Selegiline (oral): Difference between revisions
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| image2 = Selegiline-3D-balls.png | | image2 = Selegiline-3D-balls.png | ||
| CAS_number = 14611-51-9 | | CAS_number = 14611-51-9 | ||
| CAS_supplemental = [ | | CAS_supplemental = [14611-52-0] <small>(HCl)</small>, [2079-54-1] <small>(deprenyl.HCl)</small>, [4530-70-5] <small>((+-)-isomer)</small>, [1205-70-5] <small>((+-)-isomer, HCl)</small>, [2323-36-6] <small>(cpd w/o isomeric designation; deprenyl)</small>, [4528-51-2] <small>((S)-isomer)</small>, [4528-52-3] <small>((S)-isomer, HCl)</small> | ||
| ATC_prefix = N04 | | ATC_prefix = N04 | ||
| ATC_suffix = BD01 | | ATC_suffix = BD01 | ||
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| metabolism = liver | | metabolism = liver | ||
| elimination_half-life = 2 hours | | elimination_half-life = 2 hours | ||
| pregnancy_category = C <small>([ | | pregnancy_category = C <small>([[US]])</small> | ||
| legal_status = prescription only (unscheduled) <small>([[US]])</small> | |||
| routes_of_administration = Oral, [[transdermal]]ly | |||
}} | |||
'''Selegiline''' (l-deprenyl, Eldepryl® or Anipryl® [[veterinary]]) is a [[medication|drug]] used for the treatment of early-stage [[Parkinson's disease]] and [[senile dementia]]. In normal clinical doses it is a selective irreversible [[MAOI#Mode of action|MAO-B inhibitor]], however in larger doses (>20 [[milligram|mg]] in a typical adult) it loses its specificity and also inhibits MAO-A. Dietary restrictions are common for MAOI treatments, however, since selegiline is selective for MAO-B, special dietary restrictions for lower doses have been found to be unnecessary.<ref> | |||
{{cite journal | {{cite journal | ||
| last = Amsterdam | | last = Amsterdam | ||
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| id = | | id = | ||
| accessdate = }} | | accessdate = }} | ||
</ref> The drug was researched by [ | </ref> The drug was researched by [[Joseph Knoll]]. Selegiline is most closely related to the [[phenylethylamines]]. The only difference between the two classes of drugs is the attachment of a [[propargyl]] group (three carbons with a triple bond between the second and third carbon) to the nitrogen. | ||
==Uses== | ==Uses== | ||
It is sometimes used [ | It is sometimes used [[off-label]] to treat [[narcolepsy]] and as a [[nootropic]], as well as for its published life-extending effects among several species of mammals. It is also reported to positively affect [[libido]], particularly in older [[male]]s. As of February 28, 2006, selegiline has also been approved by the [[Food and Drug Administration]] (FDA) to treat [[clinical depression|major depression]] using a transdermal patch ([[Emsam]] Patch).<ref>http://www.fda.gov/bbs/topics/NEWS/2006/NEW01326.html</ref> Selegiline is also used (at extremely high dosages relative to humans) in [[veterinary medicine]] to treat the symptoms of [[Cushing's disease]] and so-called "cognitive dysfunction" in [[dog]]s. As of June 26, 2006, a selegiline transdermal patch is being tested for its effectiveness in treating [[ADHD]]. | ||
Several clinical studies are currently underway to evaluate Selegiline's effectiveness in helping people stop smoking [[tobacco]] or [[cannabis (drug)|marijuana]].<ref>{{cite web | |||
| last = | | last = | ||
| first = | | first = | ||
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==Mechanism of Action== | ==Mechanism of Action== | ||
Selegiline is a selective inhibitor of MAO-B; MAO-B metabolizes dopamine.<ref>Katzung, Bertram G. Basic & Clinical Pharmacology. 9th Edition. 2004. page 453. Lange Medical Books - McGraw Hill Publishers.</ref> Selegiline exhibits little therapeutic benefit when used independently, but enhances and prolongs the anti-[ | Selegiline is a selective inhibitor of MAO-B; MAO-B metabolizes dopamine.<ref>Katzung, Bertram G. Basic & Clinical Pharmacology. 9th Edition. 2004. page 453. Lange Medical Books - McGraw Hill Publishers.</ref> Selegiline exhibits little therapeutic benefit when used independently, but enhances and prolongs the anti-[[Parkinson's disease|Parkinson]] effects of [[levodopa]].<ref>Katzung. Page 453</ref> | ||
===Metabolites=== | ===Metabolites=== | ||
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====L-methamphetamine==== | ====L-methamphetamine==== | ||
Selegiline is partly [ | Selegiline is partly [[Drug metabolism|metabolized]] to l-methamphetamine, a [[stereoisomer]] of [[methamphetamine]] ''[[in vivo]]''.<ref>{{cite journal |author=Engberg G, Elebring T, Nissbrandt H |title=Deprenyl (selegiline), a selective MAO-B inhibitor with active metabolites; effects on locomotor activity, dopaminergic neurotransmission and firing rate of nigral dopamine neurons |journal=J. Pharmacol. Exp. Ther. |volume=259 |issue=2 |pages=841-7 |year=1991 |pmid=1658311 |doi=}}</ref> This stereoisomer is not considered psychoactive and has little abuse potential. The stimulatory effect on locomotor activity and dopamine synthesis may be contributed to by the action of l-methamphetamine. | ||
Due to this metabolite selegiline can cause false positives for [ | Due to this metabolite selegiline can cause false positives for [[amphetamine]]/[[methamphetamine]] on drug tests. | ||
==Legal Issues== | ==Legal Issues== | ||
Possibly due to the structural similarity to illegal [ | Possibly due to the structural similarity to illegal [[stimulant]]s, selegiline has been classified as a [[controlled substance]] in [[Japan]] and thus can only be obtained with a [[Medical prescription|prescription]] or special government license. Selegiline is not a controlled substance in the US but a prescription is required to obtain it. | ||
==EMSAM== | ==EMSAM== | ||
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==External links== | ==External links== | ||
* [http:// | * [http://www.lef.org/prod_hp/abstracts/deprenylabs.html Collection of Research Abstracts on Deprenyl] | ||
* [http:// | * [http://www.imminst.org/forum/index.php?s=&act=ST&f=44&t=16293&st=0&#entry177446 An Interview with Dr. Joseph Knoll regarding longevity] | ||
* [http:// | * [http://lef.org/magazine/mag96/sept96_versy6.html Deprenyl Improves Learning And Memory] | ||
* [http:// | * [http://www.antiaging-magazine.com/news/news_1.html Deprenyl (Selegiline) Can Slow Parkinson's Disease Safely] According to the British Medical Journal | ||
* [http:// | * [http://www.fda.gov/bbs/topics/NEWS/2006/NEW01326.html FDA Approves Emsam (Selegiline) as First Drug Patch for Depression] | ||
{{Dopaminergic agents}} | {{Dopaminergic agents}} | ||
{{Antidepressants}} | {{Antidepressants}} | ||
[ | [[Category:Nootropics]] | ||
[ | [[Category:Monoamine oxidase inhibitors]] | ||
[ | [[Category:Antiparkinsonian agents]] | ||
[[Category:Phenethylamines]] | |||
[[de:Selegilin]] | |||
[[hu:Szelegilin]] | |||
[[sv:Selegilin]] | |||
{{WikiDoc Help Menu}} | |||
{{WikiDoc Sources}} | {{WikiDoc Sources}} | ||
Revision as of 13:05, 25 September 2011
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| File:Selegiline-2D-skeletal-alternative-view.png | |
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| Clinical data | |
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| Pregnancy category |
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| Routes of administration | Oral, transdermally |
| ATC code | |
| Legal status | |
| Legal status |
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| Pharmacokinetic data | |
| Bioavailability | 4.4% |
| Protein binding | > 99.5% |
| Metabolism | liver |
| Elimination half-life | 2 hours |
| Identifiers | |
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| CAS Number |
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| PubChem CID | |
| DrugBank | |
| E number | {{#property:P628}} |
| ECHA InfoCard | {{#property:P2566}}Lua error in Module:EditAtWikidata at line 36: attempt to index field 'wikibase' (a nil value). |
| Chemical and physical data | |
| Formula | C13H17N |
| Molar mass | 187.281 g/mol |
Selegiline (l-deprenyl, Eldepryl® or Anipryl® veterinary) is a drug used for the treatment of early-stage Parkinson's disease and senile dementia. In normal clinical doses it is a selective irreversible MAO-B inhibitor, however in larger doses (>20 mg in a typical adult) it loses its specificity and also inhibits MAO-A. Dietary restrictions are common for MAOI treatments, however, since selegiline is selective for MAO-B, special dietary restrictions for lower doses have been found to be unnecessary.[1] The drug was researched by Joseph Knoll. Selegiline is most closely related to the phenylethylamines. The only difference between the two classes of drugs is the attachment of a propargyl group (three carbons with a triple bond between the second and third carbon) to the nitrogen.
Uses
It is sometimes used off-label to treat narcolepsy and as a nootropic, as well as for its published life-extending effects among several species of mammals. It is also reported to positively affect libido, particularly in older males. As of February 28, 2006, selegiline has also been approved by the Food and Drug Administration (FDA) to treat major depression using a transdermal patch (Emsam Patch).[2] Selegiline is also used (at extremely high dosages relative to humans) in veterinary medicine to treat the symptoms of Cushing's disease and so-called "cognitive dysfunction" in dogs. As of June 26, 2006, a selegiline transdermal patch is being tested for its effectiveness in treating ADHD.
Several clinical studies are currently underway to evaluate Selegiline's effectiveness in helping people stop smoking tobacco or marijuana.[3][4]
Mechanism of Action
Selegiline is a selective inhibitor of MAO-B; MAO-B metabolizes dopamine.[5] Selegiline exhibits little therapeutic benefit when used independently, but enhances and prolongs the anti-Parkinson effects of levodopa.[6]
Metabolites
Desmethylselegiline
Desmethylselegiline may have neuroprotective antiapoptotic properties. A large multicenter study suggests a decrease of in the disease progression of parkinsonism but may have reflected other symptomatic response.[7]
L-methamphetamine
Selegiline is partly metabolized to l-methamphetamine, a stereoisomer of methamphetamine in vivo.[8] This stereoisomer is not considered psychoactive and has little abuse potential. The stimulatory effect on locomotor activity and dopamine synthesis may be contributed to by the action of l-methamphetamine.
Due to this metabolite selegiline can cause false positives for amphetamine/methamphetamine on drug tests.
Legal Issues
Possibly due to the structural similarity to illegal stimulants, selegiline has been classified as a controlled substance in Japan and thus can only be obtained with a prescription or special government license. Selegiline is not a controlled substance in the US but a prescription is required to obtain it.
EMSAM
February 28, 2006 - The Food and Drug Administration approved Emsam (selegiline), the first skin (transdermal) patch for use in treating major depression. The once a day patch works by delivering selegiline, a monoamine oxidase inhibitor or MAOI, through the skin and into the bloodstream. At its lowest strength, Emsam can be used without the dietary restrictions that are needed for all oral MAO inhibitors that are approved for treating major depression. It comes in three sizes that deliver 6, 9, or 12 mg of selegiline per 24 hours. The patch is a matrix containing three layers consisting of a backing, and adhesive drug layer, and a release liner that is placed against the skin. EMSAM was developed by Somerset Pharmaceuticals, Inc. In December 2004, Bristol-Myers Squibb and Somerset entered into an agreement that provides Bristol-Myers Squibb with distribution rights to market EMSAM after approval in the United States.
References
- ↑
Amsterdam, J. D. (2003-02). "A double-blind, placebo-controlled trial of the safety and efficacy of selegiline transdermal system without dietary restrictions in patients with major depressive disorder". Journal of Clinical Psychiatry. 64 (2): 208–214. Check date values in:
|date=(help) - ↑ http://www.fda.gov/bbs/topics/NEWS/2006/NEW01326.html
- ↑ "Effectiveness of Selegiline in Treating Marijuana Dependent Individuals". ClinicalTrials.gov. National Institute on Drug Abuse. March 2005. Retrieved 2007-2-16. Check date values in:
|accessdate=(help) - ↑ "Usefulness of Selegiline as an Aid to Quit Smoking". ClinicalTrials.gov. National Institute on Drug Abuse. July 2004. Retrieved 2007-2-16. Check date values in:
|accessdate=(help) - ↑ Katzung, Bertram G. Basic & Clinical Pharmacology. 9th Edition. 2004. page 453. Lange Medical Books - McGraw Hill Publishers.
- ↑ Katzung. Page 453
- ↑ Katzung, Bertram G. Basic & Clinical Pharmacology. 9th Edition. 2004. page 453. Lange Medical Books - McGraw Hill Publishers.
- ↑ Engberg G, Elebring T, Nissbrandt H (1991). "Deprenyl (selegiline), a selective MAO-B inhibitor with active metabolites; effects on locomotor activity, dopaminergic neurotransmission and firing rate of nigral dopamine neurons". J. Pharmacol. Exp. Ther. 259 (2): 841–7. PMID 1658311.
External links
- Collection of Research Abstracts on Deprenyl
- An Interview with Dr. Joseph Knoll regarding longevity
- Deprenyl Improves Learning And Memory
- Deprenyl (Selegiline) Can Slow Parkinson's Disease Safely According to the British Medical Journal
- FDA Approves Emsam (Selegiline) as First Drug Patch for Depression
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