Monday, October 24, 2016

Comtess 200mg film-coated tablets





Comtess 200 mg film-coated tablets



Entacapone




Read all of this leaflet carefully before you start taking this medicine.



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


  • If you have any further questions, ask your doctor 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 gets serious, or if you notice any side effects not listed in this leaflet, please tell your doctor or pharmacist.




In this leaflet:



  • 1. What Comtess is and what it is used for


  • 2. Before you take Comtess


  • 3. How to take Comtess


  • 4. Possible side effects


  • 5. How to store Comtess


  • 6. Further information





What Comtess Is And What It Is Used For



Comtess is used together with levodopa to treat Parkinson’s disease. Comtess improves the therapeutic effect of levodopa in relieving the symptoms of Parkinson's disease. Comtess has no antiparkinsonian activity without levodopa.





Before You Take Comtess




Do not take Comtess



  • if you are allergic (hypersensitive) to entacapone or any of the other ingredients of Comtess;


  • if you have a tumour of the adrenal gland (known as pheochromocytoma; this may increase the risk of severe high blood pressure);


  • if you are taking certain antidepressants (ask your doctor or pharmacist whether your antidepressive medicine can be taken together with Comtess);


  • if you have liver disease;


  • if you have ever suffered from a rare reaction to antipsychotic medicines called neuroleptic malignant syndrome (NMS) and/or a rare muscle disorder called non-traumatic rhabdomyolysis.




Take special care with Comtess



  • if you are taking a medicine which may cause low blood pressure when rising from a chair or bed;


  • if you experience diarrhoea, monitoring of your weight is recommended in order to avoid potentially excessive weight loss;


  • if you experience excessive gambling or excessive sexual activity.


  • if you experience progressive anorexia, asthenia (weakness, exhaustion) and weight decrease within a relatively short period of time, a general medical evaluation including liver function should be considered.

The dose of other antiparkinsonian medicines may need to be adjusted when you start taking Comtess. Follow the instructions that your doctor has given you.



Entacapone taken with levodopa may cause drowsiness and may cause you to sometimes suddenly fall asleep. If this happens, you should not drive or use any tools or machines (see section ”Driving and using machines”).



There have been isolated cases of neuroleptic malignant syndrome (NMS), especially when treatment with both entacapone and other dopaminergic medicines has been abruptly discontinued or reduced. For the characteristics of NMS see section 4. Your doctor may advise you to slowly discontinue the treatment with entacapone and other dopaminergic medicines.



Children



Experience with Comtess in patients under 18 years is limited. Therefore, the use of Comtess in children cannot be recommended.





Taking other medicines



Comtess may increase the effects of other medicinal products (e.g. those containing rimiterol, isoprenaline, adrenaline, noradrenaline, dopamine, dobutamine, alpha-methyldopa, and apomorphine). Please tell your doctor or pharmacist if you are taking or have recently taken other medicines, including medicines obtained without a prescription or herbal medicines.



Comtess may make it harder for you to digest iron. Therefore, do not take Comtess and iron supplements at the same time. After taking one of them, wait at least 2 to 3 hours before taking the other.





Pregnancy and breast-feeding



Do not use Comtess during pregnancy or if you are breast-feeding.





Driving and using machines



Comtess taken together with levodopa may lower your blood pressure, which may make you feel light-headed or dizzy. Be particularly careful when you drive or when you use tools or machinery.



Comtess taken with levodopa may make you feel very drowsy, or cause you to sometimes find yourself suddenly falling asleep. If this happens, you must not drive or do anything else that requires you to be alert (e.g. using tools or machines) until you are clear of such problems. Otherwise you may put yourself and others at risk of serious injury or even death.






How To Take Comtess



Always take Comtess exactly as your doctor has told you. You should check with your doctor or pharmacist if you are not sure.



Comtess is taken together with preparations containing levodopa (either levodopa/carbidopa preparations or levodopa/benserazide preparations). You may also use other antiparkinsonian medicines at the same time.



The usual dose of Comtess is one 200 mg tablet with each levodopa dose. If you are receiving dialysis for renal insufficiency, your doctor may tell you to extend the interval between doses. The maximum recommended dose is 10 tablets per day, i.e. 2,000 mg of Comtess.




If you take more Comtess than you should



In the event of an overdose, consult your doctor or the nearest hospital immediately.





If you forget to take Comtess



If you forget to take the Comtess tablet with your levodopa dose, you should continue the treatment by taking the next Comtess tablet with your next levodopa dose.



Do not take a double dose to make up for a forgotten tablet.





If you stop taking Comtess



Do not stop taking Comtess unless your doctor tells you to. In such a case your doctor may need to re-adjust the dosage of your other antiparkinsonian medicines. Abrupt discontinuation of both Comtess and other antiparkinsonian medicines may result in unwanted side effects.




If you have any further questions on the use of this product, ask your doctor or pharmacist.





Possible Side Effects



Like all medicines, Comtess can cause side effects, although not everybody gets them. Usually side effects caused by Comtess are mild to moderate.




The frequencies are defined as:



Very common (affects more than 1 patient in 10)



Common (affects 1 to 10 patients in 100)



Uncommon (affects 1 to 10 patients in 1,000)



Rare (affects 1 to 10 patients in 10,000)



Very rare (affects less than 1 patient in 10,000)



Not known (frequency cannot be estimated from the available data).





Very common



Uncontrollable movements (dyskinesias), feeling sick (nausea) and harmless reddish-brown discoloration of urine.





Common



Uncontrollable movements (hyperkinesias), being sick (vomiting), worsening of symptoms of Parkinson’s disease, dizziness, diarrhoea, abdominal pain, constipation, dry mouth, hallucinations (seeing/hearing/feeling/smelling things that are not really there), prolonged muscle contractions (dystonia), tiredness, increased sweating, sleeplessness, vivid dreams, fall and confusion.





Rare



Rashes and abnormal results in liver function test.





Very rare



Mental restlessness, decreased appetite, weight decrease, hives.



The exact frequencies of these side effects are not known but are based on reports received since the product has been on the market: colitis (inflammation of the colon), hepatitis and skin, hair, beard and nail discolorations.



The side effects are often caused by the increased effects of levodopa therapy and are most common at the start of treatment. Some, such as uncontrollable movements, nausea and abdominal pain, may also be more common with higher doses (1,400 to 2,000 mg per day). If you experience such effects at the start of treatment with Comtess you should contact your doctor, who may decide to adjust your dosage of levodopa.



Excessive daytime drowsiness has been reported in rare cases in patients receiving Comtess with levodopa and there have been isolated cases of sudden sleep onset episodes.



A few cases of neuroleptic malignant syndrome (NMS) and rhabdomyolysis have been reported. NMS is a rare severe reaction to medicines used to treat disorders of the central nervous system and characterised by stiffness, muscle twitching, shaking, mental changes, coma, high body temperature, increased heart rate, and unstable blood pressure. Rhabdomyolysis is a rare severe muscle disorder.



Behavioural changes such as urge to gamble (pathological gambling) or increased sexual desire and urges (increased libido and hypersexuality) have been reported in patients receiving dopaminergic medicines including Comtess with levodopa.




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





How To Store Comtess



Keep out of the reach and sight of children.



Do not use Comtess after the expiry date which is stated on the carton and on the bottle label. The expiry date refers to the last day of that month.



This medicinal product does not require any special storage conditions.





Further Information




What Comtess contains



  • The active substance is entacapone. Each tablet contains 200 mg of entacapone.

  • The other ingredients in the tablet core are microcrystalline cellulose, croscarmellose sodium, povidone and magnesium stearate.

  • The film-coating contains partly hydrolysed polyvinyl alcohol, talc, macrogol, soybean lecithin, yellow iron oxide (E 172), red iron oxide (E 172) and titanium dioxide (E 171).




What Comtess looks like and contents of the pack



Comtess 200 mg film-coated tablets are brownish-orange, oval tablets with "COMT" engraved on one side. They are packed in bottles.



There are four different pack sizes (bottles containing 30, 60, 100 or 175 tablets). Not all pack sizes may be marketed.





Marketing Authorisation Holder and Manufacturer:




Orion Corporation

Orionintie 1

FI-02200 Espoo

Finland




For further information about this medicine, please contact the local representative of the Marketing Authorisation Holder:




























































United Kingdom

Orion Pharma (UK) Ltd.

Tel:+44 1635 520 300




This leaflet was last approved on 05 August 2009



Detailed information on this medicine is available on the European Medicine’s Agency (EMEA) web site: http://www.emea.europa.eu






Capozide LS Tablets




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





CAPOZIDE LS TABLETS



Captopril/Hydrochlorothiazide


Your doctor has prescribed Capozide LS tablets for you. Please read this leaflet before you take your medicine. It gives a summary of information about your medicine. If you want to know more, or are not sure about anything, ask your doctor or pharmacist.



REMEMBER:


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




What Is In Capozide Ls Tablets?


The active ingredients in Capozide LS tablets are captopril 25mg and hydrochlorothiazide 12.5mg. Captopril is a member of a group of medicines called Angiotensin Converting Enzyme (ACE) Inhibitors. ACE inhibitors reduce constriction of blood vessels, which makes it easier for the blood to flow through them. Hydrochlorothiazide is a member of the group of medicines called diuretics or "water tablets".


The tablets are packaged in blister packs of 28 tablets.


The other ingredients are lactose, magnesium stearate, pregelatinised maize starch, microcrystalline cellulose and stearic acid.



Who supplies Capozide LS Tablets?



United Kingdom



E R Squibb & Sons Ltd

Uxbridge Business Park

Sanderson Road

Uxbridge

Middlesex

UB8 1DH

Tel:0800 7311736



MANUFACTURER:



Bristol-Myers Squibb SARL

Avenue du Dr. Gilles

28230 Epernon

France




What is this medicine for?


Capozide LS tablets are used in the treatment of high blood pressure.





Before Taking Your Medicine:



Should you be taking this medicine?


Do NOT take these tablets if you answer YES to any of the following questions. Go back to your doctor for advice as soon as possible.


  • 1. Are you pregnant or planning to become pregnant?

  • 2. Are you breast feeding?

  • 3. Have you had an allergic reaction to any ingredients of Capozide LS or to any other medicines?

  • 4. Have you ever had a reaction which included swelling of the hands, lips, face or tongue, where the cause was unknown?

  • 5. Do you suffer from a type of disease known as a "collagen vascular disease", such as rheumatoid arthritis, systemic lupus erythematosus or scleroderma, that your doctor does not know about?

  • 6. Have you suffered from heart, kidney or liver disease that your doctor does not know about?



Can you take other medicines?


Do not take other medicines while you are taking Capozide LS tablets, unless you have told your doctor or pharmacist and asked their advice. These include medicines from pharmacies for colds, coughs, hay fever or sinus problems as these may increase your blood pressure. If you are also taking anti-inflammatory painkillers (e.g. indomethacin, ibuprofen), lithium, carbenoxolone, corticosteroids, corticotrophin (ACTH), some laxatives, injections of an antifungal (amphotericin), muscle relaxants (given at the time of surgery), cholestyramine resin, colestipol, allopurinol (treatment for gout), procainamide and digoxin (treatment for irregular heartbeats), immunosuppressants (e.g. azathioprine and cyclophosphamide), calcium salts, potassium supplements or salt substitutes containing potassium, diuretics (water tablets), other drugs which can increase potassium in your body, such as heparin, drugs that cause dilation of the blood vessels (e.g. minoxidil), clonidine, drugs used in diabetes, drugs used to treat psychotic conditions and some of the older antidepressants, or any other treatment for high blood pressure, remind your doctor before taking Capozide LS tablets.




Do you have high blood sugar (diabetes)?


The amount of insulin or other anti-diabetic medicines you need to use may change when using Capozide, especially during the first month of treatment - ask your doctor for advice.




Is it all right to drink alcohol?


Moderate amounts of alcohol will not affect Capozide LS. However, you should check with your doctor whether drinking is advisable for you.




Is it all right to drive?


Capozide LS tablets do not usually affect your ability to drive. However, if you feel light-headed or dizzy, do not drive and check with your doctor.




What if you have lactose intolerance?


Each tablet contains 35mg lactose. Therefore, Capozide should not be taken by patients with inherited lactose intolerance.




Who should you tell that you are taking Capozide LS?


Doctor - before having surgery or emergency treatment, if he prescribes any new treatment or if you are to have desensitisation treatment for wasp or bee stings. Tell your doctor you are taking Capozide LS before you have any blood or urine tests as Capozide LS may interfere with the results of some tests.


Dentist - before having dental surgery.


Pharmacist - before buying any medicines.




How much exercise should you take?


As you start feeling better you may try to do too much and feel faint, especially in hot weather. Make sure you discuss with your doctor a safe amount of exercise for you.




What if you are using dialysis?


There have been some reports of allergic-type reactions seen when people using drugs such as Capozide undergo dialysis. Tell your doctor before your next dialysis treatment.





Taking Your Medicine:



How should you take Capozide LS tablets?


You should try to take Capozide LS at about the same time each morning. The usual dose will be one or two tablets daily. If you are elderly or you have diabetes or kidney problems your doctor will probably start you on one tablet daily.




Can you take the tablets before or after meals?


It does not matter.




How long should you take them for?


Continue with Capozide LS tablets until your doctor tells you otherwise. Keep your doctor's appointments even if you feel well.




What if you take too many or a child swallows some?


Go to your nearest hospital Casualty Department or tell your doctor immediately. If you are going to the hospital, take the empty container and any remaining tablets with you. If the person has fainted, lay them down and raise their feet higher than their head.




What if you miss or forget to take a dose?


If you miss a dose do not worry. Just carry on taking your normal dose when the next one is due. DO NOT take a double dose to make up for the one you missed.





Undesirable Effects



Are there any unwanted effects of Capozide LS?


All medicines may cause some unwanted or "side-effects" in a few persons.


If you experience any of the following


STOP TAKING YOUR MEDICINE AND TELL YOUR DOCTOR IMMEDIATELY:


Swelling of the hands, face, lips or tongue, difficulty in breathing, sore throat or fever, severe dizziness or fainting, severe abdominal pain, unusually fast or irregular heart beat, jaundice (yellow skin/eyes), a sudden, unexpected rash or burning, red or peeling skin.


Sometimes Capozide LS causes dizziness, itching, rashes, hair loss, flushing or pale skin, taste impairment, anorexia, sore mouth, mouth ulcers, dry mouth, upset stomach, sickness, abdominal pain, diarrhoea or constipation, pins and needles, cold extremities, cough, sleep disorders, drowsiness, headache, respiratory problems, generalised weakness and restlessness. If these symptoms persist or become troublesome you should tell your doctor.


Other unwanted effects sometimes seen with Capozide LS include purpura (purplish or reddish-brown discolouration of the skin), necrotising angiitis (inflammation of the blood vessels), xanthopsia ("yellow vision"), gout, thrombocytopenia (which causes unusual bruising or bleeding), neutropenia or agranulocytosis (which may cause infection, sore throat or fever due to a lack of white cells).


Sometimes patients may feel dizzy after taking the first one or two doses of Capozide. If this happens to you, lie down till these symptoms disappear.


Rarely disorders of the blood, kidney or liver, and emergence of diabetes mellitus can occur. Your doctor may need to give you blood or urine tests to monitor your condition.


Very rarely, the following have been reported: confusion, depression, chest pain, heart attack, stroke, blurred vision, runny nose, swollen salivary glands, stomach ulcers, sensitivity of the skin to light, pains in the muscles and joints, muscle spasm, fatigue, swelling of the breasts, impotence, changes in the amount of chemicals in the blood.


Tell your doctor or pharmacist if you notice any other troublesome side-effects.



Note: The hydrochlorothiazide in this medicine would produce a positive anti-doping test result.


You will see an "Expiry date" on the outer packaging of Capozide LS. Do not use the tablets after this date.


Keep all your medicines where children cannot reach them, preferably in a locked cupboard or medicine cabinet. Keep Capozide LS tablets below 30°C. They should not get too hot or damp; so do not leave your tablets near a radiator on a window sill, or in the bathroom.


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


Date of last revision : June 2005






Clomifene 50mg Tablets (Wockhardt UK Ltd)





1. Name Of The Medicinal Product



Clomifene 50mg Tablets


2. Qualitative And Quantitative Composition



Each tablet contain 50mg of Clomifene Citrate



Excipient: Also contains lactose



For full list of excipients, see section 6.1



3. Pharmaceutical Form



Tablet



White, round tablets with HG C50 on one side and a breakline on the other side.



4. Clinical Particulars



4.1 Therapeutic Indications



The treatment of anovulatory infertility in women.



4.2 Posology And Method Of Administration



Route of administration : Oral



(i) Dosage Schedule



The recommended dose for the first course of treatment is 50mg (one tablet) daily for five days, starting within the first five days of spontaneous or induced menstrual bleeding. Therapy may be started as an arbitrary time in patients who have had no recent menstrual bleeding.



If ovulation occurs but is not followed by pregnancy, subsequent courses at the same dosage may be given up to a maximum of three cycles.



The majority of patients who are going to respond will respond to the first course of therapy, and three courses should constitute an adequate therapeutic trial. If ovulatory menses have not yet occurred, the diagnosis should be re-evaluated. Treatment beyond this is not recommended in the patient who does not exhibit evidence of ovulation.



Long-term cyclic therapy: Not recommended.



The relative safety of long-term cyclic therapy has not been conclusively demonstrated and, since the majority of patients will ovulate following three courses, long-term cyclic therapy is not recommended, i.e. beyond a total of about six cycles (including three ovulatory cycles).



(ii) Types of Patient



Not intended for children.



Not intended for elderly patients.



Only for women of reproductive age with anovulatory infertility.



4.3 Contraindications



Hypersensitivity to clomifene



Pregnancy



Liver disease or a history of liver dysfunction



Abnormal uterine bleeding until the cause has been determined



Pituitary or ovarian tumours



Ovarian cysts (other than in association with polycystic ovary syndrome)



4.4 Special Warnings And Precautions For Use



There have been rare reports of ovarian cancer with fertility drugs; infertility itself is a primary risk factor. Epidemiological data suggest that prolonged use of clomifene 50mg tablets may increase this risk. Therefore the recommended duration of treatment should not be exceeded (see section 4.2).



Patients with rare hereditary problems of galactose intolerance, the Lapp lactase deficiency or glucose-galactose malabsorption should not take this medicine.



Causes of infertility other than ovarian dysfunction should be excluded before the start of treatment.



Hyperstimulation of the ovary, with excessive ovarian enlargement, may occur rarely. Patients undergoing therapy with clomifene, particularly those with polycystic ovary syndrome, should receive the lowest possible doses to minimise ovarian enlargement or cyst formation. The patient should be instructed to report any abdominal or pelvic pain and should be evaluated for the presence of ovarian cysts before each cycle of treatment. Pelvic examination, which should be carried out with care, will reveal the diagnosis. The dose of clomifene should be reduced. Further courses should not be given until the ovaries have returned to pre-treatment size.



The incidence of multiple pregnancies is increased when conception takes place during a clomifene-stimulated cycle.



In order to avoid inadvertent administration of clomifene in early pregnancy, the basal body temperature should be monitored. In the absence of expected menses, a sensitive pregnancy test should be performed and only if negative should the patient be given the course of clomifene.



Clomifene should be used with caution:



• in patients with uterine fibroids, because of the risk of further enlargement of the fibroids



• in patients suffering from mental depression, because of the risk of exacerbation



• in patients with or susceptible to thrombophlebitis.



Clomifene therapy should be withdrawn if the patient experiences visual disturbances and a full ophthalmologic examination should be performed.



4.5 Interaction With Other Medicinal Products And Other Forms Of Interaction



None known.



4.6 Pregnancy And Lactation



Use during pregnancy is contraindicated.



It is not known whether clomifene is distributed into breast milk. However, the drug may suppress lactation.



4.7 Effects On Ability To Drive And Use Machines



Drowsiness or sedation do not occur, but patients should be warned that visual symptoms particularly blurring of vision occasionally occur during clomifene therapy and may affect their ability to drive or operate machinery. Onset is gradual.



4.8 Undesirable Effects



Side effects, when they occur, are generally mild. They are dose related.



Side effects are reversible on drug withdrawal.



Eye: Visual disturbances, including after-images and blurred vision may occur. Ocular side effects usually disappear within a few days or weeks after withdrawal of clomifene (see 4.4 Special warnings and precautions for use).



Gastro-intestinal: Nausea, vomiting.



General: Dizziness, lightheadedness, fatigue and insomnia.



Hepato-biliary: Jaundice



Metabolic: Weight gain



Neurological: Headache. Convulsions have been reported. Patients with a history of seizures may be predisposed.



Pregnancy: Ectopic or heterotopic pregnancies have occurred following treatment with clomifene. Patients should be warned that there is a risk of multiple pregnancies (rarely more than twins).



Psychiatric: Depression.



Reproductive: Among those reported, which are of low frequency at the recommended doses are ovarian hyperstimulation syndrome with ovarian enlargement and ovarian cyst formation (see 4.4 Special warnings and precautions for use), intermenstrual bleeding, menorrhagia, endometriosis, abdominal pelvic discomfort, hot flushes, breast tenderness or discomfort. Very rarely and only at much higher doses than those recommended, massive ovarian enlargement has been reported.



Skin: Rash, alopecia.



Tumours/neoplasms: Isolated reports have been received on the occurrence of endocrine-related or dependent neoplasms or their aggravation. Ovarian cancer: see section 4.4



4.9 Overdose



There is no experience with overdosage



5. Pharmacological Properties



5.1 Pharmacodynamic Properties



Clomifene is used to induce ovulation in women with anovulatory cycles. This agent is an anti-oestrogen and is believed to act by binding to oestrogen receptors in the hypothalamus and allowing follicle stimulating hormone (FSH) to rise in order to stimulate follicular development and ultimately result in ovulation.



It is probable that clomifene additionally exerts a direct effect on ovarian function.



5.2 Pharmacokinetic Properties



Clomifene is absorbed from the gastrointestinal tract and slowly excreted through the liver into the bile. The biological half life is reported to be about five days. Enterohepatic recirculation takes place.



5.3 Preclinical Safety Data



Nothing of relevance to the prescriber which dose not appear elsewhere in the SPC.



6. Pharmaceutical Particulars



6.1 List Of Excipients



Magnesium stearate



Maize starch



Lactose



6.2 Incompatibilities



Not applicable



6.3 Shelf Life



Five years



6.4 Special Precautions For Storage



Do not store above 25°C.



Store in original packaging.



6.5 Nature And Contents Of Container



Blister packs of 10 tablets manufactured from 250 micron white opaque PVC and 20 micron hard temper aluminium foil



Pack Sizes: 10, 20, 30, 100 tablets (1,2,3 or 10 strips) in an outer carton.



6.6 Special Precautions For Disposal And Other Handling



None



7. Marketing Authorisation Holder



Wockhardt UK Ltd,



Ash Road North,



Wrexham,



LL13 9UF,



UK.



8. Marketing Authorisation Number(S)



PL29831/0037



9. Date Of First Authorisation/Renewal Of The Authorisation



24 July 2007



10. Date Of Revision Of The Text



09 /11/2010




CAMCOLIT 250





1. Name Of The Medicinal Product



CAMCOLIT 250 mg, Lithium Carbonate


2. Qualitative And Quantitative Composition



The active ingredient is Lithium Carbonate; 250mg/tablet



3. Pharmaceutical Form



White film coated tablets engraved "CAMCOLIT" around one face and having a breakline on the reverse. For oral administration.



4. Clinical Particulars



4.1 Therapeutic Indications



The treatment and prophylaxis of mania, manic depressive illness and recurrent depression, and the treatment of aggressive or self mutilating behaviour.



4.2 Posology And Method Of Administration



CAMCOLIT 250mg tablets are usually administered according to a twice daily regimen. When lithium levels have stabilised, a once daily regimen may be preferred.



4.2.1 Dosage



Lithium carbonate has a narrow therapeutic window. Regular monitoring of plasma lithium concentration is always obligatory when Lithium is used; lithium therapy should not be initiated unless adequate facilities for routine monitoring of plasma concentrations are available. On initiation of treatment, plasma therapy concentrations should be measured weekly until stabilisation is achieved, then weekly for one month and at monthly intervals thereafter.



Additional measurements should be made if signs of lithium toxicity occur, on dosage alteration, development of significant intercurrent disease, signs of manic depressions or depressive relapse and if significant change in sodium or fluid intake occurs. More frequent monitoring is required if patients are receiving any drug treatment that affects renal clearance of lithium e.g. diuretics and NSAID (See section 4.4 and section 4.5). As bioavailability may vary between formulations, should a change of preparations be made, blood levels should be monitored weekly until restabilisation is achieved.



Toxic symptoms are usually associated with concentrations exceeding 1.5 mmol/l and levels above 1.5mmol/l should be avoided. In the event of toxicity, lithium should be withdrawn immediately.



However if lithium is to be discontinued for other reasons the dose should be reduced gradually over a suitable period of time, e.g. 2 weeks, to prevent the risk of relapse.



Acute mania:



Adults: Treatment should be initiated in hospital where regular monitoring of plasma lithium levels can be conducted. The dosage of Camcolit should be adjusted to produce a plasma lithium level between 0.6 and 1.0 mmol/l 12 hours after the last dose. The required plasma lithium level may be achieved in one of two ways but, whichever is adopted, regular estimations must be carried out to ensure maintenance of levels within the therapeutic range. For consistent results it is essential that the blood samples for plasma lithium estimations are taken 12 hours after the last dose of lithium.



1. 1,000-1,500 mg of lithium carbonate are administered daily for the first five days. A blood sample for plasma lithium estimation is taken 12 hours after the last dose on the fifth day, and the dosage of Camcolit is adjusted to keep the plasma lithium level within the therapeutic range. Subsequently, regular plasma lithium estimations must be carried out and, where necessary, the dosage of Camcolit adjusted accordingly. The precise initial dose of lithium should be decided in the light of the age and weight of the patient; young patients often require a dose higher than average and older patients a lower dose.



2. A lithium clearance test is carried out and the initial dosage calculated from the results. Even when the initial dosage is calculated in this way, it is still desirable that plasma lithium levels should be determined at weekly intervals during the first three weeks of treatment, and any necessary adjustments to dosage made as a result of the levels actually obtained.



Most of the above applies in the treatment of hypomania as well as mania, but the patient (if not too ill) can be started on treatment as an outpatient provided that facilities for regular plasma lithium monitoring are available, and assays are initiated within one week.



Prophylaxis of recurrent affective disorders:



Adults: (Including unipolar mania & unipolar depressions and bipolar manic-depressive illness): A low dose of 300-400 mg of lithium carbonate can be administered daily for the first seven days. A blood sample for plasma lithium estimation is then taken 12 hours after the last dose, and the dosage of Camcolit is adjusted to keep the plasma lithium level within the range of 0.4-0.8 mmol/l.



Aggressive and self-mutilating behaviour:



Adults: Dosage is at the lower end of the range for the treatment for manic depressive illness.



4.2.2 Special Populations



Elderly: Elderly patients often require lower lithium dosage to achieve therapeutic serum levels. As for prophylaxis above, but 12 hour lithium levels should be kept in the range of 0.4-0.7 mmol/l as toxic symptoms are likely with plasma concentrations above 1.0 mmol/l. Toxic symptoms are more likely at lower concentrations than in the general population.



Children: Not recommended.



4.3 Contraindications



• A history of hypersensitivity to lithium or any of the excipients.



• Severely impaired renal function



• Untreated or untreatable hypothyroidism.



• Cardiac disease associated with rhythm disorder.



• Low body sodium levels for example dehydrated patients, those on low sodium diets, or those with Addison's disease.



• Breast feeding.



4.4 Special Warnings And Precautions For Use



Lithium carbonate has a narrow therapeutic window. The dose required for treatment must be titrated and adjusted on the basis of regular monitoring of serum concentration of lithium. Lithium therapy should not be initiated unless adequate facilities for routine monitoring of plasma concentrations are available.



Elderly patients are particularly liable to lithium toxicity. Use with care as lithium excretion may also be reduced. They may also exhibit adverse reactions at serum levels ordinarily tolerated by younger patients (see section 4.2).



Lithium excretion is reduced in the presence of renal impairment. This increases the risk of toxicity. Lithium is contra-indicated in patients with severe renal impairment (see section 4.3). If patients with mild or moderate renal impairment are being treated with lithium, serum levels should be closely monitored.



Renal function should be monitored in patients with renal impairment, and in patients with polyuria and polydipsia.



Before beginning a lithium treatment



-It is important to ensure that renal function is evaluated (see section 4.3 and 4.4)



-Cardiac function should be assessed especially in patients with cardiovascular disease.



-Thyroid function should be evaluated. Patients should be euthyroid before initiation of lithium therapy.



-Renal, cardiac and thyroid functions should be re-assessed periodically.



Monitoring of blood lithium levels



Serum concentration of lithium should be measured on a sample taken just prior to the time when a dose of lithium is due to be taken (i.e. at trough level 12 hours following the last dose).



Toxic effects may be expected at serum-lithium concentrations of about 1.5 mmol/litre, although they can appear at lower concentrations. They call for immediate withdrawal of treatment and should always be considered very seriously



Serum lithium concentrations should be monitored more frequently (revert to weekly monitoring) in the following circumstances:



- Dosage alteration or change of lithium formulation (bioavailability may differ)



- Significant intercurrent disease



- Intercurrent infection



- Significant change in sodium intake



- Significant change in fluid intake



- Treatment with drugs altering renal clearance of lithium



- Treatment with drugs likely to upset electrolyte balance.



Patients should also be warned to report if polyuria or polydipsia develops. Episodes of nausea and vomiting or other conditions leading to salt/water depletion (including severe dieting) should also be reported. Patients should be advised to maintain their usual salt and fluid intake.



Concomitant administration of antipsychotics should be avoided.



Lithium should be stopped 24 hours before major surgery, but the normal dose can be continued for minor surgery if fluids and electrolytes are carefully monitored



Warnings to be given to patients about signs and symptoms of toxicity



Clear instructions regarding the symptoms of impending toxicity should be given by the doctor to all patients receiving long-term lithium therapy (see Section 4.9 for symptoms of intoxication) and advice given for the need for urgency in seeking medical assistance if these symptoms appear.



4.5 Interaction With Other Medicinal Products And Other Forms Of Interaction



Interactions may occur as a result of increased or decreased lithium levels, or may act through other mechanisms, the most important being neurotoxicity which may occur at therapeutic levels when other drugs which act centrally on the CNS are taken concurrently.



Interactions which increase lithium concentrations



Co-administration of the following drugs with lithium may lead to increased lithium concentrations and a risk of toxicity:



• any drug which may cause renal impairment has the potential to cause lithium levels to rise, thereby causing toxicity. If the use of the drug is unavoidable, carefully monitor lithium blood level and adapt dosage as necessary.



• antibiotics (metronidazole, tetracyclines, co-trimoxazole, trimethoprim), N.B. Toxic symptoms may also occur at low or normal levels when used in conjunction with co-trimoxazole or trimethoprim. non-steroidal anti-inflammatory drugs (including selective cyclo-oxygenase (COX) II inhibitors.



• drugs affecting the renin angiotensin system (ACE inhibitors, Angiotensin II receptor antagonists).



• Diuretics (including herbal preparations). In addition to the effects noted above, thiazide diuretics show a paradoxical antidiuretic effect resulting in possible water retention and lithium intoxication. Loop diuretics (furosemide and bumetanide, seem less likely to cause lithium retention, although caution is warranted.



• Other drugs affecting electrolyte balance, e.g. steroids, may alter lithium excretion and should therefore be avoided.



Interactions which decrease serum lithium concentrations:



Co-administration of the following drugs with lithium may lead to decreased lithium concentrations and a risk of loss of efficacy:



• xanthine derivatives (e.g. theophylline, caffeine).



• products containing large quantities of sodium e.g. sodium bicarbonate.



• carbonic anhydrase inhibitors.



• Urea.



Interactions which may not be associated with increased or reduced lithium levels:



Concomitant use of the following drugs may precipitate symptoms of toxicity when the lithium level is within the normal range.



• antipsychotics, including the atypical antipsychotics olanzapine, clozapine and haloperidol at high doses.



• carbamazepine



• phenytoin



• methyldopa



• clonazepam



• tricyclic and tetracyclic antidepressants



• calcium channel blockers. These drugs may cause neurotoxic reactions at therapeutic levels.



• neuromuscular blocking agents. Lithium may cause neurotoxic reactions at therapeutic lithium levels.



Selective serotonin re-uptake inhibitors (SSRIs): Concurrent use with lithium may precipitate a serotonergic syndrome.



Non-steroidal anti-inflammatory drugs including COX II inhibitors: monitor serum lithium concentrations more frequently if NSAID therapy is initiated or discontinued



Triptans: lithium toxicity reported suggestive of serotonin syndrome.



Drugs which prolong the QT interval



Lithium can cause an increase in the QTc interval, particularly at higher blood levels. Therefore concurrent use of drugs which have a risk of prolonging the QTc interval should be avoided, and consideration be made of other potential risk factors such as increasing age, female sex, congenital long QT syndrome, cardiac and thyroid disease and the following metabolic disturbances: hypocalcaemia, hypokalaemia, hypomagnesaemia.



The following products have a high risk of causing QT prolongation and torsade de pointes: Class Ia antiarrhythmics , (disopyramide, procainamide, quinidine), Class III antiarrhythmics (amiodarone, sotalol), arsenic trioxide, artemisinin derivatives, dolasetron mesylate, mefloquine, intravenous erythromycin, amisulpride, haloperidol, pimozide, sertindole, terfenadine, thioridazine.



ECG should be performed after initiation of treatment and at any point where the patient becomes symptomatic or when there are changes in disease or treatment which may increase the risk of interaction or arrhythmia.



Non Drug Interactions:



• Low sodium diet. Rapid reduction of sodium intake may cause raised lithium levels.



• Intercurrent illness may cause lithium toxicity.



Raised plasma levels of ADH may occur during treatment



4.6 Pregnancy And Lactation



Lithium therapy should not be used during pregnancy, especially during the first trimester, unless considered essential. There is epidemiological evidence that it may be harmful to the foetus in human pregnancy. Lithium crosses the placental barrier. In animal studies lithium has been reported to interfere with fertility, gestation and foetal development. An increase in cardiac and other abnormalities, especially Ebstein anomaly, are reported. Therefore, a pre-natal diagnosis such as ultrasound and electrocardiogram examination is strongly recommended. In certain cases where a severe risk to the patient could exist if treatment were stopped, lithium has been continued during pregnancy.



If it is considered essential to maintain lithium treatment during pregnancy, serum lithium levels should be closely monitored and measured frequently since renal function changes gradually during pregnancy and suddenly at parturition. Dosage adjustments are required. It is recommended that lithium be discontinued shortly before delivery and reinitiated a few days post-partum.



Neonates may show signs of lithium toxicity necessitating fluid therapy in the neonatal period. Neonates born with low serum lithium concentrations may have a flaccid appearance that returns to normal without any treatment.



Women of child-bearing potential



It is advisable that women treated with lithium should adopt adequate contraceptive methods. In case of a planned pregnancy, it is strongly recommended to discontinue lithium therapy.



Lactation



Since adequate human data on use during lactation, adequate animal reproduction studies are not available and as lithium is secreted in breast milk, bottle-feeding is recommended (see section 4.3 Contra-indications).



4.7 Effects On Ability To Drive And Use Machines



As lithium may cause disturbances of the CNS, patients should be warned of the possible hazards when driving or operating machinery.



4.8 Undesirable Effects



Side effects are usually related to serum lithium concentrations and are less common in patients with plasma lithium concentrations below 1.0 mmol/l.



Initial Therapy: fine tremor of the hands, polyuria and thirst may occur.



Blood and Lymphatic system disorders: leucocytosis.



Immune system disorders: increase in antinuclear antibodies.



Endocrine disorders: disturbances of thyroid function including goitre, hypothyroidism and hyperthyroidism, hyperparathyroidism, parathyroid adenoma.



Metabolism and nutrition disorders: hypercalcaemia, hypermagnesaemia, hyperglycaemia, anorexia, weight gain.



Nervous system disorders: coma, pseudotumor cerebri, syndrome of irreversible lithium effectuated neurotoxicity (SILENT), encephalopathy, stupor, seizures, neuroleptic malignant syndrome, myasthenia gravis, serotonin syndrome, parkinsonism, extrapyramidal symptoms, ataxia, dizziness, memory impairment , mild cognitive impairment may occur during long term use, giddiness, nystagmus, slurred speech, vertigo, hyperactive deep tendon reflexes, dazed feeling, fine hand tremors.



Eye Disorders: scotomata and blurred vision.



Cardiac disorders: cardiac arrest, ventricular fibrillation, ventricular tachycardia, ventricular arrhythmias, Torsade de pointes, QT interval prolongation, cardiomyopathy, arrhythmia, bradycardia, sinus node dysfunction, ECG changes.



Vascular disorders: Peripheral circulatory collapse, hypotension.



Gastrointestinal disorders: gastritis, nausea, diarrhoea, vomiting, dry mouth, excessive salivation. Lithium salts have been implicated in dysgeusia.



Skin and subcutaneous tissue disorders: Allergic rash, exacerbation of psoriasis, acneiform eruptions, alopecia, acne, papular skin disorder, folliculitis, pruritus, rash.



Musculoskeletal and connective tissue disorders: muscle weakness.



Renal and urinary disorders: symptoms of nephrogenic diabetes insipidus, impairment of renal function, permanent changes in the kidney, nephrotic syndrome, histological renal changes with interstitial fibrosis after long term treatment, polyuria, polydipsia



Reproductive system and breast disorders: sexual dysfunction..



General disorders and administration site conditions: sudden unexplained death, oedema, asthenia, lethargy, thirst, fatigue, and malaise can occur due to lithium toxicity.



Some adverse events will be seen when Lithium levels are raised – for symptoms see section 4.9 Overdose.



4.9 Overdose



Lithium carbonate has a narrow therapeutic window. Symptoms of lithium overdose (Lithium intoxication) can therefore occur due to intercurrent illness, iatrogenic causes, and self poisoning.



Any overdose in a patient who has been taking chronic lithium therapy should be regarded as potentially serious. A single acute overdose usually carries low risk and patients tend to show mild symptoms only, irrespective of their serum lithium concentration. However more severe symptoms may occur after a delay if lithium elimination is reduced because of renal impairment, particularly if a slow-release preparation has been taken. The fatal dose, in a single overdose, is probably over 5g.



Special attention must be given to the maintenance of fluid and electrolyte balance, and also adequate renal function. Sodium depleting diuretics should not be used in any circumstances.



If an acute overdose has been taken by a patient on chronic lithium therapy, this can lead to serious toxicity occurring even after a modest overdose as the extravascular tissues are already saturated with lithium.



In patients with a raised lithium concentration, the risk of toxicity is greater in those with the following underlying medical conditions: hypertension; diabetes; congestive heart failure; chronic renal failure; schizophrenia; Addison's disease.



Symptoms



The onset of symptoms may be delayed, with peak effects not occurring for as long as 24 hours, especially in patients who are not receiving chronic lithium therapy or following the use of a sustained release preparation.



Mild: Nausea, diarrhoea, blurred vision, polyuria, light headedness, fine resting tremor, muscular weakness and drowsiness.



Moderate: Increasing confusion, blackouts, fasciculation and increased deep tendon reflexes, myoclonic twitches and jerks, choreoathetoid movements, urinary or faecal incontinence, increasing restlessness followed by stupor. Hypernatraemia.



Severe: Coma, convulsions, cerebellar signs, cardiac dysrhythmias including sino-atrial block, sinus and junctional bradycardia and first degree heart block. Hypotension or rarely hypertension, circulatory collapse and renal failure.



Management



There is no known antidote to lithium poisoning.



Special attention must be given to the maintenance of fluid and electrolyte balance, and also adequate renal function. Sodium-depleting diuretics should not be used in any circumstances.



All patients should be observed for a minimum of 24 hours. ECG should be monitored in symptomatic patients. Steps should be taken to correct hypotension.



Consider gastric lavage for non-sustained-release preparations if more than 4g has been ingested by an adult within one hour or definite ingestion of a significant amount by a child. Slow-release tablets do not disintegrate in the stomach and most are too large to pass up a lavage tube. Gut decontamination is not useful for chronic accumulation. Whole bowel irrigation may be helpful in patients ingesting large quantities of a slow-release preparation.



Note: Activated charcoal does not adsorb lithium.



Haemodialysis is the treatment of choice for severe poisoning and should be considered in all patients with marked neurological features. It is the most efficient method of lowering lithium concentrations rapidly but substantial rebound increases can be expected when dialysis is stopped, and prolonged, or repeated treatments may be required.



It should be considered also in acute, acute on chronic or chronic overdose in patients with severe symptoms regardless of serum lithium concentration; discuss with your local poisons service.



Note: Clinical improvement generally takes longer than reduction of serum lithium concentrations regardless of the method used.



5. Pharmacological Properties



5.1 Pharmacodynamic Properties



The precise mechanism of action of lithium as a mood-stabilising agent remains unknown, although many cellular actions of lithium have been characterised.



5.2 Pharmacokinetic Properties



Lithium is excreted almost exclusively in the urine by the kidneys.



The pharmacokinetics of lithium are extremely well documented. A single oral dose of CAMCOLIT 250 gives a peak plasma level approximately 2-3 hours later, with the level at 24 hours being approximately 40% of peak levels. The half-life of lithium varies considerably between formulations, but generally is considered to be about 12 to 24 hours following a single dose.



Half-lives of up to 36 hours have been reported for elderly patients and 40 to 50 hours for patients with renal impairment. Steady-state concentrations may not, therefore, be attained until 4 to 7 days after starting treatment



5.3 Preclinical Safety Data



In animal studies, lithium has been reported to interfere with fertility, gestation and foetal development.



6. Pharmaceutical Particulars



6.1 List Of Excipients



Maize Starch



Magnesium Stearate



Pregelatinised Maize Starch



Hypromellose



Macrogol 400



6.2 Incompatibilities



Not applicable.



6.3 Shelf Life



The shelf life is 5 years.



6.4 Special Precautions For Storage



Do not store above 25°C. Keep the container tightly closed.



6.5 Nature And Contents Of Container



Polypropylene tablet container, containing 100 or 1000 tablets. Not all pack sizes maybe included.



6.6 Special Precautions For Disposal And Other Handling



No special requirements.



7. Marketing Authorisation Holder



Norgine Limited



Norgine House



Widewater Place



Moorhall Road



Harefield



Uxbridge



Middlesex UB9 6NS



United Kingdom



8. Marketing Authorisation Number(S)



PL 00322/5900R



9. Date Of First Authorisation/Renewal Of The Authorisation



12 June 2002



10. Date Of Revision Of The Text



August 2010




Calamine Lotion BP





1. Name Of The Medicinal Product



Calamine Lotion BP


2. Qualitative And Quantitative Composition









 
 


Calamine BP




15.0% w/v




Zinc Oxide BP




5.0% w/v



3. Pharmaceutical Form



Lotion



4. Clinical Particulars



4.1 Therapeutic Indications



For relief of the symptoms of mild sunburn and other minor skin conditions.



4.2 Posology And Method Of Administration



Topical. Applied directly to the skin.



Recommended dose and dosage schedule



The product is suitable for use by adults, children and the elderly.



Apply gently with a pad of cotton wool to the affected parts as required.



4.3 Contraindications



None known.



4.4 Special Warnings And Precautions For Use



Shake the bottle.



For external use only.



Keep all medicines away from children



4.5 Interaction With Other Medicinal Products And Other Forms Of Interaction



May mask x-ray pictures under certain circumstances.



4.6 Pregnancy And Lactation



No evidence has been found as to the safety of the product when used during pregnancy and lactation. However, the product has been used for many years without any apparent ill effects.



4.7 Effects On Ability To Drive And Use Machines



None known.



4.8 Undesirable Effects



None known



4.9 Overdose



Overdose is considered unlikely with this product. However, if large quantities have been ingested, vomiting, inflammation of mucous membranes of the mouth and stomach, weakness, mental confusion, cold sweats, depression of pulse and leg cramps may occur.



Where phenol has been swallowed it may be necessary to empty the stomach by aspiration and lavage. Castor oil or olive oil may be added to the water to dissolve the phenol and delay absorption: 50ml of oil may be left in the stomach.



The patient should be kept warm, and pulmonary oedema, systemic acidosis, respiratory failure and circulatory failure should be treated symptomatically. Respiration may have to be assisted.



5. Pharmacological Properties



5.1 Pharmacodynamic Properties



Calamine has a mild astringent action of the skin and is used as a dusting powder, cream, lotion or ointment in a variety of skin conditions.



Zinc oxide has a mildly antiseptic action and is a mild astringent, it has soothing and protective properties.



5.2 Pharmacokinetic Properties



No information available.



5.3 Preclinical Safety Data



None.



6. Pharmaceutical Particulars



6.1 List Of Excipients



Bentonite BP, sodium citrate BP, glycerol BP, phenol BP and purified water BP.



6.2 Incompatibilities



None known.



6.3 Shelf Life









 
 


100ml:




36 months unopened




200ml:




36 months unopened



6.4 Special Precautions For Storage



Store below 25°C.



6.5 Nature And Contents Of Container








100ml:




Glass bottle with polypropylene cap or white 28mm cap with tamper evident band and EPE Saranex liner




200ml:




Glass bottle with polypropylene cap or white 28mm cap with tamper evident band and EPE Saranex liner



6.6 Special Precautions For Disposal And Other Handling



None.



7. Marketing Authorisation Holder



L.C.M. Ltd.,



Linthwaite Laboratories,



Huddersfield,



HD7 5QH,



England.



8. Marketing Authorisation Number(S)



PL 12965/0003



9. Date Of First Authorisation/Renewal Of The Authorisation



25/8/1993 / 22/10/1998, 15/12/2000



10. Date Of Revision Of The Text



10/09/2010



11 DOSIMETRY (IF APPLICABLE)


Not Applicable



12 INSTRUCTIONS FOR PREPARATION OF RADIOPHARMACEUTICALS (IF APPLICABLE)


Not Applicable




Catapres Ampoules






Catapres Ampoules



150 micrograms in 1 ml Solution for Injection


(clonidine hydrochloride)




Read all of this leaflet carefully before you start taking this medicine


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

  • If you have any further questions, ask your doctor 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 gets troublesome or serious, or if you notice any side effects not listed in this leaflet, please tell your doctor or
    pharmacist.



In this leaflet:


  • 1. What CATAPRES Ampoules are and what they are used for

  • 2. Before you receive CATAPRES Ampoules

  • 3. How CATAPRES Ampoules will be given

  • 4. Possible side effects

  • 5. How to store CATAPRES Ampoules

  • 6. Further information




What Catapres Ampoules Are And What They Are Used For


The name of your medicine is CATAPRES Ampoules 150 micrograms in 1 ml Solution for Injection (called CATAPRES Ampoules in this leaflet). Your medicine is a solution for injection.


CATAPRES Ampoules contain a medicine called clonidine. This belongs to a group of medicines called antihypertensives.


CATAPRES is used to lower high blood pressure in cases of hypertensive crisis (a rapid rise in blood pressure that needs treating straight away).




Before You Receive Catapres Ampoules



You should not be given CATAPRES Ampoules if:


  • You are pregnant, likely to get pregnant or are breast-feeding

  • You are allergic (hypersensitive) to clonidine or any of the other ingredients of CATAPRES (see section 6: Further information)

  • You have a slow heart rate due to heart problems

  • You are a child

You should not receive this medicine if any of the above apply to you. If you are not sure, talk to your doctor or pharmacist before having CATAPRES Ampoules.




Take special care with CATAPRES Ampoules


Check with your doctor or pharmacist before having CATAPRES if:


  • You have Raynaud’s disease (a problem with circulation to the fingers and toes) or other blood circulation problems, including circulation to the brain

  • You have heart or kidney problems

  • You have or have ever had depression

  • You have constipation

  • You have a nerve disorder that causes your hands and feet to feel different (‘altered sensation’)

If you are not sure if any of the above apply to you, talk to your doctor or pharmacist before receiving CATAPRES Ampoules.


As you may get dry eyes whilst taking this medicine, this may be a problem if you wear contact lenses.




Taking other medicines


Please tell your doctor or pharmacist if you are taking or have recently taken any other medicines. This includes medicines obtained without a prescription and herbal medicines. This is because CATAPRES Ampoules can affect the way some other medicines work. Also some other medicines can affect the way CATAPRES Ampoules works.


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


  • Other medicines that make you drowsy

  • Non-Steroidal Anti-Inflammatory Drugs (NSAIDS) such as ibuprofen

  • Medicines for depression such as imipramine or mirtazapine

  • Medicines for severe mental illness such as schizophrenia. These are also known as ‘antipsychotics’ and include chlorpromazine and haloperidol

Please also tell your doctor or pharmacist if you are taking any of the following medicines for high blood pressure or other heart problems:


  • Beta blockers such as atenolol

  • Water tablets (‘diuretics’) such as frusemide

  • Alpha blockers such as prazosin or doxazosin. These can also be used for prostate problems in men

  • Vasodilators such as diazoxide or sodium nitroprusside

  • Calcium antagonists such as verapamil or diltiazem hydrochloride

  • ACE inhibitors such as captopril or lisinopril

  • Digitalis glycosides such as digoxin

If you are not sure if any of the above apply to you, talk to your doctor or pharmacist before receiving CATAPRES Ampoules.




Tests


If you are having any blood tests, tell the person giving the test that you are taking this medicine. This is because CATAPRES can affect results relating to your liver.




Operations


If you are going to have an operation, you will need to still receive CATAPRES Ampoules.




Having CATAPRES Ampoules with food and drink


You may feel drowsy while receiving CATAPRES Ampoules. Drinking alcohol while receiving CATAPRES Ampoules can make this worse.




Pregnancy and breast-feeding


You should not be given CATAPRES Ampoules if you are pregnant, likely to get pregnant or are breast-feeding.




Driving and using machines


You may feel drowsy while receiving CATAPRES Ampoules, especially if you have been drinking alcohol. If this happens do not drive or use any tools or machines.




Important information about some of the ingredients of CATAPRES Ampoules


CATAPRES Ampoules contain sodium chloride, the sodium content per 1 ml ampoule is less than 1 mmol (23 mg). The total sodium content if you are given 5 ampoules in 24 hours is less than 1 mmol (23 mg). This means that CATAPRES Ampoules are essentially sodium free.





How Catapres Ampoules Will Be Given


CATAPRES Ampoules are usually given by a doctor or nurse. You will normally be given 1 to 2 CATAPRES Ampoules but over 24 hours up to 5 ampoules may be given.


Your doctor will start you on a low dose but may increase the dose if you need more medicine to control your blood pressure.



Receiving the injection


  • CATAPRES Ampoules are slowly injected into a vein over 10-15 minutes

  • CATAPRES Ampoules may be diluted with other solutions if needed

CATAPRES Ampoules are not recommended for children.




If you have more CATAPRES Ampoules than you should


It is unlikely that you will be given too much of this medicine. However, tell the doctor or nurse if you think that you have been given too much.



If you have any further questions on the use of CATAPRES, ask your doctor or pharmacist.




Catapres Ampoules Side Effects


Like all medicines, CATAPRES Ampoules can cause side effects, although not everybody gets them.


The side effects described below have been experienced by people taking CATAPRES. They are listed as either very common, common, uncommon, rare or not known.


Very common (affects more than 1 in 10 people)


  • Dizziness, feeling tired and more relaxed than usual (sedation)

  • Feeling dizzy when you stand up (because your blood pressure has fallen sharply)

  • Dry mouth

Common (affects less than 1 in 10 people, more than 1 in 100 people)


  • Depression, sleeping problems

  • Headache

  • Constipation, feeling sick (nausea), pain below the ear (from the salivary gland), being sick (vomiting)

  • Erectile dysfunction

  • Fatigue

Uncommon (affects less than 1 in 100 people, more than 1 in 1,000 people)


  • Problems with understanding what is happening around you, hallucinations, nightmares

  • Your hands and feet feeling different (‘altered sensation’)

  • Regular unusually slow heart beat

  • Raynaud’s phenomenon (a problem with circulation to the fingers and toes)

  • Itching, rash, urticaria (nettle rash)

  • A feeling of discomfort and fatigue (‘malaise’)

Rare (affects less than 1 in 1,000 people, more than 1 in 10,000 people)


  • Breast growth (‘gynaecomastia’) in men

  • Dry eyes

  • Irregular heartbeat

  • Drying out of the lining of the nose

  • Pseudo-obstruction of the large bowel, which causes colicky pain, vomiting and constipation. Contact your doctor straight away if you have all these side effects.

  • Hair loss

  • Increase in your blood sugar

Not known


  • Confusion, loss of libido

  • Blurred vision

  • Abnormally slow heart beat

Two cases of hepatitis (inflammation of the liver) have also been reported. This might show up in some blood tests. Your body may also hold onto more water than usual (fluid retention).


If any of the side effects gets troublesome or serious, or if you notice any side effects not listed in the leaflet, tell your doctor or pharmacist.




How To Store Catapres Ampoules


Keep out of the reach and sight of children


The ampoules should not be stored above 30°C and should be kept in the outer carton.


CATAPRES Ampoules should not be used after the expiry date which is stated on the ampoule label and carton. The expiry date refers to the last day of that month.


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




Further Information



What CATAPRES Ampoules contain


  • The active substance is clonidine hydrochloride. Each 1 ml ampoule contains 150 micrograms of clonidine hydrochloride

  • The other ingredients in the injection are: sodium chloride, water for injections and hydrochloric acid



What CATAPRES Ampoules looks like and contents of the pack


CATAPRES Ampoules are clear glass ampoules containing a clear, colourless solution.


CATAPRES Ampoules are supplied in cartons of 5 ampoules.




Marketing Authorisation Holder and Manufacturer


The Marketing Authorisations for CATAPRES Ampoules are held by:



Boehringer Ingelheim Limited

Ellesfield Avenue

Bracknell

Berkshire

RG12 8YS

United Kingdom


and the ampoules are manufactured at



Boehringer Ingelheim Spain

TurĂ³ de can Matas

Ctra. De Rubi

San Cugat del Valles

Barcelona

Spain




This leaflet was revised in August 2009.


©Boehringer Ingelheim Limited 2009


20081008


22D030





Creon 25000 Capsules





1. Name Of The Medicinal Product



Creon® 25000 Capsules


2. Qualitative And Quantitative Composition



Each capsule contains pancreatin PhEur 300 mg equivalent to:










Lipase




25,000 PhEur units




Amylase




18,000 PhEur units




Protease




1,000 PhEur units



3. Pharmaceutical Form



Orange/colourless capsules filled with brownish minimicrospheres.



4. Clinical Particulars



4.1 Therapeutic Indications



For the treatment of pancreatic exocrine insufficiency.



4.2 Posology And Method Of Administration



Adults (including the elderly) and children:



Initially one or two capsules with each meal. Dose increases, if required, should be added slowly, with careful monitoring of response and symptomatology.



The capsules can be swallowed whole, or for ease of administration they may be opened and the granules taken with acidic fluid or soft food, but without chewing.



This could be apple sauce or yoghurt or any fruit juice with a pH less than 5.5, e.g. apple, orange or pineapple juice. If the granules are mixed with food, it is important that they are taken immediately, otherwise dissolution of the enteric coating may result. In order to protect the enteric coating, it is important that the granules are not crushed or chewed.



It is important to ensure adequate hydration of patients at all times whilst dosing Creon 25000.



Fibrosing colonopathy has been reported in patients with cystic fibrosis taking in excess of 10,000 units of lipase/kg/day (see section 4.4).



4.3 Contraindications



Hypersensitivity to pancreatin of porcine origin or to any of the excipients.



4.4 Special Warnings And Precautions For Use



Strictures of the ileo-caecum and large bowel (fibrosing colonopathy) have been reported in patients with cystic fibrosis taking high doses of pancreatin preparations. Case control studies did not reveal evidence for an association between Creon and the appearance of fibrosing colonopathy. As a precaution, unusual abdominal symptoms or changes in abdominal symptoms should be medically assessed to exclude the possibility of fibrosing colonopathy, especially if the patient is taking in excess of 10,000 units of lipase/kg/day



4.5 Interaction With Other Medicinal Products And Other Forms Of Interaction



No interaction studies have been performed.



4.6 Pregnancy And Lactation



Pregnancy



For pancreatic enzymes no clinical data on exposed pregnancies are available.



Animal studies show no evidence for any absorption of porcine pancreatic enzymes. Therefore, no reproductive or developmental toxicity is to be expected.



Caution should be exercised when prescribing to pregnant women.



Lactation



No effects on the suckling child are anticipated since animal studies suggest no systemic exposure of the breast-feeding woman to pancreatic enzymes. Pancreatic enzymes can be used during breast-feeding.



If required during pregnancy or lactation Creon should be used in doses sufficient to provide adequate nutritional status.



4.7 Effects On Ability To Drive And Use Machines



Creon has no or negligible influence on the ability to drive or use machines.



4.8 Undesirable Effects



In clinical trials, more than 600 patients with pancreatic exocrine insufficiency, due to cystic fibrosis, chronic pancreatitis, and pancreatic surgery were exposed to Creon. The most commonly reported adverse reactions were gastrointestinal disorders and were primarily mild or moderate in severity.



The following adverse reactions have been observed during placebo-controlled clinical trials with the below indicated frequencies;



Gastrointestinal disorders



Common ( nausea, vomiting, constipation, diarrhoea and abdominal distension.



Gastrointestinal disorders are mainly associated with the underlying disease. Similar or lower incidences compared to placebo were reported for abdominal pain (very common



Skin and subcutaneous tissue disorders



Uncommon ( rash



Pruritus and urticaria have been additionally identified as adverse reactions during post-approval use. Because these reactions were reported spontaneously from a population of uncertain size, it is not possible to reliably estimate their frequency.



Multiple clinical trials were conducted in other patient populations: HIV, acute pancreatitis, diabetes mellitus. No additional adverse drug reactions were identified compared to the above three patient groups.



Paediatric population



No specific adverse reactions were identified in the paediatric population. Frequency, type and severity of adverse reactions were similar in children with cystic fibrosis as compared to adults.



4.9 Overdose



Extremely high doses of pancreatin have been reported to be associated with hyperuricosuria and hyperuricaemia.



Supportive measures including stopping enzyme therapy and ensuring adequate rehydration are recommended.



5. Pharmacological Properties



5.1 Pharmacodynamic Properties



Replacement therapy in pancreatic enzyme deficiency states. The enzymes have hydrolytic activity on fat, carbohydrates and proteins.



5.2 Pharmacokinetic Properties



Pharmacokinetic data are not available as the enzymes act locally in the gastro-intestinal tract. After exerting their action, the enzymes are digested themselves in the intestine.



5.3 Preclinical Safety Data



Not applicable.



6. Pharmaceutical Particulars



6.1 List Of Excipients



Granules:



Macrogol 4000



Hypromellose phthalate



Dimeticone



Cetyl alcohol



Triethyl citrate



Capsules:



Gelatin,



Anhydrous iron (III) oxide, E172



Hydrated iron (III) oxide, E172



Titanium dioxide, E171



Sodium lauryl sulphate



6.2 Incompatibilities



None known.



6.3 Shelf Life



3 years



6.4 Special Precautions For Storage



Store below 30°C.



6.5 Nature And Contents Of Container



HDPE container with tamper-evident PP cap. Each container contains 100 capsules.



6.6 Special Precautions For Disposal And Other Handling



No special instructions.



Administrative Data


7. Marketing Authorisation Holder



Abbott Healthcare Products Limited



Mansbridge Road



West End



Southampton



SO18 3JD



United Kingdom



8. Marketing Authorisation Number(S)



PL 00512/0150



9. Date Of First Authorisation/Renewal Of The Authorisation



01 January 2001



10. Date Of Revision Of The Text



30/06/2011