Head-to-head clinical analysis & difference comparison: details on mechanism of action, dosing, half-life, interactions, and maternal-fetal safety.
TAMBOCOR vs QUINIDEX
Clinician-reviewed, head-to-head comparison of mechanism, dosing, pharmacokinetics, and safety profiles.
Last clinically reviewed: July 2026 · OpiCalc Medical Review Team
Class Ic antiarrhythmic agent; blocks sodium channels, slowing conduction velocity and prolonging refractoriness in cardiac tissues.
Class Ia antiarrhythmic agent; blocks sodium channels (fast inward sodium current) and prolongs action potential duration; also has anticholinergic and negative inotropic effects.
Treatment of documented life-threatening ventricular arrhythmias (e.g., sustained ventricular tachycardia),Suppression of symptomatic atrial fibrillation/flutter (off-label)
Conversion and prevention of atrial fibrillation/flutter,Maintenance of sinus rhythm after cardioversion,Treatment of ventricular arrhythmias (off-label)
For atrial fibrillation/flutter: 50 mg orally every 12 hours; may increase by 50 mg every 4 days up to 300 mg/day. For life-threatening ventricular arrhythmias: 100 mg orally every 12 hours; increase by 50 mg every 4 days up to 400 mg/day.
Quinidine sulfate (QUINIDEX): 200-400 mg orally every 6 hours as arrhythmia suppression; maximum 4 g/day. Route: oral, frequency: every 6 hours.
Terminal elimination half-life: 12–27 hours (mean 20 hours); prolonged to 58 hours in heart failure or renal impairment (Cr Cl < 35 m L/min).
Terminal elimination half-life is 6-8 hours in adults with normal renal and hepatic function; may be prolonged to 10-12 hours in congestive heart failure or hepatic impairment.
Hepatic metabolism via CYP2D6; active metabolite; renal excretion of unchanged drug and metabolites.
Primarily hepatic via CYP3A4 (major) and CYP2C9 (minor) to active metabolites (3-hydroxyquinidine, quinidine-N-oxide); also renal excretion of unchanged drug (20%).
Renal: 85% (30% unchanged, 55% as inactive metabolites); Fecal: 5%; Biliary: negligible.
Renal excretion accounts for approximately 20% unchanged drug; hepatic metabolism (primarily CYP3A4) accounts for 80% with metabolites excreted renally and biliarily; about 5% excreted in feces.
90–95% bound to albumin and alpha-1-acid glycoprotein.
80-90% bound to plasma proteins: primarily albumin and alpha-1-acid glycoprotein.
8–10 L/kg; extensive tissue distribution (lung, heart, liver).
2-4 L/kg; extensive tissue distribution with high affinity for myocardium (tissue-to-plasma ratio >10).
Oral: 85–90% (first-pass metabolism minimal).
70-80% for immediate-release oral; 50-70% for sustained-release formulations due to first-pass metabolism; absorption reduced by food.
Cr Cl >50 m L/min: no adjustment; Cr Cl 35-50 m L/min: 50 mg every 12 hours; Cr Cl <35 m L/min: 100 mg every 24 hours or 50 mg every 12 hours with caution.
Cr Cl 30-50 m L/min: administer 75% of normal dose every 6 hours. Cr Cl 10-29 m L/min: administer 50% of normal dose every 8 hours. Cr Cl <10 m L/min: administer 50% of normal dose every 12 hours.
Child-Pugh class A: no adjustment; Child-Pugh class B: reduce dose by 25-50%; Child-Pugh class C: contraindicated or use with extreme caution.
Child-Pugh class A: no adjustment. Child-Pugh class B: reduce dose by 50%; monitor levels. Child-Pugh class C: contraindicated or use with extreme caution; reduce dose by 75% with therapeutic drug monitoring.
Dosing not established; limited data: 1-3 mg/kg/day orally divided every 8-12 hours; maximum 6 mg/kg/day.
Oral: 15-60 mg/kg/day in 4-5 divided doses; maximum single dose 600 mg. For chronic suppression: start 30 mg/kg/day in 4-5 divided doses.
Start at 50 mg every 12 hours; increase slowly with close monitoring of plasma levels and ECG; consider lower doses due to reduced renal function.
Start at lower end of dosing range (200 mg every 8 hours) due to decreased hepatic and renal function; adjust based on plasma levels and QT interval monitoring.
May increase mortality in patients with structural heart disease (e.g., post-MI, cardiomyopathy). Reserved for life-threatening arrhythmias.
Increased mortality in treatment of non-life-threatening ventricular arrhythmias; proarrhythmic effects (torsades de pointes).
Proarrhythmic effects including new or worsened ventricular arrhythmias,Use caution in patients with conduction abnormalities (e.g., SA node dysfunction, bundle branch block),Heart failure exacerbation due to negative inotropic effects,Electrolyte disturbances (hypokalemia, hypomagnesemia) should be corrected,Plasma monitoring recommended due to narrow therapeutic index
Proarrhythmia (torsades de pointes), hepatotoxicity, cinchonism, hypersensitivity reactions, worsening of heart failure, digitalis toxicity, incomplete AV block, electrolyte disturbances.
Second- or third-degree AV block (unless pacemaker in place),Bifascicular block or distal conduction blocks,Cardiogenic shock or severe hypotension,Pre-existing prolonged QT interval,History of ventricular arrhythmias associated with structural heart disease
Hypersensitivity to quinidine or cinchona alkaloids, complete AV block or severe intraventricular conduction defects, myasthenia gravis, history of thrombocytopenia with quinidine, concurrent use with drugs that prolong QT interval (unless absolutely necessary).
Grapefruit juice increases flecainide AUC by 15-40% and should be avoided. High-fat meals may delay absorption but do not significantly alter overall exposure. No other specific dietary restrictions.
Grapefruit juice increases quinidine bioavailability and serum levels, raising toxicity risk. Avoid grapefruit and grapefruit juice. Alkaline foods (e.g., antacids, milk) may increase quinidine absorption. High-sodium diet may enhance potassium loss and worsen arrhythmias. Avoid excessive caffeine or stimulants.
FDA Pregnancy Category C. Flecainide crosses the placenta. First trimester: Limited human data; animal studies show fetal toxicity at maternally toxic doses. Second and third trimesters: Risk of fetal arrhythmia, including tachycardia or heart block; may require fetal echocardiography. Avoid in pregnancy unless benefit outweighs risk.
First trimester: Limited data, but quinidine crosses placenta. No clear increase in major malformations after first trimester exposure. Second and third trimesters: Risk of fetal QT prolongation, neonatal thrombocytopenia, and tachycardia. Fetal distress may occur. Avoid if alternative exists, but if needed, monitor fetal ECG and heart rate.
Flecainide is excreted into breast milk. Milk-to-plasma ratio approximately 2.5 (range 1.4–3.8). Infant exposure estimated at 3–5% of maternal weight-adjusted dose. Monitor infant for bradycardia, arrhythmia, and feeding difficulties. Use with caution; alternative agents preferred.
Quinidine is excreted into breast milk. M/P ratio reported as 0.57–0.78. Amount is low, but monitor infant for arrhythmias, bruising, and bleeding. Generally considered compatible with breastfeeding if maternal monitoring is done.
Increased plasma volume and renal clearance in pregnancy may reduce flecainide levels. Monitor therapeutic drug levels and ECG; dose adjustments may be needed (typically increased dose required). Titrate based on arrhythmia control and toxicity. Postpartum: dose may need reduction as clearance normalizes.
Increased volume of distribution may require dose increases. Protein binding decreases, potentially lowering total drug concentrations. Monitor free drug levels if possible. adjust dose based on therapeutic drug monitoring and clinical response. Close monitoring recommended.
Tambocor (flecainide) is a class Ic antiarrhythmic used for life-threatening ventricular arrhythmias and paroxysmal atrial fibrillation/flutter. It has a narrow therapeutic index and requires ECG monitoring for QRS prolongation (>140 ms) or new arrhythmias. Contraindicated in ischemic heart disease due to increased mortality (CAST trial). Adjust dose in renal impairment (Cr Cl < 50 m L/min: start at 50 mg q12h). Proarrhythmic risk is highest in patients with structural heart disease or reduced EF. Monitor trough levels (therapeutic range: 0.2-1.0 mcg/m L).
Quinidine (as Quinidex) is a class Ia antiarrhythmic; monitor QRS and QT intervals due to risk of torsades de pointes. It also has anticholinergic properties, causing diarrhea in up to 50% of patients, which can be dose-limiting. Drug interactions are critical: quinidine inhibits CYP2D6, increasing levels of digoxin, warfarin, and many beta-blockers. Consider checking serum quinidine levels (therapeutic: 2-6 mcg/m L) and ECG if initiating or adjusting dose.
Take exactly as prescribed; do not stop or change dose without consulting your doctor.,Report any new or worsening chest pain, palpitations, fainting, or difficulty breathing immediately.,Avoid grapefruit juice as it can increase flecainide levels and risk of side effects.,Take with or without food; maintain consistent timing to keep levels stable.,Do not crush or chew extended-release capsules; swallow whole.
Take exactly as prescribed; do not double dose if missed.,Avoid grapefruit juice as it can increase quinidine levels and toxicity.,Report new or worsening palpitations, dizziness, syncope, or irregular heartbeat immediately.,May cause diarrhea; contact your prescriber if diarrhea becomes severe or persistent.,Quinidine can cause blurred vision, tinnitus, or headache; report these to your doctor.,Avoid over-the-counter medications without consulting your doctor (especially antacids, antihistamines, and cold remedies).
No interactions on record
No interactions on record
Explore head-to-head clinical comparisons of other medications in the same therapeutic classes.
Common clinical questions about TAMBOCOR vs QUINIDEX, answered by our medical review team.
TAMBOCOR is a Antiarrhythmic Agent that works by Class Ic antiarrhythmic agent; blocks sodium channels, slowing conduction velocity and prolonging refractoriness in cardiac tissues.. QUINIDEX is a Antiarrhythmic Agent that works by Class Ia antiarrhythmic agent; blocks sodium channels (fast inward sodium current) and prolongs action potential duration; also has anticholinergic and negative inotropic effects.. They differ in pharmacokinetic profiles, FDA-approved indications, and side effect profiles.
Potency comparisons between TAMBOCOR and QUINIDEX depend on the specific clinical indication. These are both Antiarrhythmic Agent agents and are not directly interchangeable by dose. A physician or clinical pharmacist should guide any therapeutic switching decisions.
The standard adult dose of TAMBOCOR is: For atrial fibrillation/flutter: 50 mg orally every 12 hours; may increase by 50 mg every 4 days up to 300 mg/day. For life-threatening ventricular arrhythmias: 100 mg orally every 12 hours; increase by 50 mg every 4 days up to 400 mg/day.. The standard adult dose of QUINIDEX is: Quinidine sulfate (QUINIDEX): 200-400 mg orally every 6 hours as arrhythmia suppression; maximum 4 g/day. Route: oral, frequency: every 6 hours.. Dosing should always be individualized based on indication, renal and hepatic function, age, and other patient factors.
No direct drug-drug interaction has been formally documented between TAMBOCOR and QUINIDEX in current clinical databases. However, individual patient risk factors including other medications, organ function, and comorbidities should always be evaluated by a qualified healthcare provider.
The maternal-fetal safety profiles differ. TAMBOCOR is classified as Category C. FDA Pregnancy Category C. Flecainide crosses the placenta. First trimester: Limited human data; animal studies show fetal toxicity at maternally toxic doses. Second and third trime. QUINIDEX is classified as Category C. First trimester: Limited data, but quinidine crosses placenta. No clear increase in major malformations after first trimester exposure. Second and third trimesters: Risk of fetal Q. Always consult a maternal-fetal medicine specialist before taking either drug during pregnancy or lactation.