Phenelzine: Comprehensive Drug Monograph

Pharmacokinetic Profile

Plasma Half-Life

~11.6 h (single dose)

MAO Inhibition Duration

Irreversible; 2–3 weeks for MAO regeneration

Metabolism

Oxidation via MAO; minor acetylation

Tmax

~43 minutes

Excretion

73% urine (as metabolites within 96 h)

Clinical Information

Drug Class

Non-selective, irreversible MAOI (hydrazine)

Available Doses

15 mg tablets only

Route

Oral

Renal Adjustment

Contraindicated in severe renal impairment

Hepatic Adjustment

Contraindicated with liver disease or abnormal LFTs

Pregnancy

Safety not established

Lactation

Safety not established

Schedule / Legal Status

Not a controlled substance

Generic Available

Yes

Black Box Warning

Suicidality in children & young adults

Dietary Restriction

Strict low-tyramine diet required

Indications

Indication	Approved Population	Therapy Type	Status
Depression (atypical, nonendogenous, neurotic)	Adults	Second-line or later monotherapy	FDA Approved

Phenelzine is a non-selective, irreversible monoamine oxidase inhibitor of the hydrazine class, first approved in 1961. The FDA label specifically notes it is effective in patients with depression characterised as “atypical,” “nonendogenous,” or “neurotic” — patients who often present with mixed anxiety and depression, phobic features, or hypochondriacal symptoms. The label explicitly states that phenelzine should rarely be the first antidepressant used and is more suitable for patients who have failed other treatments. Despite its dietary and drug-interaction constraints, phenelzine remains one of the most effective antidepressants available, particularly for atypical depression and social anxiety disorder.

Off-Label Uses

Social anxiety disorder — Six placebo-controlled RCTs demonstrate strong efficacy; effect size among the largest of any pharmacotherapy for social anxiety (ES ~1.02). (Evidence quality: High)

Panic disorder — Effective in multiple controlled trials; generally reserved for SSRI/SNRI failures. (Evidence quality: High)

Treatment-resistant depression — Commonly used when multiple first-line agents have failed; some clinicians regard MAOIs as underutilised in this setting. (Evidence quality: Moderate)

PTSD — Limited controlled data but clinical use in veterans and trauma populations. (Evidence quality: Low)

Bulimia nervosa — Some evidence for efficacy, though SSRIs are preferred. (Evidence quality: Low)

Dose

Dosing

Adult Dosing by Clinical Scenario

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Dose	Notes
Atypical / treatment-resistant depression	15 mg TID (45 mg/day)	60–90 mg/day	90 mg/day	Increase rapidly to ≥60 mg/day as tolerated; clinical response may take ≥4 weeks at 60 mg After maximum benefit, reduce slowly to maintenance as low as 15 mg/day or QOD
Social anxiety disorder (off-label)	15 mg BID (30 mg/day)	45–90 mg/day	90 mg/day	Dose range from clinical trials: 45–90 mg/day; response typically within 6–8 weeks Start lower than for depression if tolerability is a concern
Panic disorder (off-label)	15 mg QD–BID	45–90 mg/day	90 mg/day	Some patients respond to lower doses than needed for depression Anxiolytic effects may appear earlier than antidepressant effects

Special Population Adjustments

Population	Starting Dose	Maintenance Dose	Maximum Dose	Notes
Elderly (≥65 years)	15 mg QD	Titrate cautiously	Individualize (lower doses)	Greater frequency of decreased hepatic, renal, and cardiac function Higher orthostatic hypotension risk; monitor BP closely
Hepatic impairment	Contraindicated			History of liver disease or abnormal LFTs is a contraindication per PI
Severe renal impairment	Contraindicated			Contraindicated in severe renal impairment or renal disease per PI

Clinical Pearl: Irreversible MAO Inhibition vs Plasma Half-Life

The plasma elimination half-life of phenelzine is only ~11.6 hours, but this is clinically misleading. Because phenelzine irreversibly inactivates MAO, the duration of biological effect far outlasts the drug’s presence in plasma. After discontinuation, it takes approximately 2–3 weeks for the body to synthesise sufficient new MAO enzyme to restore normal monoamine metabolism. This is why dietary restrictions and drug washout periods must continue for at least 14 days (and up to 3–4 weeks for initiating another antidepressant) after stopping phenelzine.

Phenelzine Pharmacology

Mechanism of Action

Phenelzine is a hydrazine derivative that irreversibly inhibits both isoforms of monoamine oxidase — MAO-A and MAO-B — with a slight preference for MAO-A. By inactivating these enzymes, phenelzine prevents the intraneuronal breakdown of serotonin, norepinephrine, dopamine, epinephrine, and melatonin, leading to increased concentrations of these monoamines in the synaptic cleft. Beyond monoamine oxidase inhibition, phenelzine’s metabolite phenylethylidenehydrazine (PEH) inhibits GABA-transaminase, resulting in elevated brain GABA levels. This GABAergic action is thought to contribute significantly to phenelzine’s anxiolytic and antipanic properties. Phenelzine also inhibits alanine transaminase (ALA-T), which may be related to the rare hepatotoxicity associated with hydrazine MAOIs. Additionally, phenelzine is metabolised to phenylethylamine (PEA), a trace amine that acts as a releasing agent of norepinephrine and dopamine. The antidepressant effect typically requires 2–4 weeks to manifest, reflecting the time needed for cumulative MAO inhibition and downstream neuroadaptive changes.

ADME Profile

Parameter	Value	Clinical Implication
Absorption	Rapidly absorbed; Cmax 19.8 ng/mL after 30 mg; Tmax ~43 minutes	Fast absorption allows TID dosing schedule; food effects not characterised in the PI
Distribution	Widely distributed; protein binding not formally characterised	Broad tissue distribution underlies diverse pharmacological effects throughout the body
Metabolism	Primarily by oxidation via MAO to phenylacetic acid and parahydroxyphenylacetic acid (73% urinary recovery); minor acetylation to N2-acetylphenelzine; metabolised to PEH and PEA	Phenelzine is both a substrate and an irreversible inhibitor of MAO — the drug destroys the enzyme it is metabolised by; acetylator phenotype is not a major determinant of clinical effect
Elimination	Plasma t½ ~11.6 h (single 30 mg dose); 73% recovered in urine within 96 h as metabolites; multiple-dose PK not studied	Plasma half-life does not reflect duration of biological effect (MAO inhibition is irreversible); dietary and drug restrictions must continue ≥14 days after last dose

Side Effects

The Nardil PI (approved 1961) lists adverse effects by frequency category without specific percentages from controlled trials. The estimates below are derived from published clinical experience and reviews, with the source noted. Exact incidence figures should be interpreted as approximate ranges rather than precise percentages.

Common Common (listed as “Common” in Nardil PI)

Adverse Effect	Estimated Incidence	Clinical Note
Orthostatic hypotension	20–30%	Most clinically significant common effect; peaks 10–14 days after dose increase; rise slowly from sitting or lying (PI, clinical literature)
Weight gain	15–25%	Can be substantial (average 2–3 kg, some patients much more); increased appetite and carbohydrate craving (PI)
Drowsiness / sedation	15–25%	Often improves with continued treatment; consider dosing adjustment (PI)
Sleep disturbance (insomnia / hypersomnia)	15–25%	Insomnia from serotonergic and GABA effects; hypersomnia less common; take last dose before mid-afternoon (PI)
Dizziness	15–25%	Related to orthostatic and central effects (PI)
Sexual dysfunction (anorgasmia, impotence)	20–40%	Serotonergic effect; major cause of non-adherence; dose reduction may help (PI, clinical literature)
Dry mouth	15–20%	Encourage oral hygiene, sugar-free gum (PI)
Constipation	10–20%	Increase fibre and fluids (PI)
Headache	10–15%	Distinguish from occipital headache of hypertensive crisis — latter is a medical emergency (PI)
Fatigue / weakness	10–15%	Often improves over weeks (PI)
Peripheral edema	10–15%	May respond to compression stockings or dose reduction (PI)
Tremor / twitching / myoclonic movements	5–15%	Dose-related; myoclonus may indicate serotonergic excess (PI)

Less Common Less Common (PI: “mild to moderate”)

Adverse Effect	Estimated Incidence	Clinical Note
Paresthesias	~5%	May relate to vitamin B6 depletion by hydrazine; pyridoxine supplementation can help (PI, clinical literature)
Blurred vision	~5%	Rule out glaucoma if eye pain present (PI)
Urinary retention	<5%	Caution in prostatic hypertrophy (PI)
Pruritus / skin rash	<5%	Assess for hypersensitivity (PI)
Jitteriness / euphoria	<5%	May indicate hypomanic activation (PI)
Hypernatremia	<5%	Monitor sodium if symptoms of fluid retention (PI)
Elevated transaminases	Infrequent	Usually without clinical symptoms; may rarely precede hepatotoxicity (PI)

Serious Serious (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 phenelzine immediately; IV phentolamine 5 mg; external cooling for fever; ED admission
Serotonin syndrome	Rare (with contraindicated drug combinations)	Hours after exposure to serotonergic agent	Discontinue all serotonergic agents; supportive care; cyproheptadine; ICU if severe
Hepatotoxicity (necrotizing hepatocellular)	Very rare; potentially fatal	Weeks to months	Monitor LFTs; discontinue immediately at first sign of jaundice or significant transaminase elevation
Suicidal ideation / behaviour	Uncommon (age-dependent)	First weeks to months	Close monitoring especially <25 years; consider stopping if emergent suicidality
Hypomania / mania	Uncommon	First weeks; more common in bipolar spectrum	Discontinue; assess for bipolar disorder; initiate mood stabiliser
Seizures	Rare	Variable	Discontinue phenelzine; manage seizures per protocol
Withdrawal syndrome (vivid nightmares, agitation, psychosis)	Uncommon (with abrupt discontinuation)	24–72 hours after abrupt withdrawal	Reinstitute low-dose phenelzine; taper cautiously; never stop abruptly
Leukopenia	Very rare	Variable	Check FBC; discontinue if significant cytopaenia

Discontinuation Discontinuation & Withdrawal

Withdrawal Syndrome

Taper required

Abrupt withdrawal can cause agitation, vivid nightmares, psychosis, or seizures (onset 24–72 h). Reinstitution of low-dose phenelzine followed by cautious taper is the recommended treatment.

Washout Period

≥14 days

Dietary and drug restrictions must continue for at least 14 days after the last dose. Wait 3–4 weeks before starting another antidepressant; wait at least 5 weeks after stopping fluoxetine before starting phenelzine (due to fluoxetine’s long half-life metabolite).

Hypertensive Crisis: Recognition and Emergency Treatment

Hypertensive crises are characterised by sudden-onset occipital headache (may radiate frontally), palpitations, neck stiffness, nausea, vomiting, diaphoresis, dilated pupils, and photophobia. Tachycardia or bradycardia may be present. Intracranial haemorrhage has been reported. Treatment: discontinue phenelzine immediately; administer IV phentolamine 5 mg slowly; manage fever with external cooling. 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.

Int

Drug Interactions

Phenelzine has one of the most extensive and dangerous drug interaction profiles of any medication in clinical use. Because it irreversibly inhibits MAO, interactions persist for 2–3 weeks after discontinuation. The categories below highlight the most critical interactions; prescribers should also consult a comprehensive interaction database.

MajorTyramine-Rich Foods

MechanismTyramine displaces norepinephrine from vesicles; MAO inhibition prevents degradation, causing catecholamine surge

EffectPotentially fatal hypertensive crisis

ManagementStrict avoidance of aged cheeses, pickled herring, liver, dry sausage, fava beans, sauerkraut, yogurt, beer, wine, yeast extract, and improperly stored protein-rich foods. Restrictions continue ≥14 days after stopping

FDA PI

MajorSerotonergic Drugs (SSRIs, SNRIs, TCAs, triptans, tramadol, tryptophan)

MechanismMAO inhibition + serotonin reuptake inhibition = serotonin excess

EffectLife-threatening serotonin syndrome; hyperthermia, rigidity, coma, death

ManagementContraindicated. 14-day washout both directions; 5 weeks after fluoxetine due to its long half-life metabolite

FDA PI

MajorSympathomimetics (amphetamines, methylphenidate, pseudoephedrine, cocaine)

MechanismPotentiation of catecholamine effects via MAO inhibition

EffectHypertensive crisis; includes OTC decongestants and cold preparations

ManagementContraindicated. Also includes dopamine, epinephrine, norepinephrine, methyldopa, and L-dopa

FDA PI

MajorMeperidine (Pethidine)

MechanismSerotonin reuptake inhibition by meperidine + MAO inhibition

EffectExcitation, seizures, delirium, hyperpyrexia, circulatory collapse, death — even a single dose

ManagementAbsolutely contraindicated. Other opioids carry lesser but still significant risk

FDA PI

MajorOther MAOIs, Bupropion, Buspirone

MechanismExcessive monoamine accumulation or additive serotonergic/noradrenergic effects

EffectSeizures, hypertensive crisis, serotonin syndrome

ManagementContraindicated. 14-day washout between MAOIs; elevated BP reported with buspirone

FDA PI

MajorDextromethorphan

MechanismSerotonin reuptake inhibition by dextromethorphan

EffectSerotonin syndrome; bizarre behaviour reported

ManagementContraindicated; patients must avoid all OTC cough preparations containing dextromethorphan

FDA PI

ModerateAntihypertensives / Thiazide Diuretics / Beta-Blockers

MechanismAdditive hypotensive effects

EffectExaggerated hypotension

ManagementUse with caution; monitor BP closely; dose adjustments may be needed

FDA PI

ModerateInsulin / Oral Hypoglycaemics

MechanismMAOIs may increase insulin sensitivity

EffectPotential hypoglycaemia

ManagementMonitor glucose closely; may need to reduce insulin/hypoglycaemic dose

FDA PI

Mon

Monitoring

Blood Pressure Every visit; orthostatic at baseline and during titration
Routine Orthostatic hypotension is the most common clinically significant effect. Measure lying and standing BP. Systolic drop ≥20 mmHg or diastolic drop ≥10 mmHg is significant. Also monitor for hypertensive episodes (headache, palpitations) that may signal dietary non-compliance.
Liver Function Baseline; periodically during treatment
Routine Contraindicated with abnormal LFTs or liver disease. Rare but fatal hepatocellular necrosis reported. Monitor transaminases; discontinue immediately if jaundice or significant elevation occurs.
Weight Baseline, then every 1–3 months
Routine Weight gain is common and can be substantial. Dietary counselling from treatment initiation.
Mental State Every visit for first 3 months
Routine Monitor for suicidality (especially <25 years), hypomania/mania, psychosis, and agitation. Screen for bipolar disorder before initiation.
Dietary Compliance Every visit
Routine Review tyramine-restricted diet and medication restrictions at every visit. Ensure patient has written list of prohibited foods and drugs. Assess understanding and adherence.
Vitamin B6 Status If paresthesias or neuropathic symptoms develop
Trigger-Based Phenelzine can deplete vitamin B6 via hydrazine metabolism. Pyridoxine supplementation (50–100 mg/day) may be considered if neuropathic symptoms arise. Use pyridoxine form, not pyridoxal.
Blood Glucose If diabetic
Trigger-Based MAOIs may increase insulin sensitivity. Monitor glucose closely in diabetic patients; insulin or oral hypoglycaemic dose may need reduction.

Contraindications & Cautions

Absolute Contraindications

Hypersensitivity to phenelzine or any component
Pheochromocytoma — catecholamine-secreting tumour; MAO inhibition causes catastrophic hypertension
Congestive heart failure
Severe renal impairment or renal disease
History of liver disease or abnormal liver function tests
Concurrent or recent use of: sympathomimetic drugs, meperidine, dextromethorphan, alcohol and CNS depressants, serotonergic agents (SSRIs, SNRIs, TCAs, triptans, tramadol, tryptophan), other MAOIs, bupropion, buspirone, linezolid, IV methylene blue, guanethidine, carbamazepine
Tyramine-containing foods — aged cheeses (cottage cheese and cream cheese are allowed), pickled herring, liver, dry sausage, fava beans, sauerkraut, yogurt, beer, wine, yeast extract; excessive amounts of chocolate and caffeine
General anaesthesia — discontinue ≥10 days before elective surgery

Relative Contraindications (Specialist Input Recommended)

Bipolar disorder (unscreened) — risk of manic switching; screen before initiation
Epilepsy — variable effect on seizure threshold; adequate precautions required
Poorly controlled diabetes — increased insulin sensitivity may cause hypoglycaemia

Use with Caution

Elderly — greater susceptibility to orthostatic hypotension; start low, go slow
Patients at risk of suicide — prescribe smallest feasible quantity; MAOI overdose is frequently fatal
Patients on antihypertensive therapy — exaggerated hypotension possible
Asthma patients — effects on sympathetic neurotransmission may alter bronchodilator response
Patients requiring surgery — discontinue ≥10 days before; avoid cocaine and local anaesthetics with sympathomimetic vasoconstrictors

FDA Boxed Warning Suicidal Thoughts and Behaviours

Antidepressants, including phenelzine, increase the risk of suicidal thinking and behaviour in children, adolescents, and young adults (<25 years). In pooled analyses, the risk was 14 additional cases per 1,000 treated in those under 18 and 5 additional per 1,000 in those aged 18–24. Phenelzine is not approved for use in paediatric patients. All patients should be monitored for clinical worsening and emergence of suicidal thoughts, especially during initial months of therapy and at dose changes.

Patient Counselling

Purpose of Therapy

Phenelzine works by preventing the breakdown of important brain chemicals (serotonin, norepinephrine, and dopamine), allowing them to build up and relieve depression and anxiety. It is typically prescribed when other antidepressants have not worked well enough. The medication requires strict dietary restrictions because certain foods and drugs can cause a dangerous spike in blood pressure when combined with phenelzine.

How to Take

Take phenelzine exactly as prescribed, typically three times daily. It may take 2–4 weeks to notice benefit, and up to 6–8 weeks for full effect. Do not stop taking phenelzine abruptly — this can cause withdrawal symptoms. When your doctor is ready to stop the medication, the dose will be reduced gradually over several weeks.

Food Restrictions (CRITICAL)

Tell patientYou MUST avoid certain foods that contain a substance called tyramine while taking this medication and for at least 2 weeks after stopping. These include: aged cheeses (cottage cheese and cream cheese are fine), cured or smoked meats, pickled herring, fava beans, sauerkraut, yogurt, beer, wine, yeast extract, and foods that have been improperly refrigerated. Excessive chocolate and caffeine should also be limited. 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 after eating — go to the emergency department.

Medication Restrictions (CRITICAL)

Tell patientMany common medications are dangerous with phenelzine, including cold and cough remedies (especially those containing pseudoephedrine or dextromethorphan), 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 and supplements.

Call prescriberBefore starting any new medication prescribed by another doctor or dentist. Inform all healthcare providers that you take an MAOI.

Dizziness & Blood Pressure Changes

Tell patientFeeling lightheaded or dizzy when standing up is common, especially in the first weeks. Stand up slowly from sitting or lying positions. This effect usually improves over time but may persist.

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

Weight Gain

Tell patientWeight gain is a common side effect. Try to maintain a balanced diet (within the tyramine-free guidelines) and stay physically active. Report significant weight changes to your prescriber.

Call prescriberIf weight gain is causing distress or affecting your willingness to continue treatment.

Sexual Side Effects

Tell patientDifficulty reaching orgasm, reduced desire, or erectile problems are common with this medication. These effects are dose-related and can sometimes be improved with dose adjustments.

Call prescriberIf sexual side effects are intolerable or are affecting your relationship or treatment adherence.

Surgery & Medical Emergencies

Tell patientPhenelzine must be stopped at least 10 days before any planned surgery. In an emergency, always tell medical staff that you take an MAOI — carry an alert card or medical ID bracelet. Certain anaesthetics and pain medications are dangerous with MAOIs.

Call prescriberWell in advance of any planned medical or dental procedures so the medication can be safely discontinued.

Ref

Sources

Regulatory (PI / SmPC)

Nardil (phenelzine sulfate) Tablets — Full Prescribing Information. Parke-Davis Division of Pfizer Inc. DailyMed Primary source for FDA-approved indication, dosing, pharmacokinetics, adverse reactions, contraindications, and drug/food interactions.

Key Clinical Trials

Liebowitz MR, Quitkin FM, Stewart JW, et al. Phenelzine v imipramine in atypical depression: a preliminary report. Arch Gen Psychiatry. 1984;41(7):669–677. DOI Landmark Columbia University trial establishing phenelzine superiority over imipramine and placebo in atypical depression (response rate 67% vs 43% vs 29%).
Heimberg RG, Liebowitz MR, Hope DA, et al. Cognitive behavioral group therapy vs phenelzine therapy for social phobia: 12-week outcome. Arch Gen Psychiatry. 1998;55(12):1133–1141. DOI RCT comparing phenelzine with CBGT for social anxiety disorder, showing both superior to placebo with phenelzine having broader response.
Blanco C, Heimberg RG, Schneier FR, et al. A placebo-controlled trial of phenelzine, cognitive behavioral group therapy, and their combination for social anxiety disorder. Arch Gen Psychiatry. 2010;67(3):286–295. DOI Follow-up RCT demonstrating combined phenelzine + CBGT is superior to either monotherapy for social anxiety disorder.
Quitkin FM, Stewart JW, McGrath PJ, et al. Phenelzine versus imipramine in the treatment of probable atypical depression: defining syndrome boundaries of selective MAOI responders. Am J Psychiatry. 1988;145(3):306–311. DOI Further defined the atypical depression phenotype responsive to phenelzine, confirming superiority over imipramine and placebo.

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. DOI APA guideline recommending MAOIs for treatment-resistant depression after failure of multiple first-line agents.
Bandelow B, Michaelis S, Wedekind D. Treatment of anxiety disorders. Dialogues Clin Neurosci. 2017;19(2):93–107. DOI Review of pharmacotherapy for anxiety disorders positioning phenelzine as a highly effective but second-line option for social anxiety.

Mechanistic / Basic Science

Baker GB, Coutts RT, McKenna KF, Sherry-McKenna RL. Insights into the mechanisms of action of the MAO inhibitors phenelzine and tranylcypromine: a review. J Psychiatry Neurosci. 1992;17(5):206–214. PubMed Review of phenelzine’s mechanisms beyond MAO inhibition, including GABA-transaminase inhibition and metabolite pharmacology.
Bortolato M, Chen K, Shih JC. Monoamine oxidase inactivation: from pathophysiology to therapeutics. Adv Drug Deliv Rev. 2008;60(13–14):1527–1533. DOI Comprehensive review of MAO-A and MAO-B biochemistry and the pharmacological basis of irreversible MAO inhibition.

Pharmacokinetics / Special Populations

Robinson DS, Nies A, Ravaris CL, Lamborn KR, Korson L. A multiple-dose controlled study of phenelzine in depression-anxiety states. Arch Gen Psychiatry. 1976;33(3):347–350. DOI Early controlled dose-response study establishing therapeutic dose range and side-effect profile of phenelzine.
Blanco C, Schneier FR, Schmidt A, et al. Pharmacological treatment of social anxiety disorder: a meta-analysis. Depress Anxiety. 2003;18(1):29–40. DOI Meta-analysis showing phenelzine had the largest effect size (1.02) among medications studied for social anxiety disorder.
Sunderland T, Mueller EA, Cohen RM, et al. Tyramine pressor sensitivity changes during deprenyl treatment. Psychopharmacology (Berl). 1985;86(4):432–437. DOI Study characterising tyramine pressor sensitivity during MAO inhibition, informing dietary restriction guidelines.
Gillman PK. Monoamine oxidase inhibitors, opioid analgesics and serotonin toxicity. Br J Anaesth. 2005;95(4):434–441. DOI Definitive review of MAOI-opioid interactions, clarifying which opioids are safe and which are contraindicated with phenelzine.