How much Doxorubin will you receive and how • allergic reactions e.g. fever, nettle rash, often: increased heartbeat, breathing problems, Adults dizziness

•    The dosage will depend on the type of cancer • stomach problems, nausea, vomiting, being treated, other medicines you are diarrhoea

receiving, your age, height, weight and your • kidney and bladder problems e.g. general medical condition inflammation and bleeding of the bladder,

•    The most commonly used dosage is blood in the urine, changed pattern of 60 - 75 mg/m² every 3 weeks urination, pain during urination

•    If you are being treated for cancer of the • liver problems, e.g. yellow eyes and skin, bladder the usual dose is 50 mg/50 ml every abnormal liver enzymes, inflamed liver. week and later on, every month

•    Your treatment schedule may be modified There is a chance that Doxorubin might cause depending on your body's response or other unwanted effects that may not occur until medication you are receiving months or years after the medicine is used. These

•    While you are being given Doxorubin your delayed effects may include certain types of doctor may want to monitor your heart cancer, such as leukaemia. Discuss these possible function. Your condition will also be closely effects with your doctor.

monitored during treatment. This will involve

blood tests Doxorubin may cause your urine to turn red in

•    Other medicines may be given during a course colour for a couple of days after each dose. of Doxorubin to treat or prevent side effects.

Medicines like Doxorubin often cause temporary Children hair loss. After treatment your normal hair Children may be given lower doses than those growth should return. used in adults.

If any of the side effects get serious, or if you If you have any questions about your treatment notice any side effects not listed in this leaflet, ask your doctor or nurse. please tell your doctor or nurse.

If you receive more Doxorubin than you should

As a doctor or nurse will be giving you your HOW TO STORE DOXORUBIN medicine, it is unlikely that you will receive an

incorrect dose. If you receive too much Doxorubin Keep out of the reach and sight of children. you may suffer from side effects sooner. Tell your The vials should be stored in a fridge and be doctor or nurse if you have any concerns about protected from light. Diluted solutions of the amount of medicine that you receive. Doxorubin should be stored in a fridge for 24

hours, and be protected from light. Do not use

If you miss a dose of Doxorubin Doxorubin after the expiry date that is stated on It is important that you do not miss an the outer packaging. The expiry date refers to appointment/injection. If you do miss an the last day of that month. injection, you should ensure that you receive your missed dose as soon as possible.

FURTHER INFORMATION

If you have any further questions on the use of

this product, ask your doctor or nurse. What Doxorubin contains:

• The active ingredient is doxorubicin hydrochloride

POSSIBLE SIDE EFFECTS • The other ingredients are sodium chloride,

hydrochloric acid/sodium hydroxide and water Like all medicines, Doxorubin can cause side for injections. effects. You should discuss them with your

doctor who will explain the risks and benefits of What Doxorubin looks like and contents of the your treatment. Some of the side effects can be pack:

lessened or treated by other medicines or • Doxorubin 0.2% comes as a red-orange therapy. solution for injection in vials of 5 ml (10 mg

doxorubicin hydrochloride per vial), 10 ml

Although not all of these side effects may occur, (20 mg doxorubicin hydrochloride per vial), if they do occur, they may need medical 25 ml (50 mg doxorubicin hydrochloride per attention. vial) and 100 ml (200 mg doxorubicin

hydrochloride per vial)

Tell your doctor immediately if any of the • Doxorubin 0.2% is supplied in packs of 1 or following occur: 10 vials.

•    blood problems, characterised by fever or

chills, sore throat, ulcers in the mouth or Marketing Authorisation Holder and throat, tiredness or weakness, unusual Manufacturer

bleeding or unexplained bruising Marketing Authorisation holder and company

•    heart problems, characterised by irregular responsible for manufacture: Pharmachemie B.V., heartbeat, problems with the heart muscle. Haarlem, The Netherlands.

After you have completed your course of This leaflet was last revised: September 2011

treatment, you should tell your doctor or nurse

immediately if you notice difficulty in breathing, PL 04946/0016

swelling of the feet or legs, or an irregular or

rapid heart beat.

The following side effects have also been reported:

•    inflammation, ulceration or swelling of the nose, mouth, or throat

•    flushing of the face

•    inflammation of a vein with a blood clot

•    conjunctivitis

•    pain, swelling or warmth around the vein where Doxorubin is being injected

r

4.7    Effects on ability to drive and use machines 5.2 Pharmacokinetic properties

Due to the frequent occurrence of nausea and The intravenous administration of doxorubicin is vomiting, driving and operation of machinery should followed by a rapid plasma clearance (t1/2 = 10 min.) be discouraged. and significant tissue binding. The terminal half-life is

approximately 30 hours. Doxorubicin is partly

4.8    Undesirable effects metabolised, mainly to doxorubicinol and to a lesser Dose limiting toxicities of therapy are extent, to the aglycon, and is conjugated to the myelosuppression and cardiotoxicity. glucuronide and sulphate. Biliary and faecal excretion Myelosuppression includes a transient leukopenia, presents the major excretion route. About 5 % of anaemia and thrombocytopenia, reaching its nadir at the dose is eliminated by renal excretion. Plasma

10 to 14 days after treatment. protein binding of doxorubicin ranges from 50-85 %. Cardiotoxicity may occur as arrhythmias directly The volume of distribution is 800-3500 l/irP. following drug administration; eCg changes, Doxorubicin is not absorbed after oral including T-wave flattening and S-T depression, may administration; it does not cross the blood-brain last up to 2 weeks after administration. barrier. Impairment of liver function may decrease The risk of cardiomyopathy increases at cumulative the clearance of doxorubicin and its metabolites. doses higher than 550 mg/m2. Age over 70 or below

15 years should be regarded as a risk factor. Also, 5.3 Preclinical safety data concomitant or previous treatment with mitomycin None stated.

C, cyclophosphamide or dacarbazine has been

reported to potentiate doxorubicin induced 6. Pharmaceutical Particulars cardiomyopathy. 6.1 List of excipients

Cardiotoxicity may be encountered several weeks or Sodium chloride, hydrochloric acid/sodium months after discontinuation of doxorubicin therapy. hydroxide, water for injections.

Other adverse reactions reported are: a generally

reversible alopecia; gastrointestinal disturbances, 6.2 Incompatibilities

including nausea, vomiting and diarrhoea. Mucositis Doxorubicin should not be mixed with 5-fluorouracil (stomatitis or oesophagitis) may occur 5 to 10 days or heparin. Contact with aluminium should be after administration. avoided.

Hypersensitivity reactions, such as fever, urticaria

and anaphylaxis have been occasionally reported. 6.3 Shelf-life

Doxorubicin influences and potentiates normal tissue Following the special precautions for storage (see reactions to radiation. Also, late ("recall") reactions section 6.4) the shelf-life of the 5 ml, and 25 ml vials may occur when doxorubicin is administered some is 36 months and the shelf-life of the 100 ml vial is time after irradiation. Facial flushing may occur if the 24 months as printed on the label. injection is given too rapidly Thrombophlebitis and The injection may be diluted with 0.9% sodium conjunctivitis have been reported. chloride solution or 5% glucose solution. Chemical Slight transient increases of liver enzymes have been and physical in-use stability has been demonstrated reported. Concomitant irradiation of the liver may for 7 days at room temperature (15-25°C) and cause severe hepatoxicity, sometimes progressing to protected from light.

cirrhosis. From a biological point of view, the product should As with other cytotoxic agents, myelodysplastic be used immediately. If not used immediately, in-use syndrome and acute myeloid leukaemia have been storage times and conditions prior to use are the observed after treatment with combination therapy responsibility of the user and would normally not be including doxorubicin. With topoisomerase II longer than 24 hours at 2 to 8°C, unless inhibitors, secondary leukaemias have been reported reconstitution/dilution (etc) has taken place in more frequently than expected in the form of acute controlled and validated aseptic conditions. myeloid leukaemia classification 2, 3 and 4. These

forms of leukaemia can have a short period of 6.4 Special precautions for storage

latency (1 to 3 years). They can be cured when Doxorubin 0.2%, injection should be stored at

detected at an early stage and with an appropriate 2-8°C, protected from light.

curative treatment (see section 4.4 "Special warnings

and special precautions for use"). 6.5 Nature and contents of container

Intravesical administration may cause the following Doxorubicin 0.2%, injection is supplied as a red-adverse reactions: haematuria, vesical and urethral orange, sterile solution in injection vials containing irritation, stranguria and pollakisuria. These reactions 5 ml (10 mg), 25 ml (50 mg), or 100 ml (200 mg), are usually of moderate severity and of short respectively, of doxorubicin hydrochloride 2 mg/ml. duration. Intravesical administration of doxorubicin

may cause a sometimes haemorrhagic cystitis; this 6.6 Instructions for use/handling may cause a decrease in bladder capacity. Any contact with the solution should be avoided. Doxorubicin may impart a red colouration to the During preparation and reconstitution a strictly urine. aseptic working technique should be used; protective

measures should include the use of gloves, mask,

4.9    Overdosage safety goggles and protective clothing.

Acute overdosage of doxorubicin enhances the toxic Use of a vertical laminar airflow (LAF) hood is effects of mucositis, leukopenia and recommended.

thrombocytopenia. Gloves should be worn during administration. Overdosage at intravesical administration may cause Waste-disposal procedures should take into account severe cystitis. Treatment of acute overdosage the cytotoxic nature of this substance. consists of treatment of the severely myelosuppressed If the doxorubicin solution contacts skin, mucosae or patient with hospitalisation, antibiotics and eyes, immediately wash thoroughly with water. Soap transfusions after consultation with an oncologist. may be used for skin cleansing.

Chronic overdosage with cumulative doses exceeding

550 mg/m2 increases the risk of cardiomyopathy and 7. Marketing Authorisation Holder resultant congestive heart failure. Treatment consists Pharmachemie B.V., of vigorous management of congestive heart failure Swensweg 5, with digitalis preparations and diuretics. Postbus 552,

Administration of a very high single dose may cause 2003 RN Haarlem, myocardial degeneration within 24 hours. The Netherlands.

5. Pharmacological Properties 8. Marketing Authorisation Number 5.1 Pharmacodynamic properties PL 04946/0016 Doxorubicin is a cytotoxic anthracycline antibiotic

isolated from cultures of Streptomyces peucetius var. 9. Date of First Authorisation/Renewal of caesius. Animal studies have shown a cytotoxic Authorisation action in several solid and haematologic tumours. 4 January 1996.

The mechanism of action is not completely elucidated.

A major mechanism is probably inhibition of 10. Date of (Partial) Revision of the Text

topoisomerase II, resulting in DNA breakage. January 2001.

Intercalation and free-radical formation is probably

of minor importance. Drug resistance, due to ^{Distributed by TEVA UK} Uirrite^ ^Ea^stbourne^, increased expression of the MDR-1 gene encoding BN22 9AG. for a multidrug efflux pump, has been reported

regularly. 67918-K 93.130.570-D