Wednesday, 28 September 2016

Zicron 40mg Tablets





1. Name Of The Medicinal Product



Gliclazide 40mg Tablets



Zicron 40mg Tablets


2. Qualitative And Quantitative Composition



Gliclazide 40mg



For Excipients, see 6.1



3. Pharmaceutical Form



Tablet



White to off-white, circular, flat, bevelled edged, uncoated tablets with “40” on one side, plain on reverse.



4. Clinical Particulars



4.1 Therapeutic Indications



Non insulin dependant diabetes mellitus.



4.2 Posology And Method Of Administration



For oral administration.



Adults:



The total daily dose may vary from 40 to 320 mg taken orally. The dose should be adjusted according to the individual patient's response, commencing with 40-80 mg daily (1 – 2 tablets) and increasing until adequate control is achieved. A single dose should not exceed 160 mg (4 tablets). When higher doses are required, gliclazide should be taken twice daily and according to the main meals of the day.



In obese patients or those not showing adequate response to gliclazide alone, additional therapy may be required.



Elderly:



Plasma clearance of gliclazide is not altered in the elderly and steady state plasma levels can therefore be expected to be similar to those in adults under 65 years. Clinical experience in the elderly to date shows that gliclazide is effective and well tolerated. Care should be exercised, however, when prescribing sulphonylureas in the elderly due to a possible age-related increased risk of hypoglycaemia.



Children:



Gliclazide as with other sulphonylureas, is not indicated for the treatment of juvenile onset diabetes mellitus.



4.3 Contraindications



Gliclazide should not be used in:



- Juvenile onset diabetes.



- Diabetes complicated by ketosis and acidosis.



- Pregnancy.



- Diabetes undergoing surgery, after severe trauma or during infections.



- Patients known to have hypersensitivity to other sulphonylureas and related drugs or any of the other tablet ingredients.



- Diabetic pre-coma and coma.



- Severe renal or hepatic insufficiency.



4.4 Special Warnings And Precautions For Use



- Hypoglycaemia: all sulphonylurea drugs are capable of producing moderate or severe hypoglycaemia, particularly in the following conditions:



- in patients controlled by diet alone,



- in cases of accidental overdose,



- When calorie or glucose intake is deficient,



- in patients with hepatic and/or renal impairment; however, in long-term clinical trials, patients with renal insufficiency have been treated satisfactorily, using gliclazide at reduced doses.



In order to reduce the risk of hypoglycaemia it is therefore recommended:



- to initiate treatment for non-insulin dependant diabetes by diet alone, if this is possible,



- to take into account the age of the patient: blood sugar levels not strictly controlled by diet alone might be acceptable in the elderly,



- to adjust the dose of gliclazide according to the blood glucose response and to the 24 hour urinary glucose during the first days of treatment.



Dosage adjustments may be necessary:



- on the occurrence of mild symptoms of hypoglycaemia (sweating, pallor, hunger pangs, tachycardia, sensation of malaise). Such findings should be treated with oral glucose and adjustments made in drug dosage and/or meal patterns,



- on the occurrence of severe hypoglycaemic reactions (coma or neurological impairment, see overdose),



- loss of control of blood glucose (hyperglycaemia). When a patient stabilised on any diabetic regimen is exposed to stress such as fever, trauma, infection or surgery, a loss of control may occur. At such times, it may be necessary to increase progressively the dosage of gliclazide and it this is insufficient, to discontinue the treatment with gliclazide and to administer insulin. As with other sulphonylureas, hypoglycaemia will occur if the patient's dietary intake is reduced or of they are receiving a larger dose of gliclazide than required.



- Care should be exercised in patients with hepatic and/or renal impairment and a small starting dose should be used with careful patient monitoring.



4.5 Interaction With Other Medicinal Products And Other Forms Of Interaction



Care should be taken when giving gliclazide with drugs which are known to alter the diabetic state or potentiate the drug's action.



The hypoglycaemic effect of gliclazide may be potentiated by phenylbutazone, salicylates, sulphonamides, coumarin derivatives, MAOIs, beta adrenergic blocking agents, tetracycline compounds, chloramphenicol, clofibrate, disopyramide, miconazole (oral forms) and cimetidine.



It may be diminished by corticosteroids, oral contraceptives, thiazide diuretics, Phenothiazine derivatives, thyroid hormones and abuse of laxatives.



4.6 Pregnancy And Lactation



Pregnancy:



Gliclazide is contraindicated during pregnancy (see section 4.3 contra-indications).



Lactation:



It has not been established whether gliclazide is transferred to human milk. However, other sulphonylureas have been found in milk and there is no evidence to suggest that gliclazide differs from the group in this respect. Gliclazide should, therefore, not be taken while the mother is breast-feeding.



4.7 Effects On Ability To Drive And Use Machines



Patients should be informed that their concentration may be affected if their diabetes is not satisfactorily controlled, especially at the beginning of treatment (see special warnings and precautions).



4.8 Undesirable Effects



- Hypoglycaemia (see special warnings and precautions).



- Abnormalities of hepatic function are not uncommon during gliclazide therapy. There are rare reports of hepatic failure, hepatitis and jaundice following treatment with gliclazide.



- Mild gastro-intestinal disturbances including nausea, dyspepsia, diarrhoea, constipation have been reported but this type of adverse reaction can be avoided if gliclazide is taken during a meal.



- Skin reactions including rash, pruritus, Erythema, bullous eruption; blood dyscrasia including anaemia, leukopenia, thrombocytopenia and granulocytopenia have been observed during treatment with gliclazide but are not known to be directly attributable to the drug.



4.9 Overdose



The symptoms to be expected of overdose would be hypoglycaemia. The treatment is gastric lavage and correction of the hypoglycaemia by appropriate means with continual monitoring of the patient's blood sugar until the effect of the drug has ceased.



5. Pharmacological Properties



5.1 Pharmacodynamic Properties



A10B B09 Oral Blood Glucose Lowering Drugs



Gliclazide is a hypoglycaemic sulphonylurea differing from other related compounds by the addition of an azabicyclo-octane ring.



In man, apart from having similar hypoglycaemic effect to the other sulphonylureas, gliclazide has been shown to reduce platelet adhesiveness and aggregation and increase fibrinolytic activity. These factors are thought to be implicated in the pathogenesis of long-term complications of diabetes mellitus.



Gliclazide primarily enhances the first phase of insulin secretion, but also to a lesser degree its second phase. Both phases are diminished in non-insulin dependant diabetes mellitus.



5.2 Pharmacokinetic Properties



The drug is well absorbed and its half-life in man is approximately 10-12 hours. Gliclazide is metabolised in the liver; less than 5% of the dose is excreted unchanged in the urine.



5.3 Preclinical Safety Data



No data of relevance which is additional to that already included in other sections of the SPC.



6. Pharmaceutical Particulars



6.1 List Of Excipients



Lactose monohydrate



Microcrystalline cellulose



Magnesium stearate



Purified talc



Croscarmellose sodium



Povidone



6.2 Incompatibilities



Not applicable



6.3 Shelf Life



2 years



6.4 Special Precautions For Storage







Blisters:
Do not store above 25ºC. Store in the original package.

Tablet containers:
Do not store above 25ºC. Keep the container tightly closed.


6.5 Nature And Contents Of Container



Al/PVC/PVDC blister, pack sizes of 20, 28, 56, 60, 84, 100 tablets.



HDPE tablet containers, pack sizes of 100, 250, 500 or 1000 tablets.



Not all pack sizes may be marketed.



6.6 Special Precautions For Disposal And Other Handling



No special requirements.



7. Marketing Authorisation Holder



Bristol Laboratories Limited



Unit 3, Canalside



Northbridge Road



Berkhamsted



Hertfordshire



HP4 1EG



8. Marketing Authorisation Number(S)



PL 17907/0067



9. Date Of First Authorisation/Renewal Of The Authorisation



12/06/2007



10. Date Of Revision Of The Text



July 2008




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Tuesday, 27 September 2016

Mezzopram 20 mg Dispersible Gastro-resistant Tablets





1. Name Of The Medicinal Product



Mezzopram 20 mg Dispersible Gastro-resistant Tablets


2. Qualitative And Quantitative Composition



Each gastro-resistant tablet contains 20 mg omeprazole (as omeprazole magnesium).



Excipients: glucose, sucrose



For a full list of excipients, see section 6.1.



3. Pharmaceutical Form



Gastro-resistant tablet



Pink, oval film-coated tablet with a breaking notch on both sides. The tablet can be divided into equal halves.



4. Clinical Particulars



4.1 Therapeutic Indications



Mezzopram Dispersible gastro-resistant tablets are indicated for:



Adults



• Treatment of duodenal ulcers



• Prevention of relapse of duodenal ulcers



• Treatment of gastric ulcers



• Prevention of relapse of gastric ulcers



• In combination with appropriate antibiotics, Helicobacter pylori (H. pylori) eradication in peptic ulcer disease



• Treatment of NSAID-associated gastric and duodenal ulcers



• Prevention of NSAID-associated gastric and duodenal ulcers in patients at risk



• Treatment of reflux oesophagitis



• Long-term management of patients with healed reflux oesophagitis



• Treatment of symptomatic gastro-oesophageal reflux disease



• Treatment of Zollinger-Ellison syndrome



Paediatric use



Children over 1 year of age and



• Treatment of reflux oesophagitis



• Symptomatic treatment of heartburn and acid regurgitation in gastro-oesophageal reflux disease



Children and adolescents over 4 years of age



• In combination with antibiotics in treatment of duodenal ulcer caused by H. pylori



4.2 Posology And Method Of Administration



Posology in adults



Treatment of duodenal ulcers



The recommended dose in patients with an active duodenal ulcer is Mezzopram 20 mg once daily. In most patients healing occurs within two weeks. For those patients who may not be fully healed after the initial course, healing usually occurs during a further two weeks treatment period. In patients with poorly responsive duodenal ulcer Mezzopram 40 mg once daily is recommended and healing is usually achieved within four weeks.



Prevention of relapse of duodenal ulcers



For the prevention of relapse of duodenal ulcer in H. pylori negative patients or when H. pylori eradication is not possible the recommended dose is Mezzopram 20 mg once daily. In some patients a daily dose of 10 mg may be sufficient. In case of therapy failure, the dose can be increased to 40 mg.



Treatment of gastric ulcers



The recommended dose is Mezzopram 20 mg once daily. In most patients healing occurs within four weeks. For those patients who may not be fully healed after the initial course, healing usually occurs during a further four weeks treatment period. In patients with poorly responsive gastric ulcer Mezzopram 40 mg once daily is recommended and healing is usually achieved within eight weeks.



Prevention of relapse of gastric ulcers



For the prevention of relapse in patients with poorly responsive gastric ulcer the recommended dose is Mezzopram 20 mg once daily. If needed the dose can be increased to Mezzopram 40 mg once daily.



H. pylori eradication in peptic ulcer disease



For the eradication of H. pylori the selection of antibiotics should consider the individual patient's drug tolerance, and should be undertaken in accordance with national, regional and local resistance patterns and treatment guidelines.



• Mezzopram 20 mg + clarithromycin 500 mg + amoxicillin 1,000 mg, each twice daily for one week, or



• Mezzopram 20 mg + clarithromycin 250 mg (alternatively 500 mg) + metronidazole 400 mg (or 500 mg or tinidazole 500 mg), each twice daily for one week, or



• Mezzopram 40 mg once daily with amoxicillin 500 mg and metronidazole 400 mg (or 500 mg or tinidazole 500 mg), both three times a day for one week.



In each regimen, if the patient is still H. pylori positive, therapy may be repeated.



Treatment of NSAID-associated gastric and duodenal ulcers



For the treatment of NSAID-associated gastric and duodenal ulcers, the recommended dose is Mezzopram 20 mg once daily. In most patients healing occurs within four weeks. For those patients who may not be fully healed after the initial course, healing usually occurs during a further four weeks treatment period.



Prevention of NSAID-associated gastric and duodenal ulcers in patients at risk



For the prevention of NSAID associated gastric ulcers or duodenal ulcers in patients at risk (age> 60, previous history of gastric and duodenal ulcers, previous history of upper GI bleeding) the recommended dose is Mezzopram 20 mg once daily.



Treatment of reflux oesophagitis



The recommended dose is Mezzopram 20 mg once daily. In most patients healing occurs within four weeks. For those patients who may not be fully healed after the initial course, healing usually occurs during a further four weeks treatment period.



In patients with severe oesophagitis Mezzopram 40 mg once daily is recommended and healing is usually achieved within eight weeks.



Long-term management of patients with healed reflux oesophagitis



For the long-term management of patients with healed reflux oesophagitis the recommended dose is Mezzopram 10 mg once daily. If needed, the dose can be increased to Mezzopram 20-40 mg once daily.



Treatment of symptomatic gastro-esophageal reflux disease



The recommended dose is Mezzopram 20 mg daily. Patients may respond adequately to 10 mg daily, and therefore individual dose adjustment should be considered.



If symptom control has not been achieved after 4 weeks treatment with Mezzopram 20 mg daily, further investigation is recommended.



Treatment of Zollinger-Ellison syndrome



In patients with Zollinger-Ellison syndrome the dose should be individually adjusted and treatment continued as long as clinically indicated. The recommended initial dose is Mezzopram 60 mg daily. All patients with severe disease and inadequate response to other therapies have been effectively controlled and more than 90% of the patients maintained on doses of Mezzopram 20–120 mg daily. When dose exceed Mezzopram 80 mg daily, the dose should be divided and given twice daily.



Posology in children



Children over 1 year of age and



Treatment of reflux oesophagitis



Symptomatic treatment of heartburn and acid regurgitation in gastro-esophageal reflux disease



The posology recommendations are as follows:













Age


Weight


Posology





10-20 kg


10 mg once daily. The dose can be increased to 20 mg once daily if needed





> 20 kg


20 mg once daily. The dose can be increased to 40 mg once daily if needed


Reflux oesophagitis: The treatment time is 4–8 weeks.



Symptomatic treatment of heartburn and acid regurgitation in gastro-esophageal reflux disease: The treatment time is 2–4 weeks. If symptom control has not been achieved after 2–4 weeks the patient should be investigated further.



Children and adolescents over 4 years of age



Treatment of duodenal ulcer caused by H. pylori



When selecting appropriate combination therapy, consideration should be given to official national, regional and local guidance regarding bacterial resistance, duration of treatment (most commonly 7 days but sometimes up to 14 days), and appropriate use of antibacterial agents.



The treatment should be supervised by a specialist.



The posology recommendations are as follows:












Weight


Posology


15-30 kg


Combination with two antibiotics: Mezzopram 10 mg, amoxicillin 25 mg/kg body weight and clarithromycin 7.5 mg/kg body weight are all administrated together two times daily for one week


31-40 kg


Combination with two antibiotics: Mezzopram 20 mg, amoxicillin 750 mg and clarithromycin 7.5 mg/kg body weight are all administrated two times daily for one week


> 40 kg


Combination with two antibiotics: Mezzopram 20 mg, amoxicillin 1 g and clarithromycin 500 mg are all administrated two times daily for one week.


Special populations



Impaired renal function



Dose adjustment is not needed in patients with impaired renal function (see section 5.2).



Impaired hepatic function



In patients with impaired hepatic function a daily dose of 10–20 mg may be sufficient (see section 5.2).



Elderly (> 65 years old)



Dose adjustment is not needed in the elderly (see section 5.2).



Method of administration



It is recommended to take Mezzopram tablets in the morning, swallowed whole with half a glass of water. The tablets must not be chewed or crushed.



For patients with swallowing difficulties and for children who can drink or swallow semi-solid food



Patients can break the tablet and disperse it in a spoonful of non-carbonated water and if so wished, mix with some fruit juices or applesauce. Patients should be advised that the dispersion should be taken immediately (or within 15 minutes)and always be stirred just before drinking and rinsed down with half a glass of water. DO NOT USE milk or carbonated water. The enteric-coated pellets must not be chewed.



4.3 Contraindications



Hypersensitivity to omeprazole, substituted benzimidazoles or to any of the excipients.



Omeprazole like other proton pump inhibitors must not be used concomitantly with nelfinavir (see section 4.5).



4.4 Special Warnings And Precautions For Use



In the presence of any alarm symptom (e.g. significant unintentional weight loss, recurrent vomiting, dysphagia, haematemesis or melena) and when gastric ulcer is suspected or present, malignancy should be excluded, as treatment may alleviate symptoms and delay diagnosis.



Co-administration of atazanavir with proton pump inhibitors is not recommended (see section 4.5). If the combination of atazanavir with a proton pump inhibitor is judged unavoidable, close clinical monitoring (e.g virus load) is recommended in combination with an increase in the dose of atazanavir to 400 mg with 100 mg of ritonavir; omeprazole 20 mg should not be exceeded.



Omeprazole, as all acid-blocking medicines, may reduce the absorption of vitamin B12 (cyanocobalamin) due to hypo- or achlorhydria. This should be considered in patients with reduced body stores or risk factors for reduced vitamin B12 absorption on long-term therapy.



Omeprazole is a CYP2C19 inhibitor. When starting or ending treatment with omeprazole, the potential for interactions with drugs metabolised through CYP2C19 should be considered. An interaction is observed between clopidogrel and omeprazole (see section 4.5). The clinical relevance of this interaction is uncertain. As a precaution, concomitant use of omeprazole and clopidogrel should be discouraged.



Some children with chronic illnesses may require long-term treatment although it is not recommended.



Treatment with proton pump inhibitors may lead to slightly increased risk of gastrointestinal infections such as Salmonella and Campylobacter (see section 5.1).



As in all long-term treatments, especially when exceeding a treatment period of 1 year, patients should be kept under regular surveillance.



Mezzopram Dispersible gastro-resistant tablets contain sucrose and glucose. Patients with rare fructose intolerance, glucose-galactose malabsorption or sucrase-isomaltase insufficiency should not take this medicine.



4.5 Interaction With Other Medicinal Products And Other Forms Of Interaction



Effects of omeprazole on the pharmacokinetics of other active substances



Active substances with pH dependent absorption



The decreased intragastric acidity during treatment with omeprazole might increase or decrease the absorption of active substances with a gastric pH dependent absorption.



Nelfinavir, atazanavir



The plasma levels of nelfinavir and atazanavir are decreased in case of co-administration with omeprazole.



Concomitant administration of omeprazole with nelfinavir is contraindicated (see section 4.3). Co-administration of omeprazole (40 mg once daily) reduced mean nelfinavir exposure by ca. 40% and the mean exposure of the pharmacologically active metabolite M8 was reduced by ca. 75-90%. The interaction may also involve CYP2C19 inhibition.



Concomitant administration of omeprazole with atazanavir is not recommended (see section 4.4). Concomitant administration of omeprazole (40 mg once daily) and atazanavir 300 mg/ritonavir 100 mg to healthy volunteers resulted in a 75% decrease of the atazanavir exposure. Increasing the atazanavir dose to 400 mg did not compensate for the impact of omeprazole on atazanavir exposure. The co-administration of omeprazole (20 mg once daily) with atazanavir 400 mg/ritonavir 100 mg to healthy volunteers resulted in a decrease of approximately 30% in the atazanavir exposure as compared to atazanavir 300 mg/ritonavir 100 mg once daily.



Digoxin



Concomitant treatment with omeprazole (20 mg daily) and digoxin in healthy subjects increased the bioavailability of digoxin by 10%. Digoxin toxicity has been rarely reported. However caution should be exercised when omeprazole is given at high doses in elderly patients. Therapeutic drug monitoring of digoxin should be then be reinforced.



Clopidogrel



In a crossover clinical study, clopidogrel (300 mg loading dose followed by 75 mg/day) alone and with omeprazole (80 mg at the same time as clopidogrel) were administered for 5 days. The exposure to the active metabolite of clopidogrel was decreased by 46% (Day 1) and 42% (Day 5) when clopidogrel and omeprazole were administered together. Mean inhibition of platelet aggregation (IPA) was diminished by 47% (24 hours) and 30% (Day 5) when clopidogrel and omeprazole were administered together. In another study it was shown that administering clopidogrel and omeprazole at different times did not prevent their interaction that is likely to be driven by the inhibitory effect of omeprazole on CYP2C19. Inconsistent data on the clinical implications of this PK/PD interaction in terms of major cardiovascular events have been reported from observational and clinical studies.



Other active substances



The absorption of posaconazole, erlotinib, ketoconazol and itraconazol is significantly reduced and thus clinical efficacy may be impaired. For posaconazol and erlotinib concomitant use should be avoided.



Active substances metabolised by CYP2C19



Omeprazole is a moderate inhibitor of CYP2C19, the major omeprazole metabolising enzyme. Thus, the metabolism of concomitant active substances also metabolised by CYP2C19, may be decreased and the systemic exposure to these substances increased. Examples of such drugs are R-warfarin and other vitamin K antagonists, cilostazol, diazepam and phenytoin.



Cilostazol



Omeprazole, given in doses of 40 mg to healthy subjects in a cross-over study, increased Cmax and AUC for cilostazol by 18% and 26% respectively, and one of its active metabolites by 29% and 69% respectively.



Phenytoin



Monitoring phenytoin plasma concentration is recommended during the first two weeks after initiating omeprazole treatment and, if a phenytoin dose adjustment is made, monitoring and a further dose adjustment should occur upon ending omeprazole treatment.



Unknown mechanism



Saquinavir



Concomitant administration of omeprazole with saquinavir/ritonavir resulted in increased plasma levels up to approximately 70% for saquinavir associated with good tolerability in HIV-infected patients.



Tacrolimus



Concomitant administration of omeprazole has been reported to increase the serum levels of tacrolimus. A reinforced monitoring of tacrolimus concentrations as well as renal function (creatinine clearance) should be performed, and dosage of tacrolimus adjusted if needed.



Effects of other active substances on the pharmacokinetics of omeprazole



Inhibitors of CYP2C19 and/or CYP3A4



Since omeprazole is metabolised by CYP2C19 and CYP3A4, active substances known to inhibit CYP2C19 or CYP3A4 (such as clarithromycin and voriconazole) may lead to increased omeprazole serum levels by decreasing omeprazole's rate of metabolism. Concomitant voriconazole treatment resulted in more than doubling of the omeprazole exposure. As high doses of omeprazole have been well-tolerated adjustment of the omeprazole dose is not generally required. However, dose adjustment should be considered in patients with severe hepatic impairment and if long-term treatment is indicated.



Inducers of CYP2C19 and/or CYP3A4



Active substances known to induce CYP2C19 or CYP3A4 or both (such as rifampicin and St John's wort) may lead to decreased omeprazole serum levels by increasing omeprazole's rate of metabolism.



4.6 Pregnancy And Lactation



Results from three prospective epidemiological studies (more than 1000 exposed outcomes) indicate no adverse effects of omeprazole on pregnancy or on the health of the foetus/newborn child. Omeprazole can be used during pregnancy.



Omeprazole is excreted in breast milk but is not likely to influence the child when therapeutic doses are used.



4.7 Effects On Ability To Drive And Use Machines



Mezzopram is not likely to affect the ability to drive or use machines. Adverse drug reactions such as dizziness and visual disturbances may occur (see section 4.8). If affected, patients should not drive or operate machinery.



4.8 Undesirable Effects



The most common side effects (1-10% of patients) are headache, abdominal pain, constipation, diarrhoea, flatulence and nausea/vomiting.



The following adverse drug reactions have been identified or suspected in the clinical trials programme for omeprazole and post-marketing. None was found to be dose-related. Adverse reactions listed below are classified according to frequency and System Organ Class (SOC). Frequency categories are defined according to the following convention: Very common (




























































































SOC/frequency


Adverse reaction


Blood and lymphatic system disorders


  


Rare:


Leukopenia, thrombocytopenia


Very rare:


Agranulocytosis, pancytopenia


Immune system disorders


  


Rare:


Hypersensitivity reactions e.g. fever, angioedema and anaphylactic reaction/shock


Metabolism and nutrition disorders


  


Rare:


Hyponatraemia


Very rare:


Hypomagnesaemia


Psychiatric disorders


  


Uncommon:


Insomnia


Rare:


Agitation, confusion, depression


Very rare:


Aggression, hallucinations


Nervous system disorders


  


Common:


Headache


Uncommon:


Dizziness, paraesthesia, somnolence


Rare:


Taste disturbance


Eye disorders


  


Rare:


Blurred vision


Ear and labyrinth disorders


  


Uncommon:


Vertigo


Respiratory, thoracic and mediastinal disorders


  


Rare:


Bronchospasm


Gastrointestinal disorders


  


Common:


Abdominal pain, constipation, diarrhoea, flatulence, nausea/vomiting


Rare:


Dry mouth, stomatitis, gastrointestinal candidiasis


Hepatobiliary disorders


  


Uncommon:


Increased liver enzymes


Rare:


Hepatitis with or without jaundice


Very rare:


Hepatic failure, encephalopathy in patients with pre-existing liver disease


Skin and subcutaneous tissue disorders


  


Uncommon:


Dermatitis, pruritus, rash, urticaria


Rare:


Alopecia, photosensitivity


Very rare:


Erythema multiforme, Stevens-Johnson syndrome, toxic epidermal necrolysis (TEN)


Musculoskeletal and connective tissue disorders


  


Rare:


Arthralgia, myalgia


Very rare:


Muscular weakness


Renal and urinary disorders


  


Rare:


Interstitial nephritis


Reproductive system and breast disorders


  


Very rare:


Gynaecomastia


General disorders and administration site conditions


  


Uncommon:


Malaise, peripheral oedema


Rare:


Increased sweating


Paediatric population



The safety of omeprazole has been assessed in a total of 310 children aged 0 to 16 years with acid-related disease. There are limited long term safety data from 46 children who received maintenance therapy of omeprazole during a clinical study for severe erosive oesophagitis for up to 749 days. The adverse event profile was generally the same as for adults in short- as well as in long-term treatment. There are no long term data regarding the effects of omeprazole treatment on puberty and growth.



4.9 Overdose



There is limited information available on the effects of overdoses of omeprazole in humans. In the literature, doses of up to 560 mg have been described, and occasional reports have been received when single oral doses have reached up to 2,400 mg omeprazole (120 times the usual recommended clinical dose). Nausea, vomiting, dizziness, abdominal pain, diarrhoea and headache have been reported. Also apathy, depression and confusion have been described in single cases.



The symptoms described in connection to omeprazole overdose have been transient, and no serious outcome has been reported. The rate of elimination was unchanged (first order kinetics) with increased doses. Treatment, if needed, is symptomatic.



5. Pharmacological Properties



5.1 Pharmacodynamic Properties



Pharmacotherapeutic group: Proton pump inhibitors, ATC code: A02BC01



Mechanism of action



Omeprazole, a racemic mixture of two enantiomers reduces gastric acid secretion through a highly targeted mechanism of action. It is a specific inhibitor of the acid pump in the parietal cell. It is rapidly acting and provides control through reversible inhibition of gastric acid secretion with once daily dosing.



Omeprazole is a weak base and is concentrated and converted to the active form in the highly acidic environment of the intracellular canaliculi within the parietal cell, where it inhibits the enzyme H+ K+-ATPase - the acid pump. This effect on the final step of the gastric acid formation process is dose-dependent and provides for highly effective inhibition of both basal acid secretion and stimulated acid secretion, irrespective of stimulus.



Pharmacodynamic effects



All pharmacodynamic effects observed can be explained by the effect of omeprazole on acid secretion.



Effect on gastric acid secretion



Oral dosing with omeprazole once daily provides for rapid and effective inhibition of daytime and night-time gastric acid secretion with maximum effect being achieved within 4 days of treatment. With omeprazole 20 mg, a mean decrease of at least 80% in 24-hour intragastric acidity is then maintained in duodenal ulcer patients, with the mean decrease in peak acid output after pentagastrin stimulation being about 70% 24 hours after dosing.



Oral dosing with omeprazole 20 mg maintains an intragastric pH of



As a consequence of reduced acid secretion and intragastric acidity, omeprazole dose-dependently reduces/normalizes acid exposure of the esophagus in patients with gastro-esophageal reflux disease.



The inhibition of acid secretion is related to the area under the plasma concentration-time curve (AUC) of omeprazole and not to the actual plasma concentration at a given time.



No tachyphylaxis has been observed during treatment with omeprazole.



Effect on H. pylori



H. pylori is associated with peptic ulcer disease, including duodenal and gastric ulcer disease. H. pylori is a major factor in the development of gastritis. H. pylori together with gastric acid are major factors in the development of peptic ulcer disease. H. pylori is a major factor in the development of atrophic gastritis which is associated with an increased risk of developing gastric cancer.



Eradication of H. pylori with omeprazole and antimicrobials is associated with high rates of healing and long-term remission of peptic ulcers



Dual therapies have been tested and found to be less effective than triple therapies. They could, however, be considered in cases where known hypersensitivity precludes use of any triple combination.



Other effects related to acid inhibition



During long-term treatment gastric glandular cysts have been reported in a somewhat increased frequency. These changes are a physiological consequence of pronounced inhibition of acid secretion, are benign and appear to be reversible.



Decreased gastric acidity due to any means including proton pump inhibitors, increases gastric counts of bacteria normally present in the gastrointestinal tract. Treatment with acid-reducing drugs may lead to slightly increased risk of gastrointestinal infections such as Salmonella and Campylobacter.



Paediatric use



In a non-controlled study in children (1 to 16 years of age) with severe reflux oesophagitis, omeprazole at doses of 0.7 to 1.4 mg/kg improved oesophagitis level in 90% of the cases and significantly reduced reflux symptoms. In a single-blind study, children aged 0–24 months with clinically diagnosed gastro-esophageal reflux disease were treated with 0.5, 1.0 or 1.5 mg omeprazole/kg. The frequency of vomiting/regurgitation episodes decreased by 50% after 8 weeks of treatment irrespective of the dose.



Eradication of H. pylori in children



A randomised, double blind clinical study (Héliot study) concluded that omeprazole, in combination with two antibiotics (amoxicillin and clarithromycin), was safe and effective in the treatment of H. pylori infection in children age 4 years old and above with gastritis: H. pylori eradication rate: 74.2% (23/31 patients) with omeprazole + amoxicillin + clarithromycin versus 9.4% (3/32 patients) with amoxicillin + clarithromycin. However, there was no evidence of any clinical benefit with respect to dyspeptic symptoms. This study does not support any information for children aged less than 4 years.



5.2 Pharmacokinetic Properties



Absorption



Omeprazole and omeprazole magnesium are acid labile and are therefore administered orally as enteric-coated granules in capsules or tablets. Absorption of omeprazole is rapid, with peak plasma levels occurring approximately 1-2 hours after dose. Absorption of omeprazole takes place in the small intestine and is usually completed within 3-6 hours. Concomitant intake of food has no influence on the bioavailability. The systemic availability (bioavailability) from a single oral dose of omeprazole is approximately 40%. After repeated once-daily administration, the bioavailability increases to about 60%.



Distribution



The apparent volume of distribution in healthy subjects is approximately 0.3 l/kg body weight. Omeprazole is 97% plasma protein bound.



Metabolism



Omeprazole is completely metabolised by the cytochrome P450 system (CYP). The major part of its metabolism is dependent on the polymorphically expressed CYP2C19, responsible for the formation of hydroxyomeprazole, the major metabolite in plasma. The remaining part is dependent on another specific isoform, CYP3A4, responsible for the formation of omeprazole sulphone. As a consequence of high affinity of omeprazole to CYP2C19, there is a potential for competitive inhibition and metabolic drug-drug interactions with other substrates for CYP2C19. However, due to low affinity to CYP3A4, omeprazole has no potential to inhibit the metabolism of other CYP3A4 substrates. In addition, omeprazole lacks an inhibitory effect on the main CYP enzymes.



Approximately 3% of the Caucasian population and 15-20% of Asian populations lack a functional CYP2C19 enzyme and are called poor metabolisers. In such individuals the metabolism of omeprazole is probably mainly catalysed by CYP3A4. After repeated once-daily administration of 20 mg omeprazole, the mean AUC was 5 to 10 times higher in poor metabolisers than in subjects having a functional CYP2C19 enzyme (extensive metabolisers). Mean peak plasma concentrations were also higher, by 3 to 5 times. These findings have no implications for the posology of omeprazole.



Excretion



The plasma elimination half-life of omeprazole is usually shorter than one hour both after single and repeated oral once-daily dosing. Omeprazole is completely eliminated from plasma between doses with no tendency for accumulation during once-daily administration. Almost 80% of an oral dose of omeprazole is excreted as metabolites in the urine, the remainder in the faeces, primarily originating from bile secretion.



The AUC of omeprazole increases with repeated administration. This increase is dose-dependent and results in a non-linear dose-AUC relationship after repeated administration. This time- and dose-dependency is due to a decrease of first pass metabolism and systemic clearance probably caused by an inhibition of the CYP2C19 enzyme by omeprazole and/or its metabolites (e.g. the sulphone).



No metabolite has been found to have any effect on gastric acid secretion.



Special populations



Impaired hepatic function



The metabolism of omeprazole in patients with liver dysfunction is impaired, resulting in an increased AUC. Omeprazole has not shown any tendency to accumulate with once-daily dosing.



Impaired renal function



The pharmacokinetics of omeprazole, including systemic bioavailability and elimination rate, are unchanged in patients with reduced renal function.



Elderly



The metabolism rate of omeprazole is somewhat reduced in elderly subjects (75-79 years of age).



Paediatric patients



During treatment with the recommended doses to children from the age of 1 year, similar plasma concentrations were obtained as compared to adults. In children younger than 6 months, clearance of omeprazole is low due to low capacity to metabolise omeprazole.



5.3 Preclinical Safety Data



Gastric ECL-cell hyperplasia and carcinoids, have been observed in life-long studies in rats treated with omeprazole. These changes are the result of sustained hypergastrinaemia secondary to acid inhibition. Similar findings have been made after treatment with H2-receptor antagonists, proton pump inhibitors and after partial fundectomy. Thus, these changes are not from a direct effect of any individual active substance.



6. Pharmaceutical Particulars



6.1 List Of Excipients



Tablet core



Sucrose



Maize starch



Glucose



Copovidone



Povidone



Talc



Titanium dioxide (E 171)



Methacrylic acid-ethyl acrylate copolymer (1:1)



Glycerol monostearate



Propylene glycol



Stearic acid



Polysorbate 80



Simeticone



Cellulose, microcrystalline



Macrogol 6000



Crospovidone



Silica colloidal anhydrous



Magnesium stearate



Tablet coating



Hypromellose



Macrogol 6000



Titanium dioxide (E 171)



Talc



Iron oxide, red (E 172)



6.2 Incompatibilities



Not applicable.



6.3 Shelf Life



HDPE containers:



18 months



shelf life after first opening: 6 months



Do not store above 25 °C after first opening of the container. Keep the container tightly closed, in order to protect from moisture.



Aluminium/aluminium blister:



18 months



Aclar/aluminium blister:



1 year



6.4 Special Precautions For Storage



HDPE containers:



This medicinal product does not require any special storage conditions.



For storage conditions of the medicinal product after first opening of the HDPE container, see section 6.3.



Aluminium/aluminium blister:



This medicinal product does not require any special storage conditions.



Aclar/aluminium blister:



Do not store above 30 °C.



6.5 Nature And Contents Of Container



HDPE container with a polypropylene screw-cap with 7, 14, 15, 28, 30, 56, 98, 100 gastro-resistant tablets



Aluminium/aluminium blister with 5, 7, 10, 14, 15, 20, 28, 30, 49, 50, 56, 60, 90, 98, 100 gastro-resistant tablets.



Aclar/aluminium blister with 5, 7, 10, 14, 15, 20, 28, 30, 49, 50, 56, 60, 90, 98, 100 gastro-resistant tablets.



Not all pack sizes may be marketed.



6.6 Special Precautions For Disposal And Other Handling



No special requirements.



7. Marketing Authorisation Holder



Sandoz Limited



Frimley Business Park,



Frimley,



Camberley,



Surrey,



GU16 7SR.



United Kingdom



8. Marketing Authorisation Number(S)



PL 04416/1078



9. Date Of First Authorisation/Renewal Of The Authorisation



05/07/2010



10. Date Of Revision Of The Text



26/04/2011




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Emthex




Emthex may be available in the countries listed below.


Ingredient matches for Emthex



Methotrexate

Methotrexate is reported as an ingredient of Emthex in the following countries:


  • Myanmar

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Mogadon 5 mg Tablets






Mogadon 5 mg Tablets


Nitrazepam




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 you experience any side effect and this becomes serious, tell your doctor or pharmacist.



In this leaflet:


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

  • 2. Before you take Mogadon Tablets

  • 3. How to take Mogadon Tablets

  • 4. Possible side effects

  • 5. How to store Mogadon Tablets

  • 6. Further information




What Mogadon Is And What It Is Used For


Mogadon belongs to a group of medicines known as benzodiazepines, which are tranquillisers (medicines that have a calming effect).


Mogadon shortens the time taken to fall asleep and lengthens the duration of sleep.


Mogadon Tablets are used for the short term treatment of sleeplessness (also known as insomnia) when it is severe.


Mogadon Tablets help you to sleep but do not cure the underlying cause of your insomnia, which you should discuss with your doctor.




Before You Take Mogadon Tablets



Do not take Mogadon Tablets if you:


  • are allergic (hypersensitive) to nitrazepam or any of the other ingredients of Mogadon Tablets (these are listed in section 6, ˝Further Information˝).

  • are allergic (hypersensitive) to any medicine known as a benzodiazepine (e.g. flurazepam, diazepam, chlordiazepoxide or temazepam).

  • suffer from lung disease.

  • suffer from difficulty breathing while awake or asleep.

  • suffer from myasthenia gravis (a condition in which the muscles become weak and tire easily).

  • are suffering from a psychiatric illness or a personality disorder (severe mental problems).

  • have a severe liver condition.


Mogadon Tablets are not for use in anyone under 18 years of age.




Take special care with Mogadon Tablets


Tell your doctor before you take these tablets if you:


  • have a long-term lung, liver or kidney disease.

  • suffer from depression or have recently suffered the death of a close friend or relative.

  • are suffering or have suffered from a mental illness.

  • have abused alcohol or drugs. You must not drink alcohol or use drugs while taking Mogadon.

  • are pregnant or breast-feeding.

Because Mogadon Tablets relax the muscles, elderly patients should take extra care when they get up at night as there is a risk of falls and consequently of injuries including hip fractures.




Taking other medicines


Tell your doctor or pharmacist if you are taking or have recently taken any other medicines, including medicines obtained without a prescription. This is extremely important, as using more than one medicine at the same time can strengthen or weaken the effect of the medicines involved. In particular, tell your doctor if you are taking
any of the following medicines:


  • Antidepressants, other tranquillisers or sleeping pills, or other such medicines that act on the brain and nerves.

  • Medicines used to relieve pain or anaesthetics.

  • Antihistamines (used for treating allergies) that cause drowsiness (e.g. chlorphenamine).

  • Medicines for treating epilepsy (e.g. phenytoin and phenobarbital).

  • Medicines that affect the liver (e.g. the antibiotic rifampicin).



Taking Mogadon Tablets with food and drink


Do not drink alcohol for as long as you are taking Mogadon Tablets. Alcohol will increase the effects of the tablets and this can be dangerous.




Pregnancy and breast-feeding


Tell your doctor before taking Mogadon Tablets if you are pregnant, think that you are pregnant or intend to become pregnant during treatment. Your doctor will then decide whether you should take this medicine.


Tell your doctor before taking Mogadon Tablets if you are breastfeeding. Avoid taking Mogadon Tablets if you are breast-feeding as Mogadon passes into breast-milk.


If your doctor has decided that you should receive this medicine during late pregnancy or during labour, your baby might have a low body temperature, floppiness and breathing and feeding difficulties. Also, your unborn baby may be at risk of developing dependency to this medicine and after birth may be at some risk of developing withdrawal symptoms.




Driving and using machines


Mogadon Tablets may cause side effects such as reduced alertness, confusion, tiredness, dizziness, poor muscle co-ordination and double vision. This may affect your ability to drive and operate machinery. Do not drive or operate machinery if you experience any of these side effects.




Important information about some of the ingredients of Mogadon Tablets



Lactose: Mogadon tablets contain lactose. Therefore, if you have been told by your doctor that you have an intolerance to some sugars, contact your doctor before taking this medicine.





How To Take Mogadon Tablets


Your doctor will find the lowest dose to control your symptoms.


The dose that your doctor prescribes will depend on the nature of your illness, your reaction to the medicine, your age and bodyweight.


Always take Mogadon exactly as your doctor has told you. Do not change the prescribed dose yourself. You should check with your doctor or pharmacist if you are not sure how to take this medicine. If you think that the effect of your medicine is too weak or too strong, talk to your doctor.


Mogadon is not for use in children.


The usual starting dose is 5 mg (one tablet). However, if you are elderly or suffer from a lung, liver or kidney condition, or are generally unwell, your starting dose will not usually be more than 2.5 mg (half a tablet).


You may not need to take this medicine every night.


Swallow the tablet(s) whole with water or another non-alcoholic drink.


Take the medicine just before going to bed. Make sure that you can sleep without interruptions for 7 to 8 hours after taking the tablets.


Treatment will not normally be continued for more than four weeks.


Mogadon Tablets may become less effective if you take them for more than four weeks. If you think that your medicine is no longer working or your insomnia does not improve, you should consult your doctor. Also, you may become dependent on the tablets if you use them at high doses and for long periods. Therefore, Mogadon Tablets are not suitable for long-term use and after a few weeks it is worth trying to get by without these tablets. This will help to prevent you becoming used to Mogadon and reduce the risk of dependence.


Withdrawal symptoms may occur when you stop taking Mogadon Tablets (see section below When you stop taking Mogadon Tablets).


Do not stop taking Mogadon Tablets without speaking to your doctor.



If you take more Mogadon Tablets than you should


If you take too many tablets or someone else accidentally takes your medicine, contact your doctor, pharmacist or nearest hospital straight away.




If you forget to take Mogadon


Do not take a double dose to make up for a forgotten dose. Instead you should simply continue with the next dose when it is due.




When you stop taking Mogadon Tablets


Your doctor will advise you when to stop taking the tablets.


Do not stop taking Mogadon tablets abruptly. You may experience withdrawal effects if your treatment is stopped suddenly. This is less likely if your dose is gradually reduced towards the end of your treatment.


Withdrawal symptoms may include:


  • a recurrence of sleep problems

  • depression

  • nervousness

  • extreme anxiety

  • tension

  • restlessness

  • confusion

  • mood changes

  • irritability

  • sweating

  • diarrhoea

  • headaches

  • muscle weakness



In severe cases the following symptoms may occur:


  • changes in behaviour

  • numbness and tingling of the extremities

  • fits

  • over-sensitivity to light, noise and touch

  • hallucinations

If you have taken benzodiazepines for a long time, the reduction in your dosage will be over a longer period of time than would normally be required when you stop taking this medicine. You may need additional help. Your doctor will be able to discuss this with you.



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




Possible Side Effects


Like all medicines, Mogadon Tablets can cause side effects, although not everybody gets them.


Changes in behaviour may occur rarely. These changes may include aggression, excitement, confusion, restlessness, agitation, irritability, rages, hallucinations, nightmares and depression.



If these behavioural symptoms occur, you must inform your doctor. He/she may want you to stop taking this medicine.



Common side effects:


  • drowsiness during the day

  • a feeling of emptiness

  • reduced alertness

  • confusion

  • tiredness

  • headache

  • dizziness

  • muscle weakness

  • poor muscle co-ordination

  • double vision



Rare side effects:


  • giddiness

  • reduced blood pressure

  • stomach upsets

  • skin rashes

  • changes in your vision other than double vision

  • changes in the level of sexual desire

  • inability to pass urine

  • yellowing of the eyes and skin (jaundice)

  • an abnormality of the blood (blood dyscrasias)

If you are woken up soon after taking the medicine your memory may be temporarily affected.


If you are an elderly patient, you may be more susceptible to side effects. If this happens, tell your doctor and he/she may decide to change your dose.




If you are concerned about any of these side effects, or if you notice any side effects not listed in this leaflet, tell your doctor or pharmacist.




How To Store Mogadon Tablets


Store Mogadon Tablets out of the reach and sight of children.


Store the bottle or blister in the original outer carton in order to protect from light.


Store Mogadon Tablets in a dry place below 25°C.


Do not use Mogadon Tablets after the expiry date which is stated on the bottle or blister and the outer carton after ˝EXP˝. 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 to protect the environment.




Further Information



What Mogadon Tablets contain




Active substance: Nitrazepam. Each tablet contains 5 mg of nitrazepam.



Other ingredients: Lactose, maize starch and magnesium stearate.





What Mogadon Tablets look like and contents of the pack


The white tablets are round with a capital letter V over the letters "MOG5" marked on one side and a line across the other so that they can be broken in half easily.



Mogadon Tablets come in packs of 30 tablets.




Marketing Authorisation Holder



Meda Pharmaceuticals Ltd.

Skyway House

Parsonage Road

Takeley

Bishop’s Stortford

CM22 6PU

UK




Manufacturer



ICN Polfa Rzeszów S.A.

ul. Przemyslowa 2

35-959 Rzeszów

Poland



For any information about this medicine, please contact the Marketing Authorisation Holder.




This leaflet was last revised in June 2009.



562108V1130UK00


P1EU02





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Modisal 60mg XL Tablets





1. Name Of The Medicinal Product



Modisal 60 XL


2. Qualitative And Quantitative Composition



Isosorbide-5-Mononitrate 60mg.



International non-proprietary name (INN): Isosorbide Mononitrate.



Chemical name:



1,4:3,6 dianhydro-D-glucitol-5-nitrate.



3. Pharmaceutical Form



Tablets (Modified Release).



4. Clinical Particulars



4.1 Therapeutic Indications



Prophylactic treatment of angina pectoris.



4.2 Posology And Method Of Administration



Adults: One tablet (60mg) once daily given in the morning. The dose may be increased to 2 tablets (120mg), the whole dose to be given together. The dose can be titrated to minimise the possibility of headache by initiating treatment with half a tablet (30mg) for the first two to four days. The tablets should not be chewed or crushed and should be swallowed with half a glass of fluid.



Children: The safety and efficacy of Modisal 60 XL Modified Release Tablets has not been established in children.



Elderly: No need for routine dosage adjustment in the elderly has been found, but special care may be needed in those with increased susceptibility to hypo-tension or marked hepatic or renal insufficiency.



4.3 Contraindications



Severe cerebrovascular insufficiency. Hypotension.



Sildenafil has been shown to potentiate the hypotensive effects of nitrates and its co-administration with nitrates or nitric oxide donors is therefore contra-indicated.



4.4 Special Warnings And Precautions For Use



Modisal 60 XL Modified Release Tablets are not indicated for relief of acute anginal attacks; in the event of an acute attack, sublingual or buccal glyceryl trinitrate tablets should be used.



4.5 Interaction With Other Medicinal Products And Other Forms Of Interaction



There is a possibility that ISMN may enhance the hypotensive effect of hydralazine.



The hypotensive effects of nitrates are potentiated by concurrent administration of sildenafil.



4.6 Pregnancy And Lactation



The safety and efficacy of Modisal 60 XL Modified Release Tablets during pregnancy or lactation has not been established.



4.7 Effects On Ability To Drive And Use Machines



The patient should be warned not to drive or operate machinery if hypotension or dizziness occurs.



4.8 Undesirable Effects



Headache may occur when treatment is initiated, but usually disappears after 1 to 2 weeks of treatment. Hypotension with symptoms such as dizziness or nausea has occasionally been reported. These symptoms generally disappear during long-term treatment.



4.9 Overdose



Treatment should be symptomatic. The main symptom is likely to be hypotension.



5. Pharmacological Properties



5.1 Pharmacodynamic Properties



Organic nitrates (including GTN, ISDN and ISMN) are potent relaxers of smooth muscle. They have a powerful effect on vascular smooth muscle with less effect on bronchiolar, gastrointestinal, ureteral and uterine smooth muscle. Low concentrations dilate both arteries and veins.



Venous dilatation pools blood in the periphery leading to a decrease in venous return, central blood volume, and ventricular filling volumes and pressures.



Cardiac output may remain unchanged or it may decline as a result of the decrease in venous return. Arterial blood pressure usually declines secondary to a decrease in cardiac output or arteriolar vasodilatation, or both. A modest reflex increase in heart rate results from the decrease in arterial blood pressure. Nitrates can dilate epicardial coronary arteries including atherosclerotic stenoses.



The cellular mechanism of nitrate-induced smooth muscle relaxation has become apparent in recent years. Nitrates enter the smooth muscle cell and are cleaved to inorganic nitrate and eventually to nitric oxide. This cleavage requires the presence of sulphydryl groups, which apparently come from the amino acid cysteine. Nitric oxide undergoes further reduction to nitrosothiol by further interaction with sulphydryl groups. Nitrosothiol activates guanylate cyclase in the vascular smooth muscle cells, thereby generating cyclic guanosine monophosphate (CGMP). It is this latter compound, CGMP, that produces smooth muscle relaxation by accelerating the release of calcium from these cells.



5.2 Pharmacokinetic Properties



Absorption:



Isosorbide-5-mononitrate is readily absorbed from the gastro-intestinal tract.



Distribution:



Following oral administration of conventional tablets, peak plasma levels are reached in about 1 hour. Unlike isosorbide dinitrate, ISMN does not undergo first-pass hepatic metabolism and bioavailability is 100%. ISMN has a volume of distribution of about 40 litres and is not significantly protein bound.



Elimination:



ISMN is metabolised to inactive metabolites including isosorbide and isosorbide glucuronide. The pharmacokinetics are unaffected by the presence of heart failure, renal or hepatic insufficiency. Only 20% of ISMN is excreted unchanged in the urine. An elimination half life of about 4-5 hours has been reported.



5.3 Preclinical Safety Data



Not applicable.



6. Pharmaceutical Particulars



6.1 List Of Excipients



Stearic acid, carnauba wax, hydroxypropyl methylcellulose, lactose, magnesium stearate, talc, purified siliceous earth, polyethylene glycol 4000, E171 and E172.



6.2 Incompatibilities



None known.



6.3 Shelf Life



3 years.



6.4 Special Precautions For Storage



Store in a dry place below 25ºC. Protect from light.



6.5 Nature And Contents Of Container



*The tablets are packed in aluminium foil/PVC blisters packed in boxes of 28, 30, 56, 60 and 100.



6.6 Special Precautions For Disposal And Other Handling



The tablets should be swallowed whole with half a glass of water. They must not be chewed or crushed.



Administrative Data


7. Marketing Authorisation Holder



Sandoz Ltd



Woolmer Way



Bordon



Hampshire



GU35 9QE



8. Marketing Authorisation Number(S)



PL 04416/0284



9. Date Of First Authorisation/Renewal Of The Authorisation



5th March 1998



10. Date Of Revision Of The Text



9 September 2003



* Only marketed pack sizes to be included in the SPC printed for issue




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Vitamin C Genericon




Vitamin C Genericon may be available in the countries listed below.


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Ascorbic Acid

Ascorbic Acid is reported as an ingredient of Vitamin C Genericon in the following countries:


  • Austria

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Monday, 26 September 2016

MST Continus tablets 5 mg, 10 mg, 15 mg, 30 mg, 60 mg, 100 mg, 200 mg





1. Name Of The Medicinal Product



MST® CONTINUS® 5 mg, 10 mg, 15 mg, 30 mg, 60 mg, 100 mg, 200 mg prolonged release tablets.


2. Qualitative And Quantitative Composition



Tablets containing Morphine Sulphate 5 mg, 10 mg, 15 mg, 30 mg, 60 mg, 100 mg, 200 mg.



3. Pharmaceutical Form



Prolonged release, film-coated, biconvex tablets marked with the NAPP logo on one side and the strength of the preparation on the other.



MST CONTINUS tablets 5 mg are white.



MST CONTINUS tablets 10 mg are golden brown.



MST CONTINUS tablets 15 mg are green.



MST CONTINUS tablets 30 mg are purple.



MST CONTINUS tablets 60 mg are orange.



MST CONTINUS tablets 100 mg are grey.



MST CONTINUS tablets 200 mg are teal green.



4. Clinical Particulars



4.1 Therapeutic Indications



For the prolonged relief of severe and intractable pain. MST CONTINUS tablets 5 mg, 10 mg, 15 mg and 30 mg are additionally indicated for the relief of post-operative pain.



4.2 Posology And Method Of Administration



Route of administration:



Oral.



MST CONTINUS tablets should be swallowed whole and not broken, chewed or crushed. The administration of broken, chewed or crushed tablets may lead to a rapid release and absorption of a potentially fatal dose of morphine sulphate (see section 4.9, Overdose).



.



MST CONTINUS tablets should be used at 12-hourly intervals. The dosage is dependent upon the severity of the pain, the patient's age and previous history of analgesic requirements.



Adults:



A patient presenting with severe pain, uncontrolled by weaker opioids (e.g. dihydrocodeine) should normally be started on 30 mg 12-hourly. Patients previously on normal release oral morphine should be given the same total daily dose as MST CONTINUS tablets but in divided doses at 12-hourly intervals.



Increasing severity of pain will require an increased dosage of the tablets. Higher doses should be made, where possible in 30-50% increments as required. The correct dosage for any individual patient is that which is sufficient to control pain with no, or tolerable, side effects for a full 12 hours. It is recommended that the 200 mg strength is reserved for patients who have already been titrated to a stable analgesic dose using lower strengths of morphine sulphate or other opioid preparations.



Patients receiving MST CONTINUS tablets in place of parenteral morphine sulphate should be given a sufficiently increased dosage to compensate for any reduction in analgesic effects associated with oral administration. Usually such increased requirement is of the order of 100%. In such patients individual dose adjustments are required.



Children:



For children with severe cancer pain, a starting dose in the range of 0.2 to 0.8 mg morphine sulphate per kg bodyweight 12-hourly is recommended. Doses should then be titrated as for adults.



Post-operative pain:



MST CONTINUS tablets are not recommended in the first 24 hours post-operatively or until normal bowel function has returned; thereafter it is suggested that the following dosage schedule be observed at the physician's discretion:



(a) MST CONTINUS tablets 20 mg 12-hourly to patients under 70 kg



(b) MST CONTINUS tablets 30 mg 12-hourly to patients over 70 kg



(c) Elderly - a reduction in dosage may be advisable in the elderly



(d) Children - not recommended.



Supplemental parenteral morphine sulphate may be given if required but with careful attention to the total dosages of morphine sulphate, and bearing in mind the prolonged effects of morphine sulphate in this prolonged release formulation.



4.3 Contraindications



Respiratory depression, head injury, paralytic ileus, 'acute abdomen', delayed gastric emptying, obstructive airways disease, hypersensitivity to any of the tablet constituents, acute hepatic disease, concurrent administration of monoamine oxidase inhibitors or within two weeks of discontinuation of their use. Children under one year of age.



Not recommended for pre-operative use or for the first 24 hours post-operatively.



4.4 Special Warnings And Precautions For Use



As with all narcotics a reduction in dosage may be advisable in the elderly, in hypothyroidism and in patients with significantly impaired renal or hepatic function. Use with caution in patients with impaired respiratory function, severe bronchial asthma, convulsive disorders, acute alcoholism, delirium tremens, raised intracranial pressure , hypotension with hypovolaemia, severe cor pulmonale, patients with a history of substance abuse, opiate dependent patients, diseases of the biliary tract, pancreatitis, inflammatory bowel disorders, prostatic hypertrophy and adrenocortical insufficiency.



Morphine sulphate may lower the seizure threshold in patients with a history of epilepsy.



Should paralytic ileus be suspected or occur during use, MST CONTINUS tablets should be discontinued immediately. As with all morphine sulphate preparations, patients about to undergo additional pain relieving procedures (e.g. surgery, plexus blockade) should not receive MST CONTINUS tablets for 24 hours prior to the intervention. If further treatment with MST CONTINUS tablets is indicated then the dosage should be adjusted to the new post-operative requirement.



As with all oral morphine sulphate preparations, MST CONTINUS tablets should be used with caution post-operatively and following abdominal surgery, as morphine sulphate impairs intestinal motility and should not be used until the physician is assured of normal bowel function.



The major risk of opioid excess is respiratory depression.



The patient may develop tolerance to the drug with chronic use and require progressively higher doses to maintain pain control. Prolonged use of this product may lead to physical dependence and a withdrawal syndrome may occur upon abrupt cessation of therapy. When a patient no longer requires therapy with morphine sulphate, it may be advisable to taper the dose gradually to prevent symptoms of withdrawal.



Morphine sulphate has an abuse profile similar to other strong agonist opioids. Morphine sulphate may be sought and abused by people with latent or manifest addiction disorders. There is potential for development of psychological dependence (addiction) to opioid analgesics, including morphine. The product should be used with particular care in patients with a history of alcohol and drug abuse.



The prolonged release tablets must be swallowed whole, and not broken, chewed, dissolved or crushed. The administration of broken, chewed or crushed tablets may lead to a rapid release and absorption of a potentially fatal dose of morphine sulphate (see section 4.9).



Abuse of MST Continus tablets by parenteral administration can be expected to result in serious adverse events, which may be fatal.



It is not possible to ensure bioequivalence between different brands of prolonged release morphine sulphate products. Therefore, it should be emphasised that patients, once titrated to an effective dose, should not be changed from MST CONTINUS preparations to other slow, sustained or prolonged release morphine sulphate or other potent narcotic analgesic preparations without retitration and clinical assessment.



4.5 Interaction With Other Medicinal Products And Other Forms Of Interaction



Morphine sulphate potentiates the effects of tranquillisers, general anaesthetics, phenothiazines, other central nervous system depressants including hypnotics or sedatives, alcohol, muscle relaxants, antihypertensives and gabapentin. Interactive effects resulting in respiratory depression, hypotension, profound sedation, or coma may result if these drugs are taken in combination with the usual doses of morphine sulphate.



Morphine sulphate should not be co-administered with monoamine oxidase inhibitors or within two weeks of such therapy.



Medicinal products that block the action of acetylcholine, for example antihistamines, anti-parkinsons and anti-emetics, may interact with morphine sulphate to potentiate anticholinergic adverse events.



Cimetidine inhibits the metabolism of morphine sulphate.



Plasma concentrations of morphine sulphate may be reduced by rifampicin.



Although there are no pharmacokinetic data available for concomitant use of ritonavir with morphine sulphate, ritonavir induces the hepatic enzymes responsible for the glucuronidation of morphine sulphate, and may possibly decrease plasma concentrations of morphine sulphate.



4.6 Pregnancy And Lactation



MST CONTINUS tablets are not recommended during pregnancy and labour due to the risk of neonatal respiratory depression. Administration to nursing mothers is not recommended as morphine sulphate is excreted in breast milk. Withdrawal symptoms may be observed in the newborn of mothers undergoing chronic treatment.



4.7 Effects On Ability To Drive And Use Machines



Morphine sulphate may modify the patient's reactions to a varying extent depending on the dosage and susceptibility. If affected, patients should not drive or operate machinery.



4.8 Undesirable Effects



In normal doses, the commonest side effects of morphine sulphate are nausea, vomiting, constipation and drowsiness. With chronic therapy, nausea and vomiting are unusual with MST CONTINUS tablets but should they occur the tablets can be readily combined with an anti-emetic if required. Constipation may be treated with appropriate laxatives. Common (incidence of














































Undesirable Effects


Common



(


Uncommon



(< 1%)


Immune system disorders


 


Allergic reaction



Anaphylactic reaction



Anaphylactoid reaction


Psychiatric disorders


Confusion



Insomnia



Thinking disturbances


Agitation



Drug dependence



Dysphoria



Euphoria



Hallucinations



Mood altered


Nervous system disorders


Headache



Involuntary muscle contractions



Myoclonus



Somnolence


Convulsions



Hypertonia



Paraesthesia



Syncope



Vertigo


Eye disorders


 


Miosis



Visual disturbance


Cardiac disorders


 


Bradycardia



Palpitations



Tachycardia


Vascular disorders


 


Facial flushing



Hypotension



Hypertension


Respiratory, thoracic and mediastinal disorders


Bronchospasm



Cough decreased


Pulmonary oedema



Respiratory depression


Gastrointestinal disorders


Abdominal pain



Anorexia



Constipation



Dry mouth



Dyspepsia



Nausea



Vomiting


Gastrointestinal disorders



Ileus



Taste perversion


Hepatobiliary disorders


Exacerbation of pancreatitis


Biliary pain



Increased hepatic enzymes


Skin and subcutaneous tissue disorders


Hyperhidrosis



Rash


Urticaria


Renal and urinary disorders


 


Ureteric spasm



Urinary retention


Reproductive system and breast disorders


 


Amenorrhea



Decreased libido



Erectile dysfunction


General disorders and administration site conditions


Asthenia



Pruritus


Drug tolerance



Drug withdrawal syndrome



Malaise



Peripheral oedema


4.9 Overdose



Signs of morphine sulphate toxicity and overdosage are pin-point pupils, skeletal muscle flaccidity, bradycardia, respiratory depression and hypotension. Circulatory failure and deepening coma may occur in more severe cases. Overdosage can result in death. Rhabdomyolysis progressing to renal failure has been reported in opioid overdosage.



Crushing and taking the contents of a prolonged release dosage form may lead to the release of morphine sulphate in an immediate fashion; this might result in a fatal overdose.



Treatment of morphine sulphate overdosage:



Primary attention should be given to the establishment of a patent airway and institution of assisted or controlled ventilation.



The pure opioid antagonists are specific antidotes against the effects of opioid overdose. Other supportive measures should be employed as needed.



In the case of massive overdosage, administer naloxone 0.8 mg intravenously. Repeat at 2-3 minute intervals as necessary, or by an infusion of 2 mg in 500 ml of normal saline or 5% dextrose (0.004 mg/ml).



The infusion should be run at a rate related to the previous bolus doses administered and should be in accordance with the patient's response. However, because the duration of action of naloxone is relatively short, the patient must be carefully monitored until spontaneous respiration is reliably re-established. MST CONTINUS tablets will continue to release and add to the morphine sulphate load for up to 12 hours after administration and the management of morphine sulphate overdosage should be modified accordingly.



For less severe overdosage, administer naloxone 0.2 mg intravenously followed by increments of 0.1 mg every 2 minutes if required.



Naloxone should not be administered in the absence of clinically significant respiratory or circulatory depression secondary to morphine sulphate overdosage. Naloxone should be administered cautiously to persons who are known, or suspected, to be physically dependent on morphine sulphate. In such cases, an abrupt or complete reversal of opioid effects may precipitate an acute withdrawal syndrome.



Gastric contents may need to be emptied as this can be useful in removing unabsorbed drug, particularly when a prolonged release formulation has been taken.



5. Pharmacological Properties



5.1 Pharmacodynamic Properties



Pharmacotherapeutic group: natural opium alkaloid



ATC code: N02A A01



Morphine sulphate acts as an agonist at opiate receptors in the CNS, particularly Mu and, to a lesser extent, Kappa receptors. Mu receptors are thought to mediate supraspinal analgesia, respiratory depression and euphoria, and Kappa receptors, spinal analgesia, miosis and sedation.



Central Nervous System



The principal actions of therapeutic value of morphine sulphate are analgesia and sedation (i.e., sleepiness and anxiolysis). Morphine sulphate produces respiratory depression by direct action on brain stem respiratory centers.



Morphine sulphate depresses the cough reflex by direct effect on the cough centre in the medulla. Antitussive effects may occur with doses lower than those usually required for analgesia. Morphine sulphate causes miosis, even in total darkness. Pinpoint pupils are a sign of narcotic overdose but are not pathognomonic (e.g., pontine lesions of haemorrhagic or ischaemic origin may produce similar findings). Marked mydriasis rather than miosis may be seen with hypoxia in the setting of morphine sulphate overdose.



Gastrointestinal Tract and Other Smooth Muscle



Morphine sulphate causes a reduction in motility associated with an increase in smooth muscle tone in the antrum of the stomach and duodenum. Digestion of food in the small intestine is delayed and propulsive contractions are decreased. Propulsive peristaltic waves in the colon are decreased, while tone is increased to the point of spasm resulting in constipation. Morphine sulphate generally increases smooth muscle tone, especially the sphincters of the gastrointestinal and biliary tracts. Morphine sulphate may produce spasm of the sphincter of Oddi, thus raising intrabiliary pressure.



Cardiovascular System



Morphine sulphate may produce release of histamine with or without associated peripheral vasodilation. Manifestations of histamine release and/or peripheral vasodilation may include pruritus, flushing, red eyes, sweating, and/or orthostatic hypotension.



Endocrine System



Opioids may influence the hypothalamic-pituitary-adrenal or -gonadal axes. Some changes that can be seen include an increase in serum prolactin, and decreases in plasma cortisol and testosterone in association with inappropriately low or normal ACTH, LH or FSH levels. Some premenopausal women may have low oestrogen levels. Clinical symptoms may be manifest from these hormonal changes.



Other Pharmacological Effects



In vitro and animal studies indicate various effects of natural opioids, such as morphine sulphate, on components of the immune system; the clinical significance of these findings is unknown.



5.2 Pharmacokinetic Properties



Morphine sulphate is well absorbed from MST CONTINUS tablets and, in general, peak plasma concentrations are achieved 1-5 hours following administration. The availability is complete when compared to an equivalent dose of immediate release oral solution. Morphine sulphate is subject to a significant first-pass effect which results in a lower bioavailability when compared to an equivalent intravenous dose.



The major metabolic transformation of morphine sulphate is glucuronidation to morphine sulphate-3-glucuronide and morphine sulphate-6-glucuronide which then undergo renal excretion. These metabolites are excreted in bile and may be subject to hydrolysis and subsequent re-absorption.



Patients are titrated to appropriate pain control using the wide range of strengths of MST CONTINUS tablets. Consequently, there is a large inter-patient variation in required dosage, the minimum dosage being 5 mg 12-hourly, and a dose of 5.6 g 12-hourly has been recorded.



5.3 Preclinical Safety Data



There are no pre-clinical data of relevance to the prescriber which are additional to that already included in other sections of the SPC.



6. Pharmaceutical Particulars



6.1 List Of Excipients



Tablet core:



Hydroxyethylcellulose Ph Eur



Purified Water Ph Eur



Cetostearyl Alcohol Ph Eur



Magnesium Stearate Ph Eur



Purified Talc Ph Eur



Lactose Anhydrous (except for 100 mg and 200 mg tablets) NF



Hypromellose (E464) Ph Eur



Macrogol Ph Eur



The following tablets have the colourants listed below:



5 mg - Titanium dioxide (E171)



10 mg - Iron oxide (E172), Titanium dioxide (E171)



15 mg - Iron oxide (E172), brilliant blue (E133), quinoline yellow (E104), indigo carmine (E132) Titanium dioxide (E171)



30 mg - Erythrosine (E127), indigo carmine (E132), sunset yellow (E110), Titanium dioxide (E171)



60 mg - Erythrosine (E127), quinoline yellow (E104), sunset yellow (E110), Titanium dioxide (E171)



100 mg - Iron oxide (E172), indigo carmine (E132), Titanium dioxide (E171)



200 mg - Brilliant blue (E133), quinoline yellow (E104), Titanium dioxide (E171.



6.2 Incompatibilities



None stated.



6.3 Shelf Life



Five years.



6.4 Special Precautions For Storage



Do not store above 25oC.



6.5 Nature And Contents Of Container



Aluminium foil-backed PVdC/PVC blister packs. Pack size 60 tablets.



6.6 Special Precautions For Disposal And Other Handling



None.



7. Marketing Authorisation Holder



Napp Pharmaceuticals Limited



Cambridge Science Park



Milton Road



Cambridge CB4 0GW



8. Marketing Authorisation Number(S)



PL 16950/0035-0041



9. Date Of First Authorisation/Renewal Of The Authorisation



1 May 1999



10. Date Of Revision Of The Text



June 2010



11 LEGAL CATEGORY


CD (Sch 2), POM



® MST, MST CONTINUS, CONTINUS, NAPP and the NAPP devices are Registered Trade Marks.



© Napp Pharmaceuticals Ltd 2010.




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