Tranylcypromine: Comprehensive Drug Monograph

Pharmacokinetic Profile

Plasma Half-Life

~2.5 h (range 1.5–3.2 h)

MAO Inhibition Duration

Irreversible; persists up to 10 days after discontinuation

Metabolism

Hepatic; inhibits CYP2A6

Tmax

1–2 hours (biphasic possible)

Volume of Distribution

1.1–5.7 L/kg

Clinical Information

Drug Class

Non-selective, irreversible MAOI (non-hydrazine; cyclopropylamine)

Available Doses

10 mg tablets only

Route

Oral

Renal Adjustment

No guidance; use caution

Hepatic Adjustment

No guidance; monitor for CNS effects (sedation in cirrhosis)

Pregnancy

Potential risk to fetus (limited data)

Lactation

Discontinue breastfeeding

Schedule / Legal Status

Not a controlled substance

Generic Available

Yes

Black Box Warning

Suicidality + Hypertensive crisis with tyramine

Dietary Restriction

Strict low-tyramine diet required

Indications

Indication	Approved Population	Therapy Type	Status
Major Depressive Disorder (MDD)	Adults who have not responded adequately to other antidepressants	Second-line or later monotherapy	FDA Approved

Tranylcypromine is a non-hydrazine, irreversible MAOI structurally related to amphetamine (a cyclopropylamine derivative), first approved in 1961. The updated 2023 PI explicitly states it is indicated for MDD in adults who have not responded adequately to other antidepressants and is not intended for initial treatment of MDD due to the potential for serious adverse reactions, drug interactions, and the need for dietary restrictions. Despite these constraints, tranylcypromine remains a highly effective antidepressant, and some clinicians prefer it over phenelzine because of its more activating profile and potentially faster onset of action.

Off-Label Uses

Atypical depression — Well-established efficacy particularly when psychomotor retardation or endogenous features are present; may be preferred over phenelzine in this subtype. (Evidence quality: Moderate)

Treatment-resistant depression — Used after failure of SSRIs, SNRIs, and TCAs; meta-analyses support efficacy comparable to TCAs. (Evidence quality: Moderate)

Social anxiety disorder — Evidence extrapolated from phenelzine data and clinical experience. (Evidence quality: Low)

Panic disorder — Used when first-line agents fail. (Evidence quality: Low)

Dose

Dosing

Adult Dosing by Clinical Scenario

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Dose	Notes
MDD — treatment-resistant	30 mg/day in divided doses	30–60 mg/day	60 mg/day (30 mg BID)	If no response by 2 weeks, increase by 10 mg/day every 1–3 weeks Improvement may be seen within 48 h to 3 weeks (per PI); administer earlier in day to reduce insomnia
Atypical depression (off-label)	10–20 mg/day	30–60 mg/day	60 mg/day	May be preferred over phenelzine when psychomotor retardation predominates More activating profile; amphetamine-like structure may provide early energy boost
Anxiety disorders (off-label)	10 mg BID	30–40 mg/day	60 mg/day	Lower doses often sufficient for anxiolytic effect At doses >40 mg, norepinephrine reuptake inhibition adds to pharmacological profile

Special Population Adjustments

Population	Starting Dose	Maintenance Dose	Maximum Dose	Notes
Elderly (≥65 years)	10 mg QD	Titrate cautiously	Individualize (lower doses)	Greater risk of postural hypotension and other serious adverse reactions More gradual dosage increases per PI
Hepatic impairment	Use caution; no specific guidance			Sedation reported in patients with cirrhosis; monitor for increased CNS adverse reactions (PI Section 5.10)
Renal impairment	Use caution; no specific guidance			Manufacturer labelling does not provide dose adjustments

Clinical Pearl: Tranylcypromine vs Phenelzine — Key Differences

Tranylcypromine is a non-hydrazine MAOI structurally related to amphetamine. It has a much shorter plasma half-life (~2.5 h vs ~11.6 h for phenelzine) and a somewhat shorter duration of MAO inhibition after discontinuation (~10 days vs ~14–21 days for phenelzine). At higher doses (40–60 mg/day), it additionally inhibits norepinephrine reuptake, producing a more activating profile. Postural hypotension is the major dose-limiting side effect above 30 mg/day. Unlike phenelzine, it does not deplete vitamin B6 (since it is not a hydrazine), and hepatotoxicity appears to be less common.

Tranylcypromine Pharmacology

Mechanism of Action

Tranylcypromine is a non-selective, irreversible inhibitor of both MAO-A and MAO-B at therapeutic doses (20–30 mg/day). By inactivating these enzymes, it prevents the degradation of serotonin, norepinephrine, dopamine, and trace amines (particularly phenylethylamine) in the brain and periphery. At higher doses (40–60 mg/day), tranylcypromine additionally inhibits norepinephrine reuptake, an action related to its structural similarity to amphetamine. It also increases brain GABA-B receptor density and modulates phospholipid metabolism. The increase in trace amines, particularly phenylethylamine (which acts as an endogenous amphetamine-like releasing agent), may contribute to its activating properties and potentially faster onset of action compared with phenelzine. Tranylcypromine also inhibits lysine-specific demethylase 1 (LSD1), an epigenetic regulator — a property being investigated in oncology.

ADME Profile

Parameter	Value	Clinical Implication
Absorption	Rapidly absorbed; Tmax 1–2 h (biphasic absorption possible with secondary peak at 2–3 h); Cmax 50–200 ng/mL after 20 mg	Fast absorption supports twice-daily dosing; administer morning and early afternoon to minimise insomnia
Distribution	Vd 1.1–5.7 L/kg; protein binding high (not precisely characterised)	Wide interindividual variability in distribution; amphetamine-like structure may contribute to CNS penetration
Metabolism	Hepatic; metabolites include 4-hydroxytranylcypromine and N-acetyltranylcypromine (less potent MAO inhibitors); inhibits CYP2A6 at therapeutic doses; does not significantly inhibit other CYP enzymes	CYP2A6 inhibition may increase plasma nicotine levels in smokers; low potential for pharmacokinetic interactions with most drugs via CYP pathways
Elimination	Plasma t½ ~2.5 h (range 1.5–3.2 h); excretion primarily urinary, rapid within 24 h; MAO inhibition persists up to 10 days after last dose	Short plasma half-life is clinically misleading — irreversible MAO inhibition far outlasts drug presence; dietary/drug restrictions must continue for ≥2 weeks after stopping (PI Section 5.2)

Side Effects

The updated Parnate PI (revised 11/2023) provides frequency categories from clinical trial data. The most common adverse reactions (>30%) were dry mouth, dizziness, insomnia, sedation, and headache. Adverse reactions occurring in >10% additionally include overexcitement, constipation, blurred vision, and tremor.

>30%Very Common (PI: >30%)

Adverse Effect	Frequency Category	Clinical Note
Dry mouth	>30%	Anticholinergic-like effect; encourage oral hygiene, sugar-free gum (PI Section 6)
Dizziness	>30%	Orthostatic component; postural hypotension is a major side effect above 30 mg/day and may cause syncope (PI Section 5.5)
Insomnia	>30%	Related to activating/amphetamine-like properties; administer doses earlier in the day (PI Section 6)
Sedation / drowsiness	>30%	Paradoxically coexists with insomnia in some patients; caution with driving (PI Section 5.14)
Headache	>30%	Headaches without BP elevation reported; ALWAYS rule out hypertensive crisis if sudden occipital headache (PI Sections 5.2, 6)

>10%Common (PI: >10%)

Adverse Effect	Frequency Category	Clinical Note
Overexcitement / stimulation	>10%	Amphetamine-like activation; may require dose reduction; assess for hypomania (PI Sections 5.4, 6)
Constipation	>10%	Increase fibre and fluids (PI Section 6)
Blurred vision	>10%	Rule out angle closure if eye pain; nystagmus also reported (PI Section 6)
Tremor	>10%	Fine postural tremor; dose-related; myoclonic jerks also reported (PI Section 6)

Other ReportedOther Reported Adverse Reactions (PI Section 6)

Adverse Effect	Clinical Note
Postural hypotension / syncope	Major dose-limiting adverse effect above 30 mg/day; may result in syncope; monitor standing BP (PI Section 5.5)
Weight gain	Significant anorexia also reported; metabolic effects variable (PI Section 6)
Sexual dysfunction (impotence, delayed ejaculation)	Serotonergic effect; impacts adherence (PI Section 6)
Tachycardia / palpitations	Cardiovascular; obtain ECG if symptomatic (PI Section 6)
Edema	Peripheral; may respond to dose reduction (PI Section 6)
Paresthesia / numbness	Unlike phenelzine, not related to vitamin B6 depletion (non-hydrazine) (PI Section 6)
Anorexia	Significant; may be related to amphetamine-like properties (PI Section 6)
Urinary retention / frequency / incontinence	Genitourinary effects; assess for obstruction (PI Section 6)

SeriousSerious (regardless of frequency)

Adverse Effect	Estimated Frequency	Typical Onset	Required Action
Hypertensive crisis	Rare (with proper diet); potentially fatal	Minutes to hours after tyramine ingestion or drug interaction	Discontinue immediately; treat hypertensive emergency; ED admission (PI Section 5.2)
Serotonin syndrome	Rare (with contraindicated drug); potentially fatal	Hours after exposure to serotonergic agent	Discontinue all serotonergic agents; supportive care; cyproheptadine (PI Section 5.3)
Suicidal ideation / behaviour	Uncommon (age-dependent)	First weeks to months	Close monitoring especially <25 years; consider stopping if emergent suicidality (PI Section 5.1)
Hepatitis / elevated aminotransferases	Rare	Weeks to months	Monitor LFTs; discontinue if hepatotoxicity signs develop (PI Section 5.10)
Mania / hypomania	Uncommon	First weeks	Discontinue; screen for bipolar disorder (PI Section 5.4)
Seizures	Rare (reported with withdrawal and overdose)	Variable	Manage per protocol; monitor at-risk patients (PI Section 5.11)
SIADH / hyponatraemia	Rare	Weeks	Check sodium; fluid restriction; discontinue if severe (PI Section 6)
Agranulocytosis / blood dyscrasias	Very rare	Variable	Check FBC; discontinue if significant cytopaenia (PI Section 6)

DiscontinuationDiscontinuation & Withdrawal

Withdrawal Effects

Gradual taper required

Delirium reported with abrupt discontinuation. Higher daily doses and longer duration of use correlate with higher risk. Symptoms include dizziness, nausea, insomnia, anxiety, irritability, paraesthesia, and seizures (PI Section 5.8).

MAO Inhibition Persistence

Up to 10 days

Dietary and drug restrictions must continue for at least 2 weeks after the last dose (PI Section 5.2). Wait at least 1 week before starting another MAOI or contraindicated antidepressant; wait 5 weeks after stopping fluoxetine before starting tranylcypromine (PI Sections 5.9, 7.1).

Hypertensive Crisis: The Critical Safety Concern

Hypertensive emergencies (BP >180/120 mmHg with organ dysfunction) may present with severe occipital headache, palpitations, neck stiffness, nausea, sweating, dilated pupils, photophobia, and chest pain. Seizures and intracranial haemorrhage (sometimes fatal) have been reported. All patients must carry a list of prohibited foods and drugs, and should be instructed to seek emergency care immediately if they develop sudden severe headache. The PI contains two boxed warnings — one for suicidality and one specifically for hypertensive crisis with tyramine (PI Section 5.2).

Int

Drug Interactions

Tranylcypromine has an extensive contraindicated drug list (PI Tables 1, 3, and 4). Because MAO inhibition persists up to 10 days after discontinuation, interactions can occur even after the drug is stopped. Unlike phenelzine, tranylcypromine inhibits CYP2A6 at therapeutic concentrations but has low potential for other CYP-mediated interactions.

MajorTyramine-Rich Foods

MechanismTyramine causes norepinephrine release; MAO inhibition prevents degradation

EffectPotentially fatal hypertensive crisis

ManagementStrict avoidance of aged cheeses, cured meats, fava beans, sauerkraut, beer, wine, yogurt, yeast extract; restrictions continue ≥2 weeks after stopping

FDA PI (Boxed Warning)

MajorSerotonergic Drugs (SSRIs, SNRIs, TCAs, triptans, tramadol, meperidine, dextromethorphan, tryptophan, SAM-e, St John’s Wort)

MechanismMAO inhibition + serotonin reuptake blockade = serotonin excess

EffectLife-threatening serotonin syndrome; features may resemble NMS

ManagementContraindicated. Wait 4–5 half-lives of prior drug before starting TCP; 5 weeks for fluoxetine; 1 week after stopping TCP before starting another agent

FDA PI (Table 1, Section 7.1)

MajorSympathomimetics (amphetamines, pseudoephedrine, methylphenidate, dopamine, ephedrine)

MechanismPotentiation of catecholamine effects

EffectHypertensive crisis including risk of intracranial haemorrhage

ManagementContraindicated; includes OTC cold/decongestant preparations and dietary supplements

FDA PI (Tables 1, 3)

MajorOther MAOIs, Bupropion, Buspirone, Carbamazepine, Cyclobenzaprine

MechanismAdditive MAO inhibition or serotonergic effects

EffectSerotonin syndrome, hypertensive crisis, seizures

ManagementAll contraindicated; see PI Table 1 for complete list

FDA PI (Table 1)

ModerateAntihypertensives / CNS Depressants (including alcohol, opioids)

MechanismAdditive hypotensive or CNS depressant effects

EffectExaggerated hypotension, excessive sedation

ManagementUse with caution; monitor BP; adjust doses as needed

FDA PI (Table 3)

ModerateBlood Glucose-Lowering Agents

MechanismMAOIs may increase insulin sensitivity

EffectExcessive blood glucose reduction

ManagementMonitor glucose; reduce hypoglycaemic agent dose as needed

FDA PI (Section 5.12)

Mon

Monitoring

Blood PressureBaseline; every visit; orthostatic during titration
RoutinePostural hypotension is a major side effect above 30 mg/day. Also monitor for hypertensive episodes (sudden headache, palpitations) that may indicate dietary non-compliance. Assess BP before prescribing per PI Section 2.4.
Liver FunctionBaseline; periodically
RoutineHepatitis and elevated aminotransferases reported. Discontinue if signs/symptoms of hepatotoxicity develop. Monitor for sedation in patients with cirrhosis (PI Section 5.10).
Mental StateEvery visit for first 3 months
RoutineMonitor for suicidality, mania/hypomania, psychosis, overexcitement, and anxiety aggravation. Screen for bipolar disorder before initiation (PI Sections 5.1, 5.4, 5.13).
Dietary ComplianceEvery visit
RoutineReview tyramine-restricted diet and medication restrictions. Ensure patient has written list and understands the 2-week post-discontinuation restriction period.
WeightBaseline, then every 3 months
RoutineBoth weight gain and significant anorexia reported. Monitor in both directions.
Blood GlucoseIf diabetic
Trigger-BasedMAOIs may contribute to hypoglycaemia in diabetic patients (PI Section 5.12).
Renal FunctionBaseline
RoutineNo specific guidance in PI, but renal function should be assessed given primary urinary excretion.

Contraindications & Cautions

Absolute Contraindications

Pheochromocytoma or catecholamine-releasing paraganglioma (PI Section 4.2)
Concomitant or recent use of contraindicated drugs (PI Table 1): other MAOIs, SSRIs, SNRIs, TCAs, bupropion, triptans, sympathomimetics, amphetamines, meperidine, dextromethorphan, carbamazepine, cyclobenzaprine, buspirone, levodopa, methyldopa, dopamine, tryptophan, SAM-e, rasagiline, tetrabenazine, tapentadol, non-selective H1 antihistamines
Tyramine-containing foods and beverages during treatment and for 2 weeks after

Relative Contraindications (Specialist Input Recommended)

Bipolar disorder (unscreened) — risk of manic switching (PI Section 5.4)
Hyperthyroidism — greater risk of hypertensive crisis (PI Section 5.2)
Cerebrovascular or cardiovascular disease — increased risk from hypertensive complications
Hepatic impairment — sedation in cirrhosis; hepatitis reported (PI Section 5.10)

Use with Caution

Elderly — greater risk of postural hypotension and other serious reactions; start at lower doses
Patients at risk of suicide — prescribe smallest feasible quantity; MAOI overdose is frequently fatal
Patients requiring surgery — discontinue at least 10 days before elective surgery (PI Section 5.6)
Diabetic patients — hypoglycaemia risk (PI Section 5.12)
History of drug abuse — abuse potential at high doses due to amphetamine-like structure (reported at 120–600 mg/day)

FDA Boxed Warning (Dual) 1. Suicidal Thoughts and Behaviours

Antidepressants increase the risk of suicidal thinking and behaviour in paediatric and young adult patients. Risk was 14 additional patients per 1,000 treated (<18 years) and 5 additional per 1,000 (18–24 years). Tranylcypromine is not approved for paediatric use. Monitor all patients closely.

2. Hypertensive Crisis with Tyramine

Excessive consumption of foods or beverages with significant tyramine content, or use of certain drugs, can precipitate hypertensive crisis during tranylcypromine treatment or after discontinuation. Monitor blood pressure, allow for medication-free intervals, and advise patients to avoid high-tyramine foods and beverages.

Patient Counselling

Purpose of Therapy

Tranylcypromine works by blocking an enzyme (monoamine oxidase) that breaks down mood-regulating brain chemicals. This allows serotonin, norepinephrine, and dopamine to build up and improve mood. It is prescribed when other antidepressants have not worked. The medication requires strict dietary restrictions because certain foods can cause a dangerous blood pressure spike.

How to Take

Take tranylcypromine in divided doses, typically in the morning and early afternoon to reduce the risk of insomnia. It may take up to 3 weeks to notice improvement, though some patients respond within days. Do not stop the medication abruptly — your doctor will reduce the dose gradually.

Food Restrictions (CRITICAL)

Tell patientYou MUST avoid certain foods containing tyramine while taking this medication and for at least 2 weeks after stopping. These include: aged cheeses, cured or smoked meats, pickled herring, fava beans, sauerkraut, yogurt, beer, wine, yeast extract, and improperly refrigerated protein-rich foods. You will receive a complete list. Eating these foods can cause a sudden, dangerous spike in blood pressure.

Call prescriberImmediately if you develop a sudden severe headache (especially at the back of the head), rapid heartbeat, neck stiffness, nausea with sweating, or sensitivity to light — go to the emergency department.

Medication Restrictions (CRITICAL)

Tell patientMany common medications are dangerous with tranylcypromine, including cold and cough remedies, nasal decongestants, diet pills, and certain pain medications. Always check with your pharmacist or prescriber before taking ANY new medication, including over-the-counter products. Inform all healthcare providers that you take an MAOI.

Call prescriberBefore starting any new medication. Carry an MAOI alert card or medical ID bracelet at all times.

Dizziness & Blood Pressure

Tell patientLightheadedness when standing up is common, especially at higher doses. Stand up slowly. This can sometimes lead to fainting. Report persistent dizziness to your prescriber.

Call prescriberIf you faint or feel close to fainting, or if dizziness significantly limits your daily activities.

Insomnia & Overexcitement

Tell patientThis medication can be stimulating. Take your doses earlier in the day (morning and early afternoon) rather than in the evening. If you feel unusually restless, agitated, or unable to sleep, report this promptly.

Call prescriberIf insomnia is severe or persistent, or if you feel unusually excited, racing, or euphoric — these may indicate the dose is too high or a manic episode.

Surgery & Emergencies

Tell patientTranylcypromine must be stopped at least 10 days before planned surgery. In an emergency, always tell medical staff you take an MAOI — carry an alert card. Certain anaesthetics and pain medications are dangerous with this drug.

Call prescriberWell in advance of any planned medical or dental procedures.

Stopping Treatment

Tell patientDo not stop tranylcypromine suddenly — this can cause withdrawal symptoms including confusion, dizziness, and in rare cases delirium. Your prescriber will plan a gradual dose reduction. Continue to follow dietary restrictions for at least 2 weeks after the last dose.

Call prescriberIf you experience withdrawal symptoms or wish to discontinue treatment.

Ref

Sources

Regulatory (PI / SmPC)

Parnate (tranylcypromine) Tablets — Full Prescribing Information. Revised November 2023. DailyMedPrimary source for FDA-approved indication, dosing, adverse reactions (with frequency categories), contraindications, and drug/food interactions. Modern label format with Tables 1–4 for interactions.

Key Clinical Trials

Himmelhoch JM, Thase ME, Mallinger AG, Houck P. Tranylcypromine versus imipramine in anergic bipolar depression. Am J Psychiatry. 1991;148(7):910–916. DOIKey trial demonstrating tranylcypromine superiority over imipramine in anergic bipolar depression.
Thase ME, Trivedi MH, Rush AJ. MAOIs in the contemporary treatment of depression. Neuropsychopharmacology. 1995;12(3):185–219. DOIComprehensive review and meta-analysis of MAOI efficacy in depression, including tranylcypromine comparison with TCAs.
Laux G, Volz HP, Möller HJ. Newer and older monoamine oxidase inhibitors: a comparative profile. CNS Drugs. 1995;3(2):145–158. DOIComparative review of MAOIs including tranylcypromine, with efficacy and side-effect data.

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 recommending MAOIs for treatment-resistant depression after failure of multiple first-line agents.
Bauer M, Pfennig A, Severus E, et al. World Federation of Societies of Biological Psychiatry (WFSBP) guidelines for biological treatment of unipolar depressive disorders. World J Biol Psychiatry. 2013;14(5):334–385. DOIInternational guideline positioning MAOIs as a treatment option in refractory depression with evidence-graded recommendations.

Mechanistic / Basic Science

Schildkraut JJ. The catecholamine hypothesis of affective disorders: a review of supporting evidence. Am J Psychiatry. 1965;122(5):509–522. DOIFoundational paper establishing the monoamine hypothesis of depression that underpins MAOI pharmacology.
Bortolato M, Chen K, Shih JC. Monoamine oxidase inactivation: from pathophysiology to therapeutics. Adv Drug Deliv Rev. 2008;60(13–14):1527–1533. DOIComprehensive review of MAO biochemistry and the pharmacological basis of irreversible MAO inhibition.

Pharmacokinetics / Special Populations

Schiebeler H, Laux G, Möller HJ. Tranylcypromine in mind (Part I): review of pharmacology. Eur Neuropsychopharmacol. 2017;27(8):697–713. DOIDefinitive 2017 review of tranylcypromine pharmacodynamics, pharmacokinetics, drug interactions, and toxicology. Source for plasma t½ 2 h, pharmacodynamic t½ ~1 week, and CYP2A6 inhibition data.
Mallinger AG, Edwards DJ, Himmelhoch JM, Knopf S, Ehler J. Pharmacokinetics of tranylcypromine in patients who are depressed: relationship to cardiovascular effects. Clin Pharmacol Ther. 1986;40(4):444–450. DOIPK study in depressed patients linking tranylcypromine plasma levels to hypotensive effects and clinical outcome.
Gillman PK. Monoamine oxidase inhibitors, opioid analgesics and serotonin toxicity. Br J Anaesth. 2005;95(4):434–441. DOIDefinitive review of MAOI-opioid interactions, clarifying which opioids are safe and which are contraindicated.
StatPearls: Tranylcypromine. In: StatPearls [Internet]. Treasure Island, FL: StatPearls Publishing; updated January 19, 2025. NCBI BookshelfPeer-reviewed clinical summary covering indications, PK (Vd 1.1–5.7 L/kg, t½ 1.5–3.2 h), adverse effects, and monitoring.