Antiarrhythmic agent: Difference between revisions

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Many attempts have been made to classify antiarrhythmic agents.  The problem arises from the fact that many of the antiarrhythmic agents have multiple modes of action, making any classification imprecise.
Many attempts have been made to classify antiarrhythmic agents.  The problem arises from the fact that many of the antiarrhythmic agents have multiple modes of action, making any classification imprecise.


==Vaughan Williams antiarrhythmic classification==
==Vaughan Williams Antiarrhythmic Classification==


The Vaughan Williams classification, introduced in 1970,<ref>Vaughan Williams EM. "Classification of anti-arrhythmic drugs." In: ''Symposium on Cardiac Arrhythmias'', Sandfte E, Flensted-Jensen E, Olesen KH eds. Sweden, AB ASTRA, Södertälje, 1970;449-472.</ref> is one of the most widely used classification schemes for antiarrhythmic agents. This scheme classifies a drug based on the primary mechanism of its antiarrhythmic effect. However, its dependence on primary mechanism is one of the limitations of the VW classification, since many antiarrhythmic agents have multiple action mechanisms. [[Amiodarone]], for example, has effects consistent with all of the first four classes. Another limitation is the lack of consideration within the VW classification system for the effects of drug metabolites. [[Procainamide]]&mdash;a class Ia agent whose metabolite [[N-acetyl procainamide]] (NAPA) has a class III action&mdash;is one such example. A historical limitation was that drugs such as [[digoxin]] and [[adenosine]] &ndash; important antiarrhythmic agents &ndash; had no place at all in the VW classification system. This has since been rectified by the inclusion of class V.
The Vaughan Williams classification, introduced in 1970,<ref>Vaughan Williams EM. "Classification of anti-arrhythmic drugs." In: ''Symposium on Cardiac Arrhythmias'', Sandfte E, Flensted-Jensen E, Olesen KH eds. Sweden, AB ASTRA, Södertälje, 1970;449-472.</ref> is one of the most widely used classification schemes for antiarrhythmic agents. This scheme classifies a drug based on the primary mechanism of its antiarrhythmic effect. However, its dependence on primary mechanism is one of the limitations of the VW classification, since many antiarrhythmic agents have multiple action mechanisms. [[Amiodarone]], for example, has effects consistent with all of the first four classes. Another limitation is the lack of consideration within the VW classification system for the effects of drug metabolites. [[Procainamide]]&mdash;a class Ia agent whose metabolite [[N-acetyl procainamide]] (NAPA) has a class III action&mdash;is one such example. A historical limitation was that drugs such as [[digoxin]] and [[adenosine]] &ndash; important antiarrhythmic agents &ndash; had no place at all in the VW classification system. This has since been rectified by the inclusion of class V.
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* Class II agents are anti-[[sympathetic nervous system]] agents.  All agents in this class are [[beta blockers]].
* Class II agents are anti-[[sympathetic nervous system]] agents.  All agents in this class are [[beta blockers]].
* Class III agents affect [[potassium]] (K<sup>+</sup>) efflux.
* Class III agents affect [[potassium]] (K<sup>+</sup>) efflux.
* Class IV agents affect the [[AV node]].
* Class IV agents affect the [[AV node]]. They are [[calcium channel blockers]].
* Class V agents work by other or unknown mechanisms.
* Class V agents work by other or unknown mechanisms.


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*Intensity of Na<sup>+</sup> blockade
*Intensity of Na<sup>+</sup> blockade
** 1C>1A>1B (manifests as increased PR and QRS)
** 1C>1A>1B (manifests as increased PR and QRS)
*Proarrhythmia may be provoked by increased heart rate. Thus common clinical practice is to perform exercise testing following drug loading.
*Pro-arrhythmic impact of Class 1C may be reversed or attenuated with the use of beta blocking adrenergic agents.
====Cardiac Arrhythmia Suppression Trial (CAST)====
Hypothesis: Suppression of [[Ventricular Premature Complexes]] (VPC) post-MI beneficial in terms of mortality.
Result: [[Flecainide]] and [[Encainide]] associated with unexpected increase in mortality.


==== Class Ia agents ====
==== Class Ia agents ====
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Class III agents predominantly block the potassium channels, thereby prolonging repolarization.<ref>Lenz TL, Hilleman DE, Department of Cardiology, Creighton University, Omaha, Nebraska. Dofetilide, a New Class III Antiarrhythmic Agent. Pharmacotherapy 20(7):776-786, 2000. ([http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=pubmed&dopt=Abstract&list_uids=10907968 Medline abstract])</ref>  Since these agents do not affect the sodium channel, conduction velocity is not decreased.  The prolongation of the action potential duration and refractory period, combined with the maintenance of normal conduction velocity, prevent re-entrant arrhythmias. (The re-entrant rhythm is less likely to interact with tissue that has become refractory).
Class III agents predominantly block the potassium channels, thereby prolonging repolarization.<ref>Lenz TL, Hilleman DE, Department of Cardiology, Creighton University, Omaha, Nebraska. Dofetilide, a New Class III Antiarrhythmic Agent. Pharmacotherapy 20(7):776-786, 2000. ([http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=pubmed&dopt=Abstract&list_uids=10907968 Medline abstract])</ref>  Since these agents do not affect the sodium channel, conduction velocity is not decreased.  The prolongation of the action potential duration and refractory period, combined with the maintenance of normal conduction velocity, prevent re-entrant arrhythmias. (The re-entrant rhythm is less likely to interact with tissue that has become refractory).
'''All clinically available class III drugs block IKr, not IKs'''


Class III antiarrhythmic agents exhibit reverse use dependent prolongation of the action potential duration ('''Reverse use-dependence''').  This means that the refractoriness of the ventricular [[myocyte]] increases at lower [[heart rate]]s.  This increases the susceptibility of the myocardium to early after-depolarizations (EADs) at low heart rates.  Antiarrhythmic agents that exhibit reverse use-dependence are more efficacious at preventing a tachyarrhythmia than converting someone into normal sinus rhythm.  ''Because of the reverse use-dependence of class III agents, at low heart rates class III antiarrhythmic agents may paradoxically be more arrhythmogenic.''
Class III antiarrhythmic agents exhibit reverse use dependent prolongation of the action potential duration ('''Reverse use-dependence''').  This means that the refractoriness of the ventricular [[myocyte]] increases at lower [[heart rate]]s.  This increases the susceptibility of the myocardium to early after-depolarizations (EADs) at low heart rates.  Antiarrhythmic agents that exhibit reverse use-dependence are more efficacious at preventing a tachyarrhythmia than converting someone into normal sinus rhythm.  ''Because of the reverse use-dependence of class III agents, at low heart rates class III antiarrhythmic agents may paradoxically be more arrhythmogenic.''
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'''Mixed''': [[Procainamide]], [[Flecainide]] (70% hepatic), [[Quinidine]] (50-70% hepatic), [[Ibutilide]], [[Azimilide]] (not FDA approved)
'''Mixed''': [[Procainamide]], [[Flecainide]] (70% hepatic), [[Quinidine]] (50-70% hepatic), [[Ibutilide]], [[Azimilide]] (not FDA approved)
==General Principles of Antiarrhythmic drugs==
*All anti-arrhythmic drugs should be considered pro-arrhythmic.
*Pro-arrhythmia increased in presence of [[structural heart disease]], (especially [[myocardial ischemia]] and left ventricular systolic dysfunction).
*[[Beta-adrenoreceptor blockers]] are the only drug class shown definitively to improve mortality.
*[[Amiodarone]] and [[Dofetilide]] have neutral impact on mortality following [[MI]] and in the presence of [[structural heart disease]].
*Consider altered drug clearance in both renal and hepatic impairment and drug interactions.
==Specific Drugs==
===Quinidine Class 1A===
*Less commonly used now.
*Used in atrial and ventricular arrhythmias.
*Proarrhythmia is dose-independent and may occur with normal or even sub-therapeutic drug levels.
*Theraupetic effect determined with reference to the corrected QT interval.
*[[QT prolongation]] > 500msec should prompt abandonment of this drug class or decrease in the drug dose. Some degree of [[QT prolongation]] suggests anti-arrhythmic drug effect due to prolonged [[repolarization]].
*Alpha-adrenergic blocking property of quinidine, in addition to peripheral [[vasodilation]], may cause [[orthostatic hypotension]] and [[reflex tachycardia]].
*[[Quinidine]] does not cauSe clinically important negative inotropic even in the setting of severe [[left ventricular dysfunction]].
*The vagolytic effect of quinidine may enhance AV nodal blocking agent prior to starting quinidine.
*'''Avoid use of quinidine for [[atrial fibrillation]] since associated with increased mortality'''.
*'''Drug interactions'''
**Quinidine inhibits cytochrome P450-D6 and thus decreases the metabolism of [[propranolol]], [[metoprolol]], and [[propafenone]].
**[[Digoxin]]: increased levels (may be doubled in many cases) due to decreased tissue binding (lower volume of distribution) and decreased renal and biliary clearance. Therefore '''[[Digoxin]] should be halved when used with [[Quinidine]]'''
**[[Warfarin]]: the anticoagulant effect of warfarin may be increased.
**[[Heparin]]: displaces quinidine and increases the unbound fraction of the plasma.
**[[Verapamil]]: may increase quinidine levels by decreasing metabolism.
**[[Amiodarone]]: increases quinidine levels and also has an increased impact on [[QT prolongation]].
**Also interacts with [[calcium channel blockers]], [[cimetidine]], and enzyme inducing drugs ([[phenobarbital]], [[phenytoin]], and [[rifampicin]]).
*'''Side effects'''
**GI side effects (one third), most commonly [[abdominal cramping]] and [[diarrhea]].
**[[Rash]] common.
**[[Cinchonism]] (hearing decrease, tinnitus, and blurred vision - may include delirium if severe).
**[[Thrombocytopenia]] and [[Coombe's positive hemolytic anemia]]. Former usually resolves within days after drug is discontinued but can persist for more than one month.
**[[Lupus syndrome]] with [[anti-histone antibodies]].
**[[Granulomatous hepatitis]].
**Toxic levels of quinidine cause severe [[QRS widening]] and [[ventricular arrhythmias]]. (may reverse with the infusion of [[sodium lactate]] or [[sodium bicarbonate]]).
*'''Proarrhythmia'''
**Quinidine syncope most frequently due to [[VT]] (incidence 0.5 to 4.4%).
**[[VF]] (median occurence 3 days after initiation of drug) is common to all Class 1A drugs (concordance rate ~ 30%). In other words, if [[Torsade de Pointes]] or [[VF]] is observed with one class 1A agent all other class 1A agents should be avoided due to high incidence of [[Torsade de Pointes]].
**Because of risk of [[proarrhythmia]] all class 1A drugs should be initiated in hospital.
**If QTC > 500 msec stop drug.
===[[Disopyramide]] Class 1A===
*Used in atrial and ventricular arrhythmias.
*Marked negative inotropic effect related directly to plasma levels. Problematic in patients with underlying left ventricular dysfunction. Useful in patients with diastolic dysfunction or in patients with [[hypertrophic obstructive cardiomyopathy]].
*'''Drug Interactions'''
**[[Phenobarbital]], [[phenotonin]], and [[rifamycin]] increase hepatic metabolism of [[disopyramide]] and decrease plasma levels.
**The negative inotropic effect of some drugs such as beta adrenoreceptor blockers is additive when used in combination with [[disopyramide]].
**[[Erythromycin]] may increase [[disopyramide]] levels by inhibiting hepatic monoendealkalation and this has led to [[torsades de pointes]] in some patients.
*'''Side effects'''
**Anticholinergic (30%) including [[dry mouth]], [[blurred vision]], [[constipation]], and [[urinary retention]]. Bladder effects typically seen in older men and can be counteracted with [[Bethanecol]]. [[Pyridostigmine]] (90 mg twelve hourly to 180 mg every eight hours) prevents or diminishes the anticholinergic effect of disopyramide and allows high tolerated doses of the drug.
**Disopyramide-induced hypoglycemia has been reported and may be due to enhanced secretion of [[insulin]]. Predisposing factors appear to include advanced age, [[malnutrition]], and [[chronic renal failure]]. Other reported side effects includes [[nausea]], [[vomiting]], [[rash]], [[cholestatic jaundice]], and [[Agranulocytosis]].
**[[Disopyramide]] caused regular uterine contractions in all ten near term pregnant women who were studied.
*'''Proarrhythmia'''
**As with other drugs that prolong repolarization, [[disopyramide]] may cause [[VF]], [[Torsade de Pointes]]; although it appears to do less so than [[quinidine]].
===[[Procainamide]] Class 1A===
*Useful for [[atrial fibrillation]], [[atrial flutter]], [[ventricular tachycardia]], [[ventricular fibrillation]].
*50-60% renal excreted.
**[[N-acetyl-procainamide]] (metabolite) renal excretion (therefore adjust dose in [[renal impairment]]).
**IV dose 15-20 mg/kg.
**For each 1mg/kg dose given, blood level increases 0.5 mcg/ml.
*Acute IV use largely supplanted by [[amiodarone]].
*Adverse effects
**25% develop gastrointestinal side effects.
**80% +[[ANA]].
***30% develop a lupus like syndrome.
***Do not check [[ANA]] unless clinically indicated.
**Pro-arrhythmia ([[Torsade de Pointes]])
***Dose independent (similar to [[Quinidine]]).
**Infra-hisian block.
***Care with [[bundle branch block]] and [[intra-ventricular conduction delay]].
**Accelerated ventricular response to [[atrial flutter]] (use in conjunction with AV nodal blocking agent).
===[[Lidocaine]] Class 1B===
*Voltage dependent sodium channel block (enhanced action in depolarized i.e. ischemic tissue).
*Therefore, useful against arrhythmias in [[myocardial ischemia]].
*Hepatic metabolism proportional to hepatic blood flow.
**Conditions that decrease hepatic blood flow decrease clearance and increase blood levels (toxicity common with [[Congestive Heart Failure]]).
*'''Drug Interactions'''
**[[Propanolol]] and [[Metoprolol]] decrease hepatic blood flow and consequently the metabolism of [[lidocaine]] increasing plasma level by up to 80%.
**[[Phenobarbital]] decreases the plasma concentration of [[lidocaine]].
*'''Side effects'''
**CNS effects predominate and include [[peri-oral numbness]], [[paraesthesia]], [[diplopia]], [[hyperacusis]], [[slurred speech]], [[altered consciousness]], [[seizures]], [[respiratory arrest]], and [[coma]].
**Infra-His conduction block has been reported in some patients with pre-existing conduction system disease.
**Sinus node depression has occurred in patients with underlying sinus node disease.
*'''Proarrhythmia'''
**Clinically relevant proarrhythmias due to lidocaine are infrequent.
===[[Mexilitine]] Class 1B===
*Used in [[ventricular arrhythmias]].
*Minimal hemodynamic effect including little effect on [[heart rate]], [[blood pressure]], [[cardiac output]] or [[intracardiac pressures]]. In patients with severe left ventricular dysfunction, mexiletine may cause increase in [[pulmonary capillary wedge pressure]] but this effect is variable.
*[[Ejection fraction]] is generally unaltered by mexiletine even in patients with [[structural heart disease]].
*'''Drug interactions'''
**[[Phenytoin]], [[phenobarbital]] and [[Rifampicin]] increase metabolism of Mexilitine.
**[[Digoxin]] and [[Warfarin]] not affected
*'''Side Effects'''
**GI and CNS effects most prominent which are dose and concentration related.
**[[Tremor]] usually the first sign of CNS toxicity but [[blurred vision]], [[dysarthria]], [[ataxia]], and [[confusion]] may occur. [[Tremor]] may respond to beta adrenergic blocking agents.
**[[Thrombocytopenia]] reported rarely.
**Increased [[liver function tests]] and other [[blood dyscrasias]] (rare).
*'''Proarrhythmia''': Incidence of serious proarrhythmia due to mexiletine is low (<2%).
===[[Phenytoin]] Class 1B===
*Used in ventricular arrhythmias.
*[[Hypertension]] may occur during intravenous administration but probably due to dilutant in the intravenous preparation.
*No significant ventricular depressant effect.
*Worsening of sinus node function especially in patients with underlying sinus disease.
*'''Drug Interactions'''
**[[Phenytonin]] induces hepatic enzymes thereby increases metabolism of numerous drugs including [[Quinidine]], [[disopyramide]], [[lidocaine]], [[mexiletine]], and [[Theophylline]].
**Phenytoin levels are increased by [[Isoniazid]], [[Chloramphenicol]], [[disulfiram]], and some [[sulphanamides]].
**[[Antacids]] decrease absorption of [[Phenytoin]].
*'''Side Effects'''
**CNS side effects, particularly [[nystagmus]], and [[ataxia]] occur in a concentration dependent manner.
**[[Rash]], [[nausea]], [[blood dyscrasias]], [[lupus syndrome]], [[peripheral neuropathy]], [[hyperglycemia]], [[lymphadenopathy]], [[Stevens-Johnson syndrome]], [[hirsutism]], and [[osteomalacia]] may also be seen.
**[[Gingival hyperplasia]] common (incidence ~ 50%). Elimination of pre-existing periodontal disease and thorough oral hygiene may prevent.
**Extravasation during IV administration may cause serious tissue damage or limb loss.
**A rare but important reaction is [[Phenytoin Hypersensitivity Syndrome]] characterized by [[fever]], [[skin lesions]](ranging from acne form to [[erythema multiforma]]),  [[lymphadenopathy]], [[hepatosplenomegaly]], and[[leukocytosis]] with [[eosinophilia]].
===[[Flecainide]] Class 1C===
*Used in Atrial and ventricular arrhythmias
*Heart rate typically unaffected except in the presence of sinus node disease.
*Negative inotropic effect similar to disopyramide so may exacerbate CHF in patients with left ventricular dysfunction.
*No effect on ejection fraction if EF > 50%.
*'''Drug interactions'''
**Increases [[Digoxin]] levels by 25% (via decreased clearance).
**[[Amiodarone]] and [[cimetidine]] increase [[flecainide]] levels.
**[[Quinidine]] inhibits hepatic metabolism of flecainide increases elimination half life by about 20%.
*'''Side effects'''
**CNS including [[blurred vision]], [[headache]], [[ataxia]].
**[[CHF]] in patients with underlying LV systolic dysfunction.
*'''Proarrhythmia'''
**Reduced left ventricular systolic function probably also predisposes to arrhythmogenesis.
**Exercise testing recommended before hospital dismissal after achieving steady state with flecainide.
**Beta adrenergic blockade used to treat [[proarrhythmia]] due to flecainide.
**Ventricular proarrhythmia due to flecainide is rare in the treatment of [[paroxysmal atrial fibrillation]] or [[paroxysmal supraventricular tachycardia]].
**Few cases of serious proarrhythmia reported in patients with normal hearts who receive flecainide for [[supraventricular arrhythmia]]s.
===[[Propafenone]] Class 1C===
*Structurally similar to [[propranolol]] (also has weak β-blocking action).
*Useful for [[atrial fibrillation]], [[atrial flutter]], [[SVT]].
*Cautious use in [[VT]].
*Hepatic transformation to 5-OH propafenone by P450 2D6 enzyme.
**7% of United States population deficient in this enzyme.
**Increased propafenone level, increased beta blocker effect, longer half-life.
*Proarrhythmia: increased in the presence of reduced ejection fraction/ischemia.
**May manifest as increased [[VT]].
**[[Tachycardia]] provoked proarrhythmia (use dependence)
**Exercise ECG useful screening test.
*Watch for impairment of AV conduction and [[QRS]] widening.
*Increases [[digoxin]], [[warfarin]], and [[metoprolol]] levels.
===[[Amiodarone]]===
*'''Not as good as [[ICD]] for preventing sudden cardiac death.''' Amiodarone is a useful drug in suppressing symptomatic atrial and ventricular arrhythmias but is '''NO SUBSTITUTE''' for [[ICD]] therapy in patients deemed at risk of sudden cardiac arrest.
*[[Thyroid]] toxicity
**Inhibition of T4 de-iodination to T3 leading to accumulation of rT3.
**Hypothyroid (10%); Hyperthyroid (2-12%)
**[[Hypothyroidism]]: Treat with exogenous T4 or stop [[amiodarone]].
**[[Hyperthyroidism]]: More difficult to treat. Usually need to stop drug and consider specific anti-thyroid agents. Surgical removal of gland if unable to control ir if need to continue drug. I¹³¹ not useful.
*[[Pulmonary]] toxicity
**Always consider pulmonary toxicity with worsening [[CHF]] despite therapy.
**Diagnosis
***[[PFT]]'s - low [[DLCO]] and low ρO2
***High resolution CT
***[[Biopsy]]
***[[Bronchoalveolar lavage]]
*Other side effects include [[photosensitivity]], discoloration of the skin, and corneal micro deposits(these rarely cause a clinical problem).
*Drug interactions
**[[Warfarin]] - increased INR.
**[[Digoxin]] - increased [[Digoxin]]
**[[Cyclosporine]] - increased [[Cyclosporine]]
*'''Proarrhythmia'''
**Amiodarone may cause life threatening ventricular arrhythmias including [[ventricular fibrillation]] and [[Torsade de Pointes]].
**Less pro-arrhythmic than other antiarrhythmic agents.
*'''Clinical trials'''
**Canadian Amiodarone Myocardial Infarction Arrhythmia Trial (CAMIAT): This trial randomized 1,202 patients after myocardial infarction who had ten or more ventricular premature depolarizations per hour to amiodarone. Over a 1.79 year follow up, resuscitative [[ventricular fibrillation]] or arrhythmic death was less in the patients treated with amiodarone. It was concluded that amiodarone reduces ventricular fibrillation arrhythmic death after [[myocardial infarction]] with frequent or repetitive [[ventricular premature complexes]]. The absolute risk reduction was greater in patients with previous [[myocardial infarction]] or [[congestive heart failure]].
**EMIAT: The EMIAT Trial randomized 1,486 patients with ischemic ventricular dysfunction after [[myocardial infarction]], ejection fraction less than 40%. Over a 21 month follow up, all cause and cardiac mortality was similar in both groups. There was a 35% decrease in arrhythmic death in patients receiving [[amiodarone]]. [[Amiodarone]] therapy in this group of patients was not supported by the study. The conclusions of these trials differ as did their entry trials. CAMIAT focused on ventricular ectopy whereas EMIAT focused on ventricular dysfunction. Clearly, patients in EMIAT were sicker with substantially greater overall mortality. Interestingly, the details of CAMIAT indicate that like EMIAT all cause mortality was unaffected by [[amiodarone]]. The ultimate message form these trials is ambiguous but amiodarone at the very least was shown to be no worse than [[placebo]] supporting at minimum its use in patients who require antiarrhythmic therapy for other reasons.
**JESSICA Trial.
**CHF Trial.
*'''RECOMMENDATIONS FOR ROUTINE LABORATORY TESTING WITH CHRONIC AMIODARONE THERAPY'''
**[[Thyroid Function Tests]] ([[TSH]] and [[T4]]) - Baseline, 3 months and every 6 months
**[[Liver Function Tests]] - Baseline and every 6 months
**[[Chest X-ray]] - Baseline and yearly
**[[Pulmonary Function Tests]] - Baseline and if symptoms develop or change
**Ophthalmic evaluation - Baseline if visual symptoms or for symptom changes
===[[Dofetilide]]===
*Pure IKr blocker
*Approved for [[atrial fibrillation]] and [[atrial flutter]]
*Inpatient loading mandatory due to risk of [[Torsades de Pointes]] VT.
*Dosing adjusted by [[QT interval]] change (at rest).
*Careful dosing in [[renal insufficiency]] (80% renally excreted).
*20% liver (cytochrome P450)
*Initiation and Dosing
**Plan on atleast 3 days hospitalization or 12 hours after conversion to normal sinus rhythm. (whichever is greater)
**Withdraw/avoid: [[verapamil]], [[cimetidine]], [[trimethoprim]], [[ketoconazole]], [[prochlorperazine]].
**Get potassium >4.0
**Measure QTc: if >440 msec (500 msec w/Intraventricular conduction delay) find another drug.
===[[Ibutilide]]===
*Blocks IKr and slow inactivation of sodium channels (increases atrial refractoriness).
*Mostly used for acute termination of [[atrial fibrillation]] and to facilitate [[cardioversion]] in resistant cases.
*Good for [[WPW]].
*Risk of [[Torsades de Pointes]] VT is 2-3%; higher with advanced LV dysfunction (EF<20%).
*Adjunctive use of magnesium after ibutilide may prevent proarrhythmia.
===[[Dronedarone]]===
*Chemically similar to [[Amiodarone]] but has no Iodine (lower risk of pulmonary, liver and thyroid complications).
*Shorter elimination half-life (24 hours versus weeks).
*Indicated for [[atrial Flutter]] and [[atrial fibrillation]] (not ventricular arrhythmias or sudden death prevention).
*More effective than [[placebo]] in maintaining [[sinus rhythm]].
*The efficacy of dronedarone in patients with atrial fibrillation is superior to [[placebo]] but appears inferior to [[amiodarone]] and [[sotalol]].
*Reduces hospitalization due to cardiovascular events or death.
*Reduces rate of [[strokes]].
*Contraindicated in
**NYHA class IV [[heart failure]]
**NYHA II-III [[heart failure]] with recent decompensation requiring hospitalization.
**In the ANDROMEDA study dronedarone doubled the death rate in patients with moderate to severe heart failure although the precise mechanism is unknown. Because of these findings, dronedarone is contraindicated in class IV [[CHF]] or in patients with recent exacerbation of [[heart failure]].
*'''Proarrhythmia'''
**The pro-arrhythmic potential of dronedarone is low and similar to amiodarone.
*Common side effects include [[bradycardia]] and [[QT interval prolongation]] (class III effect) along with [[nausea]], [[rash]] and [[increased creatinine]].
*'''Clinical trials'''
**EURIDIS and ADONIS trials reported that when compared with placebo dronedarone was superior in maintaining sinus rhythm after electrical, pharmacologic or spontaneous conversion to sinus rhythm from [[atrial fibrillation]] or flutter with no (short term) differences in lung and thyroid function
**ANDROMEDA study reported a significant increase in the rate of death in patients with moderate to severe [[congestive heart failure]].
**ATHENA trial reported that dronedarone was significantly more effective than placebo in reducing the composite endpoint of first hospitalization due to cardiovascular events or death with a significant reduction in the rate of cardiovascular death, but not in the rate of death from any cause. A post-hoc analysis of the ATHENA- trial also showed a significant reduction in the rate of stroke although the clinical significance of this is unclear.
===[[Bretylium]] Class III===
*Used in ventricular arrhythmias (mostly VF).
*Bretylium rarely used and then only in the setting of recurrent VT or VF having failed [[lidocaine]], [[procainamide]], and [[DC cardioversion]].
*Bretylium causes initial [[norepinephrine]] release with subsequent depletion of [[norepinephrine]] from sympathetic nerve terminals. This results in [[increased blood pressure]] followed by [[orthostatic hypotension]].
*'''Side effects'''
**[[Orthostatic hypotension]] which may take several days to resolve.
**[[Nausea]]
**[[Vomiting]] during delivery of initial dose.
*'''Proarrhythmia''': Initial worsening of arrhythmias due to release of [[norepinephrine]].
===[[Sotalol]] Class III===
*Used in Atrial and ventricular arrhythmias
*Potent [[beta adrenergic blocker]] so may cause [[bradycardia]] and worsening of [[left ventricular dysfunction]].
*Anti-hypertensive effect.
*'''Drug interactions'''
**Beta blocking action may cause exacerbate effect of drugs that have AV nodal inhibitory effects such as [[digoxin]] or non vascular selective [[calcium channel blockers]] such as [[verapamil]] and [[diltiazem]].
*'''Side effects'''
**Most side effects related to beta blocking action
**[[Fatigue]] most prominent.
*'''Proarrhythmia'''
**[[QT lengthening]] can result in [[ventricular fibrillation]] or [[Torsade de pointes]].
**Proarrhythmia rates of 3-5% have been reported.
**Care in patients with Hypokalemia/Hypomagnesia (i.e.those taking diuretics) and use of higher dose ranges (greater than 160 mg twice daily) are associated with greater risk of proarrhythmia.
*SWORD Trial (Survival With Oral D Sotalol) evaluated D sotalol (a pure Ikr potassium channel blocker with no beta blocking action) in 3,121 patients with LV dysfunction and recent [[myocardial infarction]] or recent heart failure and a remote [[myocardial infarction]].
*Use of D-sotalol was associated with increased mortality over [[placebo]].
===[[Digoxin]]===
*Still commonly used.
*Effects mediated via central and peripheral augmentation of vagal tone.
*Direct action on atria and AV node only at toxic concentrations.
**Increases sympathetic tone and Calcium loading leading to increased automaticity and delayed afterdeploarisations.
*'''Electrophysiology'''
**Inotropic action via inhibition of Na-K ATPase and Na-Ca exchange.
**Minimal effects on surface ECG at therapeutic doses.
**May improve conduction in some accessory pathways (avoid in [[WPW syndrome]]).
**No effect on rate of conversion to sinus rhythm in patients with acute episode of [[atrial fibrillation]].
**Rarely effective as sole agent for rate control. Must confirm heart rate control by exercising (aim for heart rate less than 110 with moderate walking).
*'''Clinical Pharmacology'''
**60-80% oral bioavailability (decreased with [[cholestyramine]], [[antacids]], [[colestipol]]).
**P-glycoprotein: excretes absorbed digoxin back in to gut lumen (also controls renal elimination).
**'''Drug interactions'''
***[[Quinidine]]: Increase digoxin levels by displacing from binding sites and inhibiting P-glycoprotein system.
***[[Amiodarone]], [[Propafenone]], [[Verapamil]]: decrease renal and non-renal clearance.
***[[Cyclosporine]], [[anti-fungals]], [[benzodiazepines]]: inhibit P-glycoprotein.
*Dosing guided by efficacy, adverse effects, ECG intervals and serum levels (rule of thumb: do not exceed dose that prolongs [[QRS]] more than 25% or [[QT]] >550ms)\
*'''Toxicity'''
**Non-cardiac - [[anorexia]], [[nausea]], [[vomiting]], changes in color vision including [[scotoma]], halo vision and altered color perception.
**Cardiac - due to exaggerated effects on sinus and AV node and intracellular Ca loading causing delayed afterdeploarizations.
**[[Arrhythmias]]: almost any, but high grade AV block with accelerated junctional rhythm or bi-directional VT strongly suggestive.
**[[Nausea]] (common)
**[[Vomiting]] (common)
**[[Anorexia]] (common)
**[[Diarrhea]] (common)
**[[Thrombocytopenia]] (occasionally)
**[[Marrow suppression]] (occasionally)
**[[Lupus]] (rare)
**[[Fever]]
**Pro-arrhythmia (0.5-8%) - dose independent - may occur soon after initiation (i.e. when plasma levels low)
===[[Adenosine]]===
*Activates I<sub>K Ado</sub> shortens action potential duration (direct effect).
*Decreases cAMP, decreased delayed afterdeploarizations, early afterdepolarizations (indirect effect).
*All actions mediated via A1 receptor and G proteins (not present in ventricle).
*Extensive first pass metabolism.
*Re-uptake blocked by [[dipyridamole]].
*Methylxanthines block A1 receptor.
*'''Drug interactions'''
**[[Dipyridamole]]: increases effect.
**[[Methylxanthine]]s: No effect.
**Transplanted heart: increases effect.
===EKG Examples===
----
Shown below are EKG tracings showing the effect of [[adenosine]] on AV conduction, but in addition the effect on atrial refractoriness.  The first tracing is clearly [[atrial flutter]] with an atrial rate of 270/min, and a ventricular rate of 135/min. The second recording shows much faster atrial activity. The second tracing is either [[atrial fibrillation]] (a know result of [[adenosine]]) or a faster [[atrial flutter]] (type II flutter) with variable block. Both of these effects could be seen as a result of the decrease in the atrial refractory period by the stimulation of the [[adenosine]].
[[Image:Adenosine effect.jpg|center|800px]]
----
[[Image:Adenosine effect1.jpg|center|800px]]
Copyleft images obtained courtesy of ECGpedia, http://en.ecgpedia.org
----
Shown below is an EKG demonstrating a [[supraventricular tachycardia]]. It is a somewhat unusual presentation for someone with [[angina]].  The arrhythmia terminated with [[adenosine]] which has a powerful cholinergic effect that blocks conduction through the [[AV node]].
[[Image:Svtadenosine.jpg|center|800px]]
Copyleft image obtained courtesy of ECGpedia, http://en.ecgpedia.org
----
==IN HOSPITAL VERSUS OUTPATIENT INITIATION OF ANTI-ARRHYTHMIC DRUGS==
The decision to initiate anti-arrhythmic drug therapy in hospital versus the outpatient setting is determined largely by likelihood of risk versus cost and inconvenience of inpatient drug loading. In the case of [[Dofetilide]] in-hospital initiation is mandated. Unfortunately, few prospective data are available regarding safety of outpatient initiation of AAD therapy. In the case of [[atrial fibrillation]], outpatient loading should be avoided in patients with symptomatic sinus node dysfunction, AV conduction disturbance, [[bundle branch block]], [[structural heart disease]] and [[QT prolongation]]. The most important risk of AAD therapy is that that of [[proarrhythmia]], most commonly due to [[Torsades de Pointes]], but also virtually any other [[arrhythmia]] such as [[ventricular tachycardia]] and [[atrial arrhythmias]].
*In general, in the absence of significant bradycardia and with normal ventricular function, QRS and QT intervals, proarrhythmia risk is low.
*Unsuspected sinus node dysfunction that is suppressed by AA agent may lead to prolonged sinus node recovery with termination of AF leading to possible syncope.
*[[Propafenone]] and [[flecainide]] also worsen AV node and His Purkinji conduction thus if outpatient use is contemplated initial cardioversion in hospital is prudent.
*For [[Sotalol]], outpatient initiation is probably safe if baseline [[QT interval]] is less than 450ms in the absence of renal dysfunction and risk factors for [[Torsade de Pointes]].
*[[Amiodarone]] is generally considered to be safe to administer as an out-patient. Risk of pro-arrhythmia is low.
*In hospital administration of [[Dofetilide]] is mandatory.
In most cases, AAD should be started at the lowest possible dose and titrated upwards and therapeutic efficacy monitored with reference to PR interval ([[flecainide]], [[propafenone]], [[sotalol]] and [[amiodarone]]), QRS ([[flecainide]], [[propafenone]]) and QT intervals ([[sotalol]], [[amiodarone]] and [[disopyramide]]) at rest ([[sotalol]]) or with exercise (Class IC agents). Measurement of serum drug levels is rarely helpful.
==Choice of agent in [[PSVT]]==
*[[Hypotension]], Uncertain diagnosis (especially if WCT), [[Heart failure]] - [[Adenosine]]
*[[Dipyridamole]], [[Theophyllines]], [[Bronchoconstriction]], Transplanted heart, PSVT recurs post adenosine - [[Verapamil]]/[[Diltiazem]]


==Trials==
==Trials==


The ''Cardiac Arrhythmia Suppression Trial''<ref>[http://www.clinicaltrials.gov/ct/show/NCT00000526 Entry on Clinical Trials.gov]</ref> was a medical study that demonstrated that some class 1 anti-arrhythemic drugs were not helpful to people suffering from [[ventricular]] premature depolarization.  Specifically, for populations of recent heart attack survivors, the study observed lower mortality in a control population than in populations treated with encainide, flecainide or moricizine (all class 1c drugs).
The ''Cardiac Arrhythmia Suppression Trial''<ref>[http://www.clinicaltrials.gov/ct/show/NCT00000526 Entry on Clinical Trials.gov]</ref> was a medical study that demonstrated that some class 1 anti-arrhythmic drugs were not helpful to people suffering from [[ventricular]] premature depolarization.  Specifically, for populations of recent heart attack survivors, the study observed lower mortality in a control population than in populations treated with encainide, flecainide or moricizine (all class 1c drugs).


==Mnemonics==
==Mnemonics==
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Sodium channel blockers, Beta blockers, Potassium channel blockers, Calcium channel blockers
Sodium channel blockers, Beta blockers, Potassium channel blockers, Calcium channel blockers


== See also ==
== Related Chapters ==
*[[Action potential]]
*[[Action potential]]
**[[Cardiac action potential]]
**[[Cardiac action potential]]
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Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]

Overview

Antiarrhythmic agents are a group of pharmaceuticals that are used to suppress fast rhythms of the heart (cardiac arrhythmias), such as atrial fibrillation, atrial flutter, ventricular tachycardia, and ventricular fibrillation.

While the use of antiarrhythmic agents to suppress atrial arrhythmias (atrial fibrillation and atrial flutter) is still in practice, it is unclear whether suppression of atrial arrhythmias will prolong life.[1][2]

In the past, it was believed that following myocardial infarction (heart attack), suppression of ventricular arrhythmias would prolong life. However large clinical trials found that suppression of these arrhythmias would paradoxically increase mortality,[3][4] which may happen due to the proarrhythmic effect these drugs may have (CAST trial).

In individuals with atrial fibrillation, antiarrhythmics are still used to suppress arrhythmias. This is often done to relieve the symptoms that may be associated with the loss of the atrial component to ventricular filling (atrial kick) that is due to atrial fibrillation or flutter.


In individuals with ventricular arrhythmias, antiarrhythmic agents are often still in use to suppress arrhythmias. In this case, the patient may have frequent arrhythmic events or be at high risk for ventricular arrhythmias. Antiarrhythmic agents may be considered the first-line therapy in the prevention of sudden death in certain forms of structural heart disease, and failure of these agents to suppress arrhythmias may lead to implantation of an implantable cardioverter-defibrillator (ICD).

The use of antiarrhythmic agents in this population may be in conjunction with an ICD. In this case, the ICD is used to prevent sudden death due to ventricular fibrillation, while the antiarrhythmic agent(s) are used to suppress ventricular tachyarrhythmias so that the ICD doesn't shock the patient frequently.

Many attempts have been made to classify antiarrhythmic agents. The problem arises from the fact that many of the antiarrhythmic agents have multiple modes of action, making any classification imprecise.

Vaughan Williams Antiarrhythmic Classification

The Vaughan Williams classification, introduced in 1970,[5] is one of the most widely used classification schemes for antiarrhythmic agents. This scheme classifies a drug based on the primary mechanism of its antiarrhythmic effect. However, its dependence on primary mechanism is one of the limitations of the VW classification, since many antiarrhythmic agents have multiple action mechanisms. Amiodarone, for example, has effects consistent with all of the first four classes. Another limitation is the lack of consideration within the VW classification system for the effects of drug metabolites. Procainamide—a class Ia agent whose metabolite N-acetyl procainamide (NAPA) has a class III action—is one such example. A historical limitation was that drugs such as digoxin and adenosine – important antiarrhythmic agents – had no place at all in the VW classification system. This has since been rectified by the inclusion of class V.

There are five main classes in the Vaughan Williams classification of antiarrhythmic agents:

Class I agents

The class I antiarrhythmic agents interfere with the sodium (Na+) channel. Class I agents are grouped by what effect they have on the Na+ channel, and what effect they have on cardiac action potentials.

  • Intensity of Na+ blockade
    • 1C>1A>1B (manifests as increased PR and QRS)
  • Proarrhythmia may be provoked by increased heart rate. Thus common clinical practice is to perform exercise testing following drug loading.
  • Pro-arrhythmic impact of Class 1C may be reversed or attenuated with the use of beta blocking adrenergic agents.

Cardiac Arrhythmia Suppression Trial (CAST)

Hypothesis: Suppression of Ventricular Premature Complexes (VPC) post-MI beneficial in terms of mortality.

Result: Flecainide and Encainide associated with unexpected increase in mortality.

Class Ia agents

Class Ia agents block the fast sodium channel. (manifests as increased PR and QRS)

Blocking this channel depresses the phase 0 depolarization (reduces Vmax), which prolongs the action potential duration by slowing conduction.

Prolongation of repolarization due to K+ channel effect. (manifests as prolonged QT interval)

Agents in this class also cause decreased conductivity and increased refractoriness.

Indications for Class Ia agents are supraventricular tachycardia, ventricular tachycardia, symptomatic ventricular premature beats, and prevention of ventricular fibrillation.

Procainamide can be used in the treatment of atrial fibrillation in the setting of Wolff-Parkinson-White syndrome, and in the treatment of wide complex hemodynamically stable tachycardias.

While procainamide and quinidine may be used in the conversion of atrial fibrillation to normal sinus rhythm, they should only be used in conjunction with an AV node blocking agent (ie: digoxin, verapamil, or a beta blocker), because procainamide and quinidine can increase the conduction through the AV node and may cause 1:1 conduction of atrial fibrillation, causing an increase in the ventricular rate.

Class Ia agents include quinidine, procainamide and disopyramide.

Class Ib agents

Class Ib antiarrhythmic agents are sodium channel blockers. Class Ib agents have fast onset and offset kinetics, meaning that they have little or no effect at slower heart rates, and more effects at faster heart rates. Class Ib agents shorten the action potential duration and reduce refractoriness. These agents will decrease Vmax in partially depolarized cells with fast response action potentials. They either do not change the action potential duration, or they may decrease the action potential duration. Class Ib drugs tend to be much more specific for voltage gated Na channels than Ia. Lidocane in particular is highly frequency dependent, in that it has more activity with increasing heart rates. This is because lidocane selectively blocks Na channels in their open and inactive states and has little binding capability in the resting state.

Class Ib agents are indicated for the treatment of ventricular tachycardia and symptomatic premature ventricular beats, and prevention of ventricular fibrillation.

Class Ib agents include lidocaine, mexiletine, tocainide, and phenytoin.

Class Ic agents

Class Ic antiarrhythmic agents markedly depress the phase 0 depolarization (decreasing Vmax). They decrease conductivity, but have a minimal effect on the action potential duration. Of the sodium channel blocking antiarrhythmic agents (the class I antiarrhythmic agents), the class Ic agents have the most potent sodium channel blocking effects.

Class Ic agents are indicated for life-threatening ventricular tachycardia or ventricular fibrillation, and for the treatment of refractory supraventricular tachycardia (ie: atrial fibrillation). These agents are potentially pro-arrhythmic, especially in settings of structural heart disease (e.g. post-myocardial infarction), and are contraindicated in such settings.

Class Ic agents include encainide, flecainide, moricizine, and propafenone.

Class II agents

Class II agents are conventional beta blockers. They act by selectively blocking the effects of catecholamines at the β1-adrenergic receptors, thereby decreasing sympathetic activity on the heart. These agents are particularly useful in the treatment of supraventricular tachycardias. They decrease conduction through the AV node.

Class II agents include esmolol, propranolol, and metoprolol.

Class III agents

Class III agents predominantly block the potassium channels, thereby prolonging repolarization.[6] Since these agents do not affect the sodium channel, conduction velocity is not decreased. The prolongation of the action potential duration and refractory period, combined with the maintenance of normal conduction velocity, prevent re-entrant arrhythmias. (The re-entrant rhythm is less likely to interact with tissue that has become refractory).

All clinically available class III drugs block IKr, not IKs

Class III antiarrhythmic agents exhibit reverse use dependent prolongation of the action potential duration (Reverse use-dependence). This means that the refractoriness of the ventricular myocyte increases at lower heart rates. This increases the susceptibility of the myocardium to early after-depolarizations (EADs) at low heart rates. Antiarrhythmic agents that exhibit reverse use-dependence are more efficacious at preventing a tachyarrhythmia than converting someone into normal sinus rhythm. Because of the reverse use-dependence of class III agents, at low heart rates class III antiarrhythmic agents may paradoxically be more arrhythmogenic.

Amiodarone is indicated for the treatment of refractory VT or VF, particularly in the setting of acute ischemia. Amiodarone is also safe to use in individuals with cardiomyopathy and atrial fibrillation, to maintain normal sinus rhythm. Amiodarone prolongation of the action potential is uniform over a wide range of heart rates so this drug does not have reverse use-dependent action.7 In contrast, dofetilide blocks only the rapid K channels; this means that at higher heart rates, when there is increased involvement of the slow K channels, dofetilide has less of an action potential-prolonging effect. 7

Sotalol is indicated for the treatment of atrial or ventricular tachyarrhythmias, and AV re-entrant arrhythmias. Ibutilide is the only antiarrhythmic agent currently approved by the Food and Drug Administration for acute conversion of atrial fibrillation to sinus rhythm.

Class III agents include amiodarone, azimilide, bretylium, clofilium, dofetilide, tedisamil, ibutilide, sematilide, and sotalol.

Class IV agents

Class IV agents are slow calcium channel blockers. They decrease conduction through the AV node, and shorten phase two (the plateau) of the cardiac action potential. They thus reduce the contractility of the heart, so may be inappropriate in heart failure. However, in contrast to beta blockers, they allow the body to retain adrenergic control of heart rate and contractility.

Class IV agents include verapamil and diltiazem.

Class V agents

Class V agents include digoxin and adenosine. Digoxin increases vagal activity via its central action on the central nervous system, thus decreasing the conduction of electrical impulses through the AV node

Major Routes of Elimination of Antiarrhythmic drugs

Hepatic: Amiodarone, Propafenone, Lidocaine, Mexilitine, Verapamil, Diltiazem.

Renal: Sotalol, Digoxin, Dofetilide, Bretylium

Mixed: Procainamide, Flecainide (70% hepatic), Quinidine (50-70% hepatic), Ibutilide, Azimilide (not FDA approved)

General Principles of Antiarrhythmic drugs

Specific Drugs

Quinidine Class 1A

Disopyramide Class 1A

Procainamide Class 1A

Lidocaine Class 1B

Mexilitine Class 1B

Phenytoin Class 1B

Flecainide Class 1C

  • Used in Atrial and ventricular arrhythmias
  • Heart rate typically unaffected except in the presence of sinus node disease.
  • Negative inotropic effect similar to disopyramide so may exacerbate CHF in patients with left ventricular dysfunction.
  • No effect on ejection fraction if EF > 50%.
  • Drug interactions
  • Side effects
  • Proarrhythmia

Propafenone Class 1C

  • Structurally similar to propranolol (also has weak β-blocking action).
  • Useful for atrial fibrillation, atrial flutter, SVT.
  • Cautious use in VT.
  • Hepatic transformation to 5-OH propafenone by P450 2D6 enzyme.
    • 7% of United States population deficient in this enzyme.
    • Increased propafenone level, increased beta blocker effect, longer half-life.
  • Proarrhythmia: increased in the presence of reduced ejection fraction/ischemia.
    • May manifest as increased VT.
    • Tachycardia provoked proarrhythmia (use dependence)
    • Exercise ECG useful screening test.
  • Watch for impairment of AV conduction and QRS widening.
  • Increases digoxin, warfarin, and metoprolol levels.

Amiodarone

  • Not as good as ICD for preventing sudden cardiac death. Amiodarone is a useful drug in suppressing symptomatic atrial and ventricular arrhythmias but is NO SUBSTITUTE for ICD therapy in patients deemed at risk of sudden cardiac arrest.
  • Thyroid toxicity
    • Inhibition of T4 de-iodination to T3 leading to accumulation of rT3.
    • Hypothyroid (10%); Hyperthyroid (2-12%)
    • Hypothyroidism: Treat with exogenous T4 or stop amiodarone.
    • Hyperthyroidism: More difficult to treat. Usually need to stop drug and consider specific anti-thyroid agents. Surgical removal of gland if unable to control ir if need to continue drug. I¹³¹ not useful.
  • Other side effects include photosensitivity, discoloration of the skin, and corneal micro deposits(these rarely cause a clinical problem).
  • Clinical trials
    • Canadian Amiodarone Myocardial Infarction Arrhythmia Trial (CAMIAT): This trial randomized 1,202 patients after myocardial infarction who had ten or more ventricular premature depolarizations per hour to amiodarone. Over a 1.79 year follow up, resuscitative ventricular fibrillation or arrhythmic death was less in the patients treated with amiodarone. It was concluded that amiodarone reduces ventricular fibrillation arrhythmic death after myocardial infarction with frequent or repetitive ventricular premature complexes. The absolute risk reduction was greater in patients with previous myocardial infarction or congestive heart failure.
    • EMIAT: The EMIAT Trial randomized 1,486 patients with ischemic ventricular dysfunction after myocardial infarction, ejection fraction less than 40%. Over a 21 month follow up, all cause and cardiac mortality was similar in both groups. There was a 35% decrease in arrhythmic death in patients receiving amiodarone. Amiodarone therapy in this group of patients was not supported by the study. The conclusions of these trials differ as did their entry trials. CAMIAT focused on ventricular ectopy whereas EMIAT focused on ventricular dysfunction. Clearly, patients in EMIAT were sicker with substantially greater overall mortality. Interestingly, the details of CAMIAT indicate that like EMIAT all cause mortality was unaffected by amiodarone. The ultimate message form these trials is ambiguous but amiodarone at the very least was shown to be no worse than placebo supporting at minimum its use in patients who require antiarrhythmic therapy for other reasons.
    • JESSICA Trial.
    • CHF Trial.
  • RECOMMENDATIONS FOR ROUTINE LABORATORY TESTING WITH CHRONIC AMIODARONE THERAPY

Dofetilide

Ibutilide

  • Blocks IKr and slow inactivation of sodium channels (increases atrial refractoriness).
  • Mostly used for acute termination of atrial fibrillation and to facilitate cardioversion in resistant cases.
  • Good for WPW.
  • Risk of Torsades de Pointes VT is 2-3%; higher with advanced LV dysfunction (EF<20%).
  • Adjunctive use of magnesium after ibutilide may prevent proarrhythmia.

Dronedarone

  • Chemically similar to Amiodarone but has no Iodine (lower risk of pulmonary, liver and thyroid complications).
  • Shorter elimination half-life (24 hours versus weeks).
  • Indicated for atrial Flutter and atrial fibrillation (not ventricular arrhythmias or sudden death prevention).
  • More effective than placebo in maintaining sinus rhythm.
  • The efficacy of dronedarone in patients with atrial fibrillation is superior to placebo but appears inferior to amiodarone and sotalol.
  • Reduces hospitalization due to cardiovascular events or death.
  • Reduces rate of strokes.
  • Contraindicated in
    • NYHA class IV heart failure
    • NYHA II-III heart failure with recent decompensation requiring hospitalization.
    • In the ANDROMEDA study dronedarone doubled the death rate in patients with moderate to severe heart failure although the precise mechanism is unknown. Because of these findings, dronedarone is contraindicated in class IV CHF or in patients with recent exacerbation of heart failure.
  • Proarrhythmia
    • The pro-arrhythmic potential of dronedarone is low and similar to amiodarone.
  • Common side effects include bradycardia and QT interval prolongation (class III effect) along with nausea, rash and increased creatinine.
  • Clinical trials
    • EURIDIS and ADONIS trials reported that when compared with placebo dronedarone was superior in maintaining sinus rhythm after electrical, pharmacologic or spontaneous conversion to sinus rhythm from atrial fibrillation or flutter with no (short term) differences in lung and thyroid function
    • ANDROMEDA study reported a significant increase in the rate of death in patients with moderate to severe congestive heart failure.
    • ATHENA trial reported that dronedarone was significantly more effective than placebo in reducing the composite endpoint of first hospitalization due to cardiovascular events or death with a significant reduction in the rate of cardiovascular death, but not in the rate of death from any cause. A post-hoc analysis of the ATHENA- trial also showed a significant reduction in the rate of stroke although the clinical significance of this is unclear.

Bretylium Class III

Sotalol Class III

  • Used in Atrial and ventricular arrhythmias
  • Potent beta adrenergic blocker so may cause bradycardia and worsening of left ventricular dysfunction.
  • Anti-hypertensive effect.
  • Drug interactions
  • Side effects
    • Most side effects related to beta blocking action
    • Fatigue most prominent.
  • Proarrhythmia
    • QT lengthening can result in ventricular fibrillation or Torsade de pointes.
    • Proarrhythmia rates of 3-5% have been reported.
    • Care in patients with Hypokalemia/Hypomagnesia (i.e.those taking diuretics) and use of higher dose ranges (greater than 160 mg twice daily) are associated with greater risk of proarrhythmia.
  • SWORD Trial (Survival With Oral D Sotalol) evaluated D sotalol (a pure Ikr potassium channel blocker with no beta blocking action) in 3,121 patients with LV dysfunction and recent myocardial infarction or recent heart failure and a remote myocardial infarction.
  • Use of D-sotalol was associated with increased mortality over placebo.

Digoxin

  • Still commonly used.
  • Effects mediated via central and peripheral augmentation of vagal tone.
  • Direct action on atria and AV node only at toxic concentrations.
    • Increases sympathetic tone and Calcium loading leading to increased automaticity and delayed afterdeploarisations.
  • Electrophysiology
    • Inotropic action via inhibition of Na-K ATPase and Na-Ca exchange.
    • Minimal effects on surface ECG at therapeutic doses.
    • May improve conduction in some accessory pathways (avoid in WPW syndrome).
    • No effect on rate of conversion to sinus rhythm in patients with acute episode of atrial fibrillation.
    • Rarely effective as sole agent for rate control. Must confirm heart rate control by exercising (aim for heart rate less than 110 with moderate walking).
  • Clinical Pharmacology
  • Dosing guided by efficacy, adverse effects, ECG intervals and serum levels (rule of thumb: do not exceed dose that prolongs QRS more than 25% or QT >550ms)\
  • Toxicity
    • Non-cardiac - anorexia, nausea, vomiting, changes in color vision including scotoma, halo vision and altered color perception.
    • Cardiac - due to exaggerated effects on sinus and AV node and intracellular Ca loading causing delayed afterdeploarizations.
    • Arrhythmias: almost any, but high grade AV block with accelerated junctional rhythm or bi-directional VT strongly suggestive.
    • Nausea (common)
    • Vomiting (common)
    • Anorexia (common)
    • Diarrhea (common)
    • Thrombocytopenia (occasionally)
    • Marrow suppression (occasionally)
    • Lupus (rare)
    • Fever
    • Pro-arrhythmia (0.5-8%) - dose independent - may occur soon after initiation (i.e. when plasma levels low)

Adenosine

  • Activates IK Ado shortens action potential duration (direct effect).
  • Decreases cAMP, decreased delayed afterdeploarizations, early afterdepolarizations (indirect effect).
  • All actions mediated via A1 receptor and G proteins (not present in ventricle).
  • Extensive first pass metabolism.
  • Re-uptake blocked by dipyridamole.
  • Methylxanthines block A1 receptor.
  • Drug interactions

EKG Examples


Shown below are EKG tracings showing the effect of adenosine on AV conduction, but in addition the effect on atrial refractoriness. The first tracing is clearly atrial flutter with an atrial rate of 270/min, and a ventricular rate of 135/min. The second recording shows much faster atrial activity. The second tracing is either atrial fibrillation (a know result of adenosine) or a faster atrial flutter (type II flutter) with variable block. Both of these effects could be seen as a result of the decrease in the atrial refractory period by the stimulation of the adenosine.


Copyleft images obtained courtesy of ECGpedia, http://en.ecgpedia.org


Shown below is an EKG demonstrating a supraventricular tachycardia. It is a somewhat unusual presentation for someone with angina. The arrhythmia terminated with adenosine which has a powerful cholinergic effect that blocks conduction through the AV node.

Copyleft image obtained courtesy of ECGpedia, http://en.ecgpedia.org


IN HOSPITAL VERSUS OUTPATIENT INITIATION OF ANTI-ARRHYTHMIC DRUGS

The decision to initiate anti-arrhythmic drug therapy in hospital versus the outpatient setting is determined largely by likelihood of risk versus cost and inconvenience of inpatient drug loading. In the case of Dofetilide in-hospital initiation is mandated. Unfortunately, few prospective data are available regarding safety of outpatient initiation of AAD therapy. In the case of atrial fibrillation, outpatient loading should be avoided in patients with symptomatic sinus node dysfunction, AV conduction disturbance, bundle branch block, structural heart disease and QT prolongation. The most important risk of AAD therapy is that that of proarrhythmia, most commonly due to Torsades de Pointes, but also virtually any other arrhythmia such as ventricular tachycardia and atrial arrhythmias.

  • In general, in the absence of significant bradycardia and with normal ventricular function, QRS and QT intervals, proarrhythmia risk is low.
  • Unsuspected sinus node dysfunction that is suppressed by AA agent may lead to prolonged sinus node recovery with termination of AF leading to possible syncope.
  • Propafenone and flecainide also worsen AV node and His Purkinji conduction thus if outpatient use is contemplated initial cardioversion in hospital is prudent.
  • For Sotalol, outpatient initiation is probably safe if baseline QT interval is less than 450ms in the absence of renal dysfunction and risk factors for Torsade de Pointes.
  • Amiodarone is generally considered to be safe to administer as an out-patient. Risk of pro-arrhythmia is low.
  • In hospital administration of Dofetilide is mandatory.

In most cases, AAD should be started at the lowest possible dose and titrated upwards and therapeutic efficacy monitored with reference to PR interval (flecainide, propafenone, sotalol and amiodarone), QRS (flecainide, propafenone) and QT intervals (sotalol, amiodarone and disopyramide) at rest (sotalol) or with exercise (Class IC agents). Measurement of serum drug levels is rarely helpful.

Choice of agent in PSVT

Trials

The Cardiac Arrhythmia Suppression Trial[7] was a medical study that demonstrated that some class 1 anti-arrhythmic drugs were not helpful to people suffering from ventricular premature depolarization. Specifically, for populations of recent heart attack survivors, the study observed lower mortality in a control population than in populations treated with encainide, flecainide or moricizine (all class 1c drugs).

Mnemonics

Mnemonic for Class I-IV agents: SoBe PoCa (SOBE as in South Beach or the drink, POCA as in Polka)

Sodium channel blockers, Beta blockers, Potassium channel blockers, Calcium channel blockers

Related Chapters

References

  1. Wyse D, Waldo A, DiMarco J, Domanski M, Rosenberg Y, Schron E, Kellen J, Greene H, Mickel M, Dalquist J, Corley S (2002). "A comparison of rate control and rhythm control in patients with atrial fibrillation". N Engl J Med. 347 (23): 1825–33. PMID 12466506.
  2. Nichol G, McAlister F, Pham B, Laupacis A, Shea B, Green M, Tang A, Wells G (2002). "Meta-analysis of randomised controlled trials of the effectiveness of antiarrhythmic agents at promoting sinus rhythm in patients with atrial fibrillation". Heart. 87 (6): 535–43. PMID 12010934.
  3. "Preliminary report: effect of encainide and flecainide on mortality in a randomized trial of arrhythmia suppression after myocardial infarction. The Cardiac Arrhythmia Suppression Trial (CAST) Investigators". N Engl J Med. 321 (6): 406–12. 1989. PMID 2473403.
  4. "Effect of the antiarrhythmic agent moricizine on survival after myocardial infarction. The Cardiac Arrhythmia Suppression Trial II Investigators". N Engl J Med. 327 (4): 227–33. 1992. PMID 1377359.
  5. Vaughan Williams EM. "Classification of anti-arrhythmic drugs." In: Symposium on Cardiac Arrhythmias, Sandfte E, Flensted-Jensen E, Olesen KH eds. Sweden, AB ASTRA, Södertälje, 1970;449-472.
  6. Lenz TL, Hilleman DE, Department of Cardiology, Creighton University, Omaha, Nebraska. Dofetilide, a New Class III Antiarrhythmic Agent. Pharmacotherapy 20(7):776-786, 2000. (Medline abstract)
  7. Entry on Clinical Trials.gov

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