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Tikosyn

Dofetilide is a class III antiarrhythmic agent that is approved by the FDA for the maintenance of sinus rhythm in individuals prone to the formation of atrial fibrillation and flutter, and for the chemical cardioversion to sinus rhythm from atrial fibrillation and flutter. more...

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The chemical name for dofetilide is N-- methanesulphonamide. It is marketed under the trade name Tikosyn® by Pfizer, and is available in the United States in capsules containing 125, 250, and 500 µg of dofetilide. Due to the pro-arrhythmic potential of dofetilide, it is only available by prescription by physicians who have undergone specific training in the risks of treatment with dofetilide. In addition, it is only available by mail order or through specially trained local pharmacies to individuals who are prescribed dofetilide by a physician who is registered as being able to prescribe the pharmaceutical.

The elimination half-life of dofetilide is roughly 10 hours, however this is variable based on many physiologic factors (most significantly creatinine clearance), and ranges from 4.8 to 13.5 hours.

Mechanism of action

Dofetilide works by selectively blocking the rapid component of the delayed rectifier outward potassium current (IKr).

This causes prolongation of the effective refractory period of accessory pathways (both anterograde and retrograde conduction in the accessory pathway). It is this selective action on accessory pathways that makes dofetilide effective in the treatment of atrial fibrillation and flutter.

Dofetilide does not effect Vmax (The slope of the upstroke of phase 0 depolarization), conduction velocity, or the resting membrane potential.

There is a dose-dependant increase in the QT interval and the corrected QT interval (QTc). Because of this, many practitioners will initiate dofetilide therapy only on individuals under telemetry monitoring or if serial EKG measurements of QT and QTc can be performed.

Metabolism

A steady-state plasma level of dofetilide is achieved in 2-3 days.

80% of dofetilide is excreted by the kidneys, so the dose of dofetilide should be adjusted in individuals with renal insufficiency, based on creatinine clearance.

In the kidneys, dofetilide is eliminated via cation exchange (secretion). Agents that interfere with the renal cation exchange system, such as verapamil, cimetidine, hydrochlorothiazine, itraconazole, ketoconazole, prochlorperazine, and trimethoprim should not be administered to individuals taking dofetilide.

About 20 percent of dofetilide is metabolized in the liver via the CYP3A4 isoenzyme of the Cytochrome P450 enzyme system. Drugs that interfere with the activity of the CYP3A4 isoenzyme can increase serum dofetilide levels. If the renal cation exchange system is interfered with (as with the medications listed above), a larger percentage of dofetilide is cleared via the CYP3A4 isoenzyme system.

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Tikosyn
From OB/GYN News, 11/15/99 by Elizabeth Mechcatie

(dofetilide, Pfizer)

A class III antiarrhthymic for maintaining normal sinus rhythm (NSR), defined as a delay in time to recurrence of atrial fibrillation or atrial flutter (AF/AFL) in patients with AF/AFL lasting for more than 1 week, who have been converted to NSR. Also approved for conversion of AF/AFL to NSR.

* Recommended Dosage: Dosage individualized using a specific dosing algorithm, during a hospital stay of at least 3 days.

* Special Considerations: Only for people with highly symptomatic AF/AFL because of the risk of life-threatening ventricular arrhythmias. At a Food and Drug Administration hearing in January, Tikosyn investigator Dr. Jeremy Ruskin, who presented clinical data for Pfizer, said that the risk of Q-T interval prolongation and torsades de pointes (TdP) can be minimized with inpatient initiation of treatment and the use of the dosing algorithm, which takes renal function into account. Tikosyn will be provided only to physicians and hospitals who participate in a program that teaches these principles. Contraindications include concomitant use with ketoconazole, verapamil, or cimetidine.

* Comment: In trials of 996 patients, about 10% of those on 500 [mu]g of Tikosyn per day and 30% of those on 1,000 [mu]g/day converted to NSR, vs. 1% of those on placebo. The probability of remaining in NSR 1 year later ranged from 58% to 66% and 37% to 51% of those on the higher and lower doses, respectively, vs. 21%-25% of those on placebo.

In studies of people with AF and other supraventricular arrhythmias on various Tikosyn doses, the TdP rate was 0.8%. TdP rates reported in the literature are 2% with quinidine, 1%-2% with procainamide, and 0.7% with amiodarone, according to Dr. Ruskin, director of the cardiac arrhythmia service, Massachusetts General Hospital, Boston.

COPYRIGHT 1999 International Medical News Group
COPYRIGHT 2004 Gale Group

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