  8. Effect of Ca 2+ channel blockers Refractory Period 2 Ca2+ 3 0 4 4 Slope of phase 0 = Conduction velocity

  9. Drugs affecting automaticity 2 3 0 4 4 β agonist Muscarinic agonists, Adenosine

  10. Causes of Arrhythmia Automoticity -ectopic pacemakers

  11. Ways to decrease automoticity β(-), Ca++(-), Na+(-), Ca++(-) Ach, adenosine K+(-)

  12. 2 . After depolarizations Delayed Early

  13. 3. re-entry

  14. ClassActionDrugs I A. Moderate phase 0 Quinidine, procainamide I B. No change in phase 0 Lidocaine I C. Marked phase 0 Flecainide II Beta-adrenergic blockers Propranolol, esmolol III Prolong repolarization Amiodarone, Sotolol Dofetalide, ibutilide IV Calcium channel blockers Verapamil, diltiazem

  15. Class 1: Local anesthetics

  16. Sodium Channels Resting (Closed) Active (Open) Inactive m m m h h h I A R R

  17. Local anesthetics bind to and release from the Na+ channel at different rates Phasic/frequency dependent tonic

  18. Class 1A agents: Procainamide, quinidine, disopyramide Absorption and elimination (oral or iv) Effects on cardiac activity Intermediate binding offset kinetics  conduction (phase 0 of the action potential (Na+))  refractory period ( APD (K+) and  Na inactivation)  automoticity ( slope of phase 4, fast potentials)  increase threshold (Na+) Quinidine has anticholinergic (atropine like action) to speed AV conduction used with digitalis, β blocker or Ca channel blocker Quinidine is also an alpha receptor antagonist Effects on ECG QRS,  PR, QT

  19. Class 1A (cont.) Uses Wide spectrum: Quinidine : maintain sinus rhythms in atrial fibrillation and flutter and to prevent recurrent tachycardia and fibrillation      Procainamide: acute treatment of supraventricular and ventricular arrhythmias   Side effects Hypotension, reduced cardiac output Proarrhythmia (generation of a new arrhythmia) eg. Torsades de Points (QT interval)               Dizziness, confusion, insomnia, seizure (high dose)               Gastrointestinal effects (common)               Lupus-like syndrome (esp. procainamide)

  20. Examples of cardiac arrhythmias

  21. Class 1B agents: Lidocaine, mexiletine, phenytoin Absorption and elimination Lidocaine: iv only             Tocainide and mexiletine: oral Effects on cardiac activity Fast binding offset kinetics No change in phase 0 in normal tissue (no tonic block)  APD slightly decreased (normal tissue)  increase threshold (Na+)  phase 0 conduction in fast beating or ischemic tissue, Effects on ECG None in normal, in fast beating or ischemic  QRS

  22. Class 1B (cont.) Uses acute : Ventricular tachycardia and fibrillation (esp. during ischemia) Not used in atrial arrhythmias or AV junctional arrhythmias Side effects                 Less proarrhythmic than Class 1A (less QT effect)               CNS effects: dizziness, drowsiness

  23. Class 1C agents: Flecainide and propafenone Absorption and elimination oral or iv                  Effects on cardiac activity very slow binding offset kinetics (>10 s)  Substantially   phase 0 (Na+) in normal  automoticity ( threshold)  APD (K+) and  refractory period, esp in rapidly depolarizing atrial tissue. Effects on ECG  PR, QRS, QT

  24. Class 1C (cont.) Uses Wide spectrum Used for supraventricular arrhythmias (fibrillation and flutter)               Premature ventricular contractions (caused problems) Wolff-Parkenson-White syndrome Side effects Proarrhythmia and sudden death especially with chronic use (CAST study) increase ventricular response to supraventricular arrhythmias CNS and gastrointestinal effects like other local anesthetics

  25. Cardiac Arrhythmia Suppression Trial (CAST)

  26. Class II agents: propranolol, acebutolol and esmolol Absorption and elimination Propranolol: oral, iv Esmolol: iv only (very short acting T½, 9 min) Cardiac effects  APD and refractory period in AV node to slow AV conduction velocity  decrease phase 4 depolarization (catecholamine dependent) Effects on ECG  PR,  HR

  27. Class II (cont.) Uses treating sinus and catecholamine dependent tachy arrhythmias converting reentrant arrhythmias in AV protecting the ventricles from high atrial rates (slow AV conduction) Side effects        bronchospasm              hypotension               don’t use in partial AV block or ventricular failure

  28. Class III agents: amiodarone, sotalol, ibutilide, dofetilide Amiodarone Absorption and elimination oral or iv (T 1/2 about 3 months) Cardiac effects  increase refractory period and  APD (K+)  phase 0 and conduction (Na+)  threshold  phase 4 (β block and Ca++ block)  speed of AV conduction Effects on ECG  PR, QRS,  QT,  HR

  29. Class III (cont.) Amiodarone (cont.) Uses Very wide spectrum: effective for most arrhythmias Side effects: many serious that increase with time Pulmonary fibrosis Hepatic injury Increase LDL cholesterol Thyroid disease Photosensitivity May need to reduce the dose of digoxin and class 1 antiarrhythmics

  30. Class III (cont.) Sotolol Absorption oral Cardiac effects  APD and refractory period in atrial and ventricular tissue Slow phase 4 (β blocker) Slow AV conduction ECG effects  QT,  HR Uses   Wide spectrum: supraventricular and ventricular tachycardia Side effects    Proarrhythmia, fatigue, insomnia

  31. Class III (cont.) Ibutilide Absorption rapid iv infusion Cardiac effects pure Ikr channel blocker also activates inward Na+ current net result in  APD ECG effects QT Uses conversion of atrial fibrillation and flutter Side effects Torsades de pointes

  32. Class III (cont.) Dofetilide Absorption oral Cardiac effects pure Ikr channel blocker  APD and refractory period ECG effects  QT Uses maintain sinus rhythm in pts with atrial fibrillation Side effects restricted use Torsades de pointes

  33. Class IV agents: verapamil and diltiazem Administration verapamil: oral or i.v. diltiazem: oral Cardiac effects slow conduction through AV (Ca++)  refractory period in AV node  slope of phase 4 in SA to slow HR Effects on ECG  PR,  HR (depending of blood pressure response and baroreflex)

  34. Class IV (cont.) Uses control ventricles during supraventricular tachycardia convert supraventricular tachycardia (re-entry around AV) Side effects Caution when partial AV block is present. Can get asystole if β blocker is on board Caution when hypotension, decreased CO or sick sinus Some gastrointestinal problems

  35. Additional antiarrhythmic agents Adenosine Adminsitration rapid i.v. bolus, very short T1/2 (seconds) Mechanism natural nucleoside that binds A1 receptors and activates K+ currents in AV and SA node –  APD, hyperplarization → HR  Ca++ currents -  refractory period in AV node Cardiac effects Slows AV conduction Uses convert re-entrant supraventricular arrhythmias hypotension during surgery, diagnosis of CAD

  36. Digioxin (cardiac glycosides) Mechanism enhances vagal activity ( K+ currents,  Ca++ currents,  refractory period slows AV conduction and slows HR Uses treatment of atrial fibrillation and flutter Atropine Mechanism selective muscarinic antagonist Cardiac effects block vagal activity to speed AV conduction and increase HR Uses treat vagal bradycardia Magnesium treatment for tachycardia resulting from long QT

  37. DC Cardioversion (electric shock) Treatment of choice for unstable, life-threatening cardiac arrhyghmias.

  38. Ablation therapy

  39. Mechanical devices Implantable defibrillator: for sudden death has been shown to be more effective than pharmacological therapy for increasing longevity

More Related