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Rivastigmine

 
Drug Info: Rivastigmine
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Brand names: Exelon®

Chemical formula:



Rivastigmine capsules

What are rivastigmine capsules?

RIVASTIGMINE (Exelon®) helps treat the symptoms associated with Alzheimer's disease or dementia. It is not a cure for Alzheimer's disease but offers improvement in memory, attention, reason, language, and the ability to perform simple tasks. Benefits are greater in the early stages of the disease. Generic rivastigmine capsules are not yet available.

What should I tell my health care provider before I take this medicine?

They need to know if you have any of these conditions:
• asthma or other lung disease
• difficulty passing urine
• head injury
• heart disease, or irregular or slow heartbeat
• kidney disease
• liver disease
• low blood pressure
• Parkinson's disease
• seizures (convulsions)
• stomach or intestinal disease, ulcers, or stomach bleeding
• tobacco smoker
• an unusual or allergic reaction to rivastigmine, other medicines, foods, dyes, or preservatives
• pregnant or trying to get pregnant
• breast-feeding

How should I take this medicine?

Take rivastigmine capsules by mouth. Follow the directions on the prescription label. Swallow the capsules with a drink of water. Rivastigmine is usually administered twice daily with food, and is recommended to be taken with the morning and evening meals. Take your doses at regular intervals. Do not take your medicine more often than directed. Do not stop taking except on your prescriber's advice.

If your prescriber asks you to stop taking rivastigmine; do not restart this medicine until your prescriber tells you to. Follow the special instructions given by your prescriber for restarting this medicine.

Contact your pediatrician or health care professional regarding the use of this medicine in children. Special care may be needed.

What drug(s) may interact with rivastigmine?

atropine
benztropine
dicyclomine
digoxin
donepezil
galantamine
glycopyrrolate
hyoscyamine
• medications for motion sickness (examples: dimenhydrinate, scopolamine)
• medicines that relax your muscles for surgery
• non-steroidal antiinflammatory drugs (NSAIDs, such as ibuprofen)
oxybutynin
propantheline
tacrine

Tell your prescriber or health care professional about all other medicines you are taking, including non-prescription medicines, nutritional supplements, or herbal products. Also tell your prescriber or health care professional if you are a frequent user of drinks with caffeine or alcohol, if you smoke, or if you use illegal drugs. These may affect the way your medicine works. Check with your health care professional before stopping or starting any of your medicines.

What should I watch for while taking rivastigmine?

Visit your prescriber or health care professional for regular checks on your progress. Check with your prescriber or health care professional if there is no improvement in your symptoms or if they get worse.

You may get dizzy or feel faint. Do not drive, use machinery, or do anything that needs mental alertness until you know how rivastigmine affects you.

If you are going to have surgery tell your prescriber or health care professional that you are taking rivastigmine.

What side effects may I notice from taking rivastigmine?

Side effects that you should report to your prescriber or health care professional as soon as possible:
• changes in vision or balance
• diarrhea, if it is severe or does not stop
• dizziness, fainting spells, or falls
• increase in frequency of passing urine, or incontinence
• nervousness, agitation, or increased confusion
• redness, blistering, peeling or loosening of the skin, including inside the mouth
• skin rash or hives
• slow heartbeat, or palpitations
• stomach pain
• sweating
• uncontrollable movements
• vomiting
• weight loss

Side effects that usually do not require medical attention (report to your prescriber or health care professional if they continue or are bothersome):
• mild diarrhea, especially when starting treatment
• indigestion or heartburn
• loss of appetite
• nausea

Where can I keep my medicine?

Keep out of reach of children in a container that small children cannot open.

Store at room temperature between 15 degrees and 30 degrees C (59 degrees and 86 degrees F). Throw away any unused medicine after the expiration date.

Last updated: 7/1/2002

Important Disclaimer: The drug information provided here is for educational purposes only. It is intended to supplement, not substitute for, the diagnosis, treatment and advice of a medical professional. This drug information does not cover all possible uses, precautions, side effects and interactions. It should not be construed to indicate that this or any drug is safe for you. Consult your medical professional for guidance before using any prescription or over the counter drugs.

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Wikipedia: Rivastigmine
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Home > Library > Miscellaneous > Wikipedia
Rivastigmine
Systematic (IUPAC) name
(S)-N-Ethyl- N-methyl- 3-[1-(dimethylamino)ethyl]- phenyl carbamate
Identifiers
CAS number 123441-03-2
ATC code N06DA03
PubChem 77991
DrugBank APRD00321
Chemical data
Formula C14H22N2O2 
Mol. mass 250.337 g/mol
Pharmacokinetic data
Bioavailability 96%
Protein binding 40%
Metabolism Hepatic, via pseudocholinesterase
Half life 1.5 hours
Excretion Renal, 97%
Therapeutic considerations
Pregnancy cat.

B(US)
Legal status

-only(US)
Routes Oral, Transdermal
 Yes check.svgY(what is this?)  (verify)

Rivastigmine (sold under the trade name Exelon) is a parasympathomimetic or cholinergic agent for the treatment of mild to moderate dementia of the Alzheimer’s type and dementia due to Parkinson's disease. The drug can be administered orally or via a transdermal patch; the latter form reduces the prevalence of side effects,[1] which typicaly include nausea and vomiting.[2] The drug is eliminated through the urine, and appears to have relatively few drug-drug interactions.[2]

Contents

History

Rivastigmine was developed by Novartis, and has been available in capsule and liquid formulations since 1997.[3] In 2006, it became the first product approved globally for the treatment of mild to moderate dementia associated with Parkinson's Disease;[4] and in 2007 the rivastigmine transdermal patch became the first patch treatment for dementia.

Administration

Rivastigmine tartrate is a white to off-white fine crystalline powder that is both lipophilic (soluble in fats) and hydrophilic (soluble in water). Like other cholinesterase inhibitors, it requires doses to be increased gradually over several weeks; this is usually referred to as the titration phase.[2] Oral doses of rivastigmine should be titrated with a 3 mg per day increment every 2 to 4 weeks.

Rivastigmine is classified as Pregnancy category B, with insufficient data on risks associated with breastfeeding. In cases of overdose, atropine is used to reverse bradycardia. Dialysis is ineffective due to the drug's half-life.

Pharmacodynamics

Rivastigmine is a cholinesterase inhibitor that inhibits both butyrylcholinesterase and acetylcholinesterase (unlike donepezil, which selectively inhibits acetylcholinesterase). It is thought that rivastigmine works by inhibiting these cholinesterase enzymes, which would otherwise break down the brain chemical acetylcholine.[5]

Indication

The U.S. Food and Drug Administration has approved rivastigmine capsules and the rivastigmine patch for the treatment of mild to moderate dementia of the Alzheimer’s type and for mild to moderate dementia related to Parkinson's disease. It has been used in more than 6 million patients world-wide.[citation needed]

Rivastigmine has demonstrated significant treatment effects on the cognitive (thinking and memory), functional (activities of daily living) and behavioural problems that are commonly associated with Alzheimer’s[6][7][8][9] and Parkinson's disease dementias.[10]

Efficacy

In patients with either type of dementia, rivastigmine has been shown to provide meaningful symptomatic effects that may allow patients to remain independent and ‘be themselves’ for longer. In particular, rivastigmine appears to show marked treatment effects in patients showing a more aggressive course of disease, such as those with a younger age of onset, a poor nutritional status, or those experiencing symptoms such as delusions or hallucinations.[11] For example, the presence of hallucinations appears to be a predictor of especially strong responses to rivastigmine, both in Alzheimer’s and Parkinson's disease patients.[12][13] It has been proposed that these effects might reflect the additional inhibition of butyrylcholinesterase, which is implicated in symptom progression and might provide added benefits over acetylcholinesterase-selective drugs in some patients.[14][15] Multi-infarct dementia—may be slight improvement in executive functions and behaviour. There are no firm evidences supporting usage in schizophrenia patients.

Its efficacy is similar to donepezil and tacrine. Doses below 6 mg/d may be ineffective. The effects of this kind of drugs in different kinds of dementia (including Alzheimer's dementia) are modest, and it is still unclear which AcCh(ButCh) esterase inhibitor is better in Parkinson's dementia, though rivastigmine is well-studied.

Side effects

Side effects may include nausea and vomiting.[2]

It has been postulated that the strong potency of rivastigmine, provided by its dual inhibitory mechanism, leads to more nausea and vomiting during the titration phase of oral rivastigmine treatment.[2] This enforces the importance of taking oral forms of these drugs as prescribed with food.[3] However, rates of nausea and vomiting are markedly reduced with the once-daily rivastigmine patch (which can be applied at any time of the day, with or without food).

In a large clinical trial of the rivastigmine patch in 1,195 patients with Alzheimer’s disease, the target dose of 9.5 mg/24 hour patch provided similar clinical effects (e.g. memory and thinking, activities of daily living, concentration) as the highest doses of rivastigmine capsules, but with three times fewer reports of nausea and vomiting. [1].

Pharmacokinetics

When given orally, rivastigmine is well absorbed with a bioavailability of about 40% in the 3 mg dose. Pharmacokinetics are linear up to 3 mg BID but non-linear at higher doses. Elimination is through the urine. Peak plasma concentrations are seen in about one hour, with peak CSF concentrations at 1.4–3.8 hours. When given by once-daily transdermal patch, the pharmacokinetic profile of rivastigmine is much smoother, compared with capsules, with lower peak plasma concentrations and reduced fluctuations.[16] The 9.5 mg/24 h rivastigmine patch provides comparable exposure to 12 mg/day capsules (the highest recommended oral dose).[16]

The compound does cross the blood-brain barrier. Plasma protein binding is 40%.[17] The major route of metabolism for rivastigmine is by its target enzymes via cholinesterase-mediated hydrolysis. Elimination bypasses the hepatic system so hepatic cytochrome P450 (CYP) isoenzymes are not involved.[18] It has been suggested that this means there is a low potential for drug-drug interactions (which could lead to adverse effects) between rivastigmine and the many common drugs that use the cytochrome P450 metabolic pathway.[2]

See also

Notes

  1. ^ a b Winblad B, Grossberg G, Frolich L, Farlow M, Zechner S, Nagel J, Lane R. “IDEAL: a 6-month, double-blind, placebo-controlled study of the first skin patch for Alzheimer disease”. Neurology 2007 Jul 24;69(4 Suppl 1):S14–22. PMID 17646619
  2. ^ a b c d e f Inglis F. “The tolerability and safety of cholinesterase inhibitors in the treatment of dementia”. Int J Clin Pract. 2002;(127):45–63. PMID 12139367
  3. ^ a b Novartis Pharmaceuticals Corporation “Exelon Product Insert” June 2006. [1]
  4. ^ “FDA Approves the First Treatment for Dementia of Parkinson’s Disease” U.S. FDA News Release [2]
  5. ^ Camps P. Munoz-Torrero D. “Cholinergic drugs in pharmacotherapy of Alzheimer's disease”. Mini Rev Med Chem. 2002 Feb;2(1):11–25. PMID 12369954
  6. ^ Corey-Bloom J, Anand R, Veach J. “A randomized trial evaluating the efficacy and safety of ENA 713 (rivastigmine tartrate), a new acetylcholinesterase inhibitor, in patients with mild to moderately severe Alzheimer’s disease”. Int J Geriatr Psychopharmacol. 1998;1:55–65.
  7. ^ Rösler M, Anand R, Cicin-Sain A, et al. “Efficacy and safety of rivastigmine in patients with Alzheimer’s disease: international randomised controlled trial”. Br Med J. 1999;318:633–640. PMID 10066203
  8. ^ Finkel SI. “Effects of rivastigmine on behavioral and psychological symptoms of dementia in Alzheimer's disease”. Clin Ther. 2004;26:980–990. PMID 15336465
  9. ^ Rosler M, Retz W, Retz-Junginger P, Dennler HJ. ”Effects of two-year treatment with the cholinesterase inhibitor rivastigmine on behavioural symptoms in Alzheimer's disease”. Behav Neurol. 1998;11(4):211–216. PMID 11568422
  10. ^ Emre M, Aarsland D, Albanese A, et al. “Rivastigmine for dementia associated with Parkinson’s disease”. N Engl J Med. 2004;351:2509–2518. PMID 15590953
  11. ^ Gauthier S, Vellas B, Farlow M, Burn D. “An aggressive course of disease in dementia”. Alzheimer's & Dementia 2006;2:210–17.
  12. ^ Touchon J, Bergman H, Bullock R, Rapatz G, Nagel J, Lane R. Response to rivastigmine or donepezil in patients with Alzheimer’s disease and symptoms suggestive of concomitant Lewy body pathology. Curr Med Res Opin 2006;22:49–59. PMID 16393430
  13. ^ Burn D, Emre M, McKeith I, et al. “Effects of rivastigmine in patients with and without visual hallucinations in dementia associated with Parkinson's disease”. Mov Disord. 2006;21:1899–1907. PMID 16960863
  14. ^ Gauthier S, Vellas B, Farlow M, Burn D. “An aggressive course of disease in dementia”. Alzheimer's & Dementia 2006;2:210–17.
  15. ^ Touchon J, Bergman H, Bullock R, Rapatz G, Nagel J, Lane R. Response to rivastigmine or donepezil in patients with Alzheimer’s disease and symptoms suggestive of concomitant Lewy body pathology. Curr Med Res Opin 2006;22:49–59. PMID 16393430
  16. ^ a b Cummings J, Lefevre G, Small G, Appel-Dingemanse S. “Pharmacokinetic rationale for the rivastigmine patch”. Neurology. 2007 Jul 24;69(4 Suppl 1):S10–3. PMID 17646618
  17. ^ Jann MW, Shirley KL, Small GW. “Clinical pharmacokinetics and pharmacodynamics of cholinesterase inhibitors”. Clin Pharmacokinet. 2002;41(10):719–739. PMID 12162759
  18. ^ Jann MW. “Rivastigmine, a new-generation cholinesterase inhibitor for the treatment of Alzheimer's disease”. Pharmacotherapy. 2000 20(1):1–12. PMID 10641971.
v  d  e
Parasympathomimetics / cholinergic agonists / acetylcholinesterase inhibitors (N06DA, N07AA)
Direct
(at receptor)
Indirect/AIs
(in synapse)

very short acting: Edrophonium

carbamates/stigmine: Ambenonium · Rivastigmine · Distigmine · tertiary/CNS (Physostigmine) · quaternary/peripheral (Neostigmine, Pyridostigmine)

anti-dementia (Galantamine, Donepezil, Tacrine, Ladostigil)
v  d  e
Antidementia Agents (N06D)
Anticholinesterases
Others

This entry is from Wikipedia, the leading user-contributed encyclopedia. It may not have been reviewed by professional editors (see full disclaimer)

 
 
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Rivastigmine capsules
Rivastigmine skin patches
Rivastigmine Tartrate Oral capsule

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