Selegiline Patch (Emsam): Comprehensive Drug Monograph

Pharmacokinetic Profile

Delivery

Transdermal; 25–30% of patch content delivered over 24 h

MAO Selectivity

Preferential MAO-B; inhibits both MAO-A and MAO-B at antidepressant doses

Key PK Advantage

Bypasses GI tract; intestinal MAO-A preserved at 6 mg/24h

Metabolites

Lower metabolite exposure vs oral selegiline

Clinical Information

Drug Class

Irreversible MAOI (transdermal)

Available Patches

6 mg/24h (20 cm²), 9 mg/24h (30 cm²), 12 mg/24h (40 cm²)

Route

Transdermal (upper torso, thigh, or upper arm)

Renal Adjustment

No adjustment needed (mild/moderate/severe)

Hepatic Adjustment

No adjustment for mild/moderate; not studied in severe

Pregnancy

May cause fetal harm (animal data)

Lactation

Not recommended during treatment or for 5 days after final dose

Schedule

Not a controlled substance

Generic Available

No (brand Emsam only)

Boxed Warning

Suicidality; contraindicated <12 years

Dietary Restriction

6 mg/24h: NO diet restriction
9 & 12 mg/24h: Tyramine diet required

Indications

Indication	Approved Population	Therapy Type	Status
Major Depressive Disorder (MDD)	Adults	Monotherapy	FDA Approved

The selegiline transdermal system (Emsam) is the first and only transdermal MAOI approved for the treatment of MDD, receiving FDA approval in 2006. Unlike oral MAOIs (phenelzine, tranylcypromine), it is indicated as a potential first-line option — the PI does not restrict it to treatment-resistant patients. Its unique pharmacokinetic profile allows the 6 mg/24h dose to be used without any dietary tyramine restrictions, a breakthrough that addresses the primary barrier to MAOI prescribing. At the lowest effective dose, transdermal delivery bypasses the gastrointestinal tract, preserving intestinal MAO-A activity and allowing dietary tyramine to be metabolised before reaching the systemic circulation. At higher doses (9 and 12 mg/24h), systemic selegiline levels are sufficient to partially inhibit intestinal MAO-A, necessitating tyramine dietary restrictions.

Off-Label Uses

Treatment-resistant depression — Used when oral antidepressants have failed; the transdermal route offers an alternative to oral MAOIs with a more favourable safety profile at 6 mg. (Evidence quality: Moderate)

Atypical depression — MAOIs remain highly effective for this subtype; the transdermal route may improve adherence. (Evidence quality: Low – extrapolated from oral MAOI data)

Dose

Dosing

Adult Dosing by Clinical Scenario

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Dose	Notes
MDD — initial treatment	6 mg/24h patch	6 mg/24h	12 mg/24h	6 mg/24h is the starting AND target dose; no dietary restrictions at this dose Increase by 3 mg/24h every ≥2 weeks if needed; full effect may be delayed
MDD — inadequate response at 6 mg	9 mg/24h patch	9–12 mg/24h	12 mg/24h	Tyramine dietary restrictions begin on first day of 9 mg or 12 mg dosing Restrictions continue for 2 weeks after dose reduction to 6 mg or discontinuation

Application Instructions

Parameter	Instruction
Application site	Dry, intact skin on upper torso (below neck, above waist), upper thigh, or outer surface of upper arm
Frequency	Apply one patch every 24 hours; replace at approximately the same time each day
Site rotation	Do not apply to the same site on consecutive days
Patch handling	Do not cut the patch; do not wear more than one patch at a time; avoid touching the adhesive side
Heat avoidance	Do not expose the application site to heating pads, electric blankets, saunas, hot tubs, or prolonged direct sunlight (may increase drug absorption)

Special Population Adjustments

Population	Starting Dose	Maintenance Dose	Maximum Dose	Notes
Elderly (≥65 years)	6 mg/24h	6 mg/24h (recommended)	Per clinical judgement	Recommended dose is 6 mg/24h daily (PI Section 8.5) Age effect on PK not systematically evaluated
Renal impairment	No adjustment needed (mild/moderate/severe)			PK unaffected by renal impairment; not studied in ESRD (PI Section 8.8)
Hepatic impairment	No adjustment for mild/moderate			No PK differences observed; not studied in severe hepatic impairment (PI Section 8.7)
Paediatric (<12 years)	Contraindicated			Increased risk of hypertensive crisis; children may have higher selegiline exposure (PI Section 8.4)
Adolescents (12–17 years)	Not recommended			Efficacy not demonstrated in paediatric MDD trial (PI Section 8.4)

Clinical Pearl: Why No Dietary Restrictions at 6 mg/24h?

The transdermal route delivers selegiline directly into the systemic circulation, bypassing first-pass metabolism in the GI tract and liver. Since intestinal MAO is predominantly type A, and MAO-A is the enzyme responsible for metabolising dietary tyramine in the gut wall, the transdermal route preserves this intestinal “tyramine firewall” at lower doses. At 6 mg/24h, systemic selegiline concentrations are sufficient to inhibit both MAO-A and MAO-B in the brain (producing antidepressant effects) but not high enough to significantly inhibit intestinal MAO-A. At higher doses (9 and 12 mg/24h), systemic levels rise sufficiently to partially inhibit intestinal MAO-A, restoring the tyramine risk and necessitating dietary restrictions.

Selegiline Patch Pharmacology

Mechanism of Action

Selegiline is an irreversible inhibitor of monoamine oxidase with preferential affinity for MAO-B at low concentrations. However, at the doses used for depression (6–12 mg/24h transdermally), selegiline inhibits both MAO-A and MAO-B in the brain. Antidepressant activity in animal models (Forced Swim Test) was observed only at doses that inhibited both isoenzymes. By preventing the catabolism of serotonin, norepinephrine, dopamine, and phenylethylamine in the CNS, selegiline increases monoamine neurotransmitter availability. In vitro receptor binding studies also demonstrate selegiline affinity for the human α2B adrenergic receptor (Ki = 0.3 μM), suggesting an additional pharmacological mechanism. Importantly, the transdermal route delivers significantly higher selegiline exposure with significantly lower exposure to metabolites (including methamphetamine and amphetamine, which are produced by oral selegiline but minimised with transdermal delivery).

ADME Profile

Parameter	Value	Clinical Implication
Absorption	Transdermal; 25–30% of patch content delivered systemically over 24 h (range ~10–40%); bypasses GI and hepatic first-pass metabolism	GI MAO-A preserved at 6 mg/24h, enabling tyramine-free dining; interindividual variability in absorption (10–40%); avoid heat exposure at application site
Distribution	Not formally characterised for transdermal route; oral selegiline protein binding ~90%	Selegiline is highly lipophilic, facilitating CNS penetration and transdermal absorption
Metabolism	Transdermal route produces significantly lower metabolite levels vs oral; oral selegiline metabolised to desmethylselegiline, methamphetamine, and amphetamine via CYP2B6 and CYP3A4	Reduced exposure to amphetamine/methamphetamine metabolites is a key advantage of the patch; carbamazepine increases selegiline levels ~2-fold (contraindicated)
Elimination	Primarily renal (as metabolites); renal impairment does not affect PK; no clinically relevant CYP interactions at standard doses	No dose adjustment needed for renal impairment (mild/moderate/severe); ketoconazole, alprazolam, ibuprofen, olanzapine, and warfarin do not require dose adjustments when co-administered

Side Effects

Adverse reaction data are from the pooled short-term, placebo-controlled EMSAM clinical trials (PI Section 6.1; N=2,036 selegiline exposures). The side-effect profile is considerably more favourable than oral MAOIs, with application site reactions being the most distinctive adverse event.

≥10%Very Common (≥10%)

Adverse Effect	Incidence (EMSAM vs Placebo)	Clinical Note
Application site reaction	24% vs 12%	Itching, redness, swelling at patch site; usually mild-to-moderate and resolves within hours of patch removal; rotate application sites daily (PI Section 6.1)
Headache	18% vs 17%	Rate similar to placebo; distinguish from hypertensive crisis headache (occipital, sudden onset) (PI Sections 5.3, 6.1)
Insomnia	12% vs 7%	Consider applying patch earlier in the day if sleep is affected (PI Section 6.1)

2–9%Common (2–9%, greater than placebo)

Adverse Effect	Incidence (EMSAM vs Placebo)	Clinical Note
Diarrhea	9% vs 7%	Usually self-limiting (PI Section 6.1)
Dry mouth	8% vs 6%	Less prominent than with oral MAOIs (PI Section 6.1)
Dyspepsia	4% vs 3%	GI effects milder than oral route (PI Section 6.1)
Rash	4% vs 2%	Distinct from application site reaction; assess for hypersensitivity (PI Section 6.1)
Pharyngitis	3% vs 2%	Upper respiratory symptoms (PI Section 6.1)
Sinusitis	3% vs 1%	(PI Section 6.1)

SeriousSerious (regardless of frequency)

Adverse Effect	Estimated Frequency	Typical Onset	Required Action
Hypertensive crisis (at 9 & 12 mg/24h with tyramine)	Rare (with dietary compliance)	Minutes to hours after tyramine ingestion	Discontinue patch; treat hypertensive emergency; ED admission (PI Section 5.3)
Serotonin syndrome	Rare (with contraindicated drug)	Hours after exposure to serotonergic agent	Discontinue all serotonergic agents; supportive care (PI Section 5.2)
Suicidal ideation / behaviour	Uncommon (age-dependent)	First weeks to months	Close monitoring; consider stopping if emergent suicidality (PI Section 5.1)
Mania / hypomania	0.4% (8/2,036 in Phase III)	First weeks	Discontinue; screen for bipolar disorder (PI Section 5.4)

DiscontinuationDiscontinuation & Washout

After Stopping EMSAM

≥2 weeks

At least 2 weeks must elapse after stopping EMSAM before starting any contraindicated drug (PI Section 4).

Before Starting EMSAM

4–5 half-lives (~1 week)

Wait 4–5 half-lives of the prior drug; at least 5 weeks for fluoxetine due to its long-acting metabolite (PI Section 4).

Key Advantage: Milder Side-Effect Profile vs Oral MAOIs

Compared with oral MAOIs (phenelzine, tranylcypromine), the selegiline patch has a notably milder side-effect profile. Orthostatic hypotension, weight gain, and sexual dysfunction — the major tolerability issues with oral MAOIs — were not significantly more common than placebo in EMSAM trials. The most distinctive adverse event is application site reaction (24%), which is usually mild and transient. This favourable tolerability profile, combined with no dietary restrictions at 6 mg/24h, makes the selegiline patch a significantly more practical MAOI option for many patients.

Int

Drug Interactions

Although the selegiline patch has fewer dietary interactions at the lowest dose, it retains the full range of drug-drug interactions common to all MAOIs. Notably, the contraindicated drug list is specific to EMSAM and does not include ALL tricyclic antidepressants — only clomipramine and imipramine are listed. Carbamazepine raises selegiline levels approximately 2-fold and is contraindicated. Several drugs that do not interact with EMSAM have been specifically studied (alprazolam, ibuprofen, levothyroxine, olanzapine, risperidone, warfarin, ketoconazole) and require no dose adjustment.

MajorSSRIs, SNRIs

MechanismMAO inhibition + serotonin reuptake blockade

EffectLife-threatening serotonin syndrome

ManagementContraindicated. Wait ≥2 weeks after stopping EMSAM; wait 4–5 half-lives before starting EMSAM; 5 weeks for fluoxetine

FDA PI Section 4

MajorClomipramine, Imipramine, Meperidine, Tramadol, Methadone, Dextromethorphan

MechanismSerotonin reuptake inhibition + MAO inhibition

EffectSerotonin syndrome; potentially fatal with meperidine

ManagementAll contraindicated. Note: only clomipramine and imipramine are listed (not all TCAs); pentazocine and propoxyphene also contraindicated

FDA PI Section 4

MajorCarbamazepine

MechanismCarbamazepine nearly doubles selegiline plasma levels

EffectIncreased risk of hypertensive crisis at any EMSAM dose

ManagementContraindicated (PI Sections 4, 5.3, 7.4)

FDA PI (PK study)

MajorTyramine-Rich Foods (at 9 & 12 mg/24h only)

MechanismAt higher doses, systemic selegiline inhibits intestinal MAO-A; tyramine enters circulation

EffectHypertensive crisis

ManagementAvoid tyramine-rich foods during 9/12 mg treatment and for 2 weeks after reducing to 6 mg or discontinuation. Not required at 6 mg/24h

FDA PI Section 7.2

ModerateBuspirone, Amphetamines, Sympathomimetic Amines

MechanismAdditive adrenergic/serotonergic effects

EffectSubstantial increases in blood pressure

ManagementMonitor BP closely; includes pseudoephedrine, phenylephrine, phenylpropanolamine, ephedrine

FDA PI Section 5.3

MinorAlprazolam, Ibuprofen, Olanzapine, Risperidone, Warfarin, Ketoconazole, Levothyroxine

MechanismFormally studied; no clinically relevant PK interactions

EffectNo dose adjustment needed

ManagementStandard dosing (PI Section 7.5)

FDA PI (PK studies)

Mon

Monitoring

Blood PressureEvery visit; especially at 9 & 12 mg
RoutineMonitor for hypertensive episodes especially if sympathomimetic agents are co-prescribed or if taking 9/12 mg dose. Less orthostatic hypotension risk than oral MAOIs.
Application SiteEach patch change
RoutineAssess for erythema, itching, swelling. Reactions are usually mild and transient (PI Section 6.1). Rotate sites daily.
Mental StateEvery visit for first 3 months
RoutineMonitor for suicidality, mania/hypomania (0.4% in trials), agitation. Screen for bipolar disorder before initiation (PI Sections 5.1, 5.4).
Dietary ComplianceEvery visit if on 9 or 12 mg
Trigger-BasedNot required at 6 mg/24h. At 9 and 12 mg, review tyramine-restricted diet at every visit. Restrictions continue for 2 weeks after stepping down to 6 mg or stopping (PI Section 2.3).
Heat ExposureEach visit
RoutineRemind patients to avoid heating pads, saunas, prolonged sunlight on patch site. Heat may increase drug absorption and elevate selegiline levels (PI Section 5.5).

Contraindications & Cautions

Absolute Contraindications

Patients <12 years of age — increased risk of hypertensive crisis (higher selegiline exposure) (PI Section 4)
Pheochromocytoma — MAOIs may precipitate hypertensive crisis (PI Section 4)
Concurrent or recent use of contraindicated drugs: SSRIs, SNRIs, clomipramine, imipramine, meperidine, tramadol, methadone, pentazocine, propoxyphene, dextromethorphan, carbamazepine (PI Section 4)
Oral selegiline — patients should not use oral selegiline while on EMSAM (PI Section 17)

Relative Contraindications (Specialist Input Recommended)

Bipolar disorder (unscreened) — risk of mania/hypomania (0.4% in trials) (PI Section 5.4)
Adolescents (12–17 years) — not recommended; efficacy not demonstrated (PI Section 8.4)

Use with Caution

Severe hepatic impairment — not studied (PI Section 8.7)
ESRD / dialysis — not studied (PI Section 8.8)
Patients taking sympathomimetic agents or buspirone — BP monitoring required (PI Section 5.3)
Patients exposed to external heat sources — may increase drug absorption (PI Section 5.5)

FDA Boxed Warning Suicidal Thoughts and Behaviours

Antidepressants increase the risk of suicidal thinking and behaviour in paediatric and young adult patients. In pooled analyses, the risk was 14 additional patients per 1,000 treated (<18 years) and 5 additional per 1,000 (18–24 years). EMSAM is contraindicated in patients less than 12 years of age because of an increased risk of hypertensive crisis.

Patient Counselling

Purpose of Therapy

Emsam is a skin patch that delivers selegiline, a medication that increases mood-regulating brain chemicals by preventing their breakdown. It works differently from most antidepressants and is applied to the skin once daily. At the lowest dose (6 mg/24h), you do not need to follow any special diet. If your doctor increases the dose, certain foods will need to be avoided.

How to Use

Apply one patch daily to dry, clean skin on your upper body, upper thigh, or outer upper arm. Replace the patch at approximately the same time each day. Use a different area of skin each day — do not reuse the same spot on consecutive days. Do not cut the patch. Wash your hands after handling the patch.

Dietary Rules (Dose-Dependent)

Tell patientAt the 6 mg patch, you do NOT need to follow any special diet — this is a key advantage of this medication. However, if your dose is increased to 9 mg or 12 mg, you must avoid tyramine-rich foods (aged cheeses, cured meats, fermented foods, beer, wine). These dietary restrictions begin on the first day of the higher dose and continue for 2 weeks after stepping down to 6 mg or stopping the patch entirely.

Call prescriberImmediately if you develop a sudden severe headache, rapid heartbeat, neck stiffness, or nausea — go to the emergency department.

Medication Restrictions

Tell patientEven at the lowest dose, many common medications cannot be taken with this patch, including most antidepressants, certain pain medications, and cough/cold remedies containing dextromethorphan. Alcohol use is also not recommended while on EMSAM. Always check with your pharmacist before taking any new medication. Inform all healthcare providers that you use an MAOI patch.

Call prescriberBefore starting any new medication, including over-the-counter products.

Patch Application & Heat

Tell patientDo not expose the patch area to heating pads, electric blankets, saunas, hot tubs, or prolonged sunlight. Heat can cause more medication to be absorbed, which could be dangerous. Do not cut the patch or wear more than one at a time.

Call prescriberIf you notice significant skin irritation, blistering, or allergic reaction at the patch site.

Switching Medications

Tell patientIf you are switching from another antidepressant to Emsam or from Emsam to another antidepressant, there must be a waiting period between the two medications. Your prescriber will plan this transition carefully to avoid serious interactions.

Call prescriberIf you want to change or stop your medication — never switch without medical guidance.

Ref

Sources

Regulatory (PI / SmPC)

EMSAM (selegiline transdermal system) — Full Prescribing Information. Revised May 2020. Somerset Pharmaceuticals Inc. DailyMedPrimary source for all dosing, dietary modification rules, adverse reaction incidence (Table 2, N=2,036), contraindications, PK data, and clinical trial results.

Key Clinical Trials

Bodkin JA, Amsterdam JD. Transdermal selegiline in major depression: a double-blind, placebo-controlled, parallel-group study in outpatients. Am J Psychiatry. 2002;159(11):1869–1875. DOIPivotal 6-week RCT (Study 1) demonstrating selegiline patch 6 mg/24h superiority over placebo (HAM-D change −9 vs −6.5).
Amsterdam JD. A double-blind, placebo-controlled trial of the safety and efficacy of selegiline transdermal system without dietary restrictions in patients with major depressive disorder. J Clin Psychiatry. 2003;64(2):208–214. DOI8-week RCT (Study 2) showing selegiline patch efficacy at 6–12 mg/24h without dietary restrictions at 6 mg.
Amsterdam JD, Bodkin JA. Selegiline transdermal system in the prevention of relapse of major depressive disorder: a 52-week, double-blind, placebo-controlled trial. J Clin Psychopharmacol. 2006;26(6):579–586. DOI52-week relapse-prevention study (Study 3). Relapse: 16.8% EMSAM vs 29.4% placebo at week 26 (P=0.005); 17% vs 30.7% at week 52 (P=0.003).

Guidelines

American Psychiatric Association. Practice guideline for the treatment of patients with major depressive disorder, 3rd ed. Am J Psychiatry. 2010;167(10 Suppl):1–152. DOIAPA guideline referencing MAOIs including transdermal selegiline as treatment options for MDD.

Mechanistic / Basic Science

Azzaro AJ, Ziemniak J, Kemper E, Campbell BJ, VanDenBerg C. Pharmacokinetics and absolute bioavailability of selegiline following treatment of healthy subjects with the selegiline transdermal system (6 mg/24 h): a comparison with oral selegiline capsules. J Clin Pharmacol. 2007;47(10):1256–1267. DOIPK study demonstrating transdermal delivery produces higher selegiline and lower metabolite exposure vs oral, confirming the pharmacological basis for reduced tyramine interaction at 6 mg/24h.
Azzaro AJ, Ziemniak J, Kemper E, et al. Selegiline transdermal system: an examination of the potential for CYP450-dependent pharmacokinetic interactions with 3 psychotropic medications. J Clin Pharmacol. 2007;47(2):146–158. DOIPK interaction study confirming no clinically relevant interactions between EMSAM and alprazolam, olanzapine, or risperidone.

Pharmacokinetics / Special Populations

Robinson DS, Gilmor ML, Yang Y, Moonsammy G, Azzaro AJ, Oren DA, Campbell BJ. Treatment effects of selegiline transdermal system on symptoms of major depressive disorder: a meta-analysis of short-term, placebo-controlled, efficacy trials. Psychopharmacology (Berl). 2007;190(3):397–408. DOIMeta-analysis of EMSAM short-term trials confirming efficacy across symptom domains of MDD.
Lee KC, Chen JJ. Transdermal selegiline for the treatment of major depressive disorder. Neuropsychiatr Dis Treat. 2007;3(5):527–537. PMCComprehensive review of EMSAM efficacy, safety, PK properties, and drug-drug interactions for MDD treatment.
Patkar AA, Pae CU, Grier DK, Gabbard R, Masand PS. Selegiline transdermal system: a review of its use in major depressive disorder. Drugs Today (Barc). 2007;43(6):361–377. DOIClinical review discussing EMSAM’s pharmacology, tyramine sensitivity data, and practical prescribing considerations.