ANGIVENT OD Trimetazidine Hydrochloride 60mg Sustained Release Capsule 1's
RXDRUG-DR-XY41351-1pc
Discreet Packaging
FDA-registered Products
FDA-licensed Pharmacies
Indications/Uses
Used in angina pectoris & ischemia of neurosensorial tissues as in Meniere's disease.
Ischaemic heart disease (angina pectoris, sequelae of myocardial infarction).
Dosage/Direction for Use
Adults: One capsule once a day (early morning or at bedtime).
Overdosage
Trimetazidine is safe and well tolerated. The toxic dose being very high, the safety margin of this drug is wide. The most commonly encountered adverse effects are gastric discomfort, nausea, headache and vertigo.
Administration
May be taken with or without food.
Contraindications
Hypersensitivity to trimetazidine.
Special Precautions
In Impaired Renal and Hepatic Function: Appropriate dosage reductions may be done in patients with impaired renal and hepatic function.
Use in Pregnancy: There is insufficient evidence to recommend the use of trimetazidine in pregnancy. Animal studies do not reveal any teratogenic effect.
Use in Lactation: There is no information on the secretion of trimetazidine into breast milk. However, breastfeeding should be discounted if the use of trimetazidine is considered essential.
Use in Children: There is no experience with trimetazidine in children.
Use in Pregnancy: There is insufficient evidence to recommend the use of trimetazidine in pregnancy. Animal studies do not reveal any teratogenic effect.
Use in Lactation: There is no information on the secretion of trimetazidine into breast milk. However, breastfeeding should be discounted if the use of trimetazidine is considered essential.
Use in Children: There is no experience with trimetazidine in children.
Use In Pregnancy & Lactation
Use in Pregnancy: There is insufficient evidence to recommend the use of trimetazidine in pregnancy. Animal studies do not reveal any teratogenic effect.
Use in Lactation: There is no information on the secretion of trimetazidine into breast milk. However, breastfeeding should be discounted if the use of trimetazidine is considered essential.
Use in Lactation: There is no information on the secretion of trimetazidine into breast milk. However, breastfeeding should be discounted if the use of trimetazidine is considered essential.
Adverse Reactions
Generally, the drug is well tolerated.
The most commonly encountered adverse effects are gastric discomfort, nausea, headache and vertigo. Usually, the adverse effects are mild and reversible on discontinuation of therapy.
The most commonly encountered adverse effects are gastric discomfort, nausea, headache and vertigo. Usually, the adverse effects are mild and reversible on discontinuation of therapy.
Storage
Store below 25°C. Protect from light and moisture.
Shelf-Life: 24 months
Shelf-Life: 24 months
Action
Pharmacology: Pharmacodynamics: Mechanism of Action: Findings from in vitro and ex vivo studies of myocardial ischaemia have demonstrated that: Trimetazidine limits intracellular acidosis and sodium and calcium accumulation. It maintains intracellular ATP levels and reduces creatine phosphokinase release; preserves mitochondrial function; reduces myocardial fatty acid metabolism and increases myocardial glucose metabolism. Trimetazidine protects against oxygen free-radical induced membrane damage and inhibits neutrophil infiltration.
By inhibiting fatty acid metabolism and secondarily stimulating glucose metabolism, trimetazidine optimizes cardiac metabolism and thus protects the heart against the harmful effects of ischaemia.
Consistent with a cytoprotective effect, trimetazidine exhibited anti-ischaemic effects in vivo. It limited the extent of necrosis in a rat model of myocardial ischaemia and reduced the extent of nephropathy in a rat model of renal ischaemia. In addition, trimetazidine had a direct anti-ischaemic effect in patients undergoing coronary angioplasty.
Haemodynamic Effects: Data from studies in animals and in patients with coronary artery disease indicate that the anti-ischaemic effects of trimetazidine are not associated with any effects on haemodynamic determinants of myocardial oxygen consumption such as heart rate (HR) or blood pressure.
Sustained-release formulation of trimetazidine ensures adequate 24-hour control of myocardial ischaemia, which may not be adequately ensured by the conventional formulation of trimetazidine due to the problem of patient compliance of dosage. The drug exhibits significant anit-anginal effects and its efficacy is observed both during monotherapy as well as during combination therapy. Studies have also justified the use of trimetazidine to prevent reperfusion injury when used in combination with thrombolytics during the acute phase of myocardial infarction.
In addition, trimetazidine has also been shown to improve the outcome of percutaneous transluminal coronary angioplasty (PTCA) and to reduce reperfusion in patients undergoing coronary artery bypass surgery (CABG).
Pharmacokinetics: Absorption and Distribution: Following oral administration of the sustained-release (SR) preparation, trimetazidine is well absorbed from the intestinal mucosa, blood levels reaching a peak in 5 hours. The bioavailability of orally administered trimetazidine is approximately 90%. Food intake is not known to modify absorption. Trimetazidine is only weakly protein bound in plasma (approximately 16%) and therefore is widely distributed throughout the body.
Metabolism and Elimination: The major route of elimination is urinary (80% of the administered dose), with about 62% of the administered dose being eliminated in the unchanged form. Eight metabolites (including 4 phase II metabolites) have been detected in urine, but little is known of the properties of the metabolites.
By inhibiting fatty acid metabolism and secondarily stimulating glucose metabolism, trimetazidine optimizes cardiac metabolism and thus protects the heart against the harmful effects of ischaemia.
Consistent with a cytoprotective effect, trimetazidine exhibited anti-ischaemic effects in vivo. It limited the extent of necrosis in a rat model of myocardial ischaemia and reduced the extent of nephropathy in a rat model of renal ischaemia. In addition, trimetazidine had a direct anti-ischaemic effect in patients undergoing coronary angioplasty.
Haemodynamic Effects: Data from studies in animals and in patients with coronary artery disease indicate that the anti-ischaemic effects of trimetazidine are not associated with any effects on haemodynamic determinants of myocardial oxygen consumption such as heart rate (HR) or blood pressure.
Sustained-release formulation of trimetazidine ensures adequate 24-hour control of myocardial ischaemia, which may not be adequately ensured by the conventional formulation of trimetazidine due to the problem of patient compliance of dosage. The drug exhibits significant anit-anginal effects and its efficacy is observed both during monotherapy as well as during combination therapy. Studies have also justified the use of trimetazidine to prevent reperfusion injury when used in combination with thrombolytics during the acute phase of myocardial infarction.
In addition, trimetazidine has also been shown to improve the outcome of percutaneous transluminal coronary angioplasty (PTCA) and to reduce reperfusion in patients undergoing coronary artery bypass surgery (CABG).
Pharmacokinetics: Absorption and Distribution: Following oral administration of the sustained-release (SR) preparation, trimetazidine is well absorbed from the intestinal mucosa, blood levels reaching a peak in 5 hours. The bioavailability of orally administered trimetazidine is approximately 90%. Food intake is not known to modify absorption. Trimetazidine is only weakly protein bound in plasma (approximately 16%) and therefore is widely distributed throughout the body.
Metabolism and Elimination: The major route of elimination is urinary (80% of the administered dose), with about 62% of the administered dose being eliminated in the unchanged form. Eight metabolites (including 4 phase II metabolites) have been detected in urine, but little is known of the properties of the metabolites.
MedsGo Class
Anti-Anginal Drugs
Features
Brand
Angivent OD
Full Details
Dosage Strength
60mg
Drug Ingredients
- Trimetazidine
Drug Packaging
Sustained Release Capsule 1's
Generic Name
Trimetazidine Hydrochloride
Dosage Form
Sustained Release Capsule
Registration Number
DR-XY41351
Drug Classification
Prescription Drug (RX)
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