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Antiarrhythmic Drugs Types of Cardiac Arrhythmias:
Abnormalities of Impulse Formation: Rate disturbances. Ectopic activity. Abnormalities of Impulse Conduction: Heart Block Reentry.
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Causes of Cardiac Arrhythmias
Cardiac Causes: Ischemic heart disease. Inflammation. Trauma e.g. heart surgery. Congestive heart failure. Hypotension.
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Non Cardiac Causes: Electrolyte imbalance. Acid-Base imbalance.
Hypoxia. Drugs: Digitalis, Anesthetics, Tricyclic antidepressants Diuretics, Bronchodilators. G.I. and neural reflexes.
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Antiarrhythmic drugs have effects on different portions of the cardiac action potential
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Class 1: Sodium Blockers.
Class 2: Beta blockers. Class 3: Potassium Blockers. Class 4 : Calcium Blockers.
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Nonpharmacologic Therapy
Surgery. Radiofrequency Catheter Ablation. Implantable Cardioverter - Defibrillator (ICD).
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Class 1 Drugs Na Channel Blockers
Class 1A Drugs Quinidine: Prototype, Antimalarial. Cinchona tree Antipyretic. Inhibits Na+ channels. Also, inhibits and muscarinic receptors. Slows upstroke, conduction, and prolongs atrial action potential durations (APD) and QRS duration.
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Use restricted to patients with normal hearts but have atrial or ventricular arrhythmias.
Occasionally used in acute severe malaria. Side Effects: Nausea (18%), Diarrhea (33%). Headache, Dizziness, and tinnitus= Cinchonism Hypersensitivity, fever, rash, angioedema. Thrombocytopenia. Excessive prolongation of QT interval, slowed conduction and sudden death. Hypotension. Serum Digoxin levels. Warfarin effects.
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Class 1B Drugs Lidocaine: High affinity to bind with Na+ channels in ventricles. Acts selectively on ischemic tissue to promote conduction & block reentry. Not effective in atrial arrhythmias.
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Kinetics: Well absorbed, but ineffective orally, due to first pass effect. Well distributed, including the brain. Side Effects: Least cardiotoxic of the class, except for hypotension with high doses due to depression of the myocardium. CNS: parasthesia, tremor, nausea, slurred speech, and convulsions. Was routinely given to all MI patients to prevent ventricular arrhythmias Class 1C Drugs: Flecainide
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Propranolol: Class II Drugs beta blockers
Has effective antiarrhythmic activity well tolerated, and documented to reduce mortality after acute myocardial infarction by reducing arrhythmias. Decrease slope 4 repolarization. Prolong repolarization at AV node. Increase threshold potential. Effective in CA induced arrythmias
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Esmolol β1-selective. Short acting, used in intraoperative and acute arrhythmias. Given by IV infusion.
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Class III Drugs: K⁺ channel Blockers.
Amiodarone, Sotalol (β blocker & K ⁺ blocker) Amiodarone: Blocks K ⁺ channels and markedly prolongs APD. Class I actions( i.e. blocks Na+ channels). Blocks and Receptors. Ca++ blocking actions. Reserved for life-threatening atrial & ventricular arrhythmias. Only slows heart rate and AV conduction. Peripheral vasodilator (only with IV).
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Class IV Drugs: Calcium channel blockers. Verapamil Diltiazem
Effects more marked in tissues that fire frequently, & those dependant on Ca ⁺ ⁺ (SA node and AV node). Paroxysmal Supraventricular Tachycardia. Vasodilators & have negative inotropic effects. Can cause severe AV block in diseased hearts. Safe: Constipation, gastric discomfort, vertigo, headache, nervousness, pruritus.
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Adenosine: Miscellaneous Drugs Naturally occurring nucleoside.
Activates inward K ⁺ current & inhibits Ca ⁺ ⁺ current. Very short acting (t½ 10 seconds). depolarization in SA node. AV conduction. No effect on ventricles.
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causes a brief blockade of the AV nodal conduction pathway following intravenous administration.
Such a brief AV block can be used therapeutically for reliable termination of AV nodal re-entry tachycardia 90-95% effective in supraventricular tachycardia. Less effective in the presence of adenosine receptor blockers e.g. theophylline and caffeine. Can cause very short –lived flushing (20%), chest tightness, AV block, headache, hypotension, nausea, and paresthesia.
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