Which Drugs Treat Ventricular Arrhythmias in Dogs & Cats?
Amara H. Estrada, DVM, DACVIM (Cardiology), University of Florida
Profile
Most antiarrhythmic agents exert effects on normal myocardium to some extent and may have intrinsic arrhythmogenic (proarrhythmic) properties.1 In general, the author uses antiarrhythmic drugs to manage life-threatening arrhythmias and minimize risk for sudden cardiac arrest.
Antiarrhythmic classes → Classified by function
Class I: Na channel blockers
Class II: β-blocker
Class III: K channel blockers
Class IV: Ca channel blockers
Basis for objective → Control acute life-threatening arrhythmias
These arrhythmias may be hemodynamically compromising and are likely to degenerate into fatal arrhythmias.
Basis for objective → Lower risk for sudden cardiac arrest or death
Prophylactic administration of antiarrhythmic agents to patients at increased risk for cardiac arrest or death may lower that risk.
Achieving objectives → Use of different antiarrhythmics can achieve both objectives, although some may be contraindicated in certain situations.
It is important to
Understand the mechanism of action of antiarrhythmics
Ultimately appreciate the electrophysiology of arrhythmias to select a drug that will most likely abolish, suppress, or prevent an arrhythmia
Clinical necessity → Drug selection should be based on clinical necessity, as all antiarrhythmic agents are potentially proarrhythmic.
Antiarrhythmic agents
Alter the properties of myocardium and specialized conduction tissue, suppressing abnormal electrical activity therein
Affect normal myocardial and conduction tissue to some extent
Antiarrhythmic agents may have intrinsic arrhythmogenic (proarrhythmic) potential.
Class Ia Antiarrhythmic
Procainamide
Procainamide is a fast sodium channel blocker that affects the QRS complex.
Formulation → IV only
Dose (dogs) → 5–15 mg/kg over 1 min2-4
If effective in controlling the rhythm, establish 20–50 µg/kg/min CRI.2-4
Dose (cats) → 1–2 mg/kg slowly over 20 min2-4
Key Points
Procainamide effectively suppresses ventricular tachyarrhythmias via enhanced automaticity and reentry.1
The author uses procainamide only if other antiarrhythmics (eg, lidocaine [acutely], sotalol [chronically]) are ineffective.
Has some autonomic effects and can enhance sympathetic tone
At therapeutic doses, vagolytic effects seen with other class I agents are negligible.1
Contraindicated in patients with bradyarrhythmia
In humans with chronic procainamide administration, systemic lupus erythematosus is an important side effect.<sup5 sup>
Not documented in domestic animals, although changes in hair coat color with lupus-like dermatologic changes, along with thrombocytopenia, neutropenia, and pancytopenia, have been anecdotally reported.2-4
Class Ib Antiarrhythmics
Lidocaine
As a class 1b antiarrhythmic agent, lidocaine has no effect on the QRS complex.
Formulation → IV only
Oral administration not effective because lidocaine rapidly and completely metabolized by the liver on first pass
Dose (dogs) → Initiate therapy with bolus of 2 mg/kg IV.2-4
Can repeat up to 3 times in 10 minutes to control rate and malignancy of ventricular rhythm, but full eradication of ventricular arrhythmia should not be expected
If rhythm improves, establish 30–75 µg/kg/min CRI.
Titrate infusion to maintain rhythm control.
Dose (cats) → Slow bolus of 0.25–0.5 mg/kg, followed by 10–25 µg/kg/min CRI if effective in controlling rhythm2-4
Definitive IV antiarrhythmic agents rarely needed in cats (see Cautions below for contraindications)
Oral products (eg, sotalol) usually sufficient
Key Points
Lidocaine is considered the drug of choice for controlling all types of acute ventricular tachyarrhythmias, but especially those resulting from ischemic myopathy.1-4
Clinical application
Can be used in patients with dangerous and sustained ventricular dysrhythmias causing hemodynamic compromise1-4
Because lidocaine does not depress contractility or produce vasodilation, can be safely used in patients with congestive heart failure (CHF)2-4
Effectiveness depends on extracellular potassium concentrations.
Low concentrations antagonize depressant actions.
High concentrations increase conduction velocity depression, membrane responsiveness, and automaticity.
Cautions
Contraindicated in patients with bradyarrhythmias because can suppress subsidiary pacemaker cells1
Severe adverse events uncommon
Nausea and inappetence not uncommon
GI side effects most noticeable
More common in cats, so dose should be carefully calculated and side effects carefully monitored
CNS excitability can occur in both dogs and cats, resulting in seizures.
Cats very sensitive to CNS effects
Diazepam can be used if lidocaine toxicity suspected6
Mexiletine
Mexiletine is used in dogs only. Like lidocaine, it has no effect on the QRS complex.7
The author uses mexiletine when other antiarrhythmic medications (eg, sotalol) might be contraindicated because of systolic dysfunction or myocardial failure (eg, Doberman pinscher with dilated cardiomyopathy and ventricular arrhythmias, boxer with severe myocardial dysfunction and ventricular arrhythmias).
Formulation → Oral
Dose (dogs) → 4–8 mg/kg PO q8h2-4
Effective after oral administration and slowly metabolized by liver, resulting in elimination half-life of 5–7 hours
Key Points
Mexiletine has electrophysiologic, hemodynamic, and toxic properties almost identical to those of lidocaine.
Shown to effectively suppress ventricular arrhythmias in dogs,8,9 but effects on survival unknown
To increase efficacy, commonly combined with atenolol9
May cause anorexia, diarrhea, or other GI disturbances
Class II Antiarrhythmic
Atenolol
Atenolol is a cardioselective β-adrenergic blocker, also categorized as a β1-receptor antagonist.
Formulation → Oral
Dose (dogs) → 0.2–2 mg/kg q12–24h2-4
Dose (cats) → 6.25–12.5 mg total dose per cat q12–24h2-4
Can be formulated into suspension
Key Points
Because of apparent lack of efficacy, generally not used as monotherapy for ventricular arrhythmias in dogs but commonly used in combination with other antiarrhythmic agents (eg, mexiletine)9
Can be used in cats with less severe ventricular arrhythmias2-4
If good antiarrhythmic control of the ventricular rhythm difficult to maintain, select more effective ventricular antiarrhythmic agent (eg, sotalol).
Cautions
Although atenolol does not block all β-receptors, it has significant β-blocking effects and should therefore be used with caution.
Slowly titrate in patients with significant ventricular systolic dysfunction.2-4
Should not be combined with another β-blocker
Should be used carefully in conjunction with other drugs that block atrioventricular node (eg, calcium channel blockers)
Class III Antiarrhythmics
Sotalol
Sotalol blocks potassium channels and increases the effective refractory period of myocardial cells by prolonging repolarization.
Formulation → Oral
Dose (dogs) → 1–3 mg/kg q12h2-4
Dose (cats) → 1–3 mg/kg q12h2-4
Can be reconstituted into liquid formulation
Key Points
Clinical applications
Author initiates sotalol therapy when dangerous ventricular rhythm identified but hemodynamic compromise not present
In author’s experience, therapy also indicated in at-risk breeds (eg, boxer) with single monomorphic ventricular premature complexes and history of possible cardiovascular collapse
Sotalol also exhibits potent nonselective class II activity (adrenergic antagonist).
Especially useful in reducing frequency and malignant characteristics/grade of ventricular arrhythmias and syncopal events in boxers with arrhythmogenic right ventricular cardiomyopathy
Impact on long-term survival in boxers with this disease remains unknown.10
Useful in suppressing sustained refractory ventricular tachycardias in cats with arrhythmogenic right ventricular cardiomyopathy
Cautions
Although not pure β-adrenergic blocker, has significant β-blocking effects
Use with caution and slowly titrate in patients with significant ventricular systolic dysfunction.2-4
Most side effects attributed to drug’s β-blocking properties
Amiodarone
Amiodarone, an agent used in dogs only, prolongs action potential and increases effective refractory period of cardiac tissue by blocking potassium channels and slowing repolarization.
Formulation → Oral
Dose (dogs only) → 10–20 mg/kg PO q24h for 7–10 days, then reduced to 3–15 mg/kg PO q24–48h2-4
Use low end of dose range first; slowly titrate only if necessary.
Because of potential side effects, use lowest dose possible.
Key Points
For ventricular arrhythmias refractory to aforementioned antiarrhythmic agents, amiodarone is typically initiated in lieu of, or carefully in addition to, other antiarrhythmic agents.
Antiarrhythmic profile superior to other antiarrhythmic agents
In both humans11-13 and dogs,14,15 toxicity and adverse reactions to long-term administration are common.
Blocks fast sodium channels (class I effect), noncompetitively blocks α- and β-adrenergic receptors (class II effect), and blocks slow calcium channels (class IV effect)
Efficacy generally thought to exceed that of other antiarrhythmic compounds; however, with chronic use side effects are significant and/or severe.11
May cause anorexia from elevated liver enzymes
Liver enzymes should be evaluated before starting, periodically while administering amiodarone, and if anorexia develops.
May cause neutropenia of unknown clinical significance, neurologic signs, and/or ataxia, especially at higher doses and with prolonged use11
Can be combined with β-adrenergic blocker
Does not appear to have significant negative inotropic effects
Safe to use in patients with ventricular myocardial dysfunction11
CHF = congestive heart failure