Tri-Adcortyl Cream

The wording of leaflets is regularly updated. This electronic text is the most up-to-date version and may differ from the leaflet in your pack. If you have any questions about the information provided, please ask your doctor or pharmacist.

TRI-ADCORTYL CREAM

Your doctor has prescribed Tri-Adcortyl cream for you. This leaflet gives a summary of information about your medicine. If you want to know more, or are not sure about anything, ask your doctor or pharmacist.

REMEMBER: This medicine is for YOU. Only a doctor can prescribe it. Never give it to anyone else. It may harm them even if they have the same symptoms as you.

What Is In Tri-Adcortyl Cream?

This cream contains four active ingredients: triamcinolone acetonide which belongs to a group of medicines called steroids which are used to reduce inflammation, nystatin which is a member of a group of medicines called anti-fungal agents, neomycin and gramicidin which are antibiotics.

Each gram of Tri-Adcortyl contains 0.1% of triamcinolone acetonide, nystatin 100,000 units, neomycin 1625 units (0.25%) and gramicidin 0.025% and is supplied in tubes of 30g.

The other ingredients are: aluminium hydroxide, antifoam emulsion, benzyl alcohol, ethanol, ethylenediamine, hydrochloric acid, macrogol ether, perfume verley, polysorbate 60, propylene glycol, sorbitol, titanium dioxide, white soft paraffin, water.

Who Supplies This Cream?

Product Licence Holder:

E. R. Squibb & Sons Ltd

Uxbridge Business Park

Sanderson Road

Uxbridge

Middlesex

UB8 1DH

England

Tel:0800 7311736

Manufacturer:

Bristol-Myers Squibb SpA

Contrada Fontana Del Ceraso

03012 Anagni (Fr)

Italy

What is this medicine for ?

Tri-Adcortyl cream is prescribed for infected and inflammed skin conditions including eczema.

Before Using Your Medicine

Should you be using Tri-Adcortyl cream?

This cream has been prescribed to treat the skin problem that you showed your doctor. DO NOT use it on any other skin problems as it may make them worse.

DO NOT use Tri-Adcortyl cream if you have any of the following skin conditions:

• Tuberculosis (TB) of the skin;


• viral infections e.g. cold sores, herpes, chickenpox


• acne


• inflammation around the mouth (perioral dermatitis)


• a condition called rosacea (flushed, red face)

Tri-Adcortyl cream should not be used:

• inside the ears of patients with perforated eardrums (holes in eardrums)


• for long periods of time


• over large areas of the body


• in the eyes

This cream should not be used if you have had an allergic reaction to any product containing the same ingredients as Tri-Adcortyl cream. If Tri-Adcortyl cream is to be used on the face, or on children, treatment should not be longer than 5 days and the treated area should not be covered with any airtight or waterproof plasters/dressings.

This medicine should not be used in children under one year of age.

What if I am pregnant or breast feeding ?

You should always tell your doctor if you are pregnant, planning to become pregnant or breast feeding and let him decide if it is wise for you to use this medicine.

Do you have problems with your ears or hearing?

Make sure that your doctor knows about any problems you have with your ears before you start using Tri-Adcortyl. Neomycin, which is one of the active ingredients, may be harmful to the ears, particularly if used in large amounts and for long periods of time.

Using Your Medicine

How should I apply Tri-Adcortyl cream?

This cream should be applied to the affected area two or occasionally three times daily. In the elderly this cream should be used sparingly and for short periods of time. If after 7 days little or no improvement occurs then tell your doctor.

If you are using this cream on burnt skin that has become infected or ulcerated skin, make sure you use a small amount of cream, as these skin conditions may make it easier for the active ingredients in the cream to pass through the skin into the blood stream and may increase the possibility of side-effects.

Are there special directions for children?

As children are more likely to get side effects, they should not normally be treated for longer than 5 days, unless your doctor has told you to to do so.

What if Tri-Adcortyl cream is swallowed?

If this cream is swallowed tell your doctor immediately or go to your nearest hospital casualty department.

What happens if you miss an application?

If you forget to use your cream, apply it as soon as possible. However, if it is nearly time for your next application skip the missed dose and continue as before.

What should you do if you put Tri-Adcortyl cream on areas of normal or healthy skin?

Remove the cream with a clean tissue and wash the area with plenty of water.

Undesirable Effects

Are there any unwanted effects of Tri-Adcortyl cream?

If absorbed into the bloodstream, the active ingredient neomycin can damage the ears or kidney. Check with your doctor if you notice any of the following side effects: blistering, burning, itching, peeling, dryness or other signs of skin irritation not present before using this cream.

If the cream is used for a long time additional side effects may occur. Check with your doctor as soon as possible if you notice any of these: acne or oily skin, increased facial hair growth, increased sweating, lightheadedness on standing, reddish purple lines on arms, face, legs, trunk or groin; thinning of skin with easy bruising or wounds that are slow to heal, rashes consisting of slightly raised rounded red patches. It may also cause changes in your body's sugar levels. If you have skin reaction tests, eg for allergies, the steroid contained in this cream may affect the result by reducing the reaction. If you notice any other unwanted effect tell your doctor or pharmacist.

Looking After Your Medicine

Do not use your medicine after the expiry date which you will find on both the Cream tube and carton.

Keep all your medicines out of reach and sight of children, preferably in a locked cupboard or medicine cabinet. Do not store Tri-Adcortyl cream above 25°C and avoid freezing.

If your doctor decides to stop the cream, ask your pharmacist to tell you what to do with any you have left.

DATE OF LAST REVISION June 2005

Betadine Standardised Antiseptic Solution (Molnlycke Health Care )

1. Name Of The Medicinal Product

Standardised Betadine Antiseptic Solution.

2. Qualitative And Quantitative Composition

Povidone Iodine 10.00% w/v.

3. Pharmaceutical Form

Aqueous solution.

4. Clinical Particulars

4.1 Therapeutic Indications

For use as a pre-operative and post-operative antiseptic skin cleanser for major and minor surgical procedures.

4.2 Posology And Method Of Administration

Route of administration: Topical. Adults, the elderly and children: Apply full strength as a pre-operative and post-operative antiseptic skin cleanser. Avoid pooling both under the patient and in the skin folds. Wash off excess solution before using occlusive dressings. Povidone iodine is not recommended for regular use in neonates and is contraindicated in very low birth weight infants (below 1500 grams).

4.3 Contraindications

Known or suspected iodine hypersensitivity. Regular use is contraindicated in patients and users with thyroid disorders (in particular nodular colloid goitre, endemic goitre and Hashimoto's thyroiditis). Standardised Betadine Antiseptic Solution is not recommended for body cavity irrigation.

4.4 Special Warnings And Precautions For Use

Special caution is needed when regular applications to broken skin are made to patients with pre-existing renal insufficiency. Regular use should be avoided in patients on concurrent lithium therapy.

4.5 Interaction With Other Medicinal Products And Other Forms Of Interaction

Absorption of iodine from povidone iodine through either intact or damaged skin may interfere with thyroid function tests. Contamination with povidone iodine of several types of tests for the detection of occult blood in faeces or blood in urine may produce false-positive results.

4.6 Pregnancy And Lactation

Regular use of povidone iodine should be avoided in pregnant or lactating women as absorbed iodine can cross the placental barrier and can be secreted into breast milk. Although no adverse effects have been reported from limited use, caution should be recommended and therapeutic benefit must be balanced against possible effects of the absorption on foetal thyroid function and development.

4.7 Effects On Ability To Drive And Use Machines

None known.

4.8 Undesirable Effects

Povidone iodine may produce local skin reactions although it is considered to be less irritant than iodine. The application of povidone iodine to large wounds or severe burns may produce systemic adverse effects such as metabolic acidosis, hypernatraemia and impairment of renal function.

4.9 Overdose

Excess iodine can produce goitre and hypothyroidism or hyperthyroidism. Systemic absorption of iodine after repeated application of povidone iodine to large areas of wounds or burns may lead to a number of adverse effects: metallic taste in mouth, increased salivation, burning or pain in the throat or mouth, irritation and swelling of the eyes, pulmonary oedema, skin reactions, gastrointestinal upset and diarrhoea, metabolic acidosis, hypernatraemia and renal impairment.

In the case of deliberate or accidental ingestion of large quantities of Betadine, symptomatic and supportive treatment should be provided with special attention to electrolyte balance and renal and thyroid function.

5. Pharmacological Properties

5.1 Pharmacodynamic Properties

Standardised Betadine Antiseptic Solution contains povidone iodine, a complex of iodine which shows all the broad spectrum germicidal activity of elemental iodine. The germicidal activity is maintained in the presence of blood, pus, serum and necrotic tissue. Standardised Betadine Antiseptic Solution kills bacteria, viruses, fungi, spores and protozoa.

5.2 Pharmacokinetic Properties

The product is intended for topical application.

5.3 Preclinical Safety Data

None stated.

6. Pharmaceutical Particulars

6.1 List Of Excipients

Glycerol; nonoxynol 9; dibasic sodium phosphate (anhydrous); citric acid monohydrate; sodium hydroxide; potassium iodate; purified water.

6.2 Incompatibilities

None.

6.3 Shelf Life

36 months unopened.

6.4 Special Precautions For Storage

Store at a temperature not exceeding 25^oC.

6.5 Nature And Contents Of Container

High-density polyethylene bottle containing 500ml of product, fitted with a white polypropylene cap with a steran-lined wad.

6.6 Special Precautions For Disposal And Other Handling

None stated.

7. Marketing Authorisation Holder

Medlock Medical Limited, Tubiton House, Medlock Street, Oldham, OL1 3HS.

8. Marketing Authorisation Number(S)

PL 21248/0002.

9. Date Of First Authorisation/Renewal Of The Authorisation

30^th March 2005.

10. Date Of Revision Of The Text

March 2005.

Mexiletine

Dosage Form: capsule
Mexiletine HYDROCHLORIDE CAPSULES USP

Mexiletine Description

Mexiletine hydrochloride is an orally active antiarrhythmic agent. It is a white to off-white crystalline powder with slightly bitter taste, freely soluble in water and in alcohol. Mexiletine hydrochloride has a pKa of 9.2. The chemical name of Mexiletine hydrochloride is 1-methyl-2-(2,6-xylyloxy)ethylamine hydrochloride and its structural formula is:

C11H17NO•HCl M.W. 215.72

Each capsule for oral administration, contains 150 mg, 200 mg, or 250 mg of Mexiletine hydrochloride. 100 mg of Mexiletine hydrochloride is equivalent to 83.31 mg of Mexiletine base. In addition, each capsule contains the following excipients: colloidal silicon dioxide, magnesium stearate and pregelatinized starch. The capsule shell contains: FD&C Yellow #6, gelatin and titanium dioxide. The 150 mg capsule also contains: D&C Red #28 and FD&C Blue #1 and the 250 mg capsule also contains: D&C Yellow #10 and FD&C Blue #1. The imprinting ink contains: ammonium hydroxide, black iron oxide, D&C Yellow #10, ethyl alcohol, FD&C Blue #1, FD&C Blue #2, FD&C Red #40, isopropyl alcohol, n-butyl alcohol, propylene glycol and shellac.

Mexiletine - Clinical Pharmacology

Mechanism of Action

Mexiletine hydrochloride is a local anesthetic, antiarrhythmic agent, structurally similar to lidocaine, but orally active. In animal studies, Mexiletine has been shown to be effective in the suppression of induced ventricular arrhythmias, including those induced by glycoside toxicity and coronary artery ligation. Mexiletine, like lidocaine, inhibits the inward sodium current, thus reducing the rate of rise of the action potential, Phase 0. Mexiletine decreased the effective refractory period (ERP) in Purkinje fibers. The decrease in ERP was of lesser magnitude than the decrease in action potential duration (APD), with a resulting increase in the ERP/APD ratio.

Electrophysiology in Man

Mexiletine is a Class 1B antiarrhythmic compound with electrophysiologic properties in man similar to those of lidocaine, but dissimilar from quinidine, procainamide, and disopyramide.

In patients with normal conduction systems, Mexiletine has a minimal effect on cardiac impulse generation and propagation. In clinical trials, no development of second-degree or third degree AV block was observed. Mexiletine did not prolong ventricular depolarization (QRS duration) or repolarization (QT intervals) as measured by electrocardiography. Theoretically, therefore, Mexiletine may be useful in the treatment of ventricular arrhythmias associated with a prolonged QT interval.

In patients with pre-existing conduction defects, depression of the sinus rate, prolongation of sinus node recovery time, decreased conduction velocity and increased effective refractory period of the intraventricular conduction system have occasionally been observed.

The antiarrhythmic effect of Mexiletine has been established in controlled comparative trials against placebo, quinidine, procainamide and disopyramide. Mexiletine hydrochloride, at doses of 200 to 400 mg q8h, produced a significant reduction of ventricular premature beats, paired beats, and episodes of non-sustained ventricular tachycardia compared to placebo and was similar in effectiveness to the active agents. Among all patients entered into the studies, about 30% in each treatment group had a 70% or greater reduction in PVC count and about 40% failed to complete the 3 month studies because of adverse effects. Follow-up of patients from the controlled trials has demonstrated continued effectiveness of Mexiletine in long-term use.

Hemodynamics

Hemodynamic studies in a limited number of patients, with normal or abnormal myocardial function, following oral administration of Mexiletine hydrochloride, have shown small, usually not statistically significant, decreases in cardiac output and increases in systemic vascular resistance, but no significant negative inotropic effect. Blood pressure and pulse rate remain essentially unchanged. Mild depression of myocardial function, similar to that produced by lidocaine, has occasionally been observed following intravenous Mexiletine therapy in patients with cardiac disease.

Pharmacokinetics

Mexiletine is well absorbed (~90%) from the gastrointestinal tract. Unlike lidocaine, its first-pass metabolism is low. Peak blood levels are reached in two to three hours. In normal subjects, the plasma elimination half-life of Mexiletine is approximately 10 to 12 hours. It is 50 to 60% bound to plasma protein, with a volume of distribution of 5 to 7 liters/kg. Mexiletine is mainly metabolized in the liver, the primary pathway being CYP2D6 metabolism, although it is also a substrate for CYP1A2. With involvement of CYP2D6, there can be either poor or extensive metabolizer phenotypes. Since approximately 90% of Mexiletine hydrochloride is metabolized in the liver into inactive metabolites, pathological changes in the liver can restrict hepatic clearance of Mexiletine hydrochloride and its metabolites. The metabolic degradation proceeds via various pathways including aromatic and aliphatic hydroxylation, dealkylation, deamination and N-oxidation. Several of the resulting metabolites are submitted to further conjugation with glucuronic acid (phase II metabolism); among these are the major metabolites p-hydroxyMexiletine, hydroxy-methylMexiletine and N-hydroxy-Mexiletine. Approximately 10% is excreted unchanged by the kidney. While urinary pH does not normally have much influence on elimination, marked changes in urinary pH influence the rate of excretion: acidification accelerates excretion, while alkalinization retards it.

Several metabolites of Mexiletine have shown minimal antiarrhythmics activity in animal models. The most active is the minor metabolite N-methylMexiletine, which is less than 20% as potent as Mexiletine. The urinary excretion of N-methylMexiletine in man is less than 0.5%. Thus the therapeutic activity of Mexiletine is due to the parent compound.

Hepatic impairment prolongs the elimination half-life of Mexiletine. In eight patients with moderate to severe liver disease, the mean half-life was approximately 25 hours.

Consistent with the limited renal elimination of Mexiletine, little change in the half-life has been detected in patients with reduced renal function. In eight patients with creatinine clearance less than 10 mL/min, the mean plasma elimination half-life was 15.7 hours; in seven patients with creatinine clearance between 11 to 40 mL/min, the mean half-life was 13.4 hours.

The absorption rate of Mexiletine is reduced in clinical situations such as acute myocardial infarction in which gastric emptying time is increased. Narcotics, atropine and magnesium-aluminum hydroxide have also been reported to slow the absorption of Mexiletine. Metoclopramide has been reported to accelerate absorption.

Mexiletine plasma levels of at least 0.5 mcg/mL are generally required for therapeutic response. An increase in the frequency of central nervous system adverse effects has been observed when plasma levels exceed 2.0 mcg/mL. Thus the therapeutic range is approximately 0.5 to 2.0 mcg/mL. Plasma levels within the therapeutic range can be attained with either three times daily or twice daily dosing but peak to trough differences are greater with the latter regimen, creating the possibility of adverse effects at peak and arrhythmic escape at trough. Nevertheless, some patients may be transferred successfully to the twice daily regimen. (See DOSAGE AND ADMINISTRATION.)

Indications and Usage for Mexiletine

Mexiletine hydrochloride capsules are indicated for the treatment of documented ventricular arrhythmias, such as sustained ventricular tachycardia, that, in the judgment of the physician, are life-threatening. Because of the proarrhythmic effects of Mexiletine, its use with lesser arrhythmias is generally not recommended. Treatment of patients with asymptomatic ventricular premature contractions should be avoided.

Initiation of Mexiletine treatment, as with other antiarrhythmic agents used to treat life-threatening arrhythmias, should be carried out in the hospital.

Antiarrhythmic drugs have not been shown to enhance survival in patients with ventricular arrhythmias.

Contraindications

Mexiletine hydrochloride capsules are contraindicated in the presence of cardiogenic shock or pre-existing second-or third-degree AV block (if no pacemaker is present).

BOXED WARNING

WARNINGS

Mortality

In the National Heart, Lung and Blood Institute’s Cardiac Arrhythmia Suppression Trial (CAST), a long-term, multicentered, randomized, double-blind study in patients with asymptomatic non-life-threatening ventricular arrhythmias who had a myocardial infarction more than six days but less than two years previously, an excessive mortality or non-fatal cardiac arrest rate (7.7%) was seen in patients treated with encainide or flecainide compared with that seen in patients assigned to carefully matched placebo-treated groups (3.0%). The average duration of treatment with encainide or flecainide in this study was ten months.

The applicability of the CAST results to other populations (e.g., those without recent myocardial infarction) is uncertain. Considering the known proarrhythmic properties of Mexiletine and the lack of evidence of improved survival for any antiarrhythmic drug in patients without life-threatening arrhythmias, the use of Mexiletine as well as other antiarrhythmic agents should be reserved for patients with life-threatening ventricular arrhythmia.

Acute Liver Injury

In postmarketing experience abnormal liver function tests have been reported, some in the first few weeks of therapy with Mexiletine hydrochloride. Most of these have been observed in the setting of congestive heart failure or ischemia and their relationship to Mexiletine hydrochloride has not been established.

Precautions

General

If a ventricular pacemaker is operative, patients with second or third degree heart block may be treated with Mexiletine hydrochloride if continuously monitored. A limited number of patients (45 of 475 in controlled clinical trials) with pre-existing first degree AV block were treated with Mexiletine; none of these patients developed second or third degree AV block. Caution should be exercised when it is used in such patients or in patients with pre-existing sinus node dysfunction or intraventricular conduction abnormalities.

Like other antiarrhythmics Mexiletine hydrochloride can cause worsening of arrhythmias. This has been uncommon in patients with less serious arrhythmias (frequent premature beats or nonsustained ventricular tachycardia: see ADVERSE REACTIONS), but is of greater concern in patients with life-threatening arrhythmias such as sustained ventricular tachycardia. In patients with such arrhythmias subjected to programmed electrical stimulation or to exercise provocation, 10 to 15% of patients had exacerbation of the arrhythmia, a rate not greater than that of other agents.

Mexiletine should be used with caution in patients with hypotension and severe congestive heart failure because of the potential for aggravating these conditions.

Since Mexiletine is metabolized in the liver, and hepatic impairment has been reported to prolong the elimination half-life of Mexiletine, patients with liver disease should be followed carefully while receiving Mexiletine. The same caution should be observed in patients with hepatic dysfunction secondary to congestive heart failure.

Concurrent drug therapy or dietary regimens which may markedly alter urinary pH should be avoided during Mexiletine hydrochloride therapy. The minor fluctuations in urinary pH associated with normal diet do not affect the excretion of Mexiletine.

SGOT Elevation and Liver Injury

In three month controlled trials, elevations of SGOT greater than three times the upper limit of normal occurred in about 1% of both Mexiletine-treated and control patients. Approximately 2% of patients in the Mexiletine compassionate use program had elevations of SGOT greater than or equal to three times the upper limit of normal. These elevations frequently occurred in association with identifiable clinical events and therapeutic measures such as congestive heart failure, acute myocardial infarction, blood transfusions and other medications. These elevations were often asymptomatic and transient, usually not associated with elevated bilirubin levels and usually did not require discontinuation of therapy. Marked elevations of SGOT (> 1000 U/L) were seen before death in four patients with end-stage cardiac disease (severe congestive heart failure, cardiogenic shock).

Rare instances of severe liver injury, including hepatic necrosis, have been reported in association with Mexiletine treatment. It is recommended that patients in whom an abnormal liver test has occurred, or who have signs of symptoms suggesting liver dysfunction, be carefully evaluated. If persistent or worsening elevation of hepatic enzymes is detected, consideration should be given to discontinuing therapy.

Blood Dyscrasias

Among 10,867 patients treated with Mexiletine in the compassionate use program, marked leukopenia (neutrophils less than 1000/mm3) or agranulocytosis were seen in 0.06% and milder depressions of leukocytes were seen in 0.08%, and thrombocytopenia was observed in 0.16%. Many of these patients were seriously ill and receiving concomitant medications with known hematologic adverse effects. Rechallenge with Mexiletine in several cases was negative. Marked leukopenia or agranulocytosis did not occur in any patient receiving Mexiletine alone; five of the six cases of agranulocytosis were associated with procainamide (sustained release preparations in four) and one with vinblastine. If significant hematologic changes are observed, the patient should be carefully evaluated, and, if warranted, Mexiletine should be discontinued. Blood counts usually return to normal within a month of discontinuation (see ADVERSE REACTIONS).

Convulsions (seizures) did not occur in Mexiletine controlled clinical trials. In the compassionate use program, convulsions were reported in about 2 of 1000 patients. Twenty-eight percent of these patients discontinued therapy. Convulsions were reported in patients with and without a prior history of seizures. Mexiletine should be used with caution in patients with known seizure disorder.

Drug Interactions

Since Mexiletine hydrochloride is a substrate for the metabolic pathways involving CYP2D6 and CYP1A2 enzymes, inhibition or induction of either of these enzymes would be expected to alter Mexiletine plasma concentrations. In a formal, single-dose interaction study (n = 6 males) the clearance of Mexiletine was decreased by 38% following the coadministration of fluvoxamine, an inhibitor of CYP1A2. In another formal study (n = 8 extensive and n = 7 poor metabolizers of CYP2D6), coadministration of propafenone did not alter the kinetics of Mexiletine in the poor CYP2D6 metabolizer group. However, the metabolic clearance of Mexiletine in the extensive metabolizer phenotype decreased by about 70% making the poor and extensive metabolizer groups indistinguishable. In this crossover steady state study, the pharmacokinetics of propafenone were unaffected in either phenotype by the coadministration of Mexiletine. Addition of Mexiletine to propafenone did not lead to further electrocardiographic parameters changes of QRS, QTc, RR, and PR intervals than propafenone alone. When concomitant administration of either of these two drugs is initiated, the dose of Mexiletine should be slowly titrated to desired effect.

In a large compassionate use program Mexiletine has been used concurrently with commonly employed antianginal, antihypertensive, and anticoagulant drugs without observed interactions. A variety of antiarrhythmics such as quinidine or propranolol were also added, sometimes with improved control of ventricular ectopy. When phenytoin or other hepatic enzyme inducers such as rifampin and phenobarbital have been taken concurrently with Mexiletine, lowered Mexiletine plasma levels have been reported. Monitoring of Mexiletine plasma levels is recommended during such concurrent use to avoid ineffective therapy.

In a formal study, benzodiazepines were shown not to affect Mexiletine plasma concentrations. ECG intervals (PR, QRS, and QT) were not affected by concurrent Mexiletine and digoxin, diuretics, or propranolol.

Concurrent administration of cimetidine and Mexiletine has been reported to increase, decrease, or leave unchanged Mexiletine plasma levels; therefore patients should be followed carefully during concurrent therapy.

Mexiletine does not alter serum digoxin levels but magnesium-aluminum hydroxide, when used to treat gastrointestinal symptoms due to Mexiletine, has been reported to lower serum digoxin levels.

Concurrent use of Mexiletine and theophylline may lead to increased plasma theophylline levels. One controlled study in eight normal subjects showed a 72% mean increase (range

35 to 136%) in plasma theophylline levels. This increase was observed at the first test point which was the second day after starting Mexiletine. Theophylline plasma levels returned to pre-Mexiletine values within 48 hours after discontinuing Mexiletine. If Mexiletine and theophylline are to be used concurrently, theophylline blood levels should be monitored, particularly when the Mexiletine dose is changed. An appropriate adjustment in theophylline dose should be considered.

Additionally, in one controlled study in five normal subjects and seven patients, the clearance of caffeine was decreased 50% following the administration of Mexiletine.

Carcinogenesis, Mutagenesis, Impairment of Fertility

Studies of carcinogenesis in rats (24 months) and mice (18 months) did not demonstrate any tumorigenic potential. Mexiletine was found to be non-mutagenic in the Ames test. Mexiletine did not impair fertility in the rat.

Pregnancy

Teratogenic Effects

Pregnancy category C

Reproduction studies performed with Mexiletine in rats, mice and rabbits at doses up to four times the maximum human oral dose (24 mg/kg in a 50 kg patient) revealed no evidence of teratogenicity or impaired fertility but did show an increase in fetal resorption. There are no adequate and well-controlled studies in pregnant women; this drug should be used in pregnancy only if the potential benefit justifies the potential risk to the fetus.

Nursing Mothers

Mexiletine appears in human milk in concentrations similar to those observed in plasma. Therefore, if the use of Mexiletine hydrochloride is deemed essential, an alternative method of infant feeding should be considered.

Pediatric Use

Safety and effectiveness in pediatric patients have not been established.

Adverse Reactions

Mexiletine hydrochloride commonly produces reversible gastrointestinal and nervous system adverse reactions but is otherwise well tolerated. Mexiletine has been evaluated in 483 patients in one month and three month controlled studies and in over 10,000 patients in a large compassionate use program. Dosages in the controlled studies ranged from 600 to 1200 mg/day; some patients (8%) in the compassionate use program were treated with higher daily doses (1600 to 3200 mg/day). In the three month controlled trials comparing Mexiletine to quinidine, procainamide and disopyramide, the most frequent adverse reactions were upper gastrointestinal distress (41%), lightheadedness (10.5%), tremor (12.6%) and coordination difficulties (10.2%). Similar frequency and incidence were observed in the one month placebo-controlled trial. Although these reactions were generally not serious, and were dose-related and reversible with a reduction in dosage, by taking the drug with food or antacid or by therapy discontinuation, they led to therapy discontinuation in 40% of patients in the controlled trials. Table 1 presents the adverse events reported in the one-month placebo-controlled trial.

Table 1: Comparative Incidence (%) of Adverse Events Among Patients Treated with Mexiletine and Placebo in the 4 Week, Double-blind Crossover Trial

	MexiletineN = 53	PlaceboN = 49
Cardiovascular
Palpitations	7.5	10.2
Chest Pain	7.5	4.1
Increased Ventricular Arrythmia/PVCs	1.9	-
Digestive
Nausea/Vomiting/Heartburn	39.6	6.1
Central Nervous System
Dizziness/Lightheadedness	26.4	14.3
Tremor	13.2	-
Nervousness	11.3	6.1
Coordination Difficulties	9.4	-
Changes in Sleep Habits	7.5	16.3
Paresthesias/Numbness	3.8	2.0
Weakness	1.9	4.1
Fatigue	1.9	2.0
Tinnitus	1.9	4.1
Confusion/Clouded Sensorium	1.9	2.0
Other
Headache	7.5	6.1
Blurred Vision/Visual Disturbances	7.5	2.0
Dyspnea/Respiratory	5.7	10.2
Rash	3.8	2.0
Non-specific Edema	3.8	-

Table 2 presents the adverse reactions occurring in one percent or more of patients in the three month controlled studies.

Table 2: Comparative Incidence (%) of Adverse Events Among Patients Treated with Mexiletine or Control Drugs in the 12 Week Double-blind Trials

	Mexiletine N = 430	Quinidine N = 262	Procainamide N = 78	Disopyramide N = 69
Cardiovascular
Palpitations	4.3	4.6	1.3	5.8
Chest Pain	2.6	3.4	1.3	2.9
Angina/Angina-like Pain	1.7	1.9	2.6	2.9
Increased Ventricular Arrhythmias/PVCs	1.0	2.7	2.6	-
Digestive
Nausea/Vomiting/ Heartburn	39.3	21.4	33.3	14.5
Diarrhea	5.2	33.2	2.6	8.7
Constipation	4.0	-	6.4	11.6
Changes in Appetite	2.6	1.9	-	-
Abdominal Pain/Cramps/ Discomfort	1.2	1.5	-	1.4
Central Nervous System
Dizziness/Lightheadedness	18.9	14.1	14.1	2.9
Tremor	13.2	2.3	3.8	1.4
Coordination Difficulties	9.7	1.1	1.3	-
Changes in Sleep Habits	7.1	2.7	11.5	8.7
Weakness	5.0	5.3	7.7	2.9
Nervousness	5.0	1.9	6.4	5.8
Fatigue	3.8	5.7	5.1	1.4
Speech Difficulties	2.6	0.4	-	-
Confusion/Clouded Sensorium	2.6	-	3.8	-
Paresthesias/Numbness	2.4	2.3	2.6	-
Tinnitus	2.4	1.5	-	-
Depression	2.4	1.1	1.3	1.4
Other
Blurred Vision/Visual Disturbances	5.7	3.1	5.1	7.2
Headache	5.7	6.9	7.7	4.3
Rash	4.2	3.8	10.3	1.4
Dyspnea/Respiratory	3.3	3.1	5.1	2.9
Dry Mouth	2.8	1.9	5.1	14.5
Arthralgia	1.7	2.3	5.1	1.4
Fever	1.2	3.1	2.6	-

Less than 1%: Syncope, edema, hot flashes, hypertension, short-term memory loss, loss of consciousness, other psychological changes, diaphoresis, urinary hesitancy/retention, malaise, impotence/decreased libido, pharyngitis, congestive heart failure.

An additional group of over 10,000 patients has been treated in a program allowing administration of Mexiletine hydrochloride under compassionate use circumstances. These patients were seriously ill with the large majority on multiple drug therapy. Twenty-four percent of the patients continued in the program for one year or longer. Adverse reactions leading to therapy discontinuation occurred in 15 percent of patients (usually upper gastrointestinal system or nervous system effects). In general, the more common adverse reactions were similar to those in the controlled trials. Less common adverse events possibly related to Mexiletine use include:

Cardiovascular System

Syncope and hypotension, each about 6 in 1000; bradycardia, about 4 in 1000; angina/angina-like pain, about 3 in 1000; edema, atrioventricular block/conduction disturbances and hot flashes, each about 2 in 1000; atrial arrhythmias, hypertension and cardiogenic shock, each about 1 in 1000.

Central Nervous System

Short-term memory loss, about 9 in 1000 patients; hallucinations and other psychological changes, each about 3 in 1000; psychosis and convulsions/seizures, each about 2 in 1000; loss of consciousness, about 6 in 10,000.

Digestive

Dysphagia, about 2 in 1000; peptic ulcer, about 8 in 10,000; upper gastrointestinal bleeding, about 7 in 10,000; esophageal ulceration, about 1 in 10,000. Rare cases of severe hepatitis/acute hepatic necrosis.

Skin

Rare cases of exfoliative dermatitis and Stevens-Johnson syndrome with Mexiletine treatment have been reported.

Laboratory

Abnormal liver function tests, about 5 in 1000; positive ANA and thrombocytopenia, each about 2 in 1000; leukopenia (including neutropenia and agranulocytosis), about 1 in 1000; myelofibrosis, about 2 in 10,000 patients.

Other

Diaphoresis, about 6 in 1000; altered taste, about 5 in 1000; salivary changes, hair loss and impotence/decreased libido, each about 4 in 1000; malaise, about 3 in 1000; urinary hesitancy/retention, each about 2 in 1000; hiccups, dry skin, laryngeal and pharyngeal changes and changes in oral mucous membranes, each about 1 in 1000; SLE syndrome, about 4 in 10,000.

Hematology

Blood dyscrasias were not seen in the controlled trials but did occur among 10,867 patients treated with Mexiletine in the compassionate use program (see PRECAUTIONS).

Myelofibrosis was reported in two patients in the compassionate use program; one was receiving long-term thiotepa therapy and the other had pretreatment myeloid abnormalities.

In postmarketing experience, there have been isolated, spontaneous reports of pulmonary changes including pulmonary infiltration and pulmonary fibrosis during Mexiletine therapy with or without other drugs or diseases that are known to produce pulmonary toxicity. A causal relationship to Mexiletine therapy has not been established. In addition, there have been isolated reports of drowsiness, nystagmus, ataxia, dyspepsia, hypersensitivity reaction, and exacerbation of congestive heart failure in patients with pre-existing compromised ventricular function. There have been rare reports of pancreatitis associated with Mexiletine treatment.

Overdosage

Clinical findings associated with Mexiletine overdosage have included drowsiness, confusion, nausea, hypotension, sinus bradycardia, paresthesia, seizures, bundle branch block, AV heart block, asystole, ventricular tachyarrythmia, including ventricular fibrillation, cardiovascular collapse and coma. The lowest known dose in a fatality case was 4.4 g with postmortem serum Mexiletine level of 34 to 37 mcg/mL (Jequier P. et. al., Lancet 1976: 1 (7956): 429). Patients have recovered from ingestion of 4 g to 18 g of Mexiletine (Frank S. E. et. al., Am J Emerg Med 1991: 9:43-48).

There is no specific antidote for Mexiletine. Management of Mexiletine overdosage includes general supportive measures, close observation and monitoring of vital signs. In addition, the use of pharmacologic interventions (e.g., pressor agents, atropine or anticonvulsants) or transvenous cardiac pacing is suggested, depending on the patient’s clinical condition.

Mexiletine Dosage and Administration

The dosage of Mexiletine hydrochloride must be individualized on the basis of response and tolerance, both of which are dose-related. Administration with food or antacid is recommended. Initiate Mexiletine therapy with 200 mg every eight hours when rapid control of arrhythmia is not essential. A minimum of two to three days between dose adjustments is recommended. Dose may be adjusted in 50 or 100 mg increments up or down.

As with any antiarrhythmic drug, clinical and electrocardiographic evaluation (including Holter monitoring if necessary for evaluation) are needed to determine whether the desired antiarrhythmic effect has been obtained and to guide titration and dose adjustment.

Satisfactory control can be achieved in most patients by 200 to 300 mg given every eight hours with food or antacid. If satisfactory response has not been achieved at 300 mg q8h, and the patient tolerates Mexiletine well, a dose of 400 mg q8h may be tried. As the severity of CNS side effects increases with total daily dose, the dose should not exceed 1200 mg/day.

In general, patients with renal failure will require the usual doses of Mexiletine hydrochloride. Patients with severe liver disease, however, may require lower doses and must be monitored closely. Similarly, marked right-sided congestive heart failure can reduce hepatic metabolism and reduce the needed dose. Plasma level may also be affected by certain concomitant drugs (see PRECAUTIONS, Drug Interactions).

Loading Dose

When rapid control of ventricular arrhythmia is essential, an initial loading dose of 400 mg of Mexiletine hydrochloride may be administered, followed by a 200 mg dose in eight hours. Onset of therapeutic effect is usually observed within 30 minutes to two hours.

Q12H Dosage Schedule

Some patients responding to Mexiletine may be transferred to a 12 hour dosage schedule to improve convenience and compliance. If adequate suppression is achieved on a Mexiletine hydrochloride dose of 300 mg or less every eight hours, the same total daily dose may be given in divided doses every 12 hours while carefully monitoring the degree of suppression of ventricular ectopy. This dose may be adjusted up to a maximum of 450 mg every 12 hours to achieve the desired response.

Transferring to Mexiletine Hydrochloride

The following dosage schedule, based on theoretical considerations rather than experimental data, is suggested for transferring patients from other Class I oral antiarrhythmic agents to Mexiletine: Mexiletine hydrochloride treatment may be initiated with a 200 mg dose, and titrated to response as described above, 6 to 12 hours after the last dose of quinidine sulfate, 3 to 6 hours after the last dose of procainamide, 6 to 12 hours after the last dose of disopryramide or 8 to 12 hours after the last dose of tocainide.

In patients in whom withdrawal of the previous antiarrhythmic agent is likely to produce life-threatening arrhythmias, hospitalization of the patient is recommended.

When transferring from lidocaine to Mexiletine, the lidocaine infusion should be stopped when the first oral dose of Mexiletine hydrochloride is administered. The infusion line should be left open until suppression of the arrhythmia appears to be satisfactorily maintained. Consideration should be given to the similarity of the adverse effects of lidocaine and Mexiletine and the possibility that they may be additive.

How is Mexiletine Supplied

Mexiletine hydrochloride capsules USP, 150 mg are white granular powder in a hard gelatin capsule with an opaque tan cap and an opaque orange body, imprinted with N on one side and 739 and 150 on the other in black ink. They are supplied as follows: NDC 0093-8739-01 bottles of 100.

Mexiletine hydrochloride capsules USP, 200 mg are white granular powder in a hard gelatin capsule with an opaque orange cap and an opaque orange body, imprinted with N on& one side and 740 and 200 on the other in black ink. They are supplied as follows: NDC 0093-8740-01 bottles of 100.

Mexiletine hydrochloride capsules USP, 250 mg are white granular powder in a hard gelatin capsule with an opaque green cap and an opaque orange body, imprinted with N on one side and 741 and 250 on the other in black ink. They are supplied as follows: NDC 0093-8741-01 bottles of 100.

Store at 20° to 25°C (68° to 77°F) [See USP Controlled Room Temperature].

Dispense in a tight, light-resistant container as defined in the USP, with a child-resistant closure (as required).

Manufactured In Canada By:

NOVOPHARM LIMITED

Toronto, Canada M1B 2K9

Manufactured For:

TEVA PHARMACEUTICALS USA

Sellersville, PA

Fuzeon 90 mg / ml powder and solvent for solution for injection

1. Name Of The Medicinal Product

Fuzeon 90 mg/ml powder and solvent for solution for injection

2. Qualitative And Quantitative Composition

Each vial contains 108 mg enfuvirtide.

Each ml of reconstituted solution contains 90 mg enfuvirtide.

For a full list of excipients, see section 6.1.

3. Pharmaceutical Form

Powder and solvent for solution for injection.

White to off-white lyophilised powder.

4. Clinical Particulars

4.1 Therapeutic Indications

Fuzeon is indicated in combination with other antiretroviral medicinal products for the treatment of HIV-1 infected patients who have received treatment with and failed on regimens containing at least one medicinal product from each of the following antiretroviral classes: protease inhibitors, non-nucleoside reverse transcriptase inhibitors and nucleoside reverse transcriptase inhibitors, or who have intolerance to previous antiretroviral regimens. (see section 5.1)

In deciding on a new regimen for patients who have failed an antiretroviral regimen, careful consideration should be given to the treatment history of the individual patient and the patterns of mutations associated with different medicinal products. Where available, resistance testing may be appropriate. (See sections 4.4 and 5.1)

4.2 Posology And Method Of Administration

Fuzeon should be prescribed by physicians who are experienced in the treatment of HIV infection.

Fuzeon is only to be administered by subcutaneous injection.

Adults and adolescents 16 years: The recommended dose of Fuzeon is 90 mg twice daily injected subcutaneously into the upper arm, anterior thigh or abdomen.

Elderly: There is no experience in patients> 65 years old.

Children : The experience in children is limited (See section 5.2). In clinical trials the dosage regimen in table 1 below was used:

Table 1: Paediatric Dosing

Weight (kg)	Dose per bid injection (mg/dose)	Injection volume (90 mg enfuvirtide per ml)
11.0 to 15.5	27	0.3 ml
15.6 to 20.0	36	0.4 ml
20.1 to 24.5	45	0.5 ml
24.6 to 29.0	54	0.6 ml
29.1 to 33.5	63	0.7 ml
33.6 to 38.0	72	0.8 ml
38.1 to 42.5	81	0.9 ml
	90	1.0 ml

Fuzeon is not recommended for use in children below age 6 due to insufficient data on safety and efficacy (see section 5.2).

Renal impairment: No dose adjustment is required for patients with renal impairment including those receiving dialysis. (See sections 4.4 and 5.2).

Hepatic impairment: No data are available to establish a dose recommendation for patients with hepatic impairment. (See sections 4.4 and 5.2).

4.3 Contraindications

Hypersensitivity to the active substance or to any of the excipients.

4.4 Special Warnings And Precautions For Use

Fuzeon must be taken as part of a combination regimen. Please also refer to the respective summary of product characteristics of the other antiretroviral medicinal products used in the combination. As with other antiretrovirals, enfuvirtide should optimally be combined with other antiretrovirals to which the patient's virus is sensitive. (See section 5.1)

Patients must be advised that antiretroviral therapies including enfuvirtide have not been proved to prevent the risk of transmission to HIV to others through sexual contact or blood contamination. They must continue to use appropriate precautions. Patients should also be informed that Fuzeon is not a cure for HIV-1 infection.

Animal studies have shown that enfuvirtide may impair some immune functions (see section 5.3). In clinical trials, an increased rate of some bacterial infections, most notably a higher rate of pneumonia, was seen in patients treated with Fuzeon; however, an increased risk of bacterial pneumonia related to the use of Fuzeon has not been confirmed by subsequent epidemiological data.

Hypersensitivity reactions have occasionally been associated with therapy with enfuvirtide and in rare cases hypersensitivity reactions have recurred on rechallenge. Events included rash, fever, nausea and vomiting, chills, rigors, low blood pressure and elevated serum liver transaminases in various combinations, and possibly primary immune complex reaction, respiratory distress and glomerulonephritis. Patients developing signs/symptoms of a systemic hypersensitivity reaction should discontinue enfuvirtide treatment and should seek medical evaluation immediately. Therapy with enfuvirtide should not be restarted following systemic signs and symptoms consistent with a hypersensitivity reaction considered related to enfuvirtide. Risk factors that may predict the occurrence or severity of hypersensitivity to enfuvirtide have not been identified.

Liver disease: The safety and efficacy of enfuvirtide has not been specifically studied in patients with significant underlying liver disorders. Patients with chronic hepatitis B and C and treated with antiretroviral therapy are at an increased risk for severe and potentially fatal hepatic adverse events. Few patients included in the phase III trials were co-infected with hepatitis B/C. In these the addition of Fuzeon did not increase the incidence of hepatic events. In case of concomitant antiviral therapy for hepatitis B or C, please refer also to the relevant product information for these medicinal products.

Administration of Fuzeon to non-HIV-1 infected individuals may induce anti-enfuvirtide antibodies that cross-react with HIV gp41. This may result in a false positive HIV test with the anti-HIV ELISA test.

There is no experience in patients with reduced hepatic function. Data is limited in patients with moderate to severe renal impairment, and in patients maintained on dialysis. Fuzeon should be used with caution in these populations. (See sections 4.2 and 5.2)

Immune Reactivation Syndrome: In HIV-infected patients with severe immune deficiency at the time of institution of combination antiretroviral therapy (CART), an inflammatory reaction to asymptomatic or residual opportunistic pathogens may arise and cause serious clinical conditions, or aggravation of symptoms. Typically, such reactions have been observed within the first few weeks or months of initiation of CART. Relevant examples are cytomegalovirus retinitis, generalised and/or focal mycobacterial infections, and Pneumocystis carinii pneumonia. Any inflammatory symptoms should be evaluated and treatment instituted when necessary.

Osteonecrosis:

Although the aetiology is considered to be multifactorial (including corticosteroid use, alcohol consumption, severe immunosuppression, higher body mass index), cases of osteonecrosis have been reported particularly in patients with advanced HIV-disease and/or long-term exposure to CART. Patients should be advised to seek medical advice if they experience joint aches and pain, joint stiffness or difficulty in movement.

4.5 Interaction With Other Medicinal Products And Other Forms Of Interaction

Interactions studies have only been performed in adults.

No clinically significant pharmacokinetic interactions are expected between enfuvirtide and concomitantly given medicinal products metabolised by CYP450 enzymes.

Influence of enfuvirtide on metabolism of concomitant medicinal products: In an in-vivo human metabolism study enfuvirtide, at the recommended dose of 90 mg twice daily, did not inhibit the metabolism of substrates by CYP3A4 (dapsone), CYP2D6 (debrisoquine), CYP1A2 (caffeine), CYP2C19 (mephenytoin), and CYP2E1 (chlorzoxazone).

Influence of concomitant medicinal products on enfuvirtide metabolism: In separate pharmacokinetic interaction studies, co-administration of ritonavir (potent CYP3A4 inhibitor) or saquinavir in combination with a booster dose of ritonavir or rifampicin (potent CYP34A inducer) did not result in clinically significant changes of the pharmacokinetics of enfuvirtide.

4.6 Pregnancy And Lactation

There are no adequate and well-controlled studies in pregnant women. Animal studies do not indicate harmful effects with respect to foetal development. Enfuvirtide should be used during pregnancy only if the potential benefit justifies the potential risk to the foetus.

It is not known whether enfuvirtide is secreted in human milk. Mothers should be instructed not to breast-feed if they are receiving enfuvirtide because of the potential for HIV transmission and any possible undesirable effects in breast-fed infants.

4.7 Effects On Ability To Drive And Use Machines

No studies on the effects on the ability to drive and use machines have been performed. There is no evidence that enfuvirtide may alter the patient's ability to drive and use machines, however, the adverse event profile of enfuvirtide should be taken into account. (See section 4.8)

4.8 Undesirable Effects

Safety data mainly refer to 48-week data from studies TORO 1 and TORO 2 combined (see section 5.1). Safety results are expressed as the number of patients with an adverse reaction per 100 patient-years of exposure (except for injection site reactions).

Injection site reactions

Injection site reactions (ISRs) were the most frequently reported adverse reaction and occurred in 98% of the patients (Table 2). The vast majority of ISRs occurred within the first week of Fuzeon administration and were associated with mild to moderate pain or discomfort at the injection site without limitation of usual activities. The severity of the pain and discomfort did not increase with treatment duration. The signs and symptoms generally lasted equal to or less than 7 days. Infections at the injection site (including abscess and cellulitis) occurred in 1.5% of patients.

Table 2: Summary of individual signs/symptoms characterising local injection site reactions in studies TORO 1 and TORO 2 combined (% of patients)

	n=663
Withdrawal Rate due to ISRs	4%
Event Category	Fuzeon +Optimised backgrounda	% of Event comprising Grade 3 reactions	% of Event comprising Grade 4 reactions
Pain / discomfort	96.1%	11.0%b	0%b
Erythema	90.8%	23.8%c	10.5%c
Induration	90.2%	43.5%d	19.4%d
Nodules and cysts	80.4%	29.1%e	0.2%e
Pruritus	65.2%	3.9%f	NA
Ecchymosis	51.9%	8.7%g	4.7%g

^aAny severity grade.

^bGrade 3= severe pain requiring analgesics (or narcotic analgesics for

^cGrade 3=

^dGrade 3=

^eGrade 3=

^fGrade 3= refractory to topical treatment or requiring oral or parenteral treatment; Grade 4= not defined.

^gGrade 3=> 3 cm but

Other adverse reactions

The addition of Fuzeon to background antiretroviral therapy generally did not increase the frequency or severity of most adverse reactions. The most frequently reported events occurring in the TORO 1 and TORO 2 studies were diarrhoea (38 versus 73 patients with event per 100 patient years for Fuzeon + OB versus OB) and nausea (27 versus 50 patients with event per 100 patient years for Fuzeon + OB versus OB).

The following list presents events seen at a higher rate among patients receiving Fuzeon+OB regimen than among patients on the OB alone regimen with an exposure adjusted increase of at least 2 patients with event per 100 patient-years. These events are then designated frequency estimation (“very common” (

Infections and Infestations

Common : - sinusitis, skin papilloma, influenza, pneumonia, ear infection.

Blood and Lymphatic System Disorders

Common : - lymphadenopathy.

Metabolism and Nutrition Disorders

Common : - appetite decreased, anorexia, hypertriglyceridaemia, diabetes mellitus.

Psychiatric Disorders

Common : - anxiety, nightmare, irritability.

Nervous System Disorders

Very Common: - peripheral neuropathy.

Common: - hypoaesthesia, disturbance in attention, tremor.

Eye Disorders

Common : - conjunctivitis.

Ear and Labyrinth disorders

Common : - vertigo.

Respiratory, Thoracic and Mediastinal Disorders

Common : - nasal congestion.

Gastrointestinal Disorders

Common : - pancreatitis, gastro-oesophageal reflux disease.

Skin and Subcutaneous Tissue Disorders

Common : - dry skin, eczema seborrhoeic, erythema, acne.

Musculoskeletal, Connective Tissue and Bone Disorders

Common : - myalgia.

Renal and Urinary Disorders

Common : - Calculus renal.

General Disorders and Administration Site Conditions

Common : - influenza like illness, weakness.

Investigations

Very Common: - weight decreased

Common : - blood triglycerides increased, haematuria present.

In addition there have been a small number of hypersensitivity reactions attributed to enfuvirtide and in some cases recurrence has occurred upon re-challenge. (See section 4.4)

In HIV-infected patients with severe immune deficiency at the time of initiation of combination antiretroviral therapy (CART), an inflammatory reaction to asymptomatic or residual opportunistic infections may arise (see section 4.4).

Cases of osteonecrosis have been reported, particularly in patients with generally acknowledged risk factors, advanced HIV disease or long-term exposure to CART. The frequency of this is unknown (see section 4.4).

Laboratory abnormalities

The majority of patients had no change in the toxicity grade of any laboratory parameter during the study except for those listed in Table 3. Through week 48, eosinophilia [greater than the Upper Limit of Normal of> 0.7 x 10⁹/l] occurred at a higher rate amongst patients in the Fuzeon containing group (12.4 patients with event per 100 patient-years) compared with OB alone regimen (5.6 patients with event per 100 patient-years). When using a higher threshold for eosinophilia (>1.4 x 10⁹/l), the patient exposure adjusted rate of eosinophilia is equal in both groups (1.8 patients with event per 100 patient-years).

Table 3: Exposure adjusted Grade 3 & 4 laboratory abnormalities among patients on Fuzeon+OB and OB alone regimens, reported at more than 2 patients with event per 100 patient years

Laboratory Parameters Grading	Fuzeon+OB regimen Per 100 patient years	OB alone regimen Per 100 patient years
n (Total Exposure patient years)	663 (557.0)	334 (162.1)
ALAT
Gr. 3 (>5-10 x ULN)	4.8	4.3
Gr. 4 (>10 x ULN)	1.4	1.2
Haemoglobin
Gr. 3 (6.5-7.9 g/dL)	2.0	1.9
Gr. 4 (<6.5 g/dL)	0.7	1.2
Creatinine phosphokinase
Gr. 3 (>5-10 x ULN)	8.3	8.0
Gr. 4 (>10 x ULN)	3.1	8.6

4.9 Overdose

No case of overdose has been reported. The highest dose administered to 12 patients in a clinical trial was 180 mg as a single dose subcutaneously. These patients did not experience any adverse reactions that were not seen with the recommended dose. In an Early Access Program study, one patient administered 180 mg of Fuzeon as a single dose on one occasion. He did not experience an adverse reaction as a result.

There is no specific antidote for overdose with enfuvirtide. Treatment of overdose should consist of general supportive measures.

5. Pharmacological Properties

5.1 Pharmacodynamic Properties

Pharmacotherapeutic group: Other antivirals, ATC code: J05AX07

Mechanism of Action: Enfuvirtide is a member of the therapeutic class called fusion inhibitors. It is an inhibitor of the structural rearrangement of HIV-1 gp41 and functions by specifically binding to this virus protein extracellularly thereby blocking fusion between the viral cell membrane and the target cell membrane, preventing the viral RNA from entering into the target cell.

Antiviral activity in vitro: The susceptibility to enfuvirtide of 612 HIV recombinants containing the env genes from HIV RNA samples taken at baseline from patients in Phase III studies gave a geometric mean EC ₅₀ of 0.259 μg/ml (geometric mean + 2SD = 1.96 μg/ml) in a recombinant phenotype HIV entry assay. Enfuvirtide also inhibited HIV-1 envelope mediated cell-cell fusion. Combination studies of enfuvirtide with representative members of the various antiretroviral classes exhibited additive to synergistic antiviral activities and an absence of antagonism. The relationship between the in vitro susceptibility of HIV-1 to enfuvirtide and inhibition of HIV-1 replication in humans has not been established.

Antiretroviral drug resistance: Incomplete viral suppression may lead to the development of drug resistance to one or more components of the regimen.

In Vitro resistance to enfuvirtide: HIV-1 isolates with reduced susceptibility to enfuvirtide have been selected in vitro which harbour substitutions in amino acids (aa) 36-38 of the gp41 ectodomain. These substitutions were correlated with varying levels of reduced enfuvirtide susceptibility in HIV site-directed mutants.

In Vivo resistance to enfuvirtide: In phase III clinical studies HIV recombinants containing the env genes from HIV RNA samples taken up to week 24 from 187 patients showed> 4 fold reduced susceptibility to enfuvirtide compared with the corresponding pre-treatment samples. Of these, 185 (98.9%) env genes carried specific substitutions in region of aa 36 - 45 of gp41. The substitutions observed in decreasing frequency were at aa positions 38, 43, 36, 40, 42 and 45. Specific single substitutions at these residues in gp41 each resulted in a range of decreases from baseline in recombinant viral susceptibility to enfuvirtide. The geometric mean changes ranged from 15.2 fold for V38M to 41.6 fold for V38A. There were insufficient examples of multiple substitutions to determine any consistent patterns of substitutions or their effect on viral susceptibility to enfuvirtide. The relationship of these substitutions to in vivo effectiveness of enfuvirtide has not been established. Decrease in viral sensitivity was correlated to the degree of pre-treatment resistance to background therapy. (See Table 5)

Cross-resistance: Due to its novel viral target enfuvirtide is equally active in vitro against both wild-type laboratory and clinical isolates and those with resistance to 1, 2 or 3 other classes of antiretrovirals (nucleoside reverse transcriptase inhibitors, non-nucleoside reverse transcriptase inhibitors and protease inhibitors). Conversely, mutations in aa 36-45 of gp41 which give resistance to enfuvirtide would not be expected to give cross resistance to other classes of antiretrovirals.

Clinical Pharmacodynamic data

Studies in Antiretroviral Experienced Patients:The clinical activity of Fuzeon (in combination with other antiretroviral agents) on plasma HIV RNA levels and CD4 counts have been investigated in two randomised, multicentre, controlled studies (TORO 1 and TORO 2) of Fuzeon of 48 weeks duration. 995 patients comprised the intent-to-treat population. Patient demographics include a median baseline HIV-1 RNA of 5.2 log₁₀ copies/ml and 5.1 log₁₀ copies/ml and median baseline CD4 cell count of 88 cells/mm³ and 97 cells/mm³ for Fuzeon + OB and OB, respectively. Patients had prior exposure to a median of 12 antiretrovirals for a median of 7 years. All patients received an optimised background (OB) regimen consisting of 3 to 5 antiretroviral agents selected on the basis of the patient's prior treatment history, as well as baseline genotypic and phenotypic viral resistance measurements.

The proportion of patients achieving viral load of <400 copies/ml at week 48 was 30.4% among patients on the Fuzeon+OB regimen compared to 12% among patients receiving OB regimen only. The mean CD4 cell count increase was greater in patients on the Fuzeon + OB regimen than in patients on OB regimen only. (see Table 4)

Table 4 Outcomes of Randomised Treatment at Week 48 (Pooled Studies TORO 1 and TORO 2, ITT)

Outcomes	Fuzeon +OB 90 mg bid (N=661)	OB (N=334)	Treatment Difference	95% Confidence Interval	p-value
HIV-1 RNA Log Change from baseline (log10 copies/ml)*	-1.48	-0.63	LSM -0.85	-1.073, -0.628	<.0001
CD4+ cell count Change from baseline (cells/mm3 )#	+91	+45	LSM 46.4	25.1, 67.8	<.0001
HIV RNA > 1 log below Baseline**	247 (37.4%)	57 (17.1%)	Odds Ratio 3.02	2.16, 4.20	<.0001
HIV RNA <400 copies/ml**	201 (30.4%)	40 (12.0%)	Odds Ratio 3.45	2.36, 5.06	<.0001
HIV RNA <50 copies/ml**	121 (18.3%)	26 (7.8%)	Odds Ratio 2.77	1.76, 4.37	<.0001
Discontinued due to adverse reactions/intercurrent illness/labs†	9%	11%
Discontinued due to injection site reactions†	4%	N/A
Discontinued due to other reasons†φ§	13%	25%

* Based on results from pooled data of TORO 1 and TORO 2 on ITT population, week 48 viral load for subjects who were lost to follow-up, discontinued therapy, or had virological failure replaced by their last observation (LOCF).

# Last value carried forward.

** M-H test: Discontinuations or virological failure considered as failures.

^† Percentages based on safety population Fuzeon+background (N=663) and background (N=334). Denominator for non-switch patients: N=112.

^φ As per the judgment of the investigator.

^§ Includes discontinuations from loss to follow-up, treatment refusal, and other reasons.

Fuzeon+OB therapy was associated with a higher proportion of patients reaching <400 copies/ml (or <50 copies/ml) across all subgroups based on baseline CD4, baseline HIV-1 RNA, number of prior antiretrovirals (ARVs) or number of active ARVs in the OB regimen. However, subjects with baseline CD4>100 cells/mm³, baseline HIV-1 RNA <5.0 log₁₀ copies/ml,

Table 5 Proportion of Patients achieving <400 copies/ml and <50 copies/ml at Week 48 by subgroup (pooled TORO 1 and TORO 2, ITT)

Subgroups	HIV-1 RNA < 400 copies/ml	HIV-1 RNA < 50 copies/ml
Fuzeon + OB 90 mg bid (N=661)	OB (N=334)	Fuzeon + OB 90 mg bid (N=661)	OB (N=334)
BL HIV-1 RNA < 5.0 log101 copies/ml	118/269 (43.9%)	26/144 (18.1%)	77/269 (28.6%)	18/144 (12.5%)
BL HIV-1 RNA 101 copies/ml	83/392 (21.2%)	14/190 (7.4%)	44/392 (11.2%)	8/190 (4.2%)
Total prior ARVs 1	100/215 (46.5%)	29/120 (24.2%)	64/215 (29.8%)	19/120 (15.8%)
Total prior ARVs> 101	101/446 (22.6%)	11/214 (5.1%)	57/446 (12.8%)	7/214 (3.3%)
0 Active ARVs in background1,2	9/112 (8.0%)	0/53 (0%)	4/112 (3.5%)	0/53 (0%)
1 Active ARV in background1,2	56/194 (28.9%)	7/95 (7.4%)	34/194 (17.5%)	3/95 (3.2%)
1,2	130/344 (37.8%)	32/183 (17.5%)	77/334 (22.4%)	22/183 (12.0%)

¹Discontinuations or virological failures considered as failures.

²Based on GSS score.

5.2 Pharmacokinetic Properties

The pharmacokinetic properties of enfuvirtide have been evaluated in HIV-1-infected adult and paediatric patients.

Absorption: The absolute bioavailability after subcutaneous administration of enfuvirtide 90 mg in the abdomen was 84.3 ± 15.5%. Mean (± SD) C_max was 4.59 ± 1.5 μg/ml, AUC was 55.8 ± 12.1 μg*hr/ml The subcutaneous absorption of enfuvirtide is proportional to the administered dose over the 45 to 180 mg dose range. Subcutaneous absorption at the 90 mg dose is comparable when injected into abdomen, thigh or arm. In four separate studies (N = 9 to 12) the mean steady state trough plasma concentration ranged from 2.6 to 3.4 μg/ml.

Distribution: The steady state volume of distribution with intravenous administration of a 90 mg dose of enfuvirtide was 5.5 ± 1.1 l. Enfuvirtide is 92% bound to plasma proteins in HIV infected plasma over a plasma concentration range of 2 to 10 μg/ml. It is bound predominantly to albumin and to a lower extent to α-1 acid glycoprotein. In in vitro studies, enfuvirtide was not displaced from its binding sites by other medicinal products, nor did enfuvirtide displace other medicinal products from their binding sites. In HIV patients, enfuvirtide levels in the cerebrospinal fluid have been reported to be negligible.

Metabolism: As a peptide, enfuvirtide is expected to undergo catabolism to its constituent amino acids, with subsequent recycling of the amino acids in the body pool. In vitro human microsomal studies and in in vivo studies indicate that enfuvirtide is not an inhibitor of CYP450 enzymes. In in vitro human microsomal and hepatocyte studies, hydrolysis of the amide group of the C-terminus amino acid, phenylalanine results in a deamidated metabolite and the formation of this metabolite is not NADPH dependent. This metabolite is detected in human plasma following administration of enfuvirtide, with an AUC ranging from 2.4 to 15% of the enfuvirtide AUC.

Elimination: Clearance of enfuvirtide after intravenous administration 90 mg was 1.4 ± 0.28 l/h and the elimination half-life was 3.2 ± 0.42 h. Following a 90 mg subcutaneous dose of enfuvirtide the half-life of enfuvirtide is 3.8 ± 0.6 h. Mass balance studies to determine elimination pathway(s) of enfuvirtide have not been performed in humans.

Hepatic Insufficiency: The pharmacokinetics of enfuvirtide have not been studied in patients with hepatic impairment.

Renal Insufficiency: Analysis of plasma concentration data from patients in clinical trials indicated that the clearance of enfuvirtide is not affected to any clinically relevant extent in patients with mild to moderate renal impairment. In a renal impairment study AUC of enfuvirtide was increased on average by 43-62% in patients with severe or end stage renal disease compared to patients with normal renal function. Haemodialysis did not significantly alter enfuvirtide clearance. Less than 13% of the dose was removed during haemodialysis. No dose adjustment is required for patients with impaired renal function.

Elderly: The pharmacokinetics of enfuvirtide have not been formally studied in elderly patients over 65 years of age.

Gender and Weight: Analysis of plasma concentration data from patients in clinical trials indicated that the clearance of enfuvirtide is 20% low