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Selegiline - Drs. Foster and Smith Pet Prescription Medications
Animal prescription medications are available through Drs. Foster and Smith's Free-Shipping Pharmacy at prices lower than your vet for the exact same product. We'll call to get the prescription for you, and ship it out FREE. Drs. Foster and Smith Inc. is fully licensed in all 50 states. This medication can be ordered at www.drsfostersmith.com
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Drug Name Confusion: Salagen and Selegiline (Feb 2006)
The Institute for Safe Medication Practices recently described several cases where the brand name of one drug was mistaken for the generic name of another. Salagen, a brand name for pilocarpine, is used to treat the dry mouth symptoms caused by Sjogren's syndrome or radiation therapy. Selegiline is an MAO-inhibitor used to treat Parkinson's disease. Both drugs are available in 5 mg tablets. In the first case, the mix-up occurred because the names sounded alike. A home health nurse received a telephone order from a dentist for an elderly patient with problems related to a dry mouth. The dentist prescribed Salagen 5 mg, but the nurse misheard the order and called the pharmacy to request selegiline 5 mg. About 2 weeks later, another pharmacist was processing a prescription for a fentanyl patch for the same patient when the pharmacy computer system signaled an alert about a drug interaction between fentanyl and selegiline. When the pharmacist contacted the prescriber, he discovered the error. In the second case, a pharmacist reported that the similar spelling of the two drug names led him to enter "selegiline" into the computer instead of "Salagen". The error was recognized only after the patient complained that the medication was not helping his dry mouth, and this caused the pharmacist to check the patient's profile. In order to minimize these kinds of mix-ups, ISMP says to list both the brand and generic names on prescriptions. And patients who use these drugs regularly ...
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Protecting Your Brain: Nutrients, Herbs, Nootropics, & Mind-Body Practices, Dr. Richard Brown
Richard P. Brown, MD speaks at the "11th Clinical Applications for Age Management Medicine Conference" Nov. 2011, Las Vegas, Nevada The mechanisms and clinical uses of neuroprotective agents will be discussed. The first hour will cover 5 categories of neuroprotective agents: 1. Cholinergic - Huperzine, Galantamine, Centrophenoxine, Alcar, CDP-choline 2. Nutrients - S-adenosylmethionine (SAMe), Picamilon, Bio-strath, Fish oils 3. Herbs - Rhodiola rosea, Ginseng, Gingko, Sage, Saffron, Vinpocetine 4. Nootropics - Selegiline, Racetams 5. Mind-Body Practices - Biofeedback, Breathing, Movement, Meditation AMMG Conferences are the definitive events for bringing together physicians and healthcare professionals who practice Age Management Medicine as well as those new to the field. AMA PRA Category 1 CME Credits are offered at every conference. Faculty presenters are reviewed and selected by our Conference Planning Committee of prestigious medical expert industry leaders resulting in an ethical, educational and evidence-based academic agenda. Please visit www.agemed.org for the latest meeting details including conference schedule, academic agenda, faculty and e-journal archives for the latest industry news. Please visit our website www.agemed.org for the latest meeting details including conference schedule, academic agenda, faculty and e-journal archives for the latest industry news. Or contact us at conference@agemed.org
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Part 3: Deprenyl and Dopamine decline
Deprenyl: www.antiaging-systems.com otherwise known as Selegiline is primarily used to treat the symptoms of Parkinson's disease, because Deprenyl helps to improve brain levels of Dopamine, the neurotransmitter that is most affected by that disease. Whilst dosages in the treatment of Parkinson's disease can often be 20 mg. a day or higher, those utilizing deprenyl for an anti-aging program are more likely to use just a few milligrams daily.
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Antidepressants Compared
Clip thanks to www.medstores.net Selective serotonin reuptake inhibitors (SSRIs) are a class of antidepressants considered the current standard of drug treatment. A possible cause of depression is an inadequate amount of serotonin, a chemical used in the brain to transmit signals between neurons. SSRIs are said to work by preventing the reuptake of serotonin (also known as 5-hydroxytryptamine, or 5-HT) by the presynaptic neuron, thus maintaining higher levels of 5-HT in the synapse. Serotonin-norepinephrine reuptake inhibitors (SNRIs) are a newer form of antidepressant that work on both norepinephrine and 5-HT. They typically have similar side effects to the SSRIs, though there may be a withdrawal syndrome on discontinuation that may necessitate dosage tapering. Monoamine oxidase inhibitors (MAOIs) may be used if other antidepressant medications are ineffective. MAOIs work by blocking the enzyme monoamine oxidase which breaks down the neurotransmitters dopamine, serotonin, and norepinephrine (noradrenaline). Because there are potentially fatal interactions between this class of medication and certain foods (particularly those containing tyramine), as well as certain drugs, classic MAOIs are rarely prescribed anymore. However, this does not apply to Emsam, the transdermal patch form of selegiline, which due to its bypassing of the stomach has a lesser propensity to induce such events.[32] MAOIs can be as effective as tricyclic antidepressants, although they are generally ...
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New Warnings on Suicidality in Young Adults Taking Antidepressants
FDA has proposed that the makers of all antidepressant drugs warn in the product labeling that patients 18 to 24 years old who are on these drugs may be at increased risk for suicidal thinking and suicide attempts. The new warning would be added to the black box section of the label, which already warns about this risk in children and adolescents. The proposed labeling change would also state that the increased risk has not been observed in patients older than 24, and that patients over 65 taking antidepressants actually have a decreased risk of suicidality. The warning also emphasizes that psychiatric disorders themselves are the most important causes of suicide. Affected Products: • Anafranil (clomipramine) • Asendin (amoxapine) • Aventyl (nortriptyline) • Celexa (citalopram hydrobromide) • Cymbalta (duloxetine) • Desyrel (trazodone HCl) • Elavil (amitriptyline) • Effexor (venlafaxine HCl) • Emsam (selegiline) • Etrafon (perphenazine/amitriptyline) • Fluvoxamine maleate • Lexapro (escitalopram oxalate) • Limbitrol (chlordiazepoxide/amitriptyline) • Ludiomil (maprotiline) • Marplan (isocarboxazid) • Nardil (phenelzine sulfate) • Nefazodone HCl • Norpramin (desipramine HCl) • Pamelor (nortriptyline) • Parnate (tranylcypromine sulfate) • Paxil (paroxetine HCl) • Pexeva (paroxetine mesylate) • Prozac (fluoxetine HCl) • Remeron (mirtazapine) • Sarafem (fluoxetine HCl) • Seroquel (quetiapine) • Sinequan (doxepin) • Surmontil (trimipramine) • Symbyax (olanzapine/fluoxetine ...
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Remember 11 Age of Infinity -41- MAOI Hardcore anti-depressants
Monoamine oxidase inhibitors (MAOIs) are a class of antidepressant drugs prescribed for the treatment of depression. They are particularly effective in treating atypical depression. Because of potentially lethal dietary and drug interactions, monoamine oxidase inhibitors have historically been reserved as a last line of treatment, used only when other classes of antidepressant drugs (for example selective serotonin reuptake inhibitors and tricyclic antidepressants) have failed.[1] However, a transdermal patch form of the MAOI selegiline, called Emsam, was approved for use by the Food and Drug Administration in the United States on February 28, 2006.[2] When applied transdermally, the drug does not enter the gastrointestinal system, thereby decreasing the dangers of dietary interactions associated with oral administration of MAOIs.
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Optimizing the Management of Parkinson's Disease
This CME/CPE activity is jointly sponsored by the University of Florida College of Medicine and PVI, PeerView Institute for Medical Education; the activity is also co-provided by Amedco. In this two-part activity, an expert panel discusses the clinical challenges associated with the management of Parkinson's disease. Topics addressed in this activity include the management of motor symptoms in patients with early Parkinson's disease and potential strategies to minimize motor complications in the advanced disease setting. Recent data on available and emerging therapies for patients with Parkinson's disease are also discussed. www.peerviewpress.com
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Introduction to Current James Kimball Accountings
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Modafinil(nuvigil) decreases extreme sleepiness due to narcolepsy and other sleep disorders such as difficult/irregular breathing during sleep (eg, obstructive sleep apnea/hypopnea syndrome-OSAHS). It is also used to help you stay awake during work hours for people with work schedules that interfere with a normal sleep routine (shift work sleep disorder-SWSD). It is not known how modafinil works to increase wakefulness. It is thought to work by affecting certain chemicals in the brain that control the sleep/wake cycle. Modafinil does not make up for lack of sleep and should not be used to treat tiredness or hold off sleep in people who do not have a sleep disorder. Nuvigil Interactions Your healthcare professionals (eg, doctor or pharmacist) may already be aware of any possible drug interactions and may be monitoring you for it. Do not start, stop or change the dosage of any medicine before checking with them first. Before using this medication, tell your doctor or pharmacist of all prescription and nonprescription/herbal products you may use, especially of: medications for high blood pressure (eg, beta blockers such as atenolol/metoprolol, clonidine, guanabenz, methyldopa, prazosin), "blood thinners" (eg, warfarin), street drugs (eg, methamphetamine, MDMA-"ecstasy"), drugs that affect liver enzymes that remove modafinil from the body (eg, azole antifungals such as itraconazole/ketoconazole, rifamycins such as rifabutin/rifampin, anti-seizure medications such as ...
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Walgreens Accused of Prescription Drugs Scam
Clip thanks to www.medstores.net Michael Behn, a former federal prosecutor, said, "The pharmacies nationwide had a pill flipping scheme." Behn helped expose how Walgreens exploited a Medicaid loophole. To save taxpayer dollars, Medicaid limits how much it pays for popular forms of drugs. But it doesn't bother to set price-ceilings on rarely-used versions. Take generic Zantac, or ranitidine, for example. The antacid is a huge seller in tablet form. Medicaid limits payment to 34 cents apiece. The same drug as capsules has no price-ceiling because it was so rarely-prescribed. Medicaid pays $1.25 each. Walgreens figured it could pocket millions by switching patients from tablets to capsules. Behn explained to Attkisson, "These are the ranitidine capsules." "This is what was being prescribed?" Attkisson asked, pointing to the tablets. "And this is what was being given?" pointing to the capsules. Behn replied, "Correct. At three times or more the cost to taxpayers," Behn answered. The scheme was blown wide open by a whistleblower, a pharmacist who doesn't want to appear on camera. He said Walgreens rigged its computers to automatically switch to the most expensive type of pill. "The only way in which a computer system could switch from a tablet and a capsule, is if someone went in and manipulated the computer system," Behn said. Attkisson asked, "And the fact that this was done nationwide indicates this was a corporate policy?" Behn responded, "That's what we alleged." By ...
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The Dumbing Down of America via Education, Medication, Annihilation
The rate of prescription drug use among children and teens continues to rise, with a new report from Medco Health Solutions Inc. saying that at least a quarter of all US children are now regularly taking pharmaceutical drugs. And according to the report, many of these drugs were originally intended for adults, and carry with them unknown side effects for long-term use in young people. A Very Special Thanks to GKing1000 for sending me this video: www.youtube.com And most especially to Neal Fox for your time, brilliance and thought to create it: www.wireduck.com The Wall Street Journal (WSJ) reports that in addition to taking drugs for conditions like attention-deficit hyperactivity disorder (ADHD) and asthma, children are now taking things like sleeping pills, diabetes drugs and even statin drugs, which are typically only prescribed for adults. The report cites an eight-year-old boy, for example, who has been taking blood pressure medications since he was a baby. Dr. Danny Benjamin, a professor of pediatrics at Duke University, admitted to the WSJ that prescribing chronic medications to children is a serious problem. "We know we're making errors in dosing and safety," he said, noting also that parents must do more to question the safety of medicines their doctors prescribe. Experts worry that the increasing prevalence of children on prescription drugs is causing these young people serious harm, and that parents should instead seek out dietary and lifestyle changes for ...
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COMMENT ON selegiline



Selegiline
Systematic (IUPAC) name
(R)-N-methyl-N-(1-phenylpropan-2-yl)prop-1-yn-3-amine
Clinical data
Trade names Eldepryl
AHFS/Drugs.com monograph
MedlinePlus a697046
Pregnancy cat. C (US)
Legal status prescription only (unscheduled) (US)
Routes Oral, transdermal, buccal
Pharmacokinetic data
Bioavailability 4.4% (oral, fasted), 20% (oral, after food), 18% (patch)
Protein binding 90%
Metabolism liver
Half-life 1.5 hours (oral, single dose), 9 hours (oral, chronic)
Excretion urine
Identifiers
CAS number 14611-51-9 YesY [14611-52-0] (HCl)
ATC code N04BD01 QN06AX90
PubChem CID 26757
DrugBank DB01037
ChemSpider 24930 YesY
UNII 2K1V7GP655 YesY
KEGG D03731 YesY
ChEBI CHEBI:9086 YesY
ChEMBL CHEMBL972 YesY
Chemical data
Formula C13H17N 
Mol. mass 187.281 g/mol
SMILES eMolecules & PubChem
 YesY (what is this?)  (verify)

Selegiline (Anipryl, L-deprenyl, Eldepryl, Emsam, Zelapar) is a drug used for the treatment of early-stage Parkinson's disease, depression and senile dementia. In normal clinical doses it is a selective irreversible MAO-B inhibitor, however in larger doses it loses its specificity and also inhibits MAO-A. Dietary restrictions are common for MAOI treatments, but special dietary restrictions for lower doses have been found to be unnecessary,[1] and dietary restrictions appear to be unnecessary at standard doses when selegiline is taken as Emsam, the transdermal patch form, as no adverse events due to diet have ever been reported with Emsam.[2] The drug was discovered by Jozsef Knoll et al. in Hungary. Selegiline belongs to a class of drugs called phenethylamines. Selegiline is a methamphetamine derivative with a propargyl group attached to the nitrogen atom.

Contents

History

Selegiline was discovered in Hungary in the 1960s. Joseph Knoll, a chair of pharmacology at the Semmelweis University in Budapest, was interested in the physiology of "drive" and the differences between high- and low-performing individuals. For his research, he required a molecule that combined amphetamine-like psychostimulant effect with a "psycho-energic" effect of monoamine oxidase inhibitors (MAOI). To do that, he decided to combine in the same molecule the structural features of the MAOI pargyline and the psychostimulant amphetamine. Knoll was a close friend of Meszaros, the research director of Chinoin, a Hungarian pharmaceutical company (later sold off to Sanofi). For this project, Meszaros put Knoll in contact with a chemist called Ecsery who worked in Chinoin in the field of phenethylamines. Ecsery made about 30 compounds, and Knoll selected the molecule of E-250 (deprenyl) based on its surprising properties. "The great discovery" (in Knoll's words) was that the new molecule did not increase blood pressure, unlike amphetamine, and moreover, it inhibited the blood pressure raising effect of amphetamine. The first publication on deprenyl in Hungarian appeared in 1964, followed by a paper in English in 1965. Deprenyl is a racemic compound, a mixture of two isomers called enantiomers. For the further pharmaceutical development, Knoll chose the (-)-enantiomer of deprenyl, which caused less hypermotility than the opposite (+)-enantiomer. This (-)-enantiomer (l-deprenyl, R-deprenyl) later has come to be called selegiline.[3]

In 1971, Knoll showed that selegiline selectively inhibits the B-isoform of monoamine oxidase (MAO-B) and proposed that it is unlikely to cause the infamous "cheese effect" (hypertensive crisis resulting from consuming foods containing tyramine) that plagues non-selective MAO inhibitors. A few years later, two Parkinson's researchers based in Vienna, Peter Riederer and Walther Birkmayer, realized that selegiline could be useful in Parkinson's disease. One of their colleagues, Moussa Youdim, visited Knoll in Budapest and took selegiline from him to Vienna. In 1975, the Birkmayer's group published the first paper on the effect of selegiline in Parkinson's disease.[3][4]

In 1967, a Hungarian psychiatrist Ervin Varga observed that racemic deprenyl given in large doses has an antidepressant action.[5] This study was largely forgotten until the 2000s (decade) when Sommerset Pharmaceuticals developed selegiline patch for depression.

Uses

The main use of selegiline is in the treatment of Parkinson's disease. It can be used on its own or in a combination with another agent, most often L-DOPA.[6] For the newly diagnosed Parkinson's patients, some claim that selegiline slows the progression of the disease, although this claim has not been widely accepted and the methodology has been rejected by the Food and Drug Administration (FDA).[7] It delays the time point when the L-DOPA (levodopa) treatment becomes necessary from 10-12 to 18 months,[8] which is beneficial despite not being definitive evidence of neuroprotection. The idea behind adding selegiline to levodopa is to decrease the dose of levodopa and thus reduce the motor complications of levodopa therapy.[9] Comparisons of patients on levodopa + placebo vs levodopa + selegiline showed that selegiline allowed reduction of the levodopa dose by about 40%. Selegiline + levodopa also extended the time until the levodopa dose had to be increased from 2.6 to 4.9 years.[8] As a result there were fewer motor complications in selegiline groups.[9] In one trial, selegiline + levodopa completely halted the progress of Parkinson's disease over 14 months, while in the placebo + levodopa group the deterioration of the patients' condition continued. However, the interpretation of this trial as proving neuroprotective action of selegiline has been questioned.[8]

As of February 28, 2006, selegiline has also been approved by the FDA to treat major depression using a transdermal patch (Emsam Patch).[10] Selegiline (brand name Anipryl) is also used (at extremely high dosages relative to humans) in veterinary medicine to treat the symptoms of Cushing's disease and cognitive dysfunction (Canine Cognitive Dysfunction)[11][12] in dogs.[13][14][15] As of June 26, 2006, a selegiline transdermal patch is being tested for its effectiveness in treating ADHD.[16]

Several clinical studies are currently underway to evaluate selegiline's effectiveness in helping people stop smoking tobacco or cannabis.[17][18]

Side effects

Due to the primary metabolites of L-amphetamine and L-methamphetamine, selegiline shares many side effects seen with these sympathomimetic stimulants. Minor side effects such as dizziness, dry mouth, difficulty falling or staying asleep, muscle pain, rash, nausea and constipation have been seen. More serious side effects such as severe headache, tachycardia, arrhythmia, hallucinations, chorea, or difficulty breathing should be investigated by health professionals immediately.[19]

Pharmacology

Pharmacokinetics

[icon] This section requires expansion with:
please add citations detailing bioavailability.

Selegiline has a low oral bioavailability, which increases to moderate when ingested together with a high-fat meal (the molecule being liposoluble).[20]

Selegiline's oral bioavailability is drastically increased in females taking oral contraceptives (10- to 20-fold).[21] This could lead to loss of MAO-B selectivity in favor of an MAO-A selectivity, which in turn would make patients susceptible to the usual risks of unselective MAOIs such as tyramine-induced hypertensive crisis and serotonin toxicity when combined with serotonergics such as SSRIs.[21]

Mechanism of Action

Selegiline is a selective inhibitor of MAO-B; MAO-B metabolizes dopamine and phenylethylamine.[22] Selegiline exhibits little therapeutic benefit when used independently, but enhances and prolongs the anti-Parkinson effects of levodopa.[23]

Metabolites

Desmethylselegiline

Desmethylselegiline may have neuroprotective antiapoptotic properties. A large multicenter study suggests a decrease in the disease progression of parkinsonism but may have reflected other symptomatic response.[22] Desmethylselegiline is metabolized by CYP2C19.[24]

L-amphetamine and L-methamphetamine

Selegiline is partly metabolized to l-methamphetamine, one of the two enantiomers of methamphetamine in vivo.[25] A characteristic metabolic pattern was noted, exemplified by a ratio of l-methamphetamine to l-amphetamine of about 2.8.[26] These stereoisomers are considered significantly less psychoactive and have little abuse potential in contrast to their D-isomers.[27] The stimulatory effect on locomotor activity and dopamine synthesis may be contributed to by the action of l-methamphetamine, a once thought to be inactive metabolite.[25] This locomotor effect at therapeutic doses was not apparent in comparison to placebo, but both l-amphetamine and l-methamphetamine had positive effects on genetic expression for memory enhancement in rats and other animals.[28]

This metabolic action may cause persons taking selegiline to test positive for amphetamine and or methamphetamine on drug screening tests.

Interactions

Selegiline in combination with pethidine is not recommended as it can lead to severe adverse effects; selegiline in combination with the older non-selective MAOIs or in combination with the reversible MAO-A inhibitor moclobemide requires a low tyramine diet. The risk of a true serotonin syndrome with SSRIs and selegiline is quite low an the combination can be taken together without event if caution is used.[29]

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.

In E for Ecstasy[30] (a book examining the uses of the street drug Ecstasy in the UK) the writer, activist and Ecstasy advocate Nicholas Saunders highlighted test results showing that certain consignments of the drug also contained selegiline. Consignments of Ecstasy known as "Strawberry" contained what Saunders described as a "potentially dangerous combination of ketamine, ephedrine and selegiline," as did a consignment of "Sitting Duck" Ecstasy tablets.[31]

Selegiline is not a controlled substance in the US but a prescription is required to obtain it within the US.

Emsam

In February 2006 the US Food and Drug Administration approved Emsam (selegiline), the first transdermal patch for use in treating major depression. The once a day patch works by delivering selegiline through the skin and into the bloodstream. Emsam can be used without the dietary restrictions that are needed for all oral MAO inhibitors that are approved for treating major depression, although the FDA requires warnings concerning dietary restrictions for the 9 and 12 mg doses due to theoretical concerns not supported by any reports of adverse events.[2] 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, an 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.

Zelapar

Zelapar is a transmucosal preparation for human administration of selegiline. The quickly-dissolving lozenge is placed between cheek and gum and the medication enters the bloodstream directly. Because hepatic first-pass metabolism is bypassed, the effective dose is lower than oral (swallowed) selegiline. GI side effects are reportedly reduced compared to oral (swallowed) selegiline. Zelapar is manufactured by Valeant Pharmaceuticals.[32]

Chemistry

Selegiline, N-methyl-N-(2-propynyl)-2-methyl-1-phenylethyl-2-amine, is synthesized by the alkylation of (–)-methamphetamine using propargyl bromide.[33][34][35][36]

Selegiline synthesis.png

See also

References

  1. ^ 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): 208–14. doi:10.4088/JCP.v64n0216. PMID 12633131. 
  2. ^ a b Cascade EF, Kalali AH (June 2007). "EMSAM: The First Year". Psychiatry 2007. http://www.psychiatrymmc.com/emsam-the-first-year/. Retrieved 2009-11-30. 
  3. ^ a b Healy, David (2000). "The psychopharmacology of life and death. Interview with Joseph Knoll.". The Psychopharmacologists, Vol. III: Interviews. London: Arnold. pp. 81–110. ISBN 0-340-76110-5. 
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