Exemestane

Pronunciation: EX-e-MES-tane
Generic Name: Exemestane
Brand Name: Aromasin

Exemestane is used for:

Treating advanced breast cancer in women who are past menopause and whose disease has progressed after treatment with other medicines. It is also used in the treatment of early breast cancer in certain women who are past menopause and after treatment with other medicines. It may also be used for other conditions as determined by your doctor.

Exemestane is an aromatase inhibitor. It works by stopping the production of estrogen, which may decrease the size and growth of the tumor.

Do NOT use Exemestane if:

• you are allergic to any ingredient in Exemestane


• you have not undergone menopause


• you are pregnant, may become pregnant, or are breast-feeding


• you are taking any medicines that contain estrogen (eg, certain birth control pills, certain hormone replacement therapies)

Contact your doctor or health care provider right away if any of these apply to you.

Before using Exemestane:

Some medical conditions may interact with Exemestane. Tell your doctor or pharmacist if you have any medical conditions, especially if any of the following apply to you:

• if you are pregnant, planning to become pregnant, or are breast-feeding


• if you are taking any prescription or nonprescription medicine, herbal preparation, or dietary supplement


• if you have allergies to medicines, foods, or other substances


• if you have a history of liver or kidney problems, osteoporosis (weak bones), heart problems, blood vessel problems, or a stroke

Some MEDICINES MAY INTERACT with Exemestane. Tell your health care provider if you are taking any other medicines, especially any of the following:

• Carbamazepine, medicines that contain estrogen (eg, certain birth control pills, certain hormone replacement therapies), phenobarbital, phenytoin, rifampin, or St. John's wort because they may decrease Exemestane's effectiveness

This may not be a complete list of all interactions that may occur. Ask your health care provider if Exemestane may interact with other medicines that you take. Check with your health care provider before you start, stop, or change the dose of any medicine.

How to use Exemestane:

Use Exemestane as directed by your doctor. Check the label on the medicine for exact dosing instructions. Check the label on the medicine for exact dosing instructions.

• An extra patient leaflet is available with Exemestane. Talk to your pharmacist if you have questions about this information.


• Take Exemestane by mouth after a meal at the same time every day.


• Continue to take Exemestane even if you feel well. Do not miss any doses.


• If you miss a dose of Exemestane, take it as soon as possible. If it is almost time for your next dose, skip the missed dose and go back to your regular dosing schedule. Do not take 2 doses at once.

Ask your health care provider any questions you may have about how to use Exemestane.

Important safety information:

• Exemestane may cause dizziness. This effect may be worse if you take it with alcohol or certain medicines. Use Exemestane with caution. Do not drive or perform other possibly unsafe tasks until you know how you react to it.


• It may take several weeks for Exemestane to work. Do not stop taking Exemestane or take Exemestane for longer than prescribed without checking with your doctor.


• Lab tests, including complete blood cell counts, liver and kidney function, or bone density, may be performed while you take Exemestane. These tests may be used to monitor your condition or check for side effects. Be sure to keep all doctor and lab appointments.


• Exemestane should not be used in CHILDREN; safety and effectiveness in children have not been confirmed.


• PREGNANCY and BREAST-FEEDING: Do not take Exemestane if you are pregnant. It has been shown to cause harm to the fetus. Avoid becoming pregnant while you are taking it. If you may become pregnant, you must use effective birth control while you take Exemestane. Talk with your doctor about the use of effective birth control while you take Exemestane. If you think you may be pregnant, contact your doctor right away. It is not known if Exemestane is found in breast milk. Do not breast-feed while taking Exemestane.

Possible side effects of Exemestane:

All medicines may cause side effects, but many people have no, or minor, side effects. Check with your doctor if any of these most COMMON side effects persist or become bothersome:

Anxiety; back, joint, muscle, or limb pain; constipation; coughing; diarrhea; dizziness; flu-like symptoms; hair loss; headache; hot flashes; increased or decreased appetite; increased sweating; nausea; stomach pain or upset; tiredness; trouble sleeping; weight gain; vomiting.

Seek medical attention right away if any of these SEVERE side effects occur:

Severe allergic reactions (rash; hives; itching; difficulty breathing; tightness in the chest; swelling of the mouth, face, lips, or tongue); chest pain; confusion; depression; fainting; general feeling of being unwell; numbness, burning, or tingling in the skin, hands, or feet; numbness of an arm or leg; one-sided weakness; severe or sudden bone pain; severe stomach pain; shortness of breath; sudden, severe dizziness, headache, or vomiting; sudden, unusual weight gain; swelling of the hands, legs, or feet; vision or speech changes; yellowing of the skin or eyes.

This is not a complete list of all side effects that may occur. If you have questions about side effects, contact your health care provider. Call your doctor for medical advice about side effects. To report side effects to the appropriate agency, please read the Guide to Reporting Problems to FDA.

See also: Exemestane side effects (in more detail)

If OVERDOSE is suspected:

Contact 1-800-222-1222 (the American Association of Poison Control Centers), your local poison control center, or emergency room immediately.

Proper storage of Exemestane:

Store Exemestane at 77 degrees F (25 degrees C) in a tightly closed container. Brief storage at temperatures between 59 and 86 degrees F (15 and 30 degrees C) is permitted. Store away from heat, moisture, and light. Do not store in the bathroom. Keep Exemestane out of the reach of children and away from pets.

General information:

• If you have any questions about Exemestane, please talk with your doctor, pharmacist, or other health care provider.


• Exemestane is to be used only by the patient for whom it is prescribed. Do not share it with other people.


• If your symptoms do not improve or if they become worse, check with your doctor.


• Check with your pharmacist about how to dispose of unused medicine.

This information is a summary only. It does not contain all information about Exemestane. If you have questions about the medicine you are taking or would like more information, check with your doctor, pharmacist, or other health care provider.

Issue Date: February 1, 2012

Database Edition 12.1.1.002

Copyright © 2012 Wolters Kluwer Health, Inc.

More Exemestane resources

• Exemestane Side Effects (in more detail)
• Exemestane Use in Pregnancy & Breastfeeding
• Drug Images
• Exemestane Drug Interactions
• Exemestane Support Group
• 10 Reviews for Exemestane - Add your own review/rating

• Exemestane Professional Patient Advice (Wolters Kluwer)


• Exemestane Monograph (AHFS DI)


• exemestane Advanced Consumer (Micromedex) - Includes Dosage Information


• Aromasin Prescribing Information (FDA)


• Aromasin Consumer Overview

Compare Exemestane with other medications

• Breast Cancer

Xylocaine 10mg Spray

Xylocaine 10 mg Spray

lidocaine

Read all of this leaflet carefully before Xylocaine spray is given to you.

• Keep this leaflet. You may need to read it again.


• If you have any further questions, ask your doctor, dentist or pharmacist.


• This medicine has been prescribed for you. Do not pass it on to others. It may harm them, even if their symptoms are the same as yours.


• If any of the side effects get serious, or if you notice any side effects not listed in this leaflet, please tell your doctor or dentist.

In this leaflet:

• 1. What Xylocaine Spray is and what it is used for


• 2. Before Xylocaine Spray is given to you


• 3. How Xylocaine Spray is given to you


• 4. Possible side effects


• 5. How to store Xylocaine Spray


• 6. Further information

What Xylocaine Spray is and what it is used for

The name of your medicine is ‘Xylocaine 10 mg Spray’. It is referred to as ‘Xylocaine Spray’ in the rest of this leaflet.

Xylocaine Spray contains a medicine called lidocaine. This belongs to a group of medicines called local anaesthetics.

Xylocaine Spray is used to numb (anaesthetise) parts of the body. It stops pain happening during:

• Medical examinations and operations of the nose and throat.


• Childbirth, and after the birth if stitches are needed.


• Treatment at the dentist.

Before Xylocaine Spray is given to you

You must not be given Xylocaine Spray if:

• You are allergic (hypersensitive) to lidocaine or any of the other ingredients of Xylocaine Spray (see Section 6: Further information).


• You are allergic to any other local anaesthetics of the same class (such as prilocaine or bupivacaine).

You must not be given Xylocaine Spray if any of the above apply to you. If you are not sure, talk to your doctor or dentist before you are given Xylocaine Spray.

Take special care with Xylocaine Spray

Check with your doctor or dentist before having Xylocaine Spray if:

• You have any cuts, sores or ulcers in your throat, mouth or nose.


• You have a chest infection.


• You have epilepsy.


• You have heart problems such as a slow heart beat.


• You have very low blood pressure.


• You have liver or kidney problems.


• You have ever been told that you have a rare disease of the blood pigment called ‘porphyria’ or anyone in your family has it.

If you are not sure if any of the above apply to you, talk to your doctor before having Xylocaine Spray.

Taking other medicines

Please tell your doctor or dentist if you are taking, or have recently taken, any other medicines. This includes medicines that you buy without a prescription and herbal medicines. This is because Xylocaine Spray can affect the way some medicines work and some medicines can have an effect on Xylocaine Spray.

In particular, tell your doctor or dentist if you are taking any of the following medicines:

• Medicines used to treat an uneven heart beat (arrhythmia) such as mexiletine.

Pregnancy and breast-feeding

Before you are given Xylocaine Spray, tell your doctor or dentist if you are pregnant, planning to get pregnant, or if you are breast-feeding.

Ask your doctor or pharmacist for advice before taking any medicine if you are pregnant or breast-feeding.

Driving and using machines

• Xylocaine Spray may affect you being able to drive or use tools or machines. This depends on where in the body Xylocaine Spray is used and how much is used.


• Your doctor or dentist will tell you when it is safe for you to do these activities.

Important information about some of the ingredients of Xylocaine Spray

• Xylocaine Spray contains saccharin. If you have been told by your doctor that you cannot tolerate or digest some sugars (have an intolerance to some sugars), talk to your doctor before using this medicine.


• The banana flavouring in Xylocaine Spray contains propylene glycol. Propylene glycol may cause skin irritation.

How Xylocaine Spray is given to you

• Xylocaine Spray will usually be given to you by a doctor or dentist. The dose that your doctor or dentist gives you will depend on the type of pain relief that you need. It will also depend on your age and physical condition.


• If you are given Xylocaine Spray to take home, you must use the dose recommended by your doctor or dentist. Always use Xylocaine Spray exactly as your doctor or dentist has told you. You should check with them if you are not sure.

How to use Xylocaine Spray

• Do not use more than 20 sprays.


• You should use as few sprays as possible.


• Do not get the spray in your eyes.


• The spray nozzle is bent so that it works properly. Do not try to change the shape of the nozzle or it might break.

How to use Xylocaine Spray in the mouth and throat

• When Xylocaine Spray is used in the mouth and throat it causes a loss of feeling. This makes it more likely that food or liquid may go down the wrong way. Also, this may make it difficult to swallow or cause some people to accidentally bite their tongue or cheek.


• Xylocaine Spray should be used with care in the elderly, in people who are in poor general health and in children.

Cleaning the nozzle

Do not shorten the nozzle. Otherwise the spray will not work properly. If you need to clean the nozzle:

• Remove the nozzle from the spray bottle.


• Place the nozzle in boiling water for 5 minutes.


• Remove the nozzle from the water. Then dry the nozzle and replace it on top of the bottle.

If you use more Xylocaine Spray than you should

If you think you have used more Xylocaine Spray than you should, talk to your doctor or dentist immediately.

Possible side effects

Like all medicines, Xylocaine Spray may cause side effects although not everybody gets them.

Severe allergic reactions:

If you have a severe allergic reaction, tell your doctor immediately. The signs may include sudden onset of:

• Swelling of your face, lips, tongue or throat. This may make it difficult to swallow.


• Severe or sudden swelling of your hands, feet and ankles.


• Difficulty breathing.


• Severe itching of the skin (with raised lumps).

Other possible side effects:

• Irritation where Xylocaine Spray has been used.


• Feeling nervous.


• Feeling dizzy.


• Feeling sleepy.


• Loss of consciousness.


• Sore throat.


• Hoarse voice or loss of voice.


• Low blood pressure. This might make you feel dizzy or light-headed.


• Fits (seizures).


• Difficulty breathing or slow breathing.


• Slow heart beat.


• Stopped breathing or a stopped heart beat.

Do not be concerned by this list of possible side effects. You may not get any of them.

If any of the side effects get serious, or if you notice any side effects not listed in this leaflet, please tell your doctor or dentist.

How to store Xylocaine Spray

• Keep out of the reach and sight of children.


• Do not use after the expiry date which is stated on the bottle after EXP. The expiry date refers to the last day of that month.


• Do not store above 25°C. At temperatures below 8°C the spray solution may start to go solid. This will dissolve when the spray solution is warmed up gently to room temperature.


• Medicines should not be disposed of via wastewater or household waste. Ask your pharmacist how to dispose of medicines that are no longer required. These measures will help to protect the environment.

Further information

What Xylocaine Spray contains

The active ingredient is lidocaine. Each dose of spray contains 10 mg of lidocaine.

The other ingredients are ethanol, levomenthol, macrogol 400, essence of banana (contains propylene glycol), saccharin and purified water.

What Xylocaine Spray looks like and contents of the pack

Xylocaine Spray is a pump spray. It comes in a 50 ml bottle. Each bottle contains about 500 sprays.

Marketing Authorisation Holder and Manufacturer

The Marketing Authorisation for Xylocaine Spray is held by

AstraZeneca UK Ltd

600 Capability Green

Luton

LU1 3LU

UK

Xylocaine Spray is manufactured by

AstraZeneca UK Limited

Silk Road Business Park

Macclesfield

Cheshire

SK10 2NA

UK

To listen to or request a copy of this leaflet in Braille, large print or audio please call, free of charge:

0800 198 5000 (UK only)

Please be ready to give the following information:

Product name Reference Number


Xylocaine Spray 17901/0177

This is a service provided by the Royal National Institute of Blind People.

Leaflet prepared: November 2009.

© AstraZeneca 2009.

Xylocaine is a trade mark of the AstraZeneca group of companies.

PAI 09 0051a

P026382

Ophthalmic lubricants and irrigations

A drug may be classified by the chemical type of the active ingredient or by the way it is used to treat a particular condition. Each drug can be classified into one or more drug classes.

Ophthalmic lubricants are used to treat dry and irritated eyes.

See also

Medical conditions associated with ophthalmic lubricants and irrigations:

• Eye Dryness/Redness

Drug List:

Freshkote-Drops

Theratears

Tears-Again-Ointment

Lacri-Lube-S-O-P-Ointment

Artificial-Tears

Celluvisc

Clear-Eyes-Clr

Comfort-Tears

Dry-Eye-Relief

Genteal

Isopto-Tears

Lacrisert-Insert

Lubricant-Eye-Drops

Moisture-Drops

Murocel-Eye-Drops

Oasis-Tears

Opti-Free-Rewetting-Drops

Optive

Puralube-Tears-Drops

Refresh

Soothe

Sterilube

Systane

Systane-Balance

Tears-Naturale

Tears-Renew

Ultra-Fresh

Visine-Tears

Xylocaine Accordion Gel 2%

1. Name Of The Medicinal Product

Xylocaine Accordion Gel 2%.

2. Qualitative And Quantitative Composition

Each gram of gel contains lidocaine hydrochloride Ph. Eur. corresponding to lidocaine hydrochloride anhydrous 20mg.

3. Pharmaceutical Form

Topical anaesthetic gel.

4. Clinical Particulars

4.1 Therapeutic Indications

Surface anaesthesia and lubrication:

- The male and female urethra during cystoscopy, catheterisation, exploration by sound and other endourethral operations.

- Nasal and pharyngeal cavities in endoscopic procedures such as gastroscopy and bronchoscopy.

- During proctoscopy and rectoscopy.

- Intubation.

Symptomatic treatment of pain in connection with cystitis and urethritis.

4.2 Posology And Method Of Administration

As with any local anaesthetic, reactions and complications are best averted by employing the minimal effective dosage. No more than 4 doses should be given in any 24 hour period. Debilitated, elderly patients and children should be given doses commensurate with their age and physical condition. In children under 12 years of age, the dose should not exceed 6mg/kg.

Urethral anaesthesia

Surface anaesthesia of the male adult urethra: For adequate analgesia in males 20ml ( = 400mg lidocaine hydrochloride) jelly is required. The jelly is instilled slowly until almost half the syringe (10ml = 200mg lidocaine hydrochloride) is emptied. A penile clamp is then applied for several minutes at the corona; then the rest of the jelly is instilled.

When anaesthesia is especially important, e.g. during sounding or cystoscopy, a larger quantity of jelly, for example 30-40ml, may be instilled in 3-4 portions and allowed to work for 10 minutes before insertion of the instrument.

Surface anaesthesia of the female adult urethra: Instil 5-10ml in small portions to fill the whole urethra. In order to obtain adequate anaesthesia, several minutes should be allowed prior to performing urological procedures.

Endoscopy

Instillation of 10-20ml is recommended for adequate analgesia and a small amount should be applied on the instrument for lubrication.

Lubrication for endotracheal intubation

About 5ml applied on the surface of the tube just prior to insertion. Care should be taken to avoid introducing the product into the lumen of the tube.

4.3 Contraindications

Known history of hypersensitivity to local anaesthetics of the amide type or other components of the gel.

4.4 Special Warnings And Precautions For Use

Absorption from wound surfaces and mucous membranes is relatively high, especially in the bronchial tree. Xylocaine Accordion Gel 2% should be used with caution in patients with traumatised mucosa and/or sepsis in the region of the proposed application.

If the dose or site of administration is likely to result in high blood levels, lidocaine, in common with other local anaesthetics, should be used cautiously in patients with epilepsy, impaired cardiac conduction, bradycardia, impaired hepatic function and in severe shock.

The oropharyngeal use of topical anaesthetic agents may interfere with swallowing and thus enhance the danger of aspiration. This is particularly important in children because of their frequency of eating. Numbness of the tongue or buccal mucosa may increase the danger of biting trauma.

When used for endotracheal tube lubrication care should be taken to avoid introduction of the jelly into the lumen of the tube. The jelly may dry on the inner surface leaving residue which tend to clump with flexion, narrowing the lumen. There have been rare reports in which this residue has caused the lumen to occlude.

Care should be taken to avoid instillation of excessive amounts of Xylocaine Accordion Gel 2% into the rectum. This is of particular importance in infants and children. Systemic absorption of lidocaine may occur from the rectum, and large doses may result in CNS side-effects. On rare occasions convulsions have occurred in children.

4.5 Interaction With Other Medicinal Products And Other Forms Of Interaction

Lidocaine should be used with caution in patients receiving antiarrhythmic drugs since the toxic effects are additive.

4.6 Pregnancy And Lactation

There is no, or inadequate, evidence of safety of the drug in human pregnancy but it has been in wide use for many years without apparent ill consequence, animal studies having shown no hazard. If drug therapy is needed in pregnancy, this drug can be used if there is no safer alternative.

Lidocaine enters the mother's milk, but in such small quantities that there is generally no risk of affecting the child at therapeutic dose levels.

4.7 Effects On Ability To Drive And Use Machines

None known.

4.8 Undesirable Effects

In extremely rare cases local anaesthetic preparations have been associated with allergic reactions (in most severe instances anaphylactic shock).

Systemic adverse reactions are rare and may result from high plasma levels due to excessive dosage, rapid absorption or may result from hypersensitivity, idiosyncrasy or diminished tolerance on the part of the patient. Such reactions involve the central nervous system and/or the cardiovascular system.

CNS reactions are excitatory and/or depressant and may be characterised by nervousness, dizziness, convulsions, unconsciousness and possibly, respiratory arrest. The excitatory reactions may be very brief or may not occur at all, in which case the first manifestations of toxicity may be drowsiness, merging into unconsciousness and respiratory arrest.

Cardiovascular reactions are depressant and may be characterised by hypotension, myocardial depression, bradycardia and possibly cardiac arrest.

4.9 Overdose

Treatment of a patient with systemic toxicity consists of arresting convulsions and ensuring adequate ventilation with oxygen, if necessary, by assisted or controlled ventilation (respiration). If convulsions occur, they must be treated promptly by intravenous injection of thiopentone 100 or 200mg or diazepam 5 to 10mg. Alternatively succinylcholine 50 to 100mg i.v. may be used providing the clinician is capable of performing endotracheal intubation and managing a fully paralysed patient. If ventricular fibrillation or cardiac arrest occurs effective cardiopulmonary resuscitation must be instituted. Adrenaline in repeated doses and sodium bicarbonate should be given as rapidly as possible.

5. Pharmacological Properties

5.1 Pharmacodynamic Properties

Xylocaine 2% gel provides prompt and profound anaesthesia of mucous membranes and lubrication which reduces friction. Its water-miscible base, characterized by high viscosity and low surface tension, brings the anaesthetic into intimate and prolonged contact with the tissue, giving effective anaesthesia of long duration (approx. 20-30 min). Anaesthesia usually occurs rapidly (within 5 min, depending upon the area of application).

Lidocaine like other local anaesthetics, causes a reversible blockade of impulse propagation along nerve fibres by preventing the inward movement of sodium ions through the nerve membrane. Local anaesthetics of the amide type are thought to act within the sodium channels of the nerve membrane.

Local anaesthetic drugs may also have similar effects on excitable membranes in the brain and myocardium. If excessive amounts of drug reach the systemic circulation rapidly, symptoms and signs of toxicity will appear, emanating from the central nervous and cardiovascular systems.

Central nervous system toxicity (See "Overdose") usually precedes the cardiovascular effects as it occurs at lower plasma concentrations. Direct effects of local anaesthetics on the heart include slow conduction, negative inotropism and possibly cardiac arrest.

5.2 Pharmacokinetic Properties

Lidocaine is absorbed following topical administration to mucous membranes, its rate and extent of absorption being dependent upon the concentration and total dose administered, the specific site of application, and duration of exposure. In general, the rate of absorption of local anaesthetic agents following topical application is most rapid after intratracheal and bronchial administration. Lidocaine is also well-absorbed from the gastrointestinal tract, although little intact drug appears in the circulation because of biotransformation in the liver.

The plasma protein binding of lidocaine is dependent on the drug concentration, and the fraction bound decreases with increasing concentration. At concentrations of 1 to 4μg of free base per ml, 60 to 80 per cent of lidocaine is protein-bound. Binding is also dependent on the plasma concentration of the alpha-1-acid glycoprotein.

Blood concentrations of lidocaine after instillation into the urethra of doses up to 800mg are of low range and below toxic levels.

Lidocaine crosses the blood-brain and placental barriers, presumably by passive diffusion.

Lidocaine is metabolised rapidly by the liver, and metabolites and unchanged drug are excreted by the kidneys. Biotransformation includes oxidative N-dealkylation, ring hydroxylation, cleavage of the amide linkage, and conjugation. N-dealkylation, a major pathway of biotransformation yields the metabolites monoethylglycinexylidide and glycinexylidide. The pharmacological and toxicological actions of these metabolites are similar to, but less potent than, those of lidocaine. Approximately 90% of lidocaine administered is excreted in the form of various metabolites, and less than 10% is excreted unchanged. The primary metabolite in urine is a conjugate of 4-hydroxy-2, 6-dimethylaniline.

The elimination half-life of lidocaine following an intravenous bolus injection is typically 1.5 to 2.0 hours. Because of the rapid rate at which lidocaine is metabolised, any condition that affects liver function may alter lidocaine kinetics. The half-life may be prolonged two-fold or more in patients with liver dysfunction. Renal dysfunction does not affect lidocaine kinetics but may increase the accumulation of metabolites.

Factors such as acidosis and the use of CNS stimulants and depressants affect the CNS levels of lidocaine required to produce overt systemic effects. Objective adverse manifestations become increasingly apparent with increasing venous plasma levels above 6.0µg free base per ml.

5.3 Preclinical Safety Data

Lidocaine hydrochloride is a well established active ingredient.

6. Pharmaceutical Particulars

6.1 List Of Excipients

Hydroxypropyl methylcellulose, sodium hydroxide, hydrochloric acid, purified water.

6.2 Incompatibilities

None.

6.3 Shelf Life

36 months.

6.4 Special Precautions For Storage

Store below 25°C.

6.5 Nature And Contents Of Container

Disposable bellows syringes made of polypropylene.

6.6 Special Precautions For Disposal And Other Handling

None stated.

7. Marketing Authorisation Holder

Astra Pharmaceuticals Limited

Home Park

Kings Langley

Hertfordshire

WD4 8DH

8. Marketing Authorisation Number(S)

PL 0017/5037R

9. Date Of First Authorisation/Renewal Of The Authorisation

Granted 29th May 1990 following review

10. Date Of Revision Of The Text

17 May 2000

Urokinase 500,000 I.U.

1. Name Of The Medicinal Product

Urokinase medac 500,000 I.U.

Powder for solution for injection or infusion

2. Qualitative And Quantitative Composition

Each vial contains 500,000 I.U. of human urokinase extracted from human urine.

For a full list of excipients, see section 6.1.

3. Pharmaceutical Form

Powder for solution for injection or infusion

4. Clinical Particulars

4.1 Therapeutic Indications

Intravascular lysis of blood clots in the following conditions:

• extensive acute proximal deep vein thrombosis

• acute massive pulmonary embolism

• acute occlusive peripheral arterial disease with limb threatening ischemia

• thrombosed arteriovenous haemodialysis shunts

• thrombosed central venous catheters

4.2 Posology And Method Of Administration

Urokinase medac should only be used by physicians experienced in the management of thrombotic diseases in hospitals where adequate diagnostic and monitoring techniques are available.

Depending on the indication, the route of administration of Urokinase medac is by systemic intravenous infusion, by local intra-arterial catheter-directed infusion during arteriography, or by local instillation.

It must not be given by subcutaneous or intramuscular injection.

For instructions regarding reconstitution and further dilution, see section 6.6.

Adults

The dosage may be adjusted individually depending on the clinical condition. The following dose regimens should be used as a guideline.

Deep vein thrombosis

Urokinase medac should be administered by intravenous infusion into a peripheral vein using an initial dose of 4,400 I.U./kg bodyweight infused over 10 – 20 min, followed by a maintenance dose of 100,000 I.U. per hour for 2 – 3 days.

Pulmonary embolism

Urokinase medac should be administered by intravenous infusion into a peripheral vein using an initial dose of 4,400 I.U./kg bodyweight infused over 10 – 20 min, followed by a maintenance dose of 4,400 I.U./kg bodyweight per hour for 12 hours.

Occlusive peripheral arterial disease

Urokinase medac should be administered by local intra-arterial catheter-directed graded infusion using an initial dose of 4,000 I.U./min (i.e. 240,000 I.U. per hour) for 2 – 4 hours or until restoration of antegrade flow, followed by a dose of 1,000 – 2,000 I.U./min until complete lysis or a maximum of 48 hours.

Thrombosed arteriovenous haemodialysis shunts

Urokinase medac should be administered by local forced periodic infusion (pulse spray) into both branches of the shunt at a concentration of 5,000 to 25,000 I.U./ml up to a total dose of 250,000 I.U. If necessary, the application can be repeated every 30 – 45 minutes up to a maximum of 2 hours.

Thrombosed central venous catheters

Urokinase medac should be dissolved in physiological saline at a concentration of 5,000 I.U./ml. A volume sufficient to completely fill the lumen of the occluded catheter should be instilled and either locked for a duration of 20 to 60 minutes or pushed with aliquots of saline before the lysate is aspirated. The procedure may be repeated if necessary.

Special populations

• Elderly patients: Available data are limited in patients over 65 years and it is not known whether they respond differently from younger subjects. Urokinase medac should be used with caution in elderly patients (see section 4.4).

• Patients with renal or hepatic impairment: A dose reduction may be required in patients with impaired renal and/or hepatic function. In these cases, the fibrinogen level should not fall below 100 mg/dl.

Paediatric patients

There is very limited experience with urokinase in children with thromboembolic occlusive vascular disease and urokinase should not be used in this indication.

Urokinase medac may be used in children of all ages for the treatment of thrombosed central venous catheters using the same lock procedure as in adults.

Therapeutic monitoring

Before starting thrombolytic therapy, haemostasis tests should be performed including haematocrit, platelet count, thrombin time (TT) and activated partial thromboplastin time (aPTT).

If heparin has been given, it should be discontinued and the aPTT should be less than twice the normal control value before urokinase therapy is initiated.

For systemic administration, a 3 to 5 fold prolongation of the TT measured 4 hours after initiation of therapy is generally considered sufficient. However, results of coagulation tests and fibrinolytic activity do not reliably predict either efficacy or risk of bleeding.

Follow-up treatment

In order to prevent recurrent thrombosis subsequent administration of anticoagulants should be instituted provided the aPTT is less than twice the normal control value.

4.3 Contraindications

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

• Active clinically relevant bleeding

• Aneurysm and arteriovenous malformation

• Intracranial neoplasm or other neoplasm with risk of haemorrhage

• Decreased blood coagulation (haemorrhagic diathesis, concomitant therapy with anticoagulants, spontaneous fibrinolysis) and severe thrombocytopenia

• Severe uncontrolled arterial hypertension (systolic > 200 mmHg, diastolic > 100 mmHg; grade III or IV hypertensive retinopathy)

• Acute pancreatitis, pericarditis, bacterial endocarditis, sepsis

• Recent cerebrovascular accident (e.g. within 2 months)

• Recent trauma including cardiopulmonary resuscitation, thoracic surgery or neurosurgery (e.g. within 2 months)

• Recent major surgery until primary wound healing, recent organ biopsy, lumbar puncture, translumbal aortography (e.g. within 10 days)

4.4 Special Warnings And Precautions For Use

In the following conditions, the risk of bleeding may be increased and should be weighed against the anticipated benefits:

• Recent severe gastrointestinal bleeding

• Recent surgery other than thoracic or neurosurgery, recent obstetrical delivery, puncture of non-compressible vessels

• Moderate coagulation defects including those due to severe hepatic or renal diseases

• Cavernous pulmonary diseases

• Genitourinary tract diseases with existing or potential sources of bleeding (e.g. implanted bladder catheter)

• High likelihood of a left heart thrombus (e.g. mitral stenosis with atrial fibrillation) with possible risk of cerebral embolism

• Known septic thrombotic disease

• Severe cerebrovascular disease

• Elderly patients (especially those over 75 years)

Concomitant administration of urokinase with other thrombolytic agents, anticoagulants, or agents inhibiting platelet function may further increase the risk of serious bleeding (see section 4.5).

When bleeding occurs in patients receiving urokinase, it may be difficult to control. Although urokinase is intended to produce sufficient amounts of plasmin to lyse intravascular deposits of fibrin, other fibrin deposits including those which provide haemostasis (at sites of needle puncture, catheter insertion, cut, etc.) are also subject to lysis, and bleeding from such sites may result. Oozing of blood from sites of percutaneous trauma occurs frequently.

The possibility of bruising or haematoma formation, especially after intramuscular injections, is high during urokinase therapy. Intramuscular injections and unnecessary handling of the patient should be avoided. Venipunctures and invasive venous procedures should be performed as infrequently as possible and with care to minimize bleeding. If bleeding from an invasive site is not serious, urokinase therapy may be continued while closely observing the patient; local measures such as application of pressure should be initiated immediately.

Arterial invasive procedures must be avoided before and during urokinase treatment to minimise bleeding. If an arterial puncture is absolutely essential, it should be performed by a physician experienced in the procedure, using a radial or brachial rather than a femoral artery. Direct pressure should be applied at the puncture site for at least 30 minutes, a pressure dressing applied, and the site checked frequently for evidence of bleeding.

If severe bleeding occurs following systemic treatment with urokinase, infusion should be stopped immediately and measures to manage the bleeding implemented. Plasma volume expanders other than dextrans may be used to replace blood volume deficits; if blood loss has been extensive, administration of packed red blood cells is preferred to whole blood. If very rapid reversal of the fibrinolytic state is required, administration of an antifibrinolytic agent such as epsilon-aminocaproic acid may be considered (see section 4.9).

Urokinase medac is a highly purified enzyme produced from human urine. It also contains human serum albumin. Products manufactured from human source materials have the potential to transmit infectious agents. Procedures to control such risks strongly reduce but cannot completely eliminate the risk of transmitting infectious agents.

4.5 Interaction With Other Medicinal Products And Other Forms Of Interaction

Anticoagulants

Oral anticoagulants or heparin may increase the risk of haemorrhage and should not be used concomitantly with urokinase.

Active substances affecting platelet function

Due to increased risk of haemorrhage, concomitant use of urokinase and active substances that affect platelet function (e.g., acetylsalicylic acid, other non-steroidal anti-inflammatory agents, dipyridamole, dextrans) should be avoided.

Contrast agents

Contrast agents may delay fibrinolysis.

4.6 Pregnancy And Lactation

There are no adequate data from the use of urokinase in pregnant women. Animal studies are insufficient with respect to effects on pregnancy, embryonal/fetal development, parturition or postnatal development. The potential risk for humans is unknown. However, low-molecular urokinase fragments and active plasmin cross the placenta.

Urokinase should not be used during pregnancy or in the immediate post-partum period unless clearly necessary.

It is unknown whether urokinase is excreted into human breast milk. Breast-feeding should be avoided during treatment with urokinase.

4.7 Effects On Ability To Drive And Use Machines

Not relevant.

4.8 Undesirable Effects

Haemorrhage

The most frequent and severe adverse effect of urokinase therapy is haemorrhage. The haemostatic status of the patient may be more profoundly altered with urokinase therapy than with heparin or coumarin-derivative anticoagulant therapy.

Severe spontaneous bleeding, including fatalities resulting from cerebral haemorrhage, has occurred during urokinase therapy. Less severe spontaneous bleeding has occurred approximately twice as frequently as that occurring during heparin therapy. Patients with pre-existing haemostatic defects have the greatest risk of spontaneous bleeding.

Hypersensitivity reactions

In contrast to streptokinase, urokinase is reportedly non-antigenic. However, mild allergic reactions including bronchospasm and rash have been reported rarely. In addition, very rare cases of fatal anaphylaxis have been reported.

Infusion reactions

Fever and chills, including shaking chills (rigors), have been reported occasionally in patients receiving urokinase. Symptomatic treatment is usually sufficient to alleviate discomfort caused by urokinase-induced fever; however, acetylsalicylic acid should not be used.

Other infusion reactions reported with urokinase therapy include dyspnoea, cyanosis, hypoxemia, acidosis, back pain, and nausea and/or vomiting; these effects reactions generally occurred within one hour of beginning urokinase infusion.

The following frequency convention was used as a basis for the evaluation of undesirable effects:

Very common
Common:
Uncommon:
Rare:
Very rare	< 1/10,000

Immune system disorders

Rare	Hypersensitivity reactions including dyspnoea, hypotension, flushing, urticaria, rash
Very rare	Anaphylactic reactions

Vascular disorders

Very common	Haemorrhage from puncture sites, wounds
Haematoma
Epistaxis, gingival bleeding
Haematuria (microscopic)
Common	Intracranial haemorrhage
Gastrointestinal haemorrhage, retroperitoneal haemorrhage
Urogenital haemorrhage
Muscle haemorrhage
Embolism, including cholesterol embolism
Uncommon	Intrahepatic haemorrhage

General disorders and administration site conditions

Common

Fever, chills

Investigations

Very common

Decrease in haematocrit without clinically detectable haemorrhage Transient increase in transaminases

4.9 Overdose

Haemorrhage that occurs during treatment with urokinase may be controlled with local pressure and treatment continued. If severe bleeding occurs, treatment with urokinase must be stopped and inhibitors such as aprotinin, epsilon-aminocaproic acid, p-aminoethylbenzoic acid or tranexamic acid can be given. In serious cases, human fibrinogen, factor XII, packed red cells or whole blood should be given as appropriate. For correction of volume deficiency, dextrans should be avoided.

5. Pharmacological Properties

5.1 Pharmacodynamic Properties

ATC code: B01A D04, antithrombotic agent.

Urokinase medac is a highly purified form of naturally occurring human urokinase extracted from urine. Urokinase exists in two distinct molecular entities, a high molecular weight (approximately 54,000 daltons) and a low molecular weight (approximately 33,000 daltons). Urokinase medac contains more than 85 % of the HMW form.

Urokinase is a thrombolytic agent which converts plasminogen into plasmin (fibrinolysin) a proteolytic enzyme that degrades fibrin as well as fibrinogen and other plasma proteins. The activity of urokinase leads to a dose-dependent decrease in plasminogen and fibrinogen levels and to increased presence of fibrin and fibrogen degradation products, which have an anticoagulant effect and potentiate the effect of heparin. These effects persist for 12 – 24 hours after the end of urokinase infusion.

5.2 Pharmacokinetic Properties

Urokinase is eliminated rapidly from the circulation by the liver with a half-life of 10 to 20 minutes. The inactive degradation products are excreted via the bile and primarily via the kidneys.

Elimination is delayed in patients with liver disease and impaired kidney function.

5.3 Preclinical Safety Data

There is no preclinical safety data of additional value to the prescribing physician.

6. Pharmaceutical Particulars

6.1 List Of Excipients

Disodium phosphate dodecahydrate, sodium dihydrogen phosphate dihydrate, human albumin.

6.2 Incompatibilities

No information is available regarding loss of activity in PVC containers or plastic bags/syringes.

6.3 Shelf Life

34 months

Use reconstituted material immediately.

After reconstitution and dilution, chemical and physical stability has been demonstrated for 72 hours at room temperature. From a microbiological point of view, the product should be used immediately after reconstitution and dilution. If not used immediately, in-use storage times and conditions prior to use are the responsibility of the user and would normally not be longer than 24 hours at 2 °C to 8 °C.

6.4 Special Precautions For Storage

Do not store above 25 °C.

Keep the vial in the outer container to protect from light.

6.5 Nature And Contents Of Container

All presentations are contained in borosilicate clear type 1 glass vials closed with chlorobutyl rubber stoppers and sealed with an aluminium flip-off cap.

6.6 Special Precautions For Disposal And Other Handling

The powder for solution for infusion should be dissolved in water for injection and further diluted with 0.9 % sodium chloride solution or glucose 5 % or glucose 10 % solution.

The powder is to be reconstituted as follows:

For a 500,000 I.U. vial use 10 ml of water for injection.

After reconstitution the solution must be clear and colourless.

7. Marketing Authorisation Holder

medac

Gesellschaft für klinische

Spezialpräparate mbH

Fehlandtstr. 3

20354 Hamburg

Germay

Phone: +49 (0)4103 8006-0

Fax: +49 (0)4103 8006-100

8. Marketing Authorisation Number(S)

PL11587/0069

9. Date Of First Authorisation/Renewal Of The Authorisation

17/03/2010

10. Date Of Revision Of The Text

22/09/2010

Loestrin 30.

1. Name Of The Medicinal Product

Loestrin 30.

2. Qualitative And Quantitative Composition

Each Loestrin 30 tablet contains:

Norethisterone acetate Ph Eur	1.5mg
Ethinylestradiol Ph Eur	0.03mg

3. Pharmaceutical Form

Pale green convex film coated tablet.

4. Clinical Particulars

4.1 Therapeutic Indications

For the prevention of pregnancy in women who elect to use oral contraceptives. The efficacy of any contraceptive method, except sterilisation, depends upon the reliability with which it is used. Correct and consistent use of methods can result in lower failure rates.

4.2 Posology And Method Of Administration

For oral use.

One Loestrin 30 tablet should be taken daily at approximately the same time of day for three weeks and then an interval of one week allowed before commencing the second course of tablets. Second and subsequent courses should be taken for three weeks with one week without tablets between courses. Thus each new course of tablets is always started on the same day of the week. It is important that the tablets are taken as directed and should be taken without regard to menstrual bleeding except in the initial cycle.

Pill initiation

Provided that it is reasonably certain that a woman is not pregnant:

• COCs can be started at any time within 5 days of the start of menstrual bleeding without additional contraceptive precautions;

• COCs can be started at any other time in the cycle, or by women who are not menstruating, with additional contraceptive precautions for the first 7 days;

• a switch can be made from other methods of contraception, whether hormonal or not, at any time in the cycle. Additional contraceptive precautions are required for the first 7 days if changing from a non-hormonal method outside the first 5 days of the menstrual cycle.

Post-partum and post-abortum use

After pregnancy combined oral contraception can be started in non-lactating women 21 days after a vaginal delivery, provided that the patient is fully ambulant and there are no puerperal complications.

If the pill is started later than 21 days after delivery, then barriers and spermicides should be used until oral contraception is started and for the first 7 days of pill-taking. If unprotected intercourse has taken place after 21 days post-partum, then oral contraception should not be started until the first menstrual bleed after childbirth.

After a miscarriage or abortion, oral contraceptives may be started immediately.

Missed pills

• If one pill is missed during weeks 1, 2 or 3, or if a pack is started 1 day late, the pill should be taken as soon as possible and no additional contraceptive precautions need be taken.

• If more than one pill is missed during weeks 1, 2 or 3, or if a pack is started more than 1 day late, a pill should be taken immediately, daily pills should be continued and additional contraceptive precautions should be taken for the next 7 days;

• if the pills are missed in the first week and unprotected sex has taken place, the woman should discuss with a healthcare professional the use of emergency contraception;

• if the pills are missed in the third week, the current course of pills should be completed and the next pack should be started immediately.

Gastrointestinal upset

Vomiting or diarrhoea may reduce efficacy by preventing full absorption. Barriers and spermicides should therefore be used during and for 7 days after recovery and if these 7 days overrun the end of a pack, the next pack should be started without a break. In this case, a withdrawal bleed should not be expected until the end of the second pack. If the patient does not have a withdrawal bleed at the end of the second pack, she must return to the doctor to exclude the possibility of pregnancy.

4.3 Contraindications

1) Known or suspected pregnancy and lactation.

2) History of confirmed venous thromboembolism (VTE), family history of idiopathic VTE and other known risk factors for VTE.

3) Ischaemic heart disease, severe hypertension or coagulation abnormalities.

4) Liver disease including disorders of hepatic excretion e.g. Dubin-Johnson or Rotor syndromes, infective hepatitis (until liver function returns to normal), known or suspected disorders of lipid metabolism, porphyria, liver adenoma or carcinoma, gallstones or jaundice with prior pill use.

5) Sickle cell anaemia.

6) Known or suspected carcinoma of the breast or estrogen dependent neoplasms.

7) Undiagnosed abnormal vaginal bleeding.

8) History during pregnancy of idiopathic jaundice, severe pruritus, chorea, herpes or deterioration of otosclerosis.

9) Focal, severe or crescendo migraine or transient cerebral ischaemic attacks without headaches.

4.4 Special Warnings And Precautions For Use

The following information is principally based on studies in patients who used oral contraceptives with higher concentrations of estrogens and progestogens than those in common use today. The effect of long-term use of the oral contraceptives with lower concentrations of both estrogens and progestogens remains to be determined. The efficacy of any contraceptive method, except sterilisation, depends upon the reliability with which it is used. Correct and consistent use of such methods can result in lower failure rates.

Thrombo-embolism

An increased risk of thromboembolic disease (VTE) associated with the use of oral contraceptives is well established but is smaller than that associated with pregnancy, which has been estimated at 60 cases per 100,000 pregnancies. Some epidemiological studies have reported a greater risk of VTE for women using combined oral contraceptives containing desogestrel or gestodene (the so-called 'third generation' pills) than for women using pills containing levonorgestrel or norethisterone (the so-called 'second generation' pills).

The spontaneous incidence of VTE in healthy, non-pregnant women (not taking any oral contraceptive) is about 5 cases per 100,000 per year. The incidence in users of second generation pills is about 15 per 100,000 women per year of use. The incidence in third generation pills is about 25 cases per 100,000 women per year of use; this excess incidence has not been satisfactorily explained by bias or confounding. The risk of venous thromboembolism is highest during the first year a combined oral contraceptive is taken. This increased risk applies to the first time ever combined oral contraceptive use is begun rather than each time a woman starts a new type of combined oral contraceptive. The level of all these risks of VTE increases with age and is likely to be further increased in women with other known risk factors for VTE such as obesity. The suitability of combined oral contraceptives for patients with any of these risk factors should be discussed with the patient before a final decision is taken.

The physician should be alert to the earliest manifestations of these disorders (thrombophlebitis, cerebrovascular disorders, pulmonary embolism and retinal thrombosis). Should any of these occur or be suspected, Loestrin should be discontinued immediately.

Cigarette smoking increases the risk of serious cardiovascular side effects from oral contraceptive use. This risk increases with age and with heavy smoking (15 or more cigarettes a day) and is quite marked in women over 35 years of age. Women who use oral contraceptives should be strongly advised not to smoke.

Hepatic tumours

Benign hepatic tumours have been associated with oral contraceptive usage. Malignant hepatic tumours have also been reported on rare occasions in long term users of oral contraceptives. A hepatic tumour should be considered in the differential diagnosis when upper abdominal pain, enlarged liver or signs of intra-abdominal haemorrhage occur.

Ovarian, endometrial, cervical and breast cancer

Numerous epidemiological studies have been reported on the risks of ovarian, endometrial, cervical and breast cancer in women using combined oral contraceptives. The evidence is clear that combined oral contraceptives offer substantial protection against both ovarian and endometrial cancer.

The most important risk factor for cervical cancer is persistent HPV infection. Some epidemiological studies have indicated that long-term use of COCs may further contribute to this increased risk but there continues to be controversy about the extent to which this finding is attributable to confounding effects, e.g., cervical screening and sexual behaviour including use of barrier contraceptives.

A meta-analysis from 54 epidemiological studies reported that there is a slightly increased relative risk (RR = 1.24) of having breast cancer diagnosed in women who are currently using combined oral contraceptives (COCs). The observed pattern of increased risk may be due to an earlier diagnosis of breast cancer in COC users, the biological effects of COCs or, a combination of both. The additional breast cancers diagnosed in current users of COCs, or in women who have used COCs in the last ten years, are more likely to be localised to the breast than in those women who have never used COCs.

Breast cancer is rare among women under 40 years of age, whether or not they take COCs. Whilst this background risk increases with age, the excess number of breast cancer diagnoses in current and recent COC users is small in relation to the overall risk of breast cancer (see bar chart).

The most important risk factor for breast cancer in COC users is the age women discontinue the COC; the older the age at stopping, the more breast cancers are diagnosed. Duration of use is less important and the excess risk gradually disappears during the course of the ten years after stopping COC use, such that by 10 years there appears to be no excess.

The possible increase in risk of breast cancer should be discussed with the user and weighed against the benefits of COCs taking into account the evidence that they offer substantial protection against the risk of developing certain other cancers (e.g. ovarian and endometrial cancer).

Estimated cumulative numbers of breast cancers per 10,000 women diagnosed in 5 years of use and up to 10 years after stopping COCs, compared with numbers of breast cancers diagnosed in 10,000 women who had never used COCs

Reasons for stopping Loestrin immediately

1) Occurrence of migraine in patients who have never previously suffered from it. Any unusually frequent or severe headaches.

2) Any kind of visual disturbance e.g. proptosis or diplopia and migraine.

3) Suspicion of thrombosis or infarction.

4) Combined oral contraceptives should be stopped at least six weeks before elective surgery and during and following prolonged immobilisation e.g. after accidents, etc.

5) Loestrin should be discontinued if the patient becomes jaundiced or has a significant rise in blood pressure.

6) Patients with a history of depression should be carefully observed and the drug discontinued if the depression recurs to a serious degree.

7) Since the safety of Loestrin in pregnancy has not been demonstrated, it is recommended that for any patient who has missed a period, the absence of pregnancy should be established before continuing the contraceptive regimen.

8) Clear exacerbation of conditions known to be capable of deteriorating during oral contraception or pregnancy.

Assessment of women prior to starting oral contraceptives (and at regular intervals thereafter) should include a personal and family medical history of each woman. Physical examination should be guided by this and by the contraindications (section 4.3) and warnings (section 4.4) for this product. The frequency and nature of these assessments should be based upon relevant guidelines and should be adapted to the individual woman, but should include measurement of blood pressure and, if judged appropriate by the clinician, breast, abdominal and pelvic examination including cervical cytology.

In case of undiagnosed, persistent or recurrent abnormal vaginal bleeding, appropriate diagnostic measures should be conducted to rule out malignancy. Women with a strong family history of breast cancer or who have breast nodules should be monitored with particular care.

Estrogen-progestogen preparations should be used with caution in patients with a history of hypertension and some women experience an increase in blood pressure following the administration of contraceptive steroids. Pregnancy should be excluded before starting treatment. Because these agents may cause some degree of fluid retention, patients with conditions which might be influenced by this such as epilepsy, migraine, asthma, and cardiac or renal dysfunction should be carefully monitored.

A decrease in glucose tolerance has been observed in a significant percentage of patients on oral contraceptives. The mechanism of this decrease is obscure. For this reason, pre-diabetic and diabetic patients should be carefully observed whilst receiving Loestrin.

Under the influence of estrogen-progestogen preparations, pre-existing uterine fibroleiomyomata may increase in size. Loestrin may mask the onset of the climacteric.

The following conditions also require careful consideration: multiple sclerosis, porphyria, tetany, disturbed liver function, gallstones, cardiovascular disease, renal disease, chloasma or any disease that is prone to worsen during pregnancy. The deterioration or first appearance of any of these conditions may indicate that the oral contraceptive should be stopped. Contact lens wearers who develop visual changes or changes to lens tolerance should be assessed by an optometrist.

Interference with laboratory tests

The following laboratory results may be altered by the use of oral contraceptives: hepatic function (increased sulpho-bromophthalein retention and other tests); thyroid function (increased thyroid binding globulin (TBG) leading to increased circulating total thyroid hormone as measured by protein-bound iodine (PBI), T4 by column or by radioimmunoassay. Free T3 resin uptake is decreased, reflecting the elevated TBG. Free T4 concentration is unaltered); haematological tests (increased prothrombin and factors VII, VIII, IX and X, decreased antithrombin 3 and increased adrenaline induced platelet aggregation); measurement of pregnanediol excretion (reduced). Other binding proteins may be elevated in the serum, sex-binding globulins are increased, triglycerides may be increased and serum folate levels may be depressed. Therefore, if such tests are abnormal in a patient taking Loestrin, it is recommended that they be repeated after Loestrin has been withdrawn for two months. The pathologist should be advised of the administration of Loestrin when relevant specimens are submitted. Any influence of prolonged administration of Loestrin on pituitary, ovarian, adrenal, hepatic and uterine functions is unknown at present.

4.5 Interaction With Other Medicinal Products And Other Forms Of Interaction

Effects of other drugs on oral contraceptives

The effectiveness of combined oral contraceptives may be considerably reduced by interaction with drugs that induce hepatic enzyme activity e.g. carbamazepine, griseofulvin, phenytoin, phenobarbital, primidone and rifampicin. Other drugs suspected of having the capacity to reduce the efficacy of oral contraceptives include ampicillin and other broad-spectrum antibiotics.

Additional contraceptive precautions should be taken whilst taking enzyme inducing drugs and some antibiotics and for at least seven days after stopping them. If these seven days run beyond the end of the packet, the new packet should be started immediately without a break. Rifampicin is such a potent inducer that even if the course lasts for less than 7 days, the additional contraceptive precautions should be continued for at least 4 weeks after stopping it.

The herbal remedy St. John's Wort (Hypericum perforatum) should not be taken concomitantly with this medicine as this could potentially lead to a loss of contraceptive effect.

Ascorbic acid and paracetamol may increase plasma ethinylestradiol concentrations, possibly by inhibition of conjugation.

Administration of atorvastatin concomitantly with oral contraceptives containing ethinylestradiol and norethisterone acetate increased AUC values for norethisterone and ethinylestradiol by approximately 30% and 20% respectively.

Effects of oral contraceptives on other drugs:

Oral contraceptive combinations containing ethinylestradiol may inhibit the metabolism of other compounds. Increased plasma concentrations of ciclosporin, prednisolone and theophylline have been reported with concomitant administration of oral contraceptives. In addition, oral contraceptives may induce conjugation of other compounds. Decreased plasma concentrations of paracetamol have been noted when administered with oral contraceptives.

4.6 Pregnancy And Lactation

Loestrin is not recommended for use during pregnancy, suspected pregnancy and in lactating mothers. Studies do not suggest a teratogenic effect, particularly in so far as cardiac anomalies and limb reduction defects are concerned, when oral contraceptives are taken inadvertently during early pregnancy. The administration of oral contraceptives to induce withdrawal bleeding should not be used as a test for pregnancy. Oral contraceptives should not be used during pregnancy to treat threatened or habitual abortion.

4.7 Effects On Ability To Drive And Use Machines

None known.

4.8 Undesirable Effects

The following adverse effects which have been reported in patients receiving oral contraceptives are believed to be drug-related:

Nausea, vomiting, gastro-intestinal symptoms (such as abdominal cramps and bloating), breakthrough bleeding, spotting, change in menstrual flow, amenorrhoea during and after treatment, oedema, chloasma or melasma, breast changes (tenderness, enlargement and secretion), change in weight, cervical erosion and changes in cervical secretion, suppression of lactation when given immediately post-partum, cholestastic jaundice, migraine, rash (allergic), rise in blood pressure, depression, thrombo-embolic disorders, temporary infertility after discontinuation of treatment, reduced tolerance to carbohydrates, vaginal candidiasis, change in corneal curvature (steepening) and intolerance to contact lenses.

Although the following adverse effects have been reported in women taking oral contraceptives, an association has been neither confirmed nor refuted: prolonged amenorrhoea after discontinuing oral contraceptives, pre-menstrual like syndrome, headache, nervousness, dizziness, fatigue, cataract, backache, hirsutism, loss of scalp hair, erythema multiforme, erythema nodusum, haemorrhagic eruption, itching, changes in appetite, cystitis-like syndrome, vaginitis, porphyria, impaired renal function, haemolytic uraemic syndrome, Budd-Chiari syndrome, acne, changes in libido and colitis.

Menstrual changes

Breakthrough bleeding and spotting are sometimes encountered, especially during the first three months of use. Non-hormonal causes should be considered and adequate diagnostic measures taken to rule out malignancy or pregnancy in the event of breakthrough bleeding, as in the case of any abnormal vaginal bleeding. If pathology has been excluded, time or a change to another formulation may solve the problem.

4.9 Overdose

The usual effects in children are nausea and drowsiness. Slight vaginal bleeding occasionally occurs in girls. In view of the low toxicity following overdosage with oral contraceptives, it is suggested that treatment should be conservative.

5. Pharmacological Properties

5.1 Pharmacodynamic Properties

Loestrin achieves its contraceptive effect primarily by inhibition of ovulation through gonadotrophin suppression. It is possible that other sites of action such as changes in cervical mucus and in the endometrium may contribute to the efficacy of combined oral contraceptives.

5.2 Pharmacokinetic Properties

Ethinylestradiol is rapidly and almost completely absorbed and peak serum levels are usually attained within an hour of oral administration. At this time, the majority of drug is already conjugated, largely as the sulphate. These conjugates have a primary serum half-life of approximately 7 hours and a terminal half-life of 48 hours and are excreted in urine and faeces.

Norethisterone acetate undergoes rapid absorption with peak serum concentrations occurring at one hour after oral administration. Less than 5% is cleared as unchanged norethisterone; glucuronide and sulphate conjugates are excreted in urine and faeces. The terminal half-life for norethisterone conjugates has been estimated at 70 hours (range: 42 - 84 hours).

5.3 Preclinical Safety Data

The results of the preclinical tests do not add anything of further significance to the prescriber.

6. Pharmaceutical Particulars

6.1 List Of Excipients

Lactose, sucrose, maize starch, talc, powdered acacia, magnesium stearate, industrial methylated spirit*, purified water*, dichloromethane*, propylene glycol*, hypromellose 15, carnauba wax, hydroxypropylcellulose and E104, E110, E131, E132, E133, E171.

* Not present in final product

6.2 Incompatibilities

None known.

6.3 Shelf Life

3 years.

6.4 Special Precautions For Storage

Do not store above 30°C. Store in the outer carton.

6.5 Nature And Contents Of Container

Printed aluminium foil blister strip contained in a cardboard carton together with a product leaflet. Supplied in packs of 21 and 63 tablets.

6.6 Special Precautions For Disposal And Other Handling

No special instructions needed.

7. Marketing Authorisation Holder

Galen Limited

Seagoe Industrial Estate

Craigavon

BT63 5UA

UK.

8. Marketing Authorisation Number(S)

PL 27827/0024.

9. Date Of First Authorisation/Renewal Of The Authorisation

03 April 1974/11 February 2009.

10. Date Of Revision Of The Text

26 October 2011

Fluorouracil topical

Class: Skin and Mucous Membrane Agents, Miscellaneous
ATC Class: L01BC02
VA Class: DE600
Molecular Formula: C₄H₃FN₂O₂
CAS Number: 51-21-8
Brands: Carac, Efudex, Fluoroplex

Introduction

Pyrimidine antagonist; antimetabolite; antineoplastic agent.^{a b c g}

Uses for Fluorouracil

Actinic Keratoses

Used topically for the treatment of multiple actinic (solar) keratoses.^{b c e g}

Curettage or cryotherapy are preferred treatment options for isolated lesions.^a

Basal Cell Carcinoma

Used topically for the treatment of superficial basal cell carcinoma when conventional methods are impractical (e.g., in patients with multiple lesions or difficult treatment sites).^{a b g} Efficacy not established for treatment of other basal cell carcinomas; establish diagnosis before initiating treatment.^{a b g}

When lesions are isolated and easily accessible, conventional techniques (e.g., surgery, curettage and dessication, cryotherapy) are preferred because they have a higher response rate.^{a b g}

Fluorouracil Dosage and Administration

General

• 
  

  Following topical application, response is manifested by erythema, followed by scaling, tenderness, vesiculation, erosion, ulceration, necrosis, and reepithelialization.^{a b c g}

  
  


• 
  

  Complete healing of actinic keratoses lesions may not occur until 1–2 months after cessation of therapy.^{a b g}

  
  


• 
  

  Evaluate patients treated for superficial basal cell carcinoma for a reasonable period of time to determine if a cure has been obtained.^{a b g}

  
  

Administration

Topical Administration

Apply cream or solution topically with a nonmetallic applicator, clean fingertips, or gloved fingers in an amount sufficient to cover lesions.^{a b e g} If the fingers are used to apply the drug, wash hands immediately afterward.^{a b e g}

For external use only; not for ophthalmic, oral, or intravaginal use.^{e g} Avoid contact with eyes, nose, mouth, or other mucous membranes.^{a b c e f g} (See Local Inflammatory Reactions under Cautions.)

Actinic Keratoses

Apply topically to lesions as a 0.5, 1, or 5% cream or as a 2 or 5% solution.^{b c e g} Apply 0.5% cream to lesions on the face and anterior scalp.^{a e}

Apply a sufficient amount of 1–5% cream or 2–5% solution to cover lesions twice daily.^{a b c g}

Apply a thin film of 0.5% cream to lesions on face and anterior scalp once daily.^{a e f}

Wash skin and wait 10 minutes before applying 0.5% cream to affected area(s) of face and anterior scalp.^{e f}

Basal Cell Carcinoma

Apply topically as a 5% cream or solution;^{a b} apply a sufficient amount to cover lesions twice daily.^{a b}

Dosage

At equivalent concentrations, solutions are considered more effective than creams.^a

Adults

Actinic Keratoses

For multiple actinic (solar) keratoses, increased frequency of application, longer duration of treatment, or temporary, initial combination therapy with topical tretinoin may be necessary on areas other than the head and neck (e.g., hands, arms).^{a c}

Topical

Apply 1–5% cream or 2–5% solution twice daily.^{a b c g} Continue therapy until erosion, necrosis, and ulceration stage is reached, usually 2–4 weeks (for 5% cream or 2–5% solution)^{b g} or 2–6 weeks (for 1% cream)^c after initiation of treatment, then discontinue the drug.^{a b c g}

Apply 0.5% cream once daily to face and anterior scalp for up to 4 weeks as tolerated.^{a e f} Generally, local irritation resolves within 2 weeks of cessation of drug.^e

Basal Cell Carcinoma

Confirmed Superficial Basal Cell Carcinoma

Topical

Apply 5% cream or solution twice daily for at least 3–6 weeks; may require up to 10–12 weeks before the lesions are obliterated.^{a b g}

Prescribing Limits

Adults

Actinic Keratoses

Topical

0.5% cream: Maximum 4 weeks of therapy recommended.^{e f}

Special Populations

No special population dosage recommendations at this time.^g

Cautions for Fluorouracil

Contraindications

• 
  

  Known hypersensitivity to fluorouracil or any ingredient in the formulation.^{a c e g}

  
  


• 
  

  Dihydropyrimidine dehydrogenase activity deficiency.^{b e} (See Dihydropyrimidine Dehydrogenase Activity Deficiency under Cautions.)

  
  


• 
  

  Known or suspected pregnancy.^{b c e g} (See Fetal/Neonatal Morbidity and Mortality under Cautions.)

  
  

Warnings/Precautions

Warnings

Fetal/Neonatal Morbidity and Mortality

May cause fetal harm.^{b c e g} Birth defects (i.e., cleft lip and palate, ventricular septal defect) and miscarriages reported.^{b e g}

Advise women to avoid becoming pregnant during therapy.^{b f g} If used during pregnancy, or if patient becomes pregnant, apprise of potential fetal hazard.^{b e g}

Dihydropyrimidine Dehydrogenase Activity Deficiency

Deficiency of dihydropyrimidine dehydrogenase activity may cause prolonged fluorouracil clearance and toxicity.^{b e}

Risk of severe, unexpected toxic reactions including stomatitis, diarrhea, neutropenia, and neurotoxicity; life-threatening symptoms including severe abdominal pain, bloody diarrhea, vomiting, fever, and chills reported following topical application of 5% fluorouracil.^{b e} Discontinue therapy if symptoms of toxicity occur.^{b e}

Local Inflammatory Reactions

Local inflammatory reactions (e.g., swelling, scaling, pain, pruritus, burning, soreness, tenderness, suppuration, scarring, hyperpigmentation) occur in most patients.^a

Avoid application to mucous membranes due to the possibility of local inflammation and ulceration.^e

Occlusive Dressings

Occlusive dressings may increase percutaneous penetration of drug.^{b g}

Increased incidence and severity of inflammatory reactions in adjacent normal skin with use of occlusive dressings.^{b c g} If required, apply a porous gauze dressing.^{b g}

Sensitivity Reactions

Photosensitivity Reactions

Exposure to ultraviolet (UV) light increases the intensity of the inflammatory reaction.^{a b c g} (See Local Inflammatory Reactions under Cautions.) Minimize exposure to UV rays during and immediately following treatment.^{a g}

Hypersensitivity Reactions

Hypersensitivity reactions, including allergic contact dermatitis, reported.^c

Potential delayed hypersensitivity reaction; however, patch testing may be inconclusive.^{c e}

General Precautions

Precautions Related to Treatment of Actinic Keratosis

Treatment responses in areas that appear clinically normal may indicate sites of subclinical actinic keratoses.^{a c}

Topical Administration Precautions

Possible increased absorption through ulcerated or inflamed skin.^{b c e g} Possible systemic toxicity when applied to large ulcerated area(s).^a

Response in treated areas may be unsightly during therapy and, in some cases, for several weeks after therapy is discontinued.^{a b c g}

Laboratory Monitoring

If an affected area does not respond to treatment or keratotic lesion recurs following therapy, perform a biopsy to confirm the diagnosis of solar keratoses or as indicated in the management of superficial basal cell carcinoma.^{a b c e g}

Specific Populations

Pregnancy

Category X.^{b c e g} (See Fetal/Neonatal Morbidity and Mortality under Cautions.)

Lactation

Not known whether topical fluorouracil is distributed into milk.^{b c e g} Discontinue nursing or the drug.^{b c e g}

Pediatric Use

Safety and efficacy not established.^{b c e g}

Geriatric Use

No substantial differences in safety and efficacy measures were demonstrated in patients 65 years of age compared with younger adults.^e

Common Adverse Effects

Local effects (e.g., burning,^{b c e g} dryness,^e allergic contact dermatitis,^{b c g} erosions,^{b e g} erythema,^{b e g} hyperpigmentation,^{b c g} irritation,^{b c g} pain,^{b c e g} photosensitivity,^{b g} pruritus,^{b c g} scarring,^{b c g} rash,^{b g} soreness,^{b g} ulceration,^{b g} edema,^e telangiectasia),^{a c} eye irritation^e .

Fluorouracil Pharmacokinetics

Absorption

Bioavailability

Following application of fluorouracil 5% cream, approximately 6% of the topical dose is absorbed systemically, with peak plasma concentrations attained in 1 hour.^{a b e g}

Absorption of the drug into cells may be selectively greater in diseased skin than in normal skin.^a

Distribution

Extent

Not known whether fluorouracil is distributed into human milk.^{b c e g}

Elimination

Metabolism

Anabolized to active metabolites (e.g., 5-fluoro-2′-deoxyuridine-5′-monophosphate); catabolized to inactive metabolites (e.g., CO₂, urea, α-fluoro-β-alanine).^{b d g}

Stability

Storage

Topical

Creams and Solutions

Cream 0.5%: 20–25°C.^e

Cream 1%: Tight containers at 15–30°C; avoid freezing.^{a c}

Cream and solutions 2 and 5%: 25°C (may be exposed to 15–30°C);^{b g} avoid freezing.^a

ActionsActions

• 
  

  Interferes with DNA synthesis and, to a lesser extent, the formation of RNA by inhibiting the methylation of deoxyuridylic acid to thymidylic acid, a DNA precursor.^{a b e g}

  
  


• 
  

  Since DNA and RNA are essential for cell division and growth, may create a thymine deficiency, which provokes unbalanced growth and death of the cell.^{b e g}

  
  


• 
  

  Effects of DNA and RNA deprivation are most marked on cells that grow more rapidly.^{e g}

  
  

Advice to Patients

• 
  

  Importance of clinicians instructing patients about proper use of the drug, including associated precautions.^f Importance of reading manufacturer’s patient information.^f

  
  


• 
  

  Keep out of reach of children.^{e f}

  
  


• 
  

  Importance of women informing their clinician if they are or plan to become pregnant or plan to breast-feed; necessity for clinicians to advise women to avoid becoming pregnant during therapy, and advise pregnant women of risk to the fetus.^{b e f}

  
  


• 
  

  Importance of not using the drug for any disorder other than that for which it was prescribed.^{e f}

  
  


• 
  

  Risk of photosensitivity reaction;^{a b c e f g} importance of using sunscreen products and wearing protective clothing over treated areas.^f

  
  


• 
  

  Importance of washing hands immediately after application, if the drug is applied with fingers.^{b c e f g}

  
  


• 
  

  Advise patients not to apply on the eyelids or directly into the eyes, nose, or mouth.^{b c e f g}

  
  


• 
  

  Advise patients being treated for superficial basal cell carcinoma to contact their clinician if any suspicious lesion arises in the treatment area.^{b g}

  
  


• 
  

  Warn patients that the reaction in the treated areas may be unsightly during therapy and, in some cases, for several weeks after therapy is discontinued.^{a b c e f g}

  
  


• 
  

  Advise patients to continue therapy until erosion, necrosis, and ulceration stage is reached, usually 2–6 weeks after initiation of treatment, then discontinue the drug.^{a b c f}

  
  


• 
  

  Advise patients not to apply other topical medications, moisturizing creams, or cosmetics on the affected area, unless specifically directed otherwise by their clinician.^f

  
  


• 
  

  Inform patients that if abdominal pain, bloody diarrhea, vomiting, fever, or chills occur during therapy to discontinue the drug and contact their clinician.^{e f}

  
  


• 
  

  Importance of informing clinician of existing or contemplated concomitant therapy, including prescription and OTC drugs and dietary or herbal supplements, as well as any concomitant illnesses.^{e f}

  
  


• 
  

  Importance of informing patients of other important precautionary information.^{e f} (See Cautions.)

  
  

Preparations

Excipients in commercially available drug preparations may have clinically important effects in some individuals; consult specific product labeling for details.

* available from one or more manufacturer, distributor, and/or repackager by generic (nonproprietary) name

Fluorouracil

Routes	Dosage Forms	Strengths	Brand Names	Manufacturer
Topical	Cream	0.5%	Carac	Dermik
		1%	Fluroplex	Allergan
		5%	Efudex	Valeant
	Solution	2%*	Efudex	Valeant
			Fluorouracil Topical Solution	Taro
		5%*	Efudex	Valeant
			Fluorouracil Topical Solution	Taro

Comparative Pricing

This pricing information is subject to change at the sole discretion of DS Pharmacy. This pricing information was updated 03/2011. Actual costs to patients will vary depending on the use of specific retail or mail-order locations and health insurance copays.

Carac 0.5% Cream (DERMIK): 30/$209.99 or 90/$575.96

Efudex 5% Cream (VALEANT): 40/$345.99 or 120/$903.35

Efudex 5% Solution (VALEANT): 10/$126 or 30/$359.95

Fluoroplex 1% Cream (ALLERGAN DERMATOLOGICS): 30/$279.97 or 90/$779.94

Fluorouracil 2% Solution (TARO): 10/$65.99 or 30/$179.97

Fluorouracil 5% Cream (OCEANSIDE PHARMACEUTICALS): 40/$249.98 or 120/$709.91

Fluorouracil 5% Solution (TARO): 10/$101.99 or 30/$283.89

Disclaimer

This report on medications is for your information only, and is not considered individual patient advice. Because of the changing nature of drug information, please consult your physician or pharmacist about specific clinical use.

The American Society of Health-System Pharmacists, Inc. and Drugs.com represent that the information provided hereunder was formulated with a reasonable standard of care, and in conformity with professional standards in the field. The American Society of Health-System Pharmacists, Inc. and Drugs.com make no representations or warranties, express or implied, including, but not limited to, any implied warranty of merchantability and/or fitness for a particular purpose, with respect to such information and specifically disclaims all such warranties. Users are advised that decisions regarding drug therapy are complex medical decisions requiring the independent, informed decision of an appropriate health care professional, and the information is provided for informational purposes only. The entire monograph for a drug should be reviewed for a thorough understanding of the drug's actions, uses and side effects. The American Society of Health-System Pharmacists, Inc. and Drugs.com do not endorse or recommend the use of any drug. The information is not a substitute for medical care.

AHFS Drug Information. © Copyright, 1959-2011, Selected Revisions April 2009. American Society of Health-System Pharmacists, Inc., 7272 Wisconsin Avenue, Bethesda, Maryland 20814.

References

a. AHFS drug information 2008. McEvoy GK, ed. Fluorouracil. Bethesda, MD: American Society of Health-System Pharmacists; 2008: 3611.

b. Valeant Pharma. Efudex (fluorouracil 2 or 5%) cream and solution prescribing information. Costa Mesa, CA; 2005 Sept.

c. Allergan. Fluoroplex (fluorouracil 1%) topical cream prescribing information. Irvine, CA; 2003 Jan.

d. AHFS drug information 2008. McEvoy GK, ed. Fluorouracil. Bethesda, MD: American Society of Health-System Pharmacists; 2008: 1068–72.

e. Dermik. Carac (fluorouracil 0.5%) topical cream prescribing information. Bridgewater, NJ; 2006 Nov.

f. Dermik. Carac (fluorouracil 0.5%) topical cream patient information. Bridgewater, NJ; 2003 Dec.

g. Taro Pharmaceutical. Fluorouracil 2% and 5% topical solution prescribing information. Hawthorne, NY; 2003 Nov.

More Fluorouracil topical resources

• Fluorouracil topical Use in Pregnancy & Breastfeeding
• Fluorouracil topical Support Group
• 23 Reviews for Fluorouracil - Add your own review/rating

• fluorouracil topical Concise Consumer Information (Cerner Multum)


• Carac Topical Advanced Consumer (Micromedex) - Includes Dosage Information


• Carac Prescribing Information (FDA)


• Carac Cream MedFacts Consumer Leaflet (Wolters Kluwer)


• Efudex Prescribing Information (FDA)


• Fluoroplex Prescribing Information (FDA)

Compare Fluorouracil topical with other medications

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• Basal Cell Carcinoma
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