BETAPACE AFTM is a medicine that is given to patients with atrial fibrillation (irregular heartbeats). Atrial fibrillation happens when certain parts of the heart (the chambers known as atria) beat too fast or irregularly. When this happens, your heart cannot pump blood through your body as well as it should. This may make you feel weak and tired, or get out of breath easily. You may get an uncomfortable feeling in your chest and "fluttering" or "palpitations." Atrial fibrillation can be changed back (converted) to normal heart rhythm by an electric shock or by using certain medicines. However, atrial fibrillation can return. BETAPACE AFTM may help your heart stay beating regularly for a longer period of time. This information about BETAPACE AFTM was developed to ensure that you and your doctor get the right information about your type of irregular heartbeats. Consult your doctor before you accept any other sotalol product that does not provide this patient information.
Who should not take BETAPACE AFTM?
BETAPACE AFTM is not for everyone with irregular heartbeats (atrial fibrillation). This is why you and your doctor need to discuss the benefits and risks of BETAPACE AFTM and whether your symptoms are troublesome enough for you to start taking BETAPACE AFTM.
Do not take BETAPACE AFTM if you:
have serious kidney problems or are on kidney dialysis;
have lung disease causing shortness of breath (such as asthma, chronic bronchitis or emphysema);
have symptoms of heart failure (such as shortness of breath when you exercise or are physically active and swelling of the ankles or legs);
have a very slow heart beat and do not have an implanted artificial pacemaker;
Taking certain other medicines with BETAPACE AFTM can increase the chance that you will get the dangerous abnormal heartbeat discussed in "What is the most important information I should know about BETAPACE AFTM? ". These include medicines used to treat abnormal heart rhythms and some other heart problems as well as medicines used to treat depression and other mental problems, gastroesophageal reflux nighttime heartburn, asthma and infections. Therefore, you should be sure to tell your health care provider about all prescription and non-prescription medicines you are taking, as well as vitamins, dietary supplements, and any natural or herbal remedies. In addition, tell your doctor about any problems you have with your heart or kidneys. If you are pregnant, you should know that there is no information about the safety of BETAPACE AFTM in pregnant women. Some reports indicate that BETAPACE AFTM is passed into breast milk. Women who are taking BETAPACE AFTM should not breast feed a child.
Your doctor will start you on BETAPACE AFTM in the hospital and will check your heart rhythm for the first 2 or more days of treatment. This will allow your doctor to find the right dose for you. Always take the exact amount your doctor prescribes. Never change your BETAPACE AFTM dose unless your doctor tells you to. Your doctor will do regular tests to check that the amount you're taking is still right for you.
Keep taking your BETAPACE AFTM until your doctor tells you to stop. Keep taking it even if you feel fine. However, never take an extra dose of BETAPACE AFTM even if you do not feel well. When it is time to stop taking BETAPACE AFTM, your doctor will give you instructions on how to gradually reduce your dose over a period of 1 to 2 weeks.
You may take BETAPACE AFTM with or without food. However, it is important to take BETAPACE AFTM at the same time every day. This gives your heart a steady supply of the medicine. It might be helpful to take BETAPACE AFTM at the same time as something you regularly do every day.
If you are taking an antacid containing aluminum or magnesium to treat heartburn or upset stomach wait at least 2 hours after your dose of BETAPACE AFTM before you take the antacid.
Never try to make up for a missed dose of BETAPACE AFTM. You could increase your chance of getting the different type of abnormal heartbeat. If you miss taking a dose of BETAPACE AFTM, just take your normal amount at the next scheduled time.
If you take more BETAPACE AFTM than you should have, call your doctor right away. If you cannot reach your doctor, go to the nearest hospital emergency room. Take your BETAPACE AFTM tablets with you to show to the doctor or nurse.
Certain other medicines taken with BETAPACE AFTM may increase the chance that you will get the dangerous abnormal heartbeat (see "Who should not take BETAPACE AFTM ?) Do not take BETAPACE AFTM with these medicines. Before you start taking BETAPACE AFTM tell your doctor about all prescription and non-prescription medicines you are taking (see also "Who should not take BETAPACE AFTM? "). Once you begin taking BETAPACE AFTM, do not start taking any new medicines until you check with your doctor.
Carry a list of all the medicines and supplements you take. If you have to go to the hospital or are treated by new or different health care providers, tell them you are taking BETAPACE AFTM and show them the list of other medicines you take. They need this information to make sure your medicines are safe to take at the same time.
Tell your doctor or dentist you are taking BETAPACE AFTM before you have an operation or dental surgery. BETAPACE AFTM can affect how well some anesthetics work.
BETAPACE AFTM''s most serious side effect, a different type of dangerous abnormal heartbeat, is discussed in "What is the most important information I should know about BETAPACE AFTM? ". Dangerous abnormal heartbeats happen rarely. But they can be serious and, in rare instances, can even cause death.
BETAPACE AFTM most common side effects are tiredness, slow rate, shortness of breath, and dizziness.
BETAPACE AFTM can also cause other side effects. If you are concerned about these or any other side effects, ask your doctor.
BETAPACE AFTM can help you best if you take it as your doctor has prescribed it.
Take your medicine every day as prescribed
Do not miss doses or take extra doses
Call your doctor right away if you feel new fast heartbeats with lightheadedness and fainting. These can be serious and in rare instances can even cause death.
Do not take BETAPACE AFTM if you have serious kidney problems, lung disease causing shortness of
breath, uncontrolled symptoms of heart failure.
Tell your doctor and pharmacist the name of all medications (prescription, non-prescription, and natural/herbal remedies) you are taking
Do not start taking any other medicines without telling your doctor
Go for all your regular checkups
Get your refills on time
Do not stop taking BETAPACE AFTM until your doctor tells you to stop.
This leaflet provides a summary of information about BETAPACE AFTM. Your doctor or pharmacist has a longer leaflet written for healthcare professionals that you can ask to read. BETAPACE AFTM was prescribed for your particular condition. Do not use it for another condition or give it to others.
BETAPACE AFTM, (sotalol hydrochloride), is an antiarrhythmic drug with Class II (beta- adrenoreceptor blocking) and Class III (cardiac action potential duration prolongation) properties. It is supplied as a white, capsule-shaped tablet for oral administration. Sotalol hydrochloride is a white, crystalline solid with a molecular weight of 308.8. It is hydrophilic, soluble in water, propylene glycol and ethanol, but is only slightly soluble in chloroform. Chemically, sotalol hydrochloride is d,l-N-[4-[l-hydroxy-2-[(l-methylethyl) amino]ethyl]phenyl]methane-sulfonamide monohydrochloride. The molecular formula is C12H20N2O3S *HCl and is represented by the following structural formula: CH3SO2NH3/4 to be inserted at time of printing 3/4CH(OH)-CH2NHCH(CH3)2 *HCl BETAPACE AFTM tablets contain the following inactive ingredients: microcrystalline cellulose, lactose, starch, stearic acid, magnesium stearate, and colloidal silicon dioxide.
Mechanism of Action: BETAPACE AFTM (sotalol hydrochloride) has both beta- adrenoreceptor blocking (Vaughan Williams Class II) and cardiac action potential duration prolongation (Vaughan Williams Class III) antiarrhythmic properties. BETAPACE AFTM (sotalol hydrochloride) is a racemic mixture of d- and l-sotalol. Both isomers have similar Class III antiarrhythmic effects, while the l-isomer is responsible for virtually all of the beta-blocking activity. The beta-blocking effect of sotalol is non-cardioselective, half maximal at about 80 mg/day and maximal at doses between 320 and 640 mg/day. Sotalol does not have partial agonist or membrane stabilizing activity. Although significant beta-blockade occurs at oral doses as low as 25 mg, significant Class III effects are seen only at daily doses of 160 mg and above.
Sotalol hydrochloride prolongs the plateau phase of the cardiac action potential in the isolated myocyte, as well as in isolated tissue preparations of ventricular or atrial muscle (Class III activity). In intact animals it slows heart rate, slows AV nodal conduction and increases the refractory periods of atrial and ventricular muscle and conduction tissue.
In man, the Class II (beta-blockade) electrophysiological effects of BETAPACE AFTM are manifested by increased sinus cycle length (slowed heart rate), decreased AV nodal conduction and increased AV nodal refractoriness. The Class III electrophysiological effects in man include prolongation of the atrial and ventricular monophasic action potentials, and effective refractory period prolongation of atrial muscle, ventricular muscle, and atrio-ventricular accessory pathways (where present) in both the anterograde and retrograde directions. With oral doses of 160 to 640 mg/day, the surface ECG shows dose-related mean increases of 40-100 msec in QT and 10-40 msec in QTc. In a study of patients with atrial fibrillation (AFIB)/flutter (AFIB/AFL) receiving three different oral doses of BETAPACE AFTM given q12h (or q24h in patients with a reduced creatinine clearance), mean increases in QT intervals measured from 12-lead ECGs of 25 msec, 40 msec and 54 msec were found in the 80 mg, 120 mg and 160 mg dose groups, respectively. (See WARNINGS for description of relationship between QTc and torsade de pointes type arrhythmias.) No significant alteration in QRS interval is observed. In a small study (n=25) of patients with implanted defibrillators treated concurrently with sotalol the average defibrillatory threshold was 6 joules (range 2-15 joules) compared to a mean of 16 joules for a non-randomized comparative group primarily receiving amiodarone. In a dose-response trial comparing three dose levels of BETAPACE AFTM, 80 mg, 120 mg, and 160 mg with placebo given q12h (or q24h in patients with a reduced renal creatinine clearance) for the prevention of recurrence of symptomatic atrial fibrillation (AFIB)/flutter (AFL), the mean ventricular rate during recurrence of AFIB/AFL was 125, 107, 110 and 99 beats/min in the placebo, 80 mg, 120 mg and 160 mg dose groups, respectively (p<0.017 for each sotalol dose group versus placebo). In another placebo controlled trial in which BETAPACE AFTM was titrated to a dose between 160 and 320 mg/day in patients with chronic AFIB, the mean ventricular rate during recurrence of AFIB was 107 and 84 beats/min in the placebo and BETAPACE AFTM groups, respectively (p<0.001) .
: In a study of systemic hemodynamic function measured invasively in 12 patients with a mean LV ejection fraction of 37% and ventricular tachycardia (9 sustained and 3 non-sustained), a median dose of 160 mg twice daily of sotalol produced a 28% reduction in heart rate and a 24% decrease in cardiac index at 2 hours post dosing at steady-state. Concurrently, systemic vascular resistance and stroke volume showed non-significant increases of 25% and 8%, respectively. Pulmonary capillary wedge pressure increased significantly from 6.4 mmHg to 11.8 mmHg in the 11 patients
who completed the study. One patient was discontinued because of worsening congestive heart failure. Mean arterial pressure, mean pulmonary artery pressure and stroke work index did not significantly change. Exercise and isoproterenol induced tachycardia are antagonized by sotalol, and total peripheral resistance increases by a small amount. In hypertensive patients, sotalol produces significant reductions in both systolic and diastolic blood pressures. Although sotalol is usually well-tolerated hemodynamically, caution should be exercised in patients with marginal cardiac compensation as deterioration in cardiac performance may occur. (See WARNINGS: Congestive Heart Failure. ).
BETAPACE AFTM has been studied in patients with symptomatic AFIB/AFL in two principal studies, one in patients with primarily paroxysmal AFIB/AFL, the other in patients with primarily chronic AFIB. In one study, a U.S. multicenter, randomized, placebo-controlled, double-blind, dose- response trial of patients with symptomatic primarily paroxysmal AFIB/AFL, three fixed dose levels of BETAPACE AFTM (80 mg, 120 mg and 160 mg) twice daily and placebo were compared in 253 patients. In patients with reduced creatinine clearance (40-60 mL/min) the same doses were given once daily. Patients were not randomized for the following reasons: QT > 450 msec; creatinine clearance < 40 mL/min; intolerance to beta-blockers; bradycardia-tachycardia syndrome in the absence of an implanted pacemaker; AFIB/AFL was asymptomatic or was associated with syncope, embolic CVA or TIA; acute myocardial infarction within the previous 2 months; congestive heart failure; bronchial asthma or other contraindications to beta-blocker therapy; receiving potassium losing diuretics without potassium replacement or without concurrent use of ACE- inhibitors; uncorrected hypokalemia (serum potassium < 3.5 meq/L) or hypomagnesiemia (serum magnesium < 1.5 meq/L); received chronic oral amiodarone therapy for > 1 month within previous12 weeks; congenital or acquired long QT syndromes; history of torsade de pointes with other antiarrhythmic agents which increase the duration of ventricular repolarization; sinus rate < 50 bpm during waking hours; unstable angina pectoris; receiving treatment with other drugs that prolong the QT interval; and AFIB/AFL associated with the Wolff-Parkinson-White (WPW) syndrome. If the QT interval increased to 3 520 msec (or JT 3 430 msec if QRS > 100 msec) the drug was discontinued. The patient population in this trial was 64% male, and the mean age was 62 years. No structural heart disease was present in 43% of the patients . Doses were administered once daily in 20% of the patients because of reduced creatinine clearance. BETAPACE AFTM was shown to prolong the time to the first symptomatic, ECG- documented recurrence of AFIB/AFL, as well as to reduce the risk of such recurrence at both 6 and 12 months. The 120 mg dose was more effective than 80 mg, but 160 mg did not appear to have an added benefit. Note that these doses were given twice or once daily, depending on renal function. The results are shown in Figure 1 and Tables 1 and 2.
Figure 1: Study 1 - Time to First ECG-Documented Recurrence of Symptomatic AFIB/AFL Since Randomization
P-value (Betapace AFTM vs. Placebo)
Log-Rank
Recurrence - Free Survival
0.325
0.018
0.029
0.6
160mg 120mg
80mg Placebo
0.1
0 30 60 90 120 150 180 210
240 270 300 330 360
Time (Days)
Table 1: Study 1 - Patient Status At 12 Months | ||||
|---|---|---|---|---|
| Placebo | Betapace AF Dose | |||
| 80 mg | 120 mg | 160 mg | ||
| Randomized | 69 | 59 | 63 | 62 |
| On treatment in NSR at 12 months without recurrence a | 23% | 22% | 29% | 23% |
| Recurrence a , b | 67% | 58% | 49% | 42% |
| D/C for AEs | 6% | 12% | 18% | 29% |
a
Symptomatic AFIB/AFL
b
Efficacy endpoint of Study 1; study treatment stopped
Please note that columns do not add up to 100% due to discontinuations (D/C) for "other" reasons.
Table 2: Study 1 - Median Time to Recurrence of Symptomatic AFIB/AFL and Relative Risk (vs. Placebo) at 12 Months | ||||
|---|---|---|---|---|
| Placebo | Betapace AF Dose | |||
| 80 mg | 120 mg | 160 mg | ||
| p-value vs placebo | p=0.325 | p=0.018 | p=0.029 | |
| Relative Risk (RR) to placebo | 0.81 | 0.59 | 0.59 | |
| Median time to recurrence (days) | 27 | 106 | 229 | 175 |
Discontinuation because of adverse events was dose related. In a second multicenter, randomized, placebo-controlled, double-blind study of 6 months duration in 232 patients with chronic AFIB, BETAPACE AFTM was titrated over a dose range from 80 mg/day to 320 mg/day. The patient population of this trial was 70% male with a mean age of 65 years. Structural heart disease was present in 49% of the patients. All patients had chronic AFIB for >2 weeks but < 1 year at entry with a mean duration of 4.1 months. Patients were excluded if they had significant electrolyte imbalance, QTc >460 msec, QRS >140 msec, any degree of AV block or functioning pacemaker, uncompensated cardiac failure, asthma, significant renal disease (estimated creatinine clearance <50 mL/min), heart rate < 50 bpm, myocardial infarction or open heart surgery in past 2 months, unstable angina, infective endocarditis, active pericarditis or myocarditis, 3 3 DC cardioversions in the past, medications that prolonged QT interval, and previous amiodarone treatment. After successful cardioversion patients were randomized to receive placebo (n=114) or BETAPACE AFTM (n=118) at a starting dose of 80 mg twice daily. If the initial dose was not tolerated it was decreased to 80 mg once daily, but if it was tolerated it was increased to 160 mg twice daily. During the maintenance period 67% of treated patients received a dose of 160 mg twice daily, and the remainder received doses of 80 mg once daily (17%) and 80 mg twice daily (16%). Figure 2 and Tables 3 and 4 show the results of the trial. There was a longer time to ECG-documented recurrence of AFIB and a reduced risk of recurrence at 6 months compared to placebo.
Figure 2: Study 2 - Time to First ECG-Documented Recurrence of Symptomatic AFIB/AFL/Death Since Randomization
Recurrence - Free Survival
P-value (Betapace AFTM vs. Placebo) Log-Rank
0.002
Betapace AFTM
Placebo
0.3
0.2
0.1
0 30 60 90 120 150
180 *
* End of study
Table 3: Study 2 - Patient Status At 6 Months | ||
|---|---|---|
| Betapace AF | Placebo | |
| Randomized | 118 | 114 |
| On treatment in NSR at 6 months without recurrence a | 45% | 29% |
| Recurrence a , b | 49% | 67% |
| D/C for AEs | 6% | 3% |
| Death | 1% | |
a
Symptomatic or asymptomatic AFIB/AFL
b
Efficacy endpoint of Study 2; study treatment stopped
Table 4: Study 2 - Median Time to Recurrence of Symptomatic AFIB/AFL/Death and Relative Risk (vs. Placebo) at 6 Months
| Betapace AF | Placebo | |
| p-value vs placebo | p=0.002 | |
| Relative Risk (RR) to placebo | 0.55 | |
| Median time to recurrence (days) | >180 | 44 |
In a multicenter double-blind randomized study reported by D. Julian et al, the effect of sotalol 320 mg once daily was compared with that of placebo in 1456 patients (randomized 3:2, sotalol to placebo) surviving an acute myocardial infarction (MI). Treatment was started 5-14 days after infarction. Patients were followed for 12 months. The mortality rate was 7.3% in the sotalol group and 8.9% in the placebo group, not a statistically significant difference. Although the results do not show evidence of a benefit of sotalol in this population, they do not show an added risk in post MI patients receiving sotalol.
In healthy subjects, the oral bioavailability of sotalol is 90-100%. After oral administration, peak plasma concentrations are reached in 2.5 to 4 hours, and steady-state plasma concentrations are attained within 2-3 days (i.e., after 5-6 doses when administered twice daily). Over the dosage range 160-640 mg/day sotalol displays dose proportionality with respect to plasma concentrations. Distribution occurs to a central (plasma) and to a peripheral compartment, with a mean elimination half-life of 12 hours. Dosing every 12 hours results in trough plasma concentrations which are
approximately one-half of those at peak. Sotalol does not bind to plasma proteins and is not metabolized. Sotalol shows very little intersubject variability in plasma levels. The pharmacokinetics of the d and l enantiomers of sotalol are essentially identical. Sotalol crosses the blood brain barrier poorly. Excretion is predominantly via the kidney in the unchanged form, and therefore lower doses are necessary in conditions of renal impairment (see DOSAGE AND ADMINISTRATION). Age per se does not significantly alter the pharmacokinetics of sotalol , but impaired renal function in geriatric patients can increase the terminal elimination half-life, resulting in increased drug accumulation. The absorption of sotalol was reduced by approximately 20% compared to fasting when it was administered with a standard meal. Since sotalol is not subject to first-pass metabolism, patients with hepatic impairment show no alteration in clearance of sotalol.
BETAPACE AFTM is indicated for the maintenance of normal sinus rhythm [delay in time to recurrence of atrial fibrillation/atrial flutter (AFIB/AFL)] in patients with symptomatic AFIB/AFL who are currently in sinus rhythm. Because BETAPACE AFTM can cause life- threatening ventricular arrhythmias, it should be reserved for patients in whom AFIB/AFL is highly symptomatic. Patients with paroxysmal AFIB whose AFIB/AFL that is easily reversed (by Valsalva maneuver, for example) should usually not be given BETAPACE AFTM (See WARNINGS). In general, antiarrhythmic therapy for AFIB/AFL aims to prolong the time in normal sinus rhythm. Recurrence is expected in some patients (See CLINICAL STUDIES). Sotalol is also indicated for the treatment of documented life-threatening ventricular arrhythmias and is marketed under the brand name BETAPACEO (sotalol hydrochloride). BETAPACEO however, must not be substituted for BETAPACE AFTM because of significant differences in labeling (i.e. patient package insert, dosing administration and safety information).
BETAPACE AFTM (sotalol hydrochloride) is contraindicated in patients with sinus bradycardia (< 50 bpm during waking hours), sick sinus syndrome or second and third degree AV block (unless a functioning pacemaker is present), congenital or acquired long QT syndromes, baseline QT interval > 450 msec, cardiogenic shock, uncontrolled heart failure, hypokalemia (< 4 mEq/L), creatinine clearance < 40 mL/min, bronchial asthma and previous evidence of hypersensitivity to sotalol.
Proarrhythmia in Atrial Fibrillation/Atrial Flutter Patients:
In eight controlled trials of
patients with AFIB/AFL and other supraventricular arrhythmias (N=659) there were four cases of torsade de pointes reported (0.6%) during the controlled phase of treatment with BETAPACE AFTM. The incidence of torsade de pointes was significantly lower in those patients receiving total daily doses of 320 mg or less (0.3%), as summarized in Table 5 below. Both patients who had torsade de pointes in the group receiving > 320 mg/day were receiving 640 mg/day. In the group receiving 320 mg daily, one case of TdP occurred at a daily dose of 320 mg on day 4 of treatment and one case occurred on a daily dose of 160 mg on day 1 of treatment. Table 5
Incidence of Torsade de Pointes in Controlled Trials of AFIB and Other Supraventricular Arrhythmias
______________ BETAPACE AFTM (Daily Dose)__________ | |||||
|---|---|---|---|---|---|
| Any Dose | >320 mg/day | PS 320 mg/day | PS 240 mg/day | Placebo | |
| (N=659) | (N=62) | (N=597) | (N=340) | (N=358) | |
| n(%) | n (%) | n(%) | n(%) | n(%) | |
| Torsade de pointes | 4(0.6%) | 2 (3.2%) | 2 (0.3%) | 1(0.3%) | 0 |
Prolongation of the QT interval is dose related, increasing from baseline an average of 25, 40, and 50 msec in the 80, 120, and 160 mg groups, respectively, in the clinical dose- response study. In this clinical trial BETAPACE AFTM treatment was not initiated if the QT interval was greater than 450 msec and during therapy the dose was reduced or discontinued if the QT interval was 3 520 msec. Experience in patients with ventricular arrhythmias is also pertinent to the risk of torsade de pointes in patients with AFIB/AFL (see below).
hydrochloride) Package Insert].
In patients with a history of sustained ventricular
tachycardia, the incidence of torsade de pointes during sotalol treatment was 4% and worsened VT in about 1%; in patients with other less serious ventricular arrhythmias the incidence of torsade de pointes was 1% and new or worsened VT in about 0.7%. Additionally, in approximately 1% of patients, deaths were considered possibly drug related; such cases, although difficult to evaluate, may have been associated with proarrhythmic events. Torsade de pointes arrhythmias in patients with VT/VF were dose related, as was the prolongation of QT (QTc) interval, as shown in Table 6 below. Table 6
Percent Incidence of Torsade de Pointes and Mean QTc Interval by Dose For Patients With Sustained VT/VF
Daily Dose (mg) Incidence of Torsade de pointes Mean QTc * | |||
|---|---|---|---|
| (msec) | |||
| 80 | 0 | (69) | 463 (17) |
| 160 | 0.5 | (832) | 467 (181) |
| 320 | 1.6 | (835) | 473 (344) |
| 480 | 4.4 | (459) | 483 (234) |
| 640 | 3.7 | (324) | 490 (185) |
| >640 | 5.8 | (103) | 512 (62) |
( ) Number of patients assessed
*highest on-therapy value
Table 7below relates the incidence of torsade de pointes to on-therapy QTc and change in QTc from baseline. It should be noted, however, that the highest on-therapy QTc was in many cases the one obtained at the time of the torsade de pointes event, so that the table overstates the predictive value of a high QTc. Table 7
Relationship Between QTc Interval Prolongation and Torsade de Pointes
On-Therapy QTc Interval (msec)
Incidence of Torsade de pointes
Change in QTc Interval From Baseline (msec)
Incidence of Torsade de pointes
less than 500 1.3% (1787) less than 65 1.6% (1516)
500-525 3.4% (236) 65-80 3.2% (158)
525-550 5.6% (125) 80-100 4.1% (146)
>550 10.8% (157) 100-130
5.2% (115)
7.1% (99)
( ) Number of patients assessed
In addition to dose and presence of sustained VT, other risk factors for torsade de pointes were gender (females had a higher incidence), excessive prolongation of the QTc interval and history of cardiomegaly or congestive heart failure. Patients with sustained ventricular tachycardia and a history of congestive heart failure appear to have the highest risk for serious proarrhythmia (7%). Of the ventricular arrhythmia patients experiencing torsade de pointes, approximately two-thirds spontaneously reverted to their baseline rhythm. The others were either converted electrically (D/C cardioversion or overdrive pacing) or treated with other drugs (see OVERDOSAGE). It is not possible to determine whether some sudden deaths represented episodes of torsade de pointes, but in some instances sudden death did follow a documented episode of torsade de pointes. Although sotalol therapy was discontinued in most patients experiencing torsade de pointes, 17% were continued on a lower dose.
The use of BETAPACE AFTM in conjunction with other drugs that prolong the QT interval has not been studied and is not recommended. Such drugs include many antiarrhythmics, some phenothiazines, cisapride, bepridil, tricyclic antidepressants, and certain oral macrolides. Class I or Class III antiarrhythmic agents should be withheld for at least three half-lives prior to dosing with BETAPACE AFTM. In clinical trials, BETAPACE AFTM was not administered to patients previously treated with oral amiodarone for >1 month in the previous three months. Class Ia antiarrhythmic drugs, such as disopyramide, quinidine and procainamide and other Class III drugs (e.g., amiodarone) are not recommended as concomitant therapy with BETAPACE AFTM, because of their potential to prolong refractoriness (see WARNINGS). There is only limited experience with the concomitant use of Class Ib or Ic antiarrhythmics.
Sympathetic stimulation is necessary in supporting circulatory function in congestive heart failure, and beta-blockade carries the potential hazard of further depressing myocardial contractility and precipitating more severe failure. In patients who have heart failure controlled by digitalis and/or diuretics,
BETAPACE AFTM should be administered cautiously. Both digitalis and sotalol slow AV conduction. As with all beta-blockers, caution is advised when initiating therapy in patients with any evidence of left ventricular dysfunction. In a pooled data base of four placebo-controlled AFIB/AFL and PSVT studies, new or worsening CHF occurred during therapy with BETAPACE AFTM in 5 (1.2%) of 415 patients. In these studies patients with uncontrolled heart failure were excluded (i.e. NYHA Functional Classes III or IV). In other premarketing sotalol studies, new or worsened congestive heart failure (CHF) occurred in 3.3% (n=3257) of patients and led to discontinuation in approximately 1% of patients receiving sotalol. The incidence was higher in patients presenting with sustained ventricular tachycardia/fibrillation (4.6%, n=1363), or a prior history of heart failure (7.3%, n=696). Based on a life-table analysis, the one-year incidence of new or worsened CHF was 3% in patients without a prior history and 10% in patients with a prior history of CHF. NYHA Classification was also closely associated to the incidence of new or worsened heart failure while receiving sotalol (1.8% in 1395 Class I patients, 4.9% in 1254 Class II patients and 6.1% in 278 Class III or IV patients). Electrolyte Disturbances: BETAPACE AFTM should not be used in patients with hypokalemia or hypomagnesemia prior to correction of imbalance, as these conditions can exaggerate the degree of QT prolongation, and increase the potential for torsade de pointes. Special attention should be given to electrolyte and acid-base balance in patients experiencing severe or prolonged diarrhea or patients receiving concomitant diuretic drugs. Bradycardia/Heart Block:. The incidence of bradycardia (as determined by the investigators) in the supraventricular arrhythmia population treated with BETAPACE AFTM (N = 415) was 13%, and led to discontinuation in 2.4% of patients. Bradycardia itself increases the risk of torsade de pointes.
Sotalol has been used in a controlled trial following an acute myocardial infarction without evidence of increased mortality (see Safety in Patients with Structural Heart Disease). Although specific studies of its use in treating atrial arrhythmias after infarction have not been conducted, the usual precautions regarding heart failure, avoidance of hypokalemia, bradycardia or prolonged QT interval apply.
Hypersensitivity to catecholamines has been observed in patients withdrawn from beta-blocker therapy. Occasional cases of exacerbation of angina pectoris, arrhythmias and, in some cases, myocardial infarction have been reported after abrupt discontinuation of beta-blocker therapy. Therefore, it is prudent when discontinuing
chronically administered BETAPACE AFTM, particularly in patients with ischemic heart disease, to carefully monitor the patient and consider the temporary use of an alternate beta-blocker if appropriate. If possible, the dosage of BETAPACE AFTM should be gradually reduced over a period of one to two weeks. If angina or acute coronary insufficiency develops, appropriate therapy should be instituted promptly. Patients should be warned against interruption or discontinuation of therapy without the physician's advice. Because coronary artery disease is common and may be unrecognized in patients receiving BETAPACE AFTM, abrupt discontinuation in patients with arrhythmias may unmask latent coronary insufficiency.
(e.g., chronic bronchitis and emphysema):
BETA-BLOCKERS. It is prudent, if BETAPACE AFTM (sotalol hydrochloride) is to be administered, to use the smallest effective dose, so that inhibition of bronchodilation produced by endogenous or exogenous catecholamine stimulation of beta2 receptors may be minimized.
While taking beta-blockers, patients with a history of anaphylactic reaction to a variety of allergens may have a more severe reaction on repeated challenge, either accidental, diagnostic or therapeutic. Such patients may be unresponsive to the usual doses of epinephrine used to treat the allergic reaction.
The management of patients undergoing major surgery who are being treated with beta-blockers is controversial. Protracted severe hypotension and difficulty in restoring and maintaining normal cardiac rhythm after anesthesia have been reported in patients receiving beta-blockers.
Diabetes: In patients with diabetes (especially labile diabetes) or with a history of episodes of spontaneous hypoglycemia, BETAPACE AFTM should be given with caution since beta-blockade may mask some important premonitory signs of acute hypoglycemia; e.g., tachycardia. Sick Sinus Syndrome: BETAPACE AFTM should be used only with extreme caution in patients with sick sinus syndrome associated with symptomatic arrhythmias, because it may cause sinus bradycardia, sinus pauses or sinus arrest. In patients with AFIB and sinus node dysfunction, the risk of torsade de pointes with BETAPACE AFTM therapy is increased, especially after cardioversion. Bradycardia following cardioversion in these patients is associated with QTc interval prolongation which is augmented due to the reverse use dependence of the Class III effects of BETAPACE AFTM. Patients with AFIB/AFL associated with the sick sinus syndrome may be treated with BETAPACE AFTM if they have an implanted pacemaker for control of bradycardia symptoms.
Beta-blockade may mask certain clinical signs (e.g., tachycardia) of hyperthyroidism. Patients suspected of developing thyrotoxicosis should be managed carefully to avoid abrupt withdrawal of beta-blockade which might be followed by an exacerbation of symptoms of hyperthyroidism, including thyroid storm. The beta-blocking
effects of BETAPACE AFTM may be useful in controlling heart rate in AFIB associated with thyrotoxicosis but no study has been conducted to evaluate this.
BETAPACE AF
Please refer to the patient package insert.
Medications and Supplements
: Assessment of patients' medication history should
include all over-counter, prescription and herbal/natural preparations with emphasis on preparations that may affect the pharmacodynamics of BETAPACE AFTM such as other cardiac antiarrhythmic drugs, some phenothiazines, cisapride, bepridil, tricyclic antidepressants and oral macrolides (see WARNINGS and Use With Drugs That Prolong QT Interval and Antiarrhythmic Agents). Patients should be instructed to notify their health care providers of any change in over-the-counter, prescription or supplement use. If a patient is hospitalized or is prescribed a new medication for any condition, the patient must inform the health care provider of ongoing BETAPACE AFT M therapy. Patients should also check with their health care and/or pharmacist prior to taking a new over-the-counter medicine.
Electrolyte Imbalance
: If patients experience symptoms that may be associated with
altered electrolyte balance, such as excessive or prolonged diarrhea, sweating, or vomiting, or loss of appetite or thirst, these conditions should be immediately reported to their health care provider.
Dosing Schedule
: Patients should be instructed NOT to double the next dose if a dose is
missed. The next dose should be taken at the usual time.
:
involving alteration of metabolism of sotalol are not expected because hepatic CYP450
metabolizing enzymes are not involved in the disposition of sotalol. Sotalol is primarily
eliminated by renal excretion; therefore, drugs that are metabolized by CYP450 are not
expected to alter the pharmacokinetics of sotalol.
Proarrhythmic events were more common in sotalol treated patients also receiving digoxin; it is not clear whether this represents an interaction or is related to the presence of CHF, a known risk factor for proarrhythmia, in the patients receiving digoxin.
Calcium blocking drugs: BETAPACE AFTM should be administered with caution in conjunction with calcium blocking drugs because of possible additive effects on atrioventricular conduction or ventricular function. Additionally, concomitant use of these drugs may have additive effects on blood pressure, possibly leading to hypotension.
Concomitant use of catecholamine-depleting drugs, such as reserpine and guanethidine, with a beta-blocker may produce an excessive
reduction of resting sympathetic nervous tone. Patients treated with BETAPACE AFTM plus a catecholamine depletor should therefore be closely monitored for evidence of hypotension and or marked bradycardia which may produce syncope.
Hyperglycemia may occur, and the dosage of insulin or antidiabetic drugs may require adjustment. Symptoms of hypoglycemia may be masked.
Beta-agonists such as salbutamol, terbutaline and isoprenaline may have to be administered in increased dosages when used
concomitantly with BETAPACE AFTM.
Beta-blocking drugs may potentiate the rebound hypertension sometimes observed after discontinuation of clonidine; therefore, caution is advised when
discontinuing clonidine in patients receiving BETAPACE AFTM.
No pharmacokinetic interactions were observed with hydrochlorothiazide or warfarin.
Antacids: Administration of BETAPACE AFTM within 2 hours of antacids containing aluminum oxide and magnesium hydroxide should be avoided because it may result in a reduction in Cmax and AUC of 26% and 20%, respectively and consequently in a 25% reduction in the bradycardic effect at rest. Administration of the antacid two hours after BETAPACE AFTM has no effect on the pharmacokinetics or pharmacodynamics of sotalol.
The presence of sotalol in the urine may result in falsely elevated levels of urinary metanephrine when measured by fluorimetric or photometric methods. In screening patients suspected of having a pheochromocytoma and being treated with sotalol, a specific method, such as a high performance liquid chromatographic assay with solid phase extraction (e.g., J. Chromatogr. 385:241, 1987) should be employed in determining levels of catecholamines.
No evidence of carcinogenic potential was observed in rats during a 24-month study at 137-275 mg/kg/day (approximately 30 times the maximum recommended human oral dose (MRHD) as
mg/kg or 5 times the MRHD as mg/m2 ) or in mice, during a 24-month study at 4141- 7122 mg/kg/day (approximately 450-750 times the MRHD as mg/kg or 36-63 times the MRHD as mg/m2). Sotalol has not been evaluated in any specific assay of mutagenicity or clastogenicity. No significant reduction in fertility occurred in rats at oral doses of 1000 mg/kg/day (approximately 100 times the MRHD as mg/kg or 9 times the MRHD as mg/m2 ) prior to mating, except for a small reduction in the number of offspring per litter. Pregnancy Category B: Reproduction studies in rats and rabbits during organogenesis at 100 and 22 times the MRHD as mg/kg (9 and 7 times the MRHD as mg/m2), respectively, did not reveal any teratogenic potential associated with sotalol HCl. In rabbits, a high dose of sotalol HCl (160 mg/kg/day) at 16 times the MRHD as mg/kg (6 times the MRHD as mg/m2) produced a slight increase in fetal death likely due to maternal toxicity. Eight times the maximum dose (80 mg/kg/day or 3 times the MRHD as mg/m2 ) did not result in an increased incidence of fetal deaths. In rats, 1000 mg/kg/day sotalol HCl, 100 times the MRHD (18 times the MRHD as mg/m2 ), increased the number of early resorptions, while at 14 times the maximum dose (2.5 times the MRHD as mg/m2), no increase in early resorptions was noted. However, animal reproduction studies are not always predictive of human response. Although there are no adequate and well-controlled studies in pregnant women, sotalol HCl has been shown to cross the placenta, and is found in amniotic fluid. There has been a report of subnormal birth weight with sotalol. Therefore, BETAPACE AFTM should be used during pregnancy only if the potential benefit outweighs the potential risk.
Nursing Mothers:
Sotalol is excreted in the milk of laboratory animals and has been
reported to be present in human milk. Because of the potential for adverse reactions in nursing infants from BETAPACE AFTM, a decision should be made whether to discontinue nursing or to discontinue the drug, taking into account the importance of the drug to the mother. Pediatric Use: The safety and effectiveness of BETAPACE AFTM in children have not been established.
Adverse events that are clearly related to BETAPACE AFTM are those which are typical of its Class II (beta-blocking) and Class III (cardiac action potential duration prolongation) effects. The common documented beta-blocking adverse events (bradycardia, dyspnea, and fatigue) and Class III effects (QT interval prolongation) are dose related. In a pooled clinical trial population consisting of four placebo-controlled studies with 275 patients with AFIB/AFL treated with 160-320 mg doses of BETAPACE AFTM , the following adverse events were reported at a rate of 2% or more in the 160-240 mg treated patients and greater than the rate in placebo patients (see Table 8). The data are presented by incidence of events in the BETAPACE AFTM and placebo groups by body system and daily dose. No significant irreversible non-cardiac end-organ toxicity was observed. Table 8
Incidence (%) of Common Adverse Events (32% in the 160 -240 mg group and more frequent than on placebo) in Four Placebo-Controlled Studies of Patients with AFIB/AFL
Body System/
Adverse Event (Preferred Term)
Placebo
Betapace AFTM
Total Daily Dose
CARDIOVASCULAR
N=282
160 - 240
N=153
>240 - 320
N=122
Abnormality ECG 0.4 3.3 2.5
Angina Pectoris 1.1 2.0 1.6
Bradycardia 2.5 13.1 12.3
Chest pain Cardiac/Non-Anginal 4.6 4.6 2.5
Disturbance Rhythm Atrial 2.1 2.0 1.6
Disturbance Rhythm Subjective 9.9 9.8 7.4
GASTROINTESTINAL
| Appetite Decreased | 0.4 | 2.0 | 1.6 |
| Diarrhea | 2.1 | 5.2 | 5.7 |
| Distention Abdomen | 0.4 | 0.7 | 2.5 |
| Dyspepsia/Heartburn | 1.8 | 2.0 | 2.5 |
| Nausea/Vomiting | 5.3 | 7.8 | 5.7 |
| Pain Abdomen | 2.5 | 3.9 | 2.5 |
GENERAL
| Fatigue | 8.5 | 19.6 | 18.9 |
| Fever | 0.7 | 0.7 | 3.3 |
| Hyperhidrosis | 3.2 | 5.2 | 4.9 |
| Influenza | 0.4 | 2.0 | 0.8 |
| Sensation Cold | 0.7 | 2.0 | 2.5 |
| Weakness | 3.2 | 5.2 | 4.9 |
| MUSCULOSKELETAL/CONNECTIVE TISSUE | |||
| Pain Chest Musculoskeletal | 1.4 | 2.0 | 2.5 |
| Pain Musculoskeletal | 2.8 | 2.6 | 4.1 |
| NERVOUS SYSTEM | |||
| Dizziness | 12.4 | 16.3 | 13.1 |
| Headache | 5.3 | 3.3 | 11.5 |
| Insomnia | 1.1 | 2.6 | 4.1 |
| RESPIRATORY | |||
| Cough | 2.5 | 3.3 | 2.5 |
| Dyspnea | 7.4 | 9.2 | 9.8 |
| Infection Upper Respiratory | 1.1 | 2.6 | 3.3 |
| Tracheobronchitis | 0.7 | 0.7 | 3.3 |
SPECIAL SENSES
Disturbance Vision 0.7 2.6 0.8
Overall, discontinuation because of unacceptable adverse events was necessary in 17% of the patients, and occurred in 10% of patients less than two weeks after starting treatment. The most common adverse events leading to discontinuation of BETAPACE AFTM were: fatigue 4.6%, bradycardia 2.4%, proarrhythmia 2.2%, dyspnea 2%, and QT interval prolongation 1.4%. In clinical trials involving 1292 patients with sustained VT/VF, the common adverse events (occurring in 3 2% of patients) were similar to those described for the AFIB/AFL population. Occasional reports of elevated serum liver enzymes have occurred with sotalol therapy but no cause and effect relationship has been established. One case of peripheral neuropathy, which resolved on discontinuation of sotalol and recurred when the patient was rechallenged with the drug, was reported in an early dose tolerance study. Elevated blood glucose levels and increased insulin requirements can occur in diabetic patients.
Potential Adverse Effects
Foreign marketing experience with sotalol hydrochloride shows an adverse experience profile similar to that described above from clinical trials. Voluntary reports since introduction also include rare reports of: emotional lability, slightly clouded sensorium, incoordination, vertigo, paralysis, thrombocytopenia, eosinophilia, leukopenia, photosensitivity reaction, fever, pulmonary edema, hyperlipidemia, myalgia, pruritus, alopecia. The oculomucocutaneous syndrome associated with the beta-blocker practolol has not been associated with BETAPACE AFTM during investigational use and foreign marketing experience.
Intentional or accidental overdosage with sotalol has rarely resulted in death.
The most common signs to be expected are bradycardia, congestive heart failure, hypotension, bronchospasm and hypoglycemia. In cases of massive intentional overdosage (2-16 grams) of sotalol the following clinical findings were seen: hypotension, bradycardia, cardiac asystole, prolongation of QT interval, torsade de pointes, ventricular tachycardia, and premature ventricular
complexes. If overdosage occurs, therapy with BETAPACE AFTM should be discontinued and the patient observed closely. Because of the lack of protein binding, hemodialysis is useful for reducing sotalol plasma concentrations. Patients should be carefully observed until QT intervals are normalized and the heart rate returns to levels >50 bpm. The occurrence of hypotension following an overdose may be associated with an initial slow drug elimination phase (half life of 30 hours) thought to be due to a temporary reduction of renal function caused by the hypotension. In addition, if required, the following therapeutic measures are suggested:
Bradycardia or
Atropine, another anticholinergic drug, a beta-adrenergic agonist or
Cardiac Asystole:
transvenous cardiac pacing.
Heart Block:
(second and third degree) transvenous cardiac pacemaker.
Hypotension:
(depending on associated factors) epinephrine rather than
isoproterenol or norepinephrine may be useful.
Bronchospasm:
Aminophylline or aerosol beta-2-receptor stimulant.
Torsade de pointes:
DC cardioversion, transvenous cardiac pacing, epinephrine,
magnesium sulfate.
Therapy with BETAPACE AFTM must be initiated (and, if necessary, titrated) in a setting that provides continuous electrocardiographic (ECG) monitoring and in the presence of personnel trained in the management of serious ventricular arrhythmias. Patients should continue to be monitored in this way for a minimum of 3 days on the maintenance dose. In addition, patients should not be discharged within 12 hours of electrical or pharmacological conversion to normal sinus rhythm.
The QT interval is used to determine patient eligibility for BETAPACE AFTM treatment and for monitoring safety during treatment. The baseline QT interval must be PS450 msec in order for a patient to be started on BETAPACE AFTM therapy. During initiation and titration, the QT interval should be monitored 2-4 hours after each dose. If the QT interval prolongs to 500 msec or greater, the dose must be reduced or the drug discontinued.
The dose of BETAPACE AF TM must be individualized according to creatinine clearance. In patients with a creatinine clearance > 60 mL/min BETAPACE AFTM is administered twice daily (BID) while in those with a creatinine clearance between 40 and 60 mL/min, the dose is administered once daily (QD). In patients with a creatinine clearance less than 40 mL/min BETAPACE AFTM is contraindicated. The
recommended initial dose of BETAPACE AFTM is 80 mg and is initiated as shown in the dosing algorithm described below. The 80 mg dose can be titrated upward to 120 mg during initial hospitalization or after discharge on 80 mg in the event of recurrence, by rehospitalization and repeating the same steps used during the initiation of therapy (see Upward Titration of Dose). Patients with atrial fibrillation should be anticoagulated according to usual medical practice. Hypokalemia should be corrected before initiation of BETAPACE AFTM therapy (see WARNINGS, Ventricular Arrhythmia). Patients to be discharged on BETAPACE AFTM therapy from an in-patient setting should have an adequate supply of BETAPACE AFTM to allow uninterrupted therapy until the patient can fill a BETAPACE AFTM prescription.
Step 1. Electrocardiographic assessment: Prior to administration of the first dose, the QT interval must be determined using an average of 5 beats. If the baseline QT is greater than 450 msec (JT 3 330 msec if QRS over 100 msec) , BETAPACE AFTM is contraindicated.
Calculation of creatinine clearance: Prior to the administration of the first dose, the patient's creatinine clearance should be calculatedusing the following formula:
creatinine clearance (male) = (140-age) x body weight in kg 72 x serum creatinine (mg/dL) creatinine clearance (female) = (140-age) x body weight in kg x 0.85 72 x serum creatinine (mg/dL) When serum creatinine is given in mmol/L, divide the value by 88.4 (1 mg/dL = 88.4
m
mol/L)
Step 3. Starting Dose: The starting dose of BETAPACE AFTM is 80 mg twice daily (BID) if the creatinine clearance is > 60 mL/min, and 80 mg once daily (QD) if the creatinine clearance is 40-60 mL/min. If the creatinine clearance is < 40 mL/min BETAPACE AFTM is contraindicated. Step 4. Administer the appropriate daily dose of BETAPACE AFTM and begin continuous ECG monitoring with QT interval measurements 2-4 hours after each dose.
If the 80 mg dose level is tolerated and the QT interval remains < 500 msec after at least 3 days (after 5 or 6 doses if patient receiving QD dosing), the patient can be discharged. Alternatively, during hospitalization, the dose can be increased to 120 mg bid and the patient followed for 3 days on this dose (followed for 5 or 6 doses if patient receiving QD doses).
The steps described above are summarized in the following
Place Patient on Telemetry
Check Baseline QT If QT > 450 msec
BETAPACE AF(tm) is CONTRAINDICATED
If QT PS 450 msec, proceed | ||
|---|---|---|
| Calculate Creatinine Clearance (Clcr) If Clcr is < 40 mL/min BETAPACE AF(tm) is CONTRAINDICATED If Clcr is 40-60 mL/min start BETAPACE AF(tm) 80 mg QD If Clcr is > 60 mL/min start BETAPACE AF(tm) 80 mg BID | ||
| Monitor QT 2-4 hours after each dose. If QT >= 500 msec discontinue BETAPACE AF(tm). If QT < 500 msec after 3 days (after 5th or 6th dose if patient receiving QD dosing) discharge patient on current treatment. Alternatively, during hospitalization, the dose can be increased to 120 mg bid and the patient followed for 3 days on this dose (followed for 5 or 6 doses if patient receiving QD doses). | ||
diagram:
If the 80 mg dose level (given BID or QD depending upon the creatinine clearance) does not reduce the frequency of relapses of AFIB/AFL and is tolerated without excessive QT interval prolongation (i.e. 3 520 msec), the dose level may be increased to 120 mg (BID or QD depending upon the creatinine clearance). As proarrhythmic events can occur not only at initiation of therapy, but also with each upward dosage adjustment, Steps 2 through 5 used during initiation of BETAPACE AFTM therapy should be followed when increasing the dose level. In the U.S. multicenter dose-response study, the 120 mg dose (BID or QD) was found to be the most effective in prolonging the time to ECG documented symptomatic recurrence of AFIB/AFL. If the 120 mg dose does not reduce the frequency of early relapse of AFIB/AFL and is tolerated without excessive QT interval prolongation (3520 msec), an increase to 160 mg (BID or QD depending upon the creatinine clearance can be considered. Steps 2 through 5 used during the initiation of therapy should be used again to introduce such an increase.
Renal function and QT should be re-evaluated regularly if medically warranted. If QT is 520 msec or greater (JT 430 msec or greater if QRS is > 100 msec), the dose of BETAPACE AFTM therapy should be reduced and patients should be carefully monitored until QT returns to less than 520 msec. If the QT interval is 3 520 msec while on the
lowest maintenance dose level (80 mg) the drug should be discontinued. If renal function deteriorates, reduce the daily dose in half by administering the drug once daily as described in
The maximum recommended dose in patients with a calculated creatinine clearance greater than 60 mL/min is 160 mg BID, doses greater than 160 mg BID have been associated with an increased incidence of torsade de pointes and are not recommended. A patient who misses a dose should NOT double the next dose. The next dose should be taken at the usual time.
Patients with a history of symptomatic AFIB/AFL who are currently receiving Betapace(r) for the maintenance of normal sinus rhythm must should be transferred to BETAPACE AFTM because of the significant differences in labeling (i.e., patient package insert, dosing administration, and safety information).
Before starting BETAPACE AFTM, previous antiarrhythmic therapy should generally be withdrawn under careful monitoring for a minimum of 2-3 plasma half-lives if the patient's clinical condition permits (see DRUG INTERACTIONS). Treatment has been initiated in some patients receiving I.V. lidocaine without ill effect. After discontinuation of amiodarone, BETAPACE AFTM should not be initiated until the QT interval is normalized (see WARNINGS).
BETAPACE AFTM (sotalol hydrochloride); capsule-shaped white scored tablets imprinted with the strength and "BERLEX" are available as follows: NDC 50419-115-06 80 mg strength, bottle of 60 in unit use package NDC 50419-119-06 120 mg strength, bottle of 60 in unit use package NDC 50419-116-06 160 mg strength, bottle of 60 in unit use package NDC 50419-115-11 80 mg strength, carton of 100 unit dose NDC 50419-119-11 120 mg strength, carton of 100 unit dose NDC 50419-116-11 160 mg strength, carton of 100 unit dose Store at 25oC with excursions permitted between 15o-30oC. Rx only (c) 2000, Berlex Laboratories. All rights reserved. Manufactured by: Berlex(r) Laboratories, Wayne, NJ 07470