Tuesday, October 25, 2016

Starlix 60mg, 120mg, 180mg film coated tablets





Starlix 60 mg film-coated tablets



Starlix 120 mg film-coated tablet



Starlix 180 mg film-coated tablets



Nateglinide




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 Starlix is and what it is used for

  • 2. Before you take Starlix

  • 3. How to take Starlix

  • 4. Possible side effects

  • 5. How to store Starlix

  • 6. Further information





What Starlix Is And What It Is Used For



Starlix is a medicine to lower blood sugar (glucose), which is taken by mouth (these medicines are also known as oral anti-diabetics).



It is used by people with type 2 diabetes. (This kind of diabetes is also called non-insulin-dependent diabetes mellitus.)



Insulin is a substance produced by a body organ called the pancreas. It helps to decrease blood sugar levels, especially after meals. In patients with type 2 diabetes, the body may not start producing insulin quickly enough after meals. Starlix works by stimulating the pancreas to produce insulin more quickly. This helps to keep the blood sugar controlled after meals.



Your doctor will prescribe Starlix together with another oral anti-diabetic containing metformin.



Starlix tablets start to act quickly after you take them and are eliminated from the body rapidly.





Before You Take Starlix



Follow all instructions given to you by your doctor and pharmacist carefully, even if they are different from what is in this leaflet.




Do not take Starlix



  • if you are allergic (hypersensitive) to nateglinide or any of the other ingredients of Starlix.

  • if you have type 1 diabetes (i.e. your body does not produce any insulin).

  • if you know that you have a severe liver problem.

  • if you are pregnant or planning to become pregnant.

  • if you are breast-feeding.

Talk to your doctor if you have any further questions or you think that any of these may apply to you.





Take special care with Starlix



People with diabetes sometimes get symptoms of low blood sugar (also called hypoglycaemia). Medicines, including Starlix, may also produce symptoms of low blood sugar.



If you get any of these symptoms – feeling dizzy, light-headed, hungry, shaky or any of the other signs in section 4, “Possible side effects” – eat or drink something containing sugar.



Some people are more likely to get symptoms of low blood sugar than others. Take care



  • if you are over 65 years of age.

  • if you are undernourished.

  • if you have another medical condition that may cause low blood sugar (e.g. an under-active pituitary or adrenal gland).

If any of these apply to you, monitor your blood sugar levels more carefully.





Talk to your doctor



  • if you know that you have a liver problem.

  • if you have a severe kidney problem.

  • if you have problems of drug metabolism.

  • if you are due to have an operation.

  • if you have suffered a fever, an accident or an infection.

Your treatment may need to be adjusted.





Taking other medicines



Please tell your doctor or pharmacist if you are taking or have recently taken any other medicines, including medicines obtained without a prescription.



The amount of Starlix that you need may change if you take other medicines as these may cause your blood sugar levels to go up or down.



It is especially important that you tell your doctor or pharmacist if you are taking:



  • Beta blockers or angiotensin-converting enzyme inhibitors (used, for example, to treat high blood pressure and certain heart conditions).

  • Diuretics (used in the treatment of high blood pressure).

  • Corticosteroids such as prednisone and cortisone (used to treat inflammatory disorders).

  • Inhibitors of drug metabolism such as fluconazole (used to treat fungal infection), gemfibrozil (used to treat dyslipidaemia) or sulfinpyrazone (used to treat chronic gout).

Your doctor may adjust the dose of these medicines.





Food, drink and exercise



Take Starlix before meals (see section 3, “How to take Starlix”). Its effect may be delayed if it is taken during or after meals.



Even though you are taking medicines for your diabetes, it is important to keep following the diet and/or exercise your doctor has recommended for you.



Watch carefully for signs of low blood sugar, especially



  • if you have exercised more strenuously than usual.

  • if you have drunk alcohol.

Alcohol may upset the control of your blood sugar so you are advised to talk to your doctor about drinking alcohol while taking Starlix. If you do get symptoms of low blood sugar, eat or drink something containing sugar and talk to your doctor.





Starlix and older people



Starlix can be used by people over 65 years of age. Take special care to avoid low blood sugar.





Starlix and children and adolescents



Starlix is not recommended for children and adolescents (under 18 years of age) because its effects in this age group have not been studied.





Pregnancy and breast-feeding



Do not take Starlix if you are pregnant or planning to become pregnant. See your doctor as soon as possible if you become pregnant during treatment.



Do not breast-feed during treatment with Starlix.



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





Driving and using machines



You are advised to take precautions to avoid hypoglycaemia whilst driving. This is particularly important if you have reduced or absent awareness of the warning signs of hypoglycaemia or if you have frequent episodes of hypoglycaemia. The advisability of driving should be considered in these circumstances.





Important information about some of the ingredients of Starlix



Starlix tablets contain lactose monohydrate. If you have been told by your doctor that you have an intolerance to some sugars, contact your doctor before taking this medicinal product.






How To Take Starlix



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




When to take Starlix



Take Starlix before the three main meals, usually:



  • 1 dose before breakfast

  • 1 dose before lunch

  • 1 dose before dinner

It is best to take it right before a main meal but you can take it up to 30 minutes before.



Do not take it if you are not going to eat a main meal. If you miss a meal, skip that dose of Starlix and wait until your next meal.





How much to take



Take Starlix as your doctor told you to. Your doctor will determine the dosage you require.



The usual dose of Starlix to start with is 60 mg before the three main meals. In some cases your doctor may prescribe higher doses. The recommended maximum daily dose is 180 mg three times daily to be taken before the three main meals.



Swallow the tablets whole with a glass of water before the meal.





How long to take Starlix



Take Starlix daily until your doctor tells you to stop.





If you take more Starlix than you should



If you have accidentally taken too many tablets, talk to a doctor straight away. If you experience symptoms of low blood sugar – if you feel dizzy, light-headed, hungry, shaky, or any of the other signs in section 4, “Possible side effects” – eat or drink something containing sugar.



If you feel as if you are about to have a severe hypoglycaemic attack (which may lead to loss of consciousness or seizure), call for urgent medical help – or make sure that someone else does this for you.





If you forget to take Starlix



If you forget to take a tablet simply take the next one before your next meal. Do not take a double dose of Starlix to make up for the one that you missed.






Possible Side Effects



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



The most common side effects are symptoms of low blood sugar (hypoglycaemia), which are usually mild. These include



  • sweating,

  • dizziness,

  • shaking,

  • weakness,

  • hunger,

  • feeling your heart beating fast,

  • tiredness,

  • feeling sick (nausea).

They can also be caused by lack of food or too high a dose of any anti-diabetic medicine you are taking. If you do get symptoms of low blood sugar, eat or drink something containing sugar.



Abdominal pain, indigestion, diarrhoea, nausea and vomiting have been reported.



Rare effects are mild abnormalities in liver function tests and allergic (hypersensitivity) reactions such as rash and itching.



A very rare effect is skin rash with blisters affecting the lips, eyes, mouth, sometimes with headache, fever and/or diarrhoea.



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.





How To Store Starlix



Keep out of the reach and sight of children.



Store in the original package.



Do not use Starlix after the expiry date stated on the carton after EXP. The expiry date refers to the last day of that month.



Do not use any Starlix pack that is damaged or shows signs of tampering.



Do not store above 30°C.



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 Starlix contains



  • The active substance is nateglinide.

  • The other ingredients are lactose monohydrate; cellulose, microcrystalline; povidone; croscarmellose sodium; magnesium stearate and silica, colloidal anhydrous.

  • The tablet coating contains hypromellose; titanium dioxide (E171); talc; macrogol and red (60 and 180 mg tablets) or yellow (120 mg tablets) iron oxide (E172).




What Starlix looks like and contents of the pack



Starlix 60 mg film-coated tablets are pink, round tablets with “STARLIX” marked on one side and “60” on the other.



Starlix 120 mg film-coated tablets are yellow, ovaloid tablets with “STARLIX” marked on one side and “120” on the other.



Starlix 180 mg film-coated tablets are red, ovaloid tablets with “STARLIX” marked on one side and “180” on the other.



Each blister pack contains 12, 24, 30, 60, 84, 120 or 360 tablets. Not all pack sizes or tablet strengths may be available in your country.





Marketing Authorisation Holder




Novartis Europharm Limited

Wimblehurst Road

Horsham

West Sussex

RH12 5AB

United Kingdom





Manufacturer




Novartis Farma S.p.A.

Via Provinciale Schito, 131

I-80058 Torre Annunziata - Napoli

Italy




For any information about this medicinal product, please contact the local representative of the Marketing Authorisation Holder:




























































United Kingdom

Novartis Pharmaceuticals UK Ltd.

Tel:+44 1276 698370




This leaflet was last approved in: 05/11/2007






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Beafemic




Beafemic may be available in the countries listed below.


Ingredient matches for Beafemic



Mefenamic Acid

Mefenamic Acid is reported as an ingredient of Beafemic in the following countries:


  • Singapore

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Estrogen receptor antagonists


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

Estrogen receptor antagonists bind to estrogen receptors and inhibit the action of estrogen. Estrogen controls the growth of certain types of breast cancers called estrogen receptor positive cancers. So estrogen receptor antagonists are useful in treating patients with estrogen sensitive breast cancers.

See also

Medical conditions associated with estrogen receptor antagonists:

  • Breast Cancer
  • Breast Cancer, Metastatic

Drug List:

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Levocarnitine Tablet




Levocarnitine Tablets USP (330 mg)

Levocarnitine Tablet Description


Levocarnitine is a carrier molecule in the transport of long-chain fatty acids across the inner mitochondrial membrane.


The chemical name of levocarnitine is 3-carboxy-2(R)-hydroxy-N,N,N-trimethyl-1-propanaminium, inner salt. Levocarnitine is a white crystalline, hygroscopic powder. It is readily soluble in water, hot alcohol, and insoluble in acetone. The specific rotation of levocarnitine is between -29° and -32°. Its chemical structure is:



Empirical Formula:C7H15NO3


Molecular Weight: 161.20


Each Levocarnitine Tablet USP contains 330 mg of levocarnitine and the inactive ingredients magnesium stearate, microcrystalline cellulose and povidone.



Levocarnitine Tablet - Clinical Pharmacology


Levocarnitine is a naturally occurring substance required in mammalian energy metabolism. It has been shown to facilitate long-chain fatty acid entry into cellular mitochondria, thereby delivering substrate for oxidation and subsequent energy production. Fatty acids are utilized as an energy substrate in all tissues except the brain. In skeletal and cardiac muscle, fatty acids are the main substrate for energy production.


Primary systemic carnitine deficiency is characterized by low concentrations of levocarnitine in plasma, RBC, and/or tissues. It has not been possible to determine which symptoms are due to carnitine deficiency and which are due to an underlying organic acidemia, as symptoms of both abnormalities may be expected to improve with levocarnitine. The literature reports that carnitine can promote the excretion of excess organic or fatty acids in patients with defects in fatty acid metabolism and/or specific organic acidopathies that bioaccumulate acylCoA esters.1-6


Secondary carnitine deficiency can be a consequence of inborn errors of metabolism. Levocarnitine may alleviate the metabolic abnormalities of patients with inborn errors that result in accumulation of toxic organic acids. Conditions for which this effect has been demonstrated are: glutaric aciduria II, methyl malonic aciduria, propionic acidemia, and medium chain fatty acylCoA dehydrogenase deficiency.7,8 Autointoxication occurs in these patients due to the accumulation of acylCoA compounds that disrupt intermediary metabolism. The subsequent hydrolysis of the acylCoA compound to its free acid results in acidosis which can be life-threatening. Levocarnitine clears the acylCoA compound by formation of acylcarnitine, which is quickly excreted. Carnitine deficiency is defined biochemically as abnormally low plasma concentrations of free carnitine, less than 20 µmol/L at one week post term and may be associated with low tissue and/or urine concentrations. Further, this condition may be associated with a plasma concentration ratio of acylcarnitine/levocarnitine greater than 0.4 or abnormally elevated concentrations of acylcarnitine in the urine. In premature infants and newborns, secondary deficiency is defined as plasma levocarnitine concentrations below age-related normal concentrations.



PHARMACOKINETICS


In a relative bioavailability study in 15 healthy adult male volunteers, Levocarnitine Tablets were found to be bio-equivalent to levocarnitine oral solution. Following 4 days of dosing with 6 tablets of levocarnitine 330 mg b.i.d. or 2 g of levocarnitine oral solution b.i.d., the maximum plasma concentration (Cmax) was about 80 µmol/L and the time to maximum plasma concentration (Tmax) occurred at 3.3 hours.


The plasma concentration profiles of levocarnitine after a slow 3 minute intravenous bolus dose of 20 mg/kg of levocarnitine were described by a two-compartment model. Following a single i.v. administration, approximately 76% of the levocarnitine dose was excreted in the urine during the 0-24h interval. Using plasma concentrations uncorrected for endogenous levocarnitine, the mean distribution half life was 0.585 hours and the mean apparent terminal elimination half life was 17.4 hours.


Total body clearance of levocarnitine (Dose/AUC including endogenous baseline concentrations) was a mean of 4.00 L/h.


Levocarnitine was not bound to plasma protein or albumin when tested at any concentration or with any species including the human.9



METABOLISM AND EXCRETION


In a pharmacokinetic study where five normal adult male volunteers received an oral dose of [3H-methyl]-L-carnitine following 15 days of a high carnitine diet and additional carnitine supplement, 58 to 65% of the administered radioactive dose was recovered in the urine and feces in 5 to 11 days. Maximum concentration of [3H-methyl]-L-carnitine in serum occurred from 2.0 to 4.5 hr after drug administration. Major metabolites found were trimethylamine N-oxide, primarily in urine (8% to 49% of the administered dose) and [3H]-γ-butyrobetaine, primarily in feces (0.44% to 45% of the administered dose). Urinary excretion of levocarnitine was about 4 to 8% of the dose. Fecal excretion of total carnitine was less than 1% of the administered dose.10


After attainment of steady state following 4 days of oral administration of Levocarnitine Tablets (1980 mg q12h) or oral solution (2000 mg q12h) to 15 healthy male volunteers, the mean urinary excretion of levocarnitine during a single dosing interval (12h) was about 9% of the orally administered dose (uncorrected for endogenous urinary excretion).



Indications and Usage for Levocarnitine Tablet


Levocarnitine is indicated in the treatment of primary systemic carnitine deficiency. In the reported cases, the clinical presentation consisted of recurrent episodes of Reye-like encephalopathy, hypoketotic hypoglycemia, and/or cardiomyopathy. Associated symptoms included hypotonia, muscle weakness and failure to thrive. A diagnosis of primary carnitine deficiency requires that serum, red cell and/or tissue carnitine levels be low and that the patient does not have a primary defect in fatty acid or organic acid oxidation (see CLINICAL PHARMACOLOGY). In some patients, particularly those presenting with cardiomyopathy, carnitine supplementation rapidly alleviated signs and symptoms. Treatment should include, in addition to carnitine, supportive and other therapy as indicated by the condition of the patient.


Levocarnitine is also indicated for acute and chronic treatment of patients with an inborn error of metabolism which results in a secondary carnitine deficiency.



Contraindications


None known.



Warnings


None.



Precautions



General


The safety and efficacy of oral levocarnitine has not been evaluated in patients with renal insufficiency. Chronic administration of high doses of oral levocarnitine in patients with severely compromised renal function or in ESRD patients on dialysis may result in accumulation of the potentially toxic metabolites, trimethylamine (TMA) and trimethylamine-N-oxide (TMAO), since these metabolites are normally excreted in the urine.



Carcinogenesis, mutagenesis, impairment of fertility


Mutagenicity tests performed in Salmonella typhimurium, Saccharomyces cerevisiae, and Schizosaccharomyces pombe indicate that levocarnitine is not mutagenic. No long-term animal studies have been performed to evaluate the carcinogenic potential of levocarnitine.



Pregnancy


Pregnancy Category B

Reproductive studies have been performed in rats and rabbits at doses up to 3.8 times the human dose on the basis of surface area and have revealed no evidence of impaired fertility or harm to the fetus due to levocarnitine. There are, however, no adequate and well controlled studies in pregnant women.


Because animal reproduction studies are not always predictive of human response, this drug should be used during pregnancy only if clearly needed.



Nursing mothers


Levocarnitine supplementation in nursing mothers has not been specifically studied.


Studies in dairy cows indicate that the concentration of levocarnitine in milk is increased following exogenous administration of levocarnitine. In nursing mothers receiving levocarnitine, any risks to the child of excess carnitine intake need to be weighed against the benefits of levocarnitine supplementation to the mother. Consideration may be given to discontinuation of nursing or of levocarnitine treatment.



Pediatric use


See DOSAGE AND ADMINISTRATION.



Adverse Reactions


Various mild gastrointestinal complaints have been reported during the long-term administration of oral L- or D,L-carnitine; these include transient nausea and vomiting, abdominal cramps, and diarrhea. Mild myasthenia has been described only in uremic patients receiving D,L-carnitine. Decreasing the dosage often diminishes or eliminates drug-related patient body odor or gastrointestinal symptoms when present. Tolerance should be monitored very closely during the first week of administration, and after any dosage increases.


Seizures have been reported to occur in patients with or without pre-existing seizure activity receiving either oral or intravenous levocarnitine. In patients with pre-existing seizure activity, an increase in seizure frequency and/or severity has been reported.



Overdosage


There have been no reports of toxicity from levocarnitine overdosage. Levocarnitine is easily removed from plasma by dialysis. The intravenous LD50 of levocarnitine in rats is 5.4 g/kg and the oral LD50 of levocarnitine in mice is 19.2 g/kg. Large doses of levocarnitine may cause diarrhea.



Levocarnitine Tablet Dosage and Administration


Levocarnitine Tablets USP


Adults: The recommended oral dosage for adults is 990 mg two or three times a day using the 330 mg tablets, depending on clinical response.


Infants and children: The recommended oral dosage for infants and children is between 50 and 100 mg/kg/day in divided doses, with a maximum of 3 g/day. Dosage should begin at 50 mg/kg/day. The exact dosage will depend on clinical response.


Monitoring should include periodic blood chemistries, vital signs, plasma carnitine concentrations and overall clinical condition.



How is Levocarnitine Tablet Supplied


Levocarnitine Tablets USP are supplied as 330 mg tablets embossed with "LC 77" in individual blisters, packaged in boxes of 90 (NDC 50383-172-90). Store at controlled room temperature (25°C). See USP. Levocarnitine Tablets USP are distributed by Hi-Tech Pharmacal Co., Inc., Amityville, NY 11701.




Rx only.



REFERENCES


1. Bohmer, T., Rydning, A. and Solberg, H.E. 1974. Carnitine levels in human serum in health and disease. Clin. Chim. Acta 57:55-61.


2. Brooks, H., Goldberg, L., Holland, R. et al. 1977. Carnitine-induced effects on cardiac and peripheral hemodynamics. J. Clin. Pharmacol. 17:561-568.


3. Christiansen, R., Bremer, J. 1976. Active transport of butyrobetaine and carnitine into isolated liver cells. Biochim. Biophys. Acta 448:562-577.


4. Lindstedt, S. and Lindstedt, G. 1961. Distribution and excretion of carnitine in the rat. Acta Chem. Scand. 15:701-702.


5. Rebouche, C.J. and Engel, A.G. 1983. Carnitine metabolism and deficiency syndromes. Mayo Clin. Proc. 58:533-540.


6. Rebouche, C.J. and Paulson, D.J. 1986. Carnitine metabolism and function in humans. Ann. Rev. Nutr. 6:41-66.


7. Scriver, C.R., Beaudet, A.L., Sly, W.S. and Valle, D. 1989. The Metabolic Basis of Inherited Disease. New York: McGraw-Hill.


8. Schaub, J., Van Hoof, F. and Vis, H.L. 1991. Inborn Errors of Metabolism. New York: Raven Press.


9. Marzo, A., Arrigoni Martelli, E., Mancinelli, A., Cardace, G., Corbelletta, C., Bassani, E. and Solbiati, M. 1991. Protein binding of L-carnitine family components. Eur. J. Drug Met. Pharmacokin., Special Issue III: 364-368.


10. Rebouche, C.J. 1991. Quantitative estimation of absorption and degradation of a carnitine supplement by human adults. Metabolism 40:1305-1310.





Amityville, NY 11701


PREVIOUS EDITION IS OBSOLETE


Date of Issue: 11/04 GTOPI-1



PRINCIPAL DISPLAY PANEL











LEVOCARNITINE 
levocarnitine  tablet










Product Information
Product TypeHUMAN PRESCRIPTION DRUGNDC Product Code (Source)50383-172 (54482-144)
Route of AdministrationORALDEA Schedule    








Active Ingredient/Active Moiety
Ingredient NameBasis of StrengthStrength
LEVOCARNITINE (LEVOCARNITINE)LEVOCARNITINE330 mg










Inactive Ingredients
Ingredient NameStrength
MAGNESIUM STEARATE 
CELLULOSE, MICROCRYSTALLINE 
POVIDONE 


















Product Characteristics
ColorWHITEScoreno score
ShapeROUNDSize13mm
FlavorImprint CodeLC;77
Contains      














Packaging
#NDCPackage DescriptionMultilevel Packaging
150383-172-909 BLISTER PACK In 1 CARTONcontains a BLISTER PACK
110 TABLET In 1 BLISTER PACKThis package is contained within the CARTON (50383-172-90)










Marketing Information
Marketing CategoryApplication Number or Monograph CitationMarketing Start DateMarketing End Date
NDANDA01894811/01/2005


Labeler - Hi-Tech Pharmacal Co., Inc. (101196749)
Revised: 12/2009Hi-Tech Pharmacal Co., Inc.

More Levocarnitine Tablet resources


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ASS axcount




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Aspirin

Acetylsalicylic Acid is reported as an ingredient of ASS axcount in the following countries:


  • Germany

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Mesalamine Rectal Suspension




Mesalamine Rectal Suspension USP

6888

Rx only

Mesalamine Rectal Suspension Description


The active ingredient in Mesalamine Rectal Suspension USP, 4 g/60 mL, a disposable (60 mL) unit, is mesalamine, also known as 5-aminosalicylic acid (5-ASA). Chemically, mesalamine is 5-amino-2-hydroxybenzoic acid.


The structural formula is:



C7H7NO3 M.W. 153.14


Each rectal suspension unit contains 4 grams of mesalamine. In addition to mesalamine the preparation contains the inactive ingredients carbomer 934P, edetate disodium, potassium acetate, potassium metabisulfite, purified water and xanthan gum. Sodium benzoate is added as a preservative. The disposable unit consists of an applicator tip protected by a polyethylene cover and lubricated with USP white petrolatum. The unit has a one-way valve to prevent back flow of the dispensed product.



Mesalamine Rectal Suspension - Clinical Pharmacology


Sulfasalazine is split by bacterial action in the colon into sulfapyridine (SP) and mesalamine (5-ASA). It is thought that the mesalamine component is therapeutically active in ulcerative colitis [A.K. Azad Khan et al, Lancet 2:892-895 (1977)]. The usual oral dose of sulfasalazine for active ulcerative colitis in adults is two to four grams per day in divided doses. Four grams of sulfasalazine provide 1.6 g of free mesalamine to the colon. Each Mesalamine Rectal Suspension USP delivers up to 4 g of mesalamine to the left side of the colon.


The mechanism of action of mesalamine (and sulfasalazine) is unknown, but appears to be topical rather than systemic. Mucosal production of arachidonic acid (AA) metabolites, both through the cyclooxygenase pathways, i.e., prostanoids, and through the lipoxygenase pathways, i.e., leukotrienes (LTs) and hydroxyeicosatetraenoic acids (HETEs) is increased in patients with chronic inflammatory bowel disease, and it is possible that mesalamine diminishes inflammation by blocking cyclooxygenase and inhibiting prostaglandin (PG) production in the colon.



Preclinical Toxicology


Preclinical studies have shown the kidney to be the major target organ for mesalamine toxicity. Adverse renal function changes were observed in rats after a single 600 mg/kg oral dose, but not after a 200 mg/kg dose. Gross kidney lesions, including papillary necrosis, were observed after a single oral > 900 mg/kg dose, and after I.V. doses of > 214 mg/kg. Mice responded similarly. In a 13 week oral (gavage) dose study in rats, the high dose of 640 mg/kg/day mesalamine caused deaths, probably due to renal failure, and dose-related renal lesions (papillary necrosis and/or multifocal tubular injury) were seen in most rats given the high dose (males and females) as well as in males receiving lower doses 160 mg/kg/day. Renal lesions were not observed in the 160 mg/kg/day female rats. Minimal tubular epithelial damage was seen in the 40 mg/kg/day males and was reversible. In a six-month oral study in dogs, the no-observable dose level of mesalamine was 40 mg/kg/day and doses of 80 mg/kg/day and higher caused renal pathology similar to that described for the rat. In a combined 52 week toxicity and 127 week carcinogenicity study in rats, degeneration in kidneys was observed at doses of 100 mg/kg/day and above admixed with diet for 52 weeks, and at 127 weeks increased incidence of kidney degeneration and hyalinization of basement membranes and Bowman's capsule were seen at 100 mg/kg/day and above. In the 12 month eye toxicity study in dogs, Keratoconjunctivitis Sicca (KCS) occurred at oral doses of 40 mg/kg/day and above. The oral preclinical studies were done with a highly bioavailable suspension where absorption throughout the gastrointestinal tract occurred. The human dose of 4 grams represents approximately 80 mg/kg but when mesalamine is given rectally as a suspension, absorption is poor and limited to the distal colon (see Pharmacokinetics). Overt renal toxicity has not been observed (see ADVERSE REACTIONS and PRECAUTIONS), but the potential must be considered.



Pharmacokinetics


Mesalamine administered rectally is poorly absorbed from the colon and is excreted principally in the feces during subsequent bowel movements. The extent of absorption is dependent upon the retention time of the drug product, and there is considerable individual variation. At steady state, approximately 10 to 30% of the daily 4 gram dose can be recovered in cumulative 24 hour urine collections. Other than the kidney, the organ distribution and other bioavailability characteristics of absorbed mesalamine in man are not known. It is known that the compound undergoes acetylation but whether this process takes place at colonic or systemic sites has not been elucidated.


Whatever the metabolic site, most of the absorbed mesalamine is excreted in the urine as the N-acetyl-5-ASA metabolite. The poor colonic absorption of rectally administered mesalamine is substantiated by the low serum concentration of 5-ASA and N-acetyl-5-ASA seen in ulcerative colitis patients after dosage with mesalamine. Under clinical conditions patients demonstrated plasma levels 10 to 12 hours post mesalamine administration of 2 mcg/mL, about two-thirds of which was the N-acetyl metabolite. While the elimination half-life of mesalamine is short (0.5 to 1.5 h), the acetylated metabolite exhibits a half-life of 5 to 10 hours [U. Klotz, Clin. Pharmacokin. 10:285-302 (1985)]. In addition, steady state plasma levels demonstrated a lack of accumulation of either free or metabolized drug during repeated daily administrations.



Efficacy


In a placebo-controlled, international, multicenter trial of 153 patients with active distal ulcerative colitis, proctosigmoiditis or proctitis, Mesalamine Rectal Suspension reduced the overall disease activity index (DAI) and individual components as follows:


















































































EFFECT OF TREATMENT ON SEVERITY OF DISEASE DATA FROM U.S.-CANADA TRIAL COMBINED RESULTS OF EIGHT CENTERS Activity Indices, Mean

*

Percent change for overall DAI only (calculated by taking the average of the change for each individual patient).


Significant mesalamine/placebo difference. p < 0.01


Each parameter has a 4 point scale with a numerical rating: 0 = normal, 1 = mild, 2 = moderate, 3 = severe. The four parameters are added together to produce a maximum overall DAI of 12.

§

Significant mesalamine/placebo difference. p < 0.05

  N Baseline Day 22End PointChange Baseline to End point*
Overall DAI Mesalamine767.424.053.37-55.07%
Placebo777.406.035.83-21.58% 
Stool FrequencyMesalamine1.581.11§1.01-0.57*
Placebo1.921.471.50-0.41 
Rectal BleedingMesalamine1.820.590.51-1.30
Placebo1.731.211.11-0.61 
Mucosal InflammationMesalamine2.171.220.96-1.21
Placebo2.181.741.61-0.56 
Physician's Assessment of Disease SeverityMesalamine1.861.130.88-0.97
Placebo1.871.621.55-0.30 

Differences between mesalamine and placebo were also statistically different in subgroups of patients on concurrent sulfasalazine and in those having an upper disease boundary between 5 and 20 or 20 and 40 cm. Significant differences between mesalamine and placebo were not achieved in those subgroups of patients on concurrent prednisone or with an upper disease boundary between 40 and 50 cm.



Indications and Usage for Mesalamine Rectal Suspension


Mesalamine Rectal Suspension is indicated for the treatment of active mild to moderate distal ulcerative colitis, proctosigmoiditis or proctitis.



Contraindications


Mesalamine Rectal Suspension is contraindicated for patients known to have hypersensitivity to the drug or any component of this medication.



Warnings


Mesalamine Rectal Suspension contains potassium metabisulfite, a sulfite that may cause allergic-type reactions including anaphylactic symptoms and life-threatening or less severe asthmatic episodes in certain susceptible people. The overall prevalence of sulfite sensitivity in the general population is unknown but probably low. Sulfite sensitivity is seen more frequently in asthmatic or in atopic nonasthmatic persons.


Epinephrine is the preferred treatment for serious allergic or emergency situations even though epinephrine injection contains sodium or potassium metabisulfite with the above-mentioned potential liabilities. The alternatives to using epinephrine in a life-threatening situation may not be satisfactory. The presence of a sulfite(s) in epinephrine injection should not deter the administration of the drug for treatment of serious allergic or other emergency situations.



Precautions


Mesalamine has been implicated in the production of an acute intolerance syndrome characterized by cramping, acute abdominal pain and bloody diarrhea, sometimes fever, headache and a rash; in such cases prompt withdrawal is required. The patient's history of sulfasalazine intolerance, if any, should be re-evaluated. If a rechallenge is performed later in order to validate the hypersensitivity it should be carried out under close supervision and only if clearly needed, giving consideration to reduced dosage. In the literature one patient previously sensitive to sulfasalazine was rechallenged with 400 mg oral mesalamine; within eight hours she experienced headache, fever, intensive abdominal colic, profuse diarrhea and was readmitted as an emergency. She responded poorly to steroid therapy and two weeks later a pancolectomy was required.


Although renal abnormalities were not noted in the clinical trials with Mesalamine Rectal Suspension, the possibility of increased absorption of mesalamine and concomitant renal tubular damage as noted in the preclinical studies must be kept in mind. Patients on Mesalamine Rectal Suspension, especially those on concurrent oral products which liberate mesalamine and those with preexisting renal disease, should be carefully monitored with urinalysis, BUN (blood urea nitrogen), and creatinine studies.


In a clinical trial most patients who were hypersensitive to sulfasalazine were able to take mesalamine enemas without evidence of any allergic reaction. Nevertheless, caution should be exercised when mesalamine is initially used in patients known to be allergic to sulfasalazine. These patients should be instructed to discontinue therapy if signs of rash or fever become apparent.


While using Mesalamine Rectal Suspension, some patients have developed pancolitis. However, extension of upper disease boundary and/or flare-ups occurred less often in the Mesalamine Rectal Suspension treated group than in the placebo-treated group.


Worsening of colitis or symptoms of inflammatory bowel disease, including melena and hematochezia, may occur after commencing mesalamine.


Rare instances of pericarditis have been reported with mesalamine containing products including sulfasalazine. Cases of pericarditis have also been reported as manifestations of inflammatory bowel disease. In the cases reported with Mesalamine Rectal Suspension, there have been positive rechallenges with mesalamine or mesalamine containing products. In one of these cases, however, a second rechallenge with sulfasalazine was negative throughout a 2 month follow-up. Chest pain or dyspnea in patients treated with Mesalamine Rectal Suspension should be investigated with this information in mind. Discontinuation of Mesalamine Rectal Suspension may be warranted in some cases, but rechallenge with mesalamine can be performed under careful clinical observation should the continued therapeutic need for mesalamine be present.



Carcinogenesis, Mutagenesis, Impairment of Fertility


Mesalamine caused no increase in the incidence of neoplastic lesions over controls in a 2 year study of Wistar rats fed up to 320 mg/kg/day of mesalamine admixed with diet. Mesalamine is not mutagenic to Salmonella typhimurium tester strains TA98, TA100, TA1535, TA1537, TA1538. There were no reverse mutations in an assay using E. coli strain WP2UVRA. There were no effects in an in vivo mouse micronucleus assay at 600 mg/kg and in an in vivo sister chromatid exchange at doses up to 610 mg/kg. No effects on fertility were observed in rats receiving up to 320 mg/kg/day. The oligospermia and infertility in men associated with sulfasalazine has very rarely been reported among patients treated with mesalamine.



Pregnancy


Teratogenic Effects

Pregnancy (category B)


Teratologic studies have been performed in rats and rabbits at oral doses up to five and eight times respectively, the maximum recommended human dose, and have revealed no evidence of harm to the embryo or the fetus. There are, however, no adequate and well controlled studies in pregnant women for either sulfasalazine or 5-ASA. Because animal reproduction studies are not always predictive of human response, 5-ASA should be used during pregnancy only if clearly needed.



Nursing Mothers


It is not known whether mesalamine or its metabolite(s) are excreted in human milk. As a general rule, nursing should not be undertaken while a patient is on a drug since many drugs are excreted in human milk.



Pediatric Use


Safety and effectiveness in pediatric patients have not been established.



Adverse Reactions



Clinical Adverse Experience


Mesalamine Rectal Suspension is usually well tolerated. Most adverse effects have been mild and transient.






































































































































ADVERSE REACTIONS OCCURRING IN MORE THAN 0.1% OF Mesalamine Rectal Suspension TREATED PATIENTS (COMPARISON TO PLACEBO)
SYMPTOMMESALAMINE N = 815 N%PLACEBON = 128 N %
Abdominal Pain/Cramps/Discomfort668.10107.81
Headache536.501612.50
Gas/Flatulence506.1353.91
Nausea475.77129.38
Flu435.2810.78
Tired/Weak/Malaise/Fatigue283.4486.25
Fever263.1900.00
Rash/Spots232.8243.12
Cold/Sore Throat192.3397.03
Diarrhea172.0953.91
Leg/Joint Pain172.0910.78
Dizziness151.8432.34
Bloating121.4721.56
Back Pain111.3510.78
Pain on Insertion of Enema Tip111.3510.78
Hemorrhoids111.3500.00
Itching101.2310.78
Rectal Pain101.2300.00
Constipation80.9843.12
Hair Loss70.8600.00
Peripheral Edema50.61118.59
UTI/Urinary Burning50.6143.12
Rectal Pain/Soreness/Burning50.6132.34
Asthenia10.1243.12
Insomnia10.1232.34

In addition, the following adverse events have been identified during post-approval use of products which contain (or are metabolized to) mesalamine in clinical practice: nephrotoxicity, pancreatitis, fibrosing alveolitis and elevated liver enzymes. Cases of pancreatitis and fibrosing alveolitis have been reported as manifestations of inflammatory bowel disease as well. Published case reports and/or spontaneous postmarketing surveillance have described rare instances of aplastic anemia, agranulocytosis, thrombocytopenia, eosinophilia, pancytopenia, neutropenia, oligospermia, and infertility in men. Anemia, leukocytosis, and thrombocytosis can be part of the clinical presentation of inflammatory bowel disease.



Hair Loss


Mild hair loss characterized by "more hair in the comb" but no withdrawal from clinical trials has been observed in 7 of 815 mesalamine patients but none of the placebo-treated patients. In the literature there are at least six additional patients with mild hair loss who received either mesalamine or sulfasalazine. Retreatment is not always associated with repeated hair loss.



Overdosage


There have been no documented reports of serious toxicity in man resulting from massive overdosing with mesalamine. Under ordinary circumstances, mesalamine absorption from the colon is limited.



Mesalamine Rectal Suspension Dosage and Administration


The usual dosage of Mesalamine Rectal Suspension USP in 60 mL units is one rectal instillation (4 grams) once a day, preferably at bedtime, and retained for approximately eight hours. While the effect of Mesalamine Rectal Suspension USP may be seen within 3 to 21 days, the usual course of therapy would be from 3 to 6 weeks depending on symptoms and sigmoidoscopic findings. Studies available to date have not assessed if Mesalamine Rectal Suspension will modify relapse rates after the 6 week short-term treatment. Mesalamine Rectal Suspension USP is for rectal use only.


Patients should be instructed to shake the bottle well to make sure the suspension is homogeneous. The patient should remove the protective sheath from the applicator tip. Holding the bottle at the neck will not cause any of the medication to be discharged. The position most often used is obtained by lying on the left side (to facilitate migration into the sigmoid colon); with the lower leg extended and the upper right leg flexed forward for balance. An alternative is the knee-chest position. The applicator tip should be gently inserted in the rectum pointing toward the umbilicus. A steady squeezing of the bottle will discharge most of the preparation. The preparation should be taken at bedtime with the objective of retaining it all night. Patient instructions are included with every seven units.



How is Mesalamine Rectal Suspension Supplied


Mesalamine Rectal Suspension USP, 4 g/60 mL for rectal administration is a off-white to tan colored suspension. Each disposable enema bottle contains 4 grams of mesalamine in 60 mL aqueous suspension. Enema bottles are supplied in boxed, foil-wrapped trays of seven. Mesalamine Rectal Suspension USP, 4 g/60 mL is for rectal use only.


Patient instructions are included.


Store at 20º to 25ºC (68º to 77ºF) [See USP Controlled Room Temperature]. Once the foil-wrapped unit of seven bottles is opened, any bottles remaining after 14 days should be discarded. Contents of enemas removed from the foil pouch may darken with time. Slight darkening will not affect potency, however, product with dark brown contents should be discarded.


NOTE: Mesalamine Rectal Suspension USP, 4 g/60 mL will cause staining of direct contact surfaces, including but not limited to fabrics, flooring, painted surfaces, marble, granite, vinyl, and enamel. Take care in choosing a suitable location for administration of this product.


Manufactured By:


TEVA PHARMACEUTICALS USA


Sellersville, PA 18960


Rev. C 8/2008



PATIENT INSTRUCTIONS


Mesalamine Rectal Suspension USP


Rx only


How to Use this Medication.


Best results are achieved if the bowel is emptied immediately before the medication is given.


NOTE: Mesalamine Rectal Suspension USP, 4 g/60 mL will cause staining of direct contact surfaces, including but not limited to fabrics, flooring, painted surfaces, marble, granite, vinyl, and enamel. Take care in choosing a suitable location for administration of this product.


1 Remove the Bottles


a. Remove the bottles from the protective foil pouch by tearing or by using scissors as shown, being careful not to squeeze or puncture bottles. Mesalamine Rectal Suspension USP, 4 g/60 mL is an off-white to tan colored suspension. Once the foil-wrapped unit of seven bottles is opened, any bottles remaining after 14 days should be discarded. Contents of enemas removed from the foil pouch may darken with time. Slight darkening will not affect potency, however, product with dark brown contents should be discarded.



2 Prepare the Medication for Administration


a. Shake the bottle well to make sure that the medication is thoroughly mixed.


b. Remove the protective sheath from the applicator tip. Hold the bottle at the neck so as not to cause any of the medication to be discharged.



3 Assume the Correct Body Position


a. Best results are obtained by lying on the left side with the left leg extended and the right leg flexed forward for balance.



b. An alternative to lying on the left side is the "knee-chest" position as shown here.



4 Administer the Medication


a. Gently insert the lubricated applicator tip into the rectum to prevent damage to the rectal wall, pointed slightly toward the navel.


b. Grasp the bottle firmly, then tilt slightly so that the nozzle is aimed toward the back, squeeze slowly to instill the medication. Steady hand pressure will discharge most of the medication. After administering, withdraw and discard the bottle.



c. Remain in position for at least 30 minutes to allow thorough distribution of the medication internally. Retain the medication all night, if possible.


Manufactured By:


TEVA PHARMACEUTICALS USA


Sellersville, PA 18960


Rev. B 8/2008



PRINCIPAL DISPLAY PANEL




Mesalamine Rectal Suspension USP 4 g/60 mL Label Text


NDC 0093-6888-71


MESALAMINE


RECTAL SUSPENSION, USP


4 g/60 mL


FOR RECTAL USE ONLY


7x60 mL UNIT-DOSE BOTTLES


TEVA









MESALAMINE 
mesalamine  suspension










Product Information
Product TypeHUMAN PRESCRIPTION DRUGNDC Product Code (Source)0093-6888
Route of AdministrationRECTALDEA Schedule    








Active Ingredient/Active Moiety
Ingredient NameBasis of StrengthStrength
MESALAMINE (MESALAMINE)MESALAMINE4 g  in 60 mL
















Inactive Ingredients
Ingredient NameStrength
EDETATE DISODIUM 
POTASSIUM ACETATE 
POTASSIUM METABISULFITE 
WATER 
XANTHAN GUM 
SODIUM BENZOATE 


















Product Characteristics
ColorWHITE (off white to tan)Score    
ShapeSize
FlavorImprint Code
Contains      














Packaging
#NDCPackage DescriptionMultilevel Packaging
10093-6888-717 BOTTLE In 1 BOXcontains a BOTTLE, WITH APPLICATOR
160 mL In 1 BOTTLE, WITH APPLICATORThis package is contained within the BOX (0093-6888-71)










Marketing Information
Marketing CategoryApplication Number or Monograph CitationMarketing Start DateMarketing End Date
ANDAANDA07684101/21/2011


Labeler - TEVA Pharmaceuticals USA Inc (118234421)
Revised: 01/2011TEVA Pharmaceuticals USA Inc

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Monday, October 24, 2016

Isosorbide Mononitrate




Isosorbide Mononitrate Tablets, USP

Rx Only



Isosorbide Mononitrate Description


Isosorbide Mononitrate, an organic nitrate, is a vasodilator with effects on both arteries and veins. The empirical formula is C6H9NO6 and the molecular weight is 191.14. The chemical name for Isosorbide Mononitrate is 1,4:3,6-Dianhydro-D-glucitol 5-nitrate and the compound has the following structural formula:



Isosorbide Mononitrate Tablets, USP are available as 10 mg and 20 mg tablets. Each tablet also contains as inactive ingredients: lactose, talc, colloidal silicon dioxide, starch, microcrystalline cellulose and aluminum stearate.



Isosorbide Mononitrate - Clinical Pharmacology


Isosorbide Mononitrate is the major active metabolite of isosorbide dinitrate (ISDN), and most of the clinical activity of the dinitrate is attributable to the mononitrate.


The principal pharmacological action of Isosorbide Mononitrate is relaxation of vascular smooth muscle and consequent dilatation of peripheral arteries and veins, especially the latter. Dilation of the veins promotes peripheral pooling of blood and decreases venous return to the heart, thereby reducing left ventricular end-diastolic pressure and pulmonary capillary wedge pressure (preload). Arteriolar relaxation reduces systemic vascular resistance, systolic arterial pressure, and mean arterial pressure (afterload). Dilatation of the coronary arteries also occurs. The relative importance of preload reduction, afterload reduction and coronary dilatation remains undefined.



Pharmacodynamics


Dosing regimens for most chronically used drugs are designed to provide plasma concentrations that are continuously greater than a minimally effective concentration. This strategy is inappropriate for organic nitrates. Several well-controlled clinical trials have used exercise testing to assess the antianginal efficacy of continuously-delivered nitrates. In the large majority of these trials, active agents were indistinguishable from placebo after 24 hours (or less) of continuous therapy. Attempts to overcome tolerance by dose escalation, even to doses far in excess of those used acutely, have consistently failed. Only after nitrates have been absent from the body for several hours has their antianginal efficacy been restored.


The drug-free interval sufficient to avoid tolerance to Isosorbide Mononitrate has not been completely defined. In the only regimen of twice-daily Isosorbide Mononitrate that has been shown to avoid development of tolerance, the two doses of Isosorbide Mononitrate Tablets are given 7 hours apart, so there is a gap of 17 hours between the second dose of each day and the first dose of the next day. Taking account of the relatively long half-life of Isosorbide Mononitrate this result is consistent with those obtained for other organic nitrates.


The asymmetric twice-daily regimen of Isosorbide Mononitrate Tablets successfully avoided significant rebound/withdrawal effects. The incidence and magnitude of such phenomena have appeared, in studies of other nitrates, to be highly dependent upon the schedule of nitrate administration.



Pharmacokinetics


Isosorbide Mononitrate is rapidly and completely absorbed from the gastrointestinal tract. In humans, Isosorbide Mononitrate is not subject to first pass metabolism in the liver. The absolute bioavailability of Isosorbide Mononitrate from Isosorbide Mononitrate Tablets is nearly 100%. Peak plasma concentrations usually occur in about 30-60 minutes. Isosorbide Mononitrate exhibits dose proportionality over the recommended dose range. Food does not significantly affect the absorption or bioavailability of Isosorbide Mononitrate Tablets. Metoprolol coadministration did not change the pharmacokinetics of Isosorbide Mononitrate. The volume of distribution is approximately 0.6 L/kg. Plasma protein binding of Isosorbide Mononitrate was found to be less than 5%.


When radiolabelled Isosorbide Mononitrate was administered to humans in order to elucidate the metabolic fate, about half of the dose was found denitrated and renally excreted as isosorbide and sorbitol. One quarter of the dose was accounted for as conjugates of the parent drug in the urine. None of these metabolites is vasoactive. Only 2% of the dose was excreted as unchanged drug.


The overall elimination half-life of Isosorbide Mononitrate is about 5 hours. The rate of clearance is the same in healthy young adults, in patients with various degrees of renal, hepatic or cardiac dysfunction and in the elderly. When radiolabelled Isosorbide Mononitrate was administered to humans, 93% of the dose was excreted within 48 hours into the urine. Renal excretion was virtually complete after 5 days; fecal excretion amounted to only 1% of the dose.


Isosorbide Mononitrate has no known effect on renal and hepatic function. In patients with varying degrees of renal failure, dosage adjustment does not appear necessary. In patients with liver cirrhosis, the pharmacokinetic parameters after a single dose of Isosorbide Mononitrate were similar to the values found in healthy volunteers.


Isosorbide Mononitrate is significantly removed from the blood during hemodialysis; however, an additional dose to compensate for drug lost is not necessary. In patients undergoing continuous ambulatory peritoneal dialysis, blood levels are similar to patients not on dialysis.



Clinical Trials


The acute and chronic antianginal efficacy of Isosorbide Mononitrate has been confirmed in clinical trials. The clinical efficacy of Isosorbide Mononitrate was studied in 21 stable angina pectoris patients. After single dose administration of Isosorbide Mononitrate Tablets, 20 mg, the exercise capacity was increased by 42.7% after one hour, 29.6% after 6 hours, and by 25% after eight hours when compared to placebo. Controlled trials of single doses of Isosorbide Mononitrate Tablets have demonstrated that antianginal activity is present about 1 hour after dosing, with peak effect seen from 1-4 hours after dosing.


In one multicenter placebo-controlled trial, Isosorbide Mononitrate was found to be safe and effective during acute and chronic (3 weeks) treatment of angina pectoris. Two hundred fourteen (214) patients were enrolled in the trial; 54 patients were randomized to receive placebo and 106 patients were randomized to receive 10 or 20 mg of Isosorbide Mononitrate Tablets twice daily seven hours apart. The largest effect of Isosorbide Mononitrate, compared to placebo, was on day one - dose one. Although 14 hours after the first dose of day 14, the increase in exercise tolerance due to Isosorbide Mononitrate was statistically significant, the increase was about half of that seen 2 hours after the first dose of day one. On day 21, two hours after the first dose the effect of Isosorbide Mononitrate was 60 to 70% of that seen on day one.



Indications and Usage for Isosorbide Mononitrate


Isosorbide Mononitrate Tablets are indicated for the prevention and treatment of angina pectoris due to coronary artery disease. The onset of action of oral Isosorbide Mononitrate is not sufficiently rapid for this product to be useful in aborting an acute anginal episode.



Contraindications


Allergic reactions to organic nitrates are extremely rare, but they do occur. Isosorbide Mononitrate is contraindicated in patients who are allergic to it.



Warnings


Amplification of the vasodilatory effects of Isosorbide Mononitrate by sildenafil can result in severe hypotension. The time course and dose dependence of this interaction have not been studied. Appropriate supportive care has not been studied, but it seems reasonable to treat this as a nitrate overdose, with elevation of the extremities and with central volume expansion.


The benefits of Isosorbide Mononitrate in patients with acute myocardial infarction or congestive heart failure have not been established. Because the effects of Isosorbide Mononitrate are difficult to terminate rapidly, this drug is not recommended in these settings.


If Isosorbide Mononitrate is used in these conditions, careful clinical or hemodynamic monitoring must be used to avoid the hazards of hypotension and tachycardia.



Precautions



General


Severe hypotension, particularly with upright posture, may occur with even small doses of Isosorbide Mononitrate. This drug should therefore be used with caution in patients who may be volume depleted or who, for whatever reason, are already hypotensive. Hypotension induced by Isosorbide Mononitrate may be accompanied by paradoxical bradycardia and increased angina pectoris.


Nitrate therapy may aggravate the angina caused by hypertrophic cardiomyopathy. In industrial workers who have had long-term exposure to unknown (presumably high) doses of organic nitrates, tolerance clearly occurs. Chest pain, acute myocardial infarction, and even sudden death have occurred during temporary withdrawal of nitrates from these workers, demonstrating the existence of true physical dependence. The importance of these observations to the routine, clinical use of oral Isosorbide Mononitrate is not known.



Information for Patients


Patients should be told that the antianginal efficacy of Isosorbide Mononitrate Tablets can be maintained by carefully following the prescribed schedule of dosing (two doses taken seven hours apart). For most patients, this can be accomplished by taking the first dose on awakening and the second dose 7 hours later.


As with other nitrates, daily headaches sometimes accompany treatment with Isosorbide Mononitrate. In patients who get these headaches, the headaches are a marker of the activity of the drug. Patients should resist the temptation to avoid headaches by altering the schedule of their treatment with Isosorbide Mononitrate, since loss of headache may be associated with simultaneous loss of antianginal efficacy. Aspirin and/or acetaminophen, on the other hand, often successfully relieve Isosorbide Mononitrate-induced headaches with no deleterious effect on Isosorbide Mononitrate's antianginal efficacy.


Treatment with Isosorbide Mononitrate may be associated with light-headedness on standing, especially just after rising from a recumbent or seated position. This effect may be more frequent in patients who have also consumed alcohol.



Drug Interactions


The vasodilating effects of Isosorbide Mononitrate may be additive with those of other vasodilators. Alcohol, in particular, has been found to exhibit additive effects of this variety.


Marked symptomatic orthostatic hypotension has been reported when calcium channel blockers and organic nitrates were used in combination. Dose adjustments of either class of agents may be necessary.



Carcinogenesis, Mutagenesis, Impairment of Fertility


No evidence of carcinogenicity was observed in rats exposed to Isosorbide Mononitrate in their diets at doses of up to 900 mg/kg/day for the first six months and 500 mg/kg/day for the remaining duration of a study in which males were dosed for up to 121 weeks and females were dosed for up to 137 weeks. No evidence of mutagenicity was seen in vitro in the Salmonella test (Ames test), in human peripheral lymphocytes, in Chinese hamster cells (V79) or, in vivo in the rat micronucleus test. In a study on the fertility and breeding capacity of two generations of rats, Isosorbide Mononitrate had no adverse effects on fertility or general reproductive performance with oral doses up to 120 mg/kg/day. A dose of 360 mg/kg/day was associated with increased mortality in treated males and females and a reduced fertility index. (See table at end of Pregnancy section for animal-to-human dosage comparisons.)



Pregnancy


Teratogenic Effects

Pregnancy Category B


Reproduction studies performed in rats and rabbits at doses of up to 540 and 810 mg/kg/day, respectively, have revealed no evidence of harm to the fetus due to Isosorbide Mononitrate. There are, however, no adequate and well-controlled studies in pregnant women. Because animal reproduction studies are not always predictive of human response, Isosorbide Mononitrate should be used during pregnancy only if clearly needed.


Nonteratogenic Effects

Birth weights, neonatal survival and development, and incidence of stillbirths were adversely affected when pregnant rats were administered oral doses of 540 (but not 270) mg Isosorbide Mononitrate/kg/day during late gestation and lactation. This dose was associated with decreased maternal body weight gain and decreased maternal motor activity.


















SpeciesDaily Dose

(mg/kg)		Multiple of MRHD*

Based on:
Body WeightBody Surface
Calculations assume a human weight of 50 kg and human body surface area of 1.46 m2, a rabbit weight of 2 kg and rabbit body surface area of 0.163 m2, and a rat weight of 150 g and rat body surface area of 0.025 m2.

*

Maximum recommended human dose (MRHD) is 20 mg bid.

Rabbit8101013375
Rat900

540

500

360

270		1125

675

625

450

338		195

117

108

78

59

Nursing Mothers


It is not known whether Isosorbide Mononitrate is excreted in human milk. Because many drugs are excreted in human milk, caution should be exercised when Isosorbide Mononitrate is administered to a nursing woman.



Pediatric Use


Safety and effectiveness of Isosorbide Mononitrate in pediatric patients have not been established.



Geriatric Use


Clinical studies of Isosorbide Mononitrate did not include sufficient numbers of subjects aged 65 and over to determine whether they respond differently from younger subjects. Other reported clinical experience has not identified differences in responses between the elderly and younger patients. In general, dose selection for an elderly patient should be cautious, usually starting at the low end of the dosing range, reflecting the greater frequency of decreased hepatic, renal, or cardiac function, and of concomitant disease or other drug therapy.



Adverse Reactions


Headache is the most frequent side effect and was the cause of 2% of all dropouts from controlled-clinical trials. Headache decreased in incidence after the first few days of therapy.


The following table shows the frequency of adverse reactions observed in 1% or more of subjects in 6 placebo-controlled trials, conducted in the United States and abroad. The same table shows the frequency of withdrawal for these adverse reactions. In many cases the adverse reactions were of uncertain relation to drug treatment.
































































































Frequency of Adverse Reactions (Discontinuations)*
6 Placebo-Controlled Studies
DosePlacebo5 mg10 mg20 mg
Patients1605452159

*

Some individuals discontinued for multiple reasons.

Headache6% (0%)17% (0%)13% (0%)35% (5%)
Fatigue2% (0%)0% (0%)4% (0%)1% (0%)
Upper Respiratory Infection<1% (0%)0% (0%)4% (0%)1% (0%)
Pain<1% (0%)4% (0%)0% (0%)<1% (0%)
Dizziness1% (0%)0% (0%)0% (0%)4% (0%)
Nausea<1% (0%)0% (0%)0% (0%)3% (2%)
Increased Cough<1% (0%)0% (0%)2% (0%)<1% (0%)
Rash0% (0%)2% (2%)0% (0%)<1% (0%)
Abdominal Pain<1% (0%)0% (0%)2% (0%)0% (0%)
Allergic Reaction0% (0%)0% (0%)2% (0%)0% (0%)
Cardiovascular Disorder0% (0%)2% (0%)0% (0%)0% (0%)
Chest Pain<1% (0%)0% (0%)2% (0%)<1% (0%)
Diarrhea0% (0%)0% (0%)2% (0%)0% (0%)
Flushing0% (0%)0% (0%)2% (0%)0% (0%)
Emotional Lability0% (0%)2% (0%)0% (0%)0% (0%)
Pruritus1% (0%)2% (2%)0% (0%)0% (0%)

Other adverse reactions, each reported by fewer than 1% of exposed patients, and in many cases of uncertain relation to drug treatment, were:




























Cardiovascular:acute myocardial infarction, apoplexy, arrhythmias, bradycardia, edema, hypertension, hypotension, pallor, palpitations, tachycardia.
 
Dermatologic:sweating.
 
Gastrointestinal:anorexia, dry mouth, dyspepsia, thirst, vomiting, decreased weight.
 
Geritourinary:prostatic disorder.
 
Miscellaneous:amblyopia, back pain, bitter taste, muscle cramps, neck pain, paresthesia, susurrus aurium.
 
Neurologic:anxiety, impaired concentration, depression, insomnia, nervousness, nightmares, restlessness, tremor, vertigo.
 
Respiratory:asthma, dyspnea, sinusitis.

Extremely rarely, ordinary doses of organic nitrates have caused methemoglobinemia in normal-seeming patients; for further discussion of its diagnosis and treatment see under Overdosage.



Overdosage



Hemodynamic Effects


The ill effects of Isosorbide Mononitrate overdose are generally the results of Isosorbide Mononitrate's capacity to induce vasodilatation, venous pooling, reduced cardiac output, and hypotension. These hemodynamic changes may have protean manifestations, including increased intracranial pressure, with any or all of persistent throbbing headache, confusion, and moderate fever; vertigo; palpitations; visual disturbances; nausea and vomiting (possibly with colic and even bloody diarrhea); syncope (especially in the upright posture); air hunger and dyspnea, later followed by reduced ventilatory effort; diaphoresis, with the skin either flushed or cold and clammy; heart block and bradycardia; paralysis; coma; seizures and death.


Laboratory determinations of serum levels of Isosorbide Mononitrate and its metabolites are not widely available, and such determinations have, in any event, no established role in the management of Isosorbide Mononitrate overdose.


There are no data suggesting what dose of Isosorbide Mononitrate is likely to be life-threatening in humans. In rats and mice, there is significant lethality at oral doses of 1965 mg/kg and 2581 mg/kg, respectively.


No data are available to suggest physiological maneuvers (e.g., maneuvers to change the pH of the urine) that might accelerate elimination of Isosorbide Mononitrate. Isosorbide Mononitrate is significantly removed from the blood during hemodialysis.


No specific antagonist to the vasodilator effects of Isosorbide Mononitrate is known, and no intervention has been subject to controlled study as a therapy of Isosorbide Mononitrate overdose. Because the hypotension associated with Isosorbide Mononitrate overdose is the result of venodilatation and arterial hypovolemia, prudent therapy in this situation should be directed toward an increase in central fluid volume. Passive elevation of the patient's legs may be sufficient, but intravenous infusion of normal saline of similar fluid may also be necessary.


The use of epinephrine or other arterial vasoconstrictors in this setting is likely to do more harm than good.


In patients with renal disease or congestive heart failure, therapy resulting in central volume expansion is not without hazard. Treatment of Isosorbide Mononitrate overdose in these patients may be subtle and difficult, and invasive monitoring may be required.



Methemoglobinemia


Methemoglobinemia has been reported in patients receiving other organic nitrates, and it probably could also occur as a side effect of Isosorbide Mononitrate. Certainly nitrate ions liberated during metabolism of Isosorbide Mononitrate can oxidize hemoglobin into methemoglobin. Even in patients totally without cytochrome b5 reductase activity, however, and even assuming that the nitrate moiety of Isosorbide Mononitrate is quantitatively applied to oxidation of hemoglobin, about 2 mg/kg of Isosorbide Mononitrate should be required before any of these patients manifests clinically significant (≥10%) methemoglobinemia. In patients with normal reductase function, significant production of methemoglobin should require even larger doses of Isosorbide Mononitrate. In one study in which 36 patients received 2-4 weeks of continuous nitroglycerin therapy at 3.1 to 4.4 mg/hr (equivalent, in total administered dose of nitrate ions, to 7.8 – 11.1 mg of Isosorbide Mononitrate per hour), the average methemoglobin level measured was 0.2%; this was comparable to that observed in parallel patients who received placebo.


Notwithstanding these observations, there are case reports of significant methemoglobinemia in association with moderate overdoses of organic nitrates. None of the affected patients had been thought to be unusually susceptible.


Methemoglobin levels are available from most clinical laboratories. The diagnosis should be suspected in patients who exhibit signs of impaired oxygen delivery despite adequate cardiac output and adequate arterial p02. Classically, methemoglobinemic blood is described as chocolate brown, without color change on exposure to air.


When methemoglobinemia is diagnosed, the treatment of choice is methylene blue, 1-2 mg/kg intravenously.



Isosorbide Mononitrate Dosage and Administration


The recommended regimen of Isosorbide Mononitrate Tablets is 20 mg twice daily, with the doses seven hours apart. A starting dose of 5 mg (½ tablet of the 10 mg dosing strength) might be appropriate for persons of particularly small stature but should be increased to at least 10 mg by the second or third day of therapy. Dosage adjustments are not necessary for elderly patients or patients with altered hepatic or renal function.


As noted above (Clinical Pharmacology), multiple studies of organic nitrates have shown that maintenance of continuous 24-hour plasma levels results in refractory tolerance. The asymmetric (2 doses, 7 hours apart) dosing regimen for Isosorbide Mononitrate Tablets provides a daily nitrate-free interval to minimize the development of tolerance.


As also noted under Clinical Pharmacology, well-controlled studies have shown that tolerance to Isosorbide Mononitrate Tablets occurs to some extent when using the twice-daily regimen in which the two doses are given seven hours apart. This regimen has been shown to have antianginal efficacy beginning one hour after the first dose and lasting at least seven hours after the second dose. The duration (if any) of antianginal activity beyond fourteen hours has not been studied.


In clinical trials, Isosorbide Mononitrate has been administered in a variety of regimens and doses. Doses above 20 mg twice a day (with the doses seven hours apart) have not been adequately studied. Doses of 5 mg twice a day are clearly effective (effectiveness based on exercise tolerance) for only the first day of a twice-a-day (with doses 7 hours apart) regimen.



How is Isosorbide Mononitrate Supplied


Isosorbide Mononitrate 10 mg Tablets, USP are white, round, scored and engraved "10" on one side and engraved "KU 106" on the other. They are supplied as follows:


     Bottles of 100        NDC 62175-106-01


Isosorbide Mononitrate 20 mg Tablets, USP are white, round, scored and engraved "20" on one side and engraved "KU 107" on the other. They are supplied as follows:


     Bottles of 100        NDC 62175-107-01



Store at 20° - 30°C (68° - 86°F) [See USP]. Keep tightly closed.



Distributed by:

Kremers Urban Pharmaceuticals Inc.

Princeton, NJ 08540, USA


Printed in U.S.A.


Rev. 3E 06/2011



PRINCIPAL DISPLAY PANEL - 10 mg Tablet Bottle Label


100 Tablets

NDC 62175-106-01


Isosorbide

Mononitrate

Tablets, USP


10 mg


Rx Only




PRINCIPAL DISPLAY PANEL - 20 mg Tablet Bottle Label


100 Tablets

NDC 62175-107-01


Isosorbide

Mononitrate

Tablets, USP


20 mg


Rx Only










Isosorbide Mononitrate 
Isosorbide Mononitrate  tablet










Product Information
Product TypeHUMAN PRESCRIPTION DRUGNDC Product Code (Source)62175-106
Route of AdministrationORALDEA Schedule    








Active Ingredient/Active Moiety
Ingredient NameBasis of StrengthStrength
Isosorbide Mononitrate (isosorbide)Isosorbide Mononitrate10 mg














Inactive Ingredients
Ingredient NameStrength
lactose 
talc 
silicon dioxide 
cellulose, microcrystalline 
aluminum stearate 


















Product Characteristics
ColorWHITEScore2 pieces
ShapeROUNDSize7mm
FlavorImprint Code10;KU;106
Contains      










Packaging
#NDCPackage DescriptionMultilevel Packaging
162175-106-01100 TABLET In 1 BOTTLENone










Marketing Information
Marketing CategoryApplication Number or Monograph CitationMarketing Start DateMarketing End Date
NDA AUTHORIZED GENERICNDA02021506/30/1993







Isosorbide Mononitrate 
Isosorbide Mononitrate  tablet










Product Information
Product TypeHUMAN PRESCRIPTION DRUGNDC Product Code (Source)62175-107
Route of AdministrationORALDEA Schedule    








Active Ingredient/Active Moiety
Ingredient NameBasis of StrengthStrength
Isosorbide Mononitrate (isosorbide)Isosorbide Mononitrate20 mg














Inactive Ingredients
Ingredient NameStrength
lactose 
talc 
silicon dioxide 
cellulose, microcrystalline 
aluminum stearate 


















Product Characteristics
ColorWHITEScore2 pieces
ShapeROUNDSize9mm
FlavorImprint Code20;KU;107
Contains      










Packaging
#NDCPackage DescriptionMultilevel Packaging
162175-107-01100 TABLET In 1 BOTTLENone










Marketing Information
Marketing CategoryApplication Number or Monograph CitationMarketing Start DateMarketing End Date
NDA AUTHORIZED GENERICNDA02021506/30/1993


Labeler - Kremers Urban Pharmaceuticals Inc. (006422406)
Revised: 01/2012Kremers Urban Pharmaceuticals Inc.
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