Selegiline

Dosage of Selegiline varies significantly based on the formulation and the condition being treated.

Parkinson’s Disease

• Standard Oral Tablets/Capsules: The typical dose is 5 mg taken twice daily, once at breakfast and once at lunch. Taking the second dose at lunch rather than bedtime helps minimize the risk of insomnia caused by the drug's metabolites.
• Orally Disintegrating Tablets (Zelapar): The starting and maintenance dose is typically 1.25 mg once daily. This should be taken in the morning before breakfast, without liquid. Patients should avoid food or drink for 5 minutes before and after taking the tablet.

Major Depressive Disorder

• Transdermal Patch (Emsam): The recommended starting dose is 6 mg per 24 hours. If the clinical response is inadequate, a healthcare provider may increase the dose in increments of 3 mg, up to a maximum of 12 mg per 24 hours. Adjustments are usually made at intervals of no less than 2 weeks.

Selegiline is generally not approved for use in pediatric patients. For Major Depressive Disorder, the Emsam patch carries a specific warning regarding the increased risk of suicidal thoughts and behaviors in children, adolescents, and young adults. Safety and effectiveness in patients under the age of 18 have not been established for any indication.

Renal Impairment

For patients with mild to moderate kidney disease, dosage adjustments are typically not required for the oral forms. However, there is limited data on the use of Selegiline in patients with severe renal impairment or end-stage renal disease (ESRD). Healthcare providers will monitor these patients closely for signs of toxicity.

Hepatic Impairment

The liver is the primary site of Selegiline metabolism. In patients with hepatic (liver) impairment, the concentration of the drug in the blood can increase significantly. For the Emsam patch, no adjustment is usually needed for mild impairment, but caution is advised in moderate to severe cases. For oral forms, a lower dose or less frequent administration may be considered by the physician.

Elderly Patients

In clinical trials, elderly patients (over 65) did not show significant differences in safety compared to younger adults. However, because older adults are more prone to orthostatic hypotension (a drop in blood pressure when standing up) and may have age-related declines in kidney or liver function, healthcare providers often start at the lower end of the dosing range.

• Oral Tablets: Swallow whole with water. It is often recommended to take these with food to increase absorption and reduce stomach upset.
• Orally Disintegrating Tablets (ODT): Do not push the tablet through the foil. Instead, peel the backing off with dry hands. Place the tablet on the tongue and let it dissolve. Do not swallow the tablet whole. Avoid rinsing the mouth or drinking for at least 5 minutes.
• Transdermal Patch: Apply to a dry, hairless area of the upper torso, upper arm, or thigh. Use a new site every day to avoid skin irritation. Change the patch at the same time every 24 hours.
• Storage: Store all forms at room temperature (68°F to 77°F or 20°C to 25°C), away from moisture, heat, and direct sunlight.

If you miss a dose of Selegiline, take it as soon as you remember. However, if it is almost time for your next scheduled dose, skip the missed dose and return to your regular schedule. Do not double the dose to catch up. For the patch, if you forget to change it, apply a new one as soon as possible and resume your normal 24-hour cycle.

An overdose of Selegiline can be life-threatening and may mimic the symptoms of other MAO inhibitor toxicities. Signs of overdose may not appear immediately and can be delayed by 12 to 24 hours. Symptoms include:

• Severe headache
• High fever (hyperpyrexia)
• Rapid heartbeat (tachycardia) or irregular heart rhythm
• Severe agitation or hallucinations
• Seizures
• Coma

If an overdose is suspected, contact your local poison control center or seek emergency medical attention immediately.

> Important: Follow your healthcare provider's dosing instructions exactly. Do not adjust your dose or stop taking Selegiline without medical guidance, as sudden discontinuation can lead to a worsening of symptoms.

Side effects of Selegiline can vary depending on whether it is taken orally for Parkinson's or via a patch for depression. Common experiences include:

• Nausea and Stomach Upset: This is the most frequently reported side effect for oral Selegiline. It often subsides as the body adjusts to the medication.
• Dizziness and Lightheadedness: Many patients experience a 'spinning' sensation, particularly when starting the drug. This is often linked to changes in blood pressure.
• Insomnia: Because Selegiline is metabolized into amphetamine-like substances, it can cause difficulty falling or staying asleep, especially if taken late in the day.
• Application Site Reactions (Patch only): For those using the Emsam patch, redness, itching, or irritation at the site of the patch is very common.

• Orthostatic Hypotension: A sudden drop in blood pressure when standing up from a sitting or lying position, which can lead to fainting.
• Dry Mouth (Xerostomia): A persistent feeling of dryness in the mouth, which can sometimes lead to dental issues if not managed.
• Dyskinesia: In Parkinson's patients, Selegiline increases the effect of levodopa, which can sometimes lead to involuntary, jerky movements (dyskinesia).
• Abdominal Pain: Cramping or general discomfort in the stomach area.
• Headache: Mild to moderate tension-type headaches.

• Hallucinations: Seeing or hearing things that are not there, more common in elderly Parkinson's patients.
• Confusion and Disorientation: A sudden lack of clarity or inability to recognize surroundings.
• Urinary Retention: Difficulty starting or fully emptying the bladder.
• Vivid Dreams or Nightmares: Intense or disturbing sleep experiences.

> Warning: Stop taking Selegiline and call your doctor immediately if you experience any of these symptoms. These may indicate a life-threatening reaction.

• Hypertensive Crisis: Characterized by an extremely severe headache ('thunderclap' headache), chest pain, neck stiffness, nausea, vomiting, and sensitivity to light. This is often triggered by eating high-tyramine foods while on high doses of Selegiline.
• Serotonin Syndrome: A potentially fatal condition caused by too much serotonin. Symptoms include high fever, sweating, shivering, rapid heart rate, muscle rigidity, twitching, and loss of coordination.
• Suicidal Thoughts: Especially in younger patients using the patch for depression, any new or worsening thoughts of self-harm must be reported immediately.
• Severe Allergic Reaction (Anaphylaxis): Symptoms include hives, swelling of the face or throat, and difficulty breathing.
• Manic Episodes: In patients with bipolar disorder, Selegiline may trigger a shift into mania (excessive energy, racing thoughts, impulsive behavior).

With prolonged use, some patients may develop a tolerance to the drug's effects, requiring dosage adjustments. Long-term use in Parkinson's disease is generally well-tolerated, but the risk of levodopa-induced dyskinesia may increase over years of combined therapy. There is also a theoretical risk of 'impulse control disorders,' where patients develop intense urges to gamble, spend money, or engage in other repetitive behaviors, though this is more common with dopamine agonists than with Selegiline.

Suicidality in Children and Young Adults (Emsam Patch only):

The FDA has issued a black box warning for the Selegiline transdermal patch (Emsam). Antidepressants increased the risk of suicidal thoughts and behavior in children, adolescents, and young adults in short-term studies. Anyone considering the use of Emsam in a child or young adult must balance this risk with the clinical need. Families and caregivers should be advised of the need for close observation and communication with the prescriber. It is important to note that Emsam is not approved for use in pediatric patients.

Report any unusual symptoms or changes in mood to your healthcare provider promptly. Monitoring by a physician is essential for the safe long-term use of this medication.

Selegiline is a powerful medication that requires careful monitoring. Patients must be aware of the 'tyramine trap.' At standard doses for Parkinson's (10 mg/day or less), Selegiline is selective for MAO-B and usually does not require a special diet. However, at higher doses (such as the 9 mg or 12 mg Emsam patch), Selegiline loses its selectivity and inhibits MAO-A in the gut. This prevents the breakdown of tyramine, an amino acid found in aged and fermented foods. High levels of tyramine can cause a sudden, massive release of norepinephrine, leading to a hypertensive crisis.

Suicidality Warning (Transdermal Patch):

According to the FDA, Emsam (Selegiline transdermal) is associated with an increased risk of suicidal thinking and behavior in children, adolescents, and young adults (ages 18-24) during initial treatment. Healthcare providers must monitor all patients starting antidepressants for clinical worsening and emergence of suicidal thoughts, especially during the first few months of drug therapy or at times of dose changes.

• Hypertension Risk: Selegiline can increase blood pressure, especially when combined with other stimulants or high-tyramine foods. Regular blood pressure monitoring is recommended.
• Orthostatic Hypotension: Patients, particularly the elderly, are at risk of fainting or falling due to sudden drops in blood pressure when standing. Rise slowly from a sitting or lying position.
• Serotonin Syndrome: This is a major risk when Selegiline is taken with other serotonergic drugs (like SSRIs, SNRIs, or certain pain medications). A 'washout period' of 14 days is usually required when switching between these medications.
• Melanoma Risk: Some studies suggested that patients with Parkinson’s disease have a higher risk of developing melanoma (skin cancer). While it is unclear if Selegiline or the disease itself causes this, regular skin examinations by a dermatologist are advised.

Your healthcare provider may require the following during Selegiline therapy:

• Blood Pressure Checks: Frequent monitoring, especially during the first few weeks of treatment or after a dose increase.
• Skin Exams: To monitor for melanoma or other skin changes.
• Mental Status Evaluation: To check for signs of depression, anxiety, or suicidal ideation.
• Liver Function Tests: Periodic blood work to ensure the liver is processing the medication correctly, particularly in patients with pre-existing liver issues.

Selegiline may cause dizziness, hallucinations, or sudden 'sleep attacks' (somnolence). Do not drive, operate heavy machinery, or engage in dangerous activities until you know how this medication affects you. If you experience increased sleepiness during the day, consult your doctor immediately.

Alcohol should be avoided while taking Selegiline. Alcohol can increase the sedative effects of the medication and may also contain tyramine (especially tap beers and certain wines), which increases the risk of a hypertensive crisis.

Do not stop taking Selegiline abruptly. Sudden discontinuation can lead to a 'withdrawal' effect or a rapid worsening of Parkinson's symptoms (Neuroleptic Malignant-like Syndrome). If the drug must be stopped, your doctor will provide a tapering schedule to slowly reduce the dose.

> Important: Discuss all your medical conditions, including any history of high blood pressure, heart disease, or mental health issues, with your healthcare provider before starting Selegiline.

Certain drugs should NEVER be used with Selegiline due to the risk of fatal reactions:

• Meperidine (Demerol): Combination can cause cardiovascular collapse, respiratory depression, and hyperpyrexia (extreme fever).
• Other MAOIs (e.g., Phenelzine, Tranylcypromine): Using two MAOIs together can cause a massive hypertensive crisis.
• Dextromethorphan: Found in many over-the-counter cough medicines, this can cause 'serotonin syndrome' when mixed with Selegiline.
• Methadone and Tramadol: These opioid pain relievers carry a high risk of serotonin syndrome and CNS toxicity.

• SSRIs and SNRIs (e.g., Prozac, Zoloft, Effexor): These increase serotonin levels and can lead to Serotonin Syndrome. A 14-day gap (5 weeks for Prozac) is mandatory between using these and Selegiline.
• Tricyclic Antidepressants (TCAs): Can cause severe hypertension and CNS toxicity.
• Sympathomimetics: This includes 'decongestants' like pseudoephedrine and 'stimulants' like methylphenidate. These can cause a dangerous spike in blood pressure.

• Levodopa/Carbidopa: While Selegiline is used with these drugs, it potentiates their effects. This can increase the risk of side effects like dyskinesia, hallucinations, and low blood pressure. Your doctor may need to lower your levodopa dose.
• Oral Contraceptives: Birth control pills can increase the blood levels of Selegiline by inhibiting its metabolism, potentially increasing side effects.

• Tyramine-Rich Foods: At doses above 10 mg/day (or 9mg/12mg patches), you must follow a low-tyramine diet. Avoid:
• Aged cheeses (Cheddar, Swiss, Blue, Brie)
• Fermented or air-dried meats (Salami, Pepperoni)
• Sauerkraut and Kimchi
• Soy sauce and Tofu
• Fava beans or broad beans
• Tap beers and unpasteurized beers
• Caffeine: Large amounts of caffeine can increase the risk of high blood pressure and jitteriness.

• St. John’s Wort: This herbal antidepressant increases serotonin and is strictly contraindicated with Selegiline.
• Ginseng and Ephedra (Ma Huang): These can cause headaches, tremors, and high blood pressure when combined with MAOIs.
• 5-HTP and L-Tryptophan: These amino acid supplements increase serotonin and should be avoided.

Selegiline metabolites (L-methamphetamine) may cause a false positive result on urine drug screens for amphetamines. If you are required to take a drug test for employment or legal reasons, ensure the testing lab is aware you are taking Selegiline so they can perform a confirmatory test (GC/MS) to distinguish between the drug's metabolites and illicit substances.

For each major interaction, the mechanism usually involves either the inhibition of neurotransmitter breakdown (pharmacodynamic) or the competition for liver enzymes (pharmacokinetic). The clinical consequence is often an 'overload' of serotonin or norepinephrine, leading to toxicity. The management strategy is always to maintain a strict 'washout period' when changing medications and to consult a pharmacist before starting any new over-the-counter product.

> Important: Tell your doctor about ALL medications, supplements, and herbal products you are taking, including those for cough, cold, or weight loss.

Selegiline must NEVER be used in the following circumstances:

• Hypersensitivity: If you have had a prior allergic reaction to Selegiline or any components of the tablet/patch.
• Concomitant Meperidine Use: The risk of fatal CNS depression and hyperpyrexia is absolute.
• Concomitant Dextromethorphan Use: Risk of serotonin syndrome and psychosis.
• Pheochromocytoma: This is a rare tumor of the adrenal gland that secretes adrenaline. Because Selegiline increases catecholamines (like adrenaline), it could trigger a life-threatening hypertensive crisis in these patients.
• Elective Surgery: Selegiline should generally be discontinued 10 to 14 days before elective surgery involving general anesthesia to avoid interactions with anesthetic agents and narcotics.

Conditions requiring careful risk-benefit analysis by a physician:

• Peptic Ulcer Disease: Selegiline may increase gastric acid secretion, potentially worsening ulcers.
• Severe Hepatic Impairment: The drug may accumulate to toxic levels if the liver cannot break it down.
• Uncontrolled Hypertension: Because the drug can raise blood pressure, it must be used with extreme caution in those whose BP is not well-managed.
• Psychosis or Schizophrenia: Increasing dopamine levels can worsen symptoms of psychosis or trigger manic episodes.

While Selegiline is chemically distinct from other MAOIs, patients who have had severe adverse reactions to other MAO inhibitors (like Rasagiline or Safinamide) should be monitored closely for similar reactions. There is no documented cross-allergy between Selegiline and other classes of antidepressants or Parkinson's medications, but caution is always warranted when introducing a new drug to a sensitive patient.

> Important: Your healthcare provider will evaluate your complete medical history, including any history of heart rhythm problems or mental health disorders, before prescribing Selegiline. Always ensure your medical record is up to date.

Selegiline is classified as FDA Pregnancy Category C. This means that animal reproduction studies have shown an adverse effect on the fetus, but there are no adequate and well-controlled studies in humans. In animal studies, Selegiline was associated with decreased pup survival and body weight. It should be used during pregnancy only if the potential benefit justifies the potential risk to the fetus. If you are planning a pregnancy or become pregnant while taking Selegiline, consult your neurologist or psychiatrist immediately to discuss alternative treatments.

It is not known whether Selegiline or its metabolites are excreted in human milk. Because many drugs are excreted in human milk and because of the potential for serious adverse reactions in nursing infants (such as irritability or changes in blood pressure), a decision should be made whether to discontinue nursing or discontinue the drug, taking into account the importance of the drug to the mother. Most clinicians advise against breastfeeding while taking MAOIs.

Selegiline is not approved for use in children. In the case of the Emsam patch, there is a specific risk of suicidality. Furthermore, the risk of a hypertensive crisis (the 'cheese effect') may be harder to manage in children who may not adhere strictly to dietary restrictions. For Parkinson's disease, the condition is extremely rare in children, and Selegiline's safety in this context has never been studied.

Parkinson's disease primarily affects older adults, so Selegiline has been studied extensively in this population. While generally effective, elderly patients are at a higher risk for:

• Falls: Due to orthostatic hypotension.
• Hallucinations: Older brains are more sensitive to the dopamine-increasing effects of the drug.
• Polypharmacy: Older adults often take multiple medications for blood pressure or heart disease, increasing the risk of drug-drug interactions.

In patients with mild to moderate renal impairment, the pharmacokinetics of Selegiline are not significantly altered. However, for those with severe impairment or those on dialysis, the metabolites (amphetamine/methamphetamine) may accumulate. While no specific dose adjustment is mandated by the FDA, a 'start low, go slow' approach is recommended.

For patients with liver disease, the oral forms of Selegiline should be used with caution. The transdermal patch (Emsam) has been studied in patients with hepatic impairment; while mild impairment doesn't require a dose change, the 6 mg/24 hour dose is usually the maximum recommended for those with more significant liver dysfunction to prevent toxicity.

> Important: Special populations require individualized medical assessment. Never share your medication with others, especially those in these sensitive categories.

Selegiline is a 'suicide' or 'irreversible' inhibitor of Monoamine Oxidase (MAO). It works by binding to the FAD (flavin adenine dinucleotide) cofactor of the MAO enzyme. At clinical doses of 10 mg/day or less, it is highly selective for the MAO-B isoform. MAO-B is the primary enzyme responsible for the oxidative deamination of dopamine in the human striatum. By blocking this enzyme, Selegiline increases the concentration of synaptic dopamine. Additionally, Selegiline may interfere with the reuptake of dopamine from the synaptic cleft, further enhancing dopaminergic activity. At higher doses (typically >20 mg orally or the higher-strength patches), it loses selectivity and inhibits MAO-A, which is why dietary restrictions become necessary at higher doses.

The onset of MAO-B inhibition is rapid, occurring within hours of the first dose. However, the clinical 'benefit' in Parkinson's symptoms may take several weeks to become apparent. Because the inhibition is irreversible, the effect persists for approximately 10 to 14 days after the last dose is taken—this is the time required for the body to manufacture new MAO enzymes. This 'lag time' is critical when switching to other medications that might interact with Selegiline.

| Parameter | Value |

|---|---|

| Bioavailability | <10% (Oral); ~73% (Transdermal) |

| Protein Binding | 90% - 94% |

| Half-life | 1.5 - 2 hours (Parent drug); 18-25 hours (Metabolites) |

| Tmax | 0.5 - 2 hours (Oral) |

| Metabolism | Hepatic (CYP2B6, CYP3A4, CYP2C19) |

| Excretion | Renal (~73%), Fecal (~15%) |

• Molecular Formula: C13H17N (as hydrochloride: C13H18ClN)
• Molecular Weight: 187.28 g/mol (base); 223.74 g/mol (HCl salt)
• Solubility: Highly soluble in water and ethanol.
• Structure: Selegiline is a phenethylamine derivative and is the levorotatory (L-isomer) of deprenyl. Its structure is closely related to methamphetamine, but the L-isomer configuration significantly reduces its central nervous system stimulant potency compared to the D-isomer.

Selegiline is classified as a Monoamine Oxidase Type B Inhibitor [EPC]. It is part of the broader category of antiparkinsonian agents and antidepressants. Related medications include Rasagiline (Azilect) and Safinamide (Xadago), which are also selective MAO-B inhibitors, and Phenelzine (Nardil), which is a non-selective MAO inhibitor.