Clomipramine: Comprehensive Drug Monograph

Pharmacokinetic Profile

Half-Life

~32 h (CMI); ~69 h (desmethyl-CMI)

Metabolism

CYP2D6, CYP3A4, CYP1A2, CYP2C19

Protein Binding

~97% (albumin)

Bioavailability

~50%

Volume of Distribution

Extensive; distributes into CSF and brain

Clinical Information

Drug Class

Tricyclic Antidepressant (dibenzazepine)

Available Doses

Capsules: 25 mg, 50 mg, 75 mg

Route

Oral

Renal Adjustment

Not studied; use caution

Hepatic Adjustment

Use caution; monitor LFTs

Pregnancy

Neonatal withdrawal reported

Lactation

Present in breast milk; caution

Schedule / Legal Status

Not a controlled substance

Generic Available

Yes

Black Box Warning

Suicidality in children & young adults

Indications

Indication	Approved Population	Therapy Type	Status
Obsessive-Compulsive Disorder (OCD)	≥10 years	Monotherapy or adjunctive	FDA Approved

Clomipramine holds a unique position among the tricyclic antidepressants as the most potent serotonin reuptake inhibitor in its class. It was the first medication approved by the FDA for OCD (1989) and remains a cornerstone of treatment for patients who do not respond adequately to SSRIs. In pivotal trials, clomipramine produced a 35–42% reduction in Yale-Brown Obsessive Compulsive Scale (Y-BOCS) scores in adults and 37% in children and adolescents, significantly outperforming placebo. Despite its robust efficacy, it is generally reserved as a second-line agent due to its side-effect burden compared with SSRIs.

Off-Label Uses

Major depressive disorder — Clomipramine is approved for depression in many countries outside the US. Some meta-analyses suggest it may have superior efficacy to other antidepressants in severe MDD, though evidence is not conclusive. (Evidence quality: Moderate)

Panic disorder — Used at 25–150 mg/day; evidence from multiple RCTs. (Evidence quality: Moderate)

Premature ejaculation — Low-dose (25–50 mg) on-demand or daily use; well-established off-label application. (Evidence quality: Moderate)

Cataplexy (narcolepsy) — Used for anticataplectic effect via serotonergic/noradrenergic mechanisms. (Evidence quality: Low)

Body dysmorphic disorder / Trichotillomania — Related to OCD spectrum; some supporting evidence. (Evidence quality: Low)

Chronic pain syndromes — Neuropathic pain at 25–150 mg/day. (Evidence quality: Low)

Dose

Dosing

Adult Dosing by Clinical Scenario

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Dose	Notes
OCD — initial treatment	25 mg/day	100–250 mg/day	250 mg/day	Increase by 25 mg every 4–7 days; max 100 mg in first 2 weeks; divide with meals during titration, then consolidate QHS Onset of anti-OCD effect typically 6–12 weeks
OCD — SSRI augmentation	25 mg QHS	75–150 mg/day	250 mg/day	Commonly combined with an SSRI; monitor CMI levels due to CYP2D6 inhibition by SSRIs Combined CMI + DCMI target: 150–300 ng/mL
Depression (off-label)	25 mg QHS	100–150 mg/day	250 mg/day	Titrate over 2–4 weeks; bedtime dosing preferred for sedation Not FDA-approved for depression in the US
Premature ejaculation (off-label)	25 mg	25–50 mg daily or on-demand (4–6 h before intercourse)	50 mg/day	Low doses exploit serotonergic-mediated ejaculation delay On-demand use reduces overall side-effect exposure
Chronic neuropathic pain (off-label)	10–25 mg QHS	75–150 mg/day	150 mg/day	Used similarly to amitriptyline; bedtime dosing preferred Analgesic effect may precede full antidepressant response

Paediatric & Special Population Adjustments

Population	Starting Dose	Maintenance Dose	Maximum Dose	Notes
Children & adolescents (10–17 y) — OCD	25 mg/day	Up to 3 mg/kg/day or 100 mg (lower value)	3 mg/kg/day or 200 mg (lower value)	Max 100 mg in first 2 weeks; divide with meals during titration FDA-approved for OCD in ≥10 years only
Elderly (≥65 years)	10–25 mg QHS	Titrate cautiously	Individualize (lower doses)	Higher sensitivity to anticholinergic and cardiovascular effects Lower steady-state concentrations occur in younger adults vs elderly
Hepatic impairment	Low dose	Titrate cautiously	Individualize	Effects of hepatic impairment on disposition not formally studied Monitor LFTs periodically; SGOT/SGPT elevations reported in 1–3%
CYP2D6 poor metabolisers	Reduce dose	Guided by plasma levels	Individualize	Higher CMI accumulation; consider pharmacogenomic testing TDM target: combined CMI + DCMI 150–300 ng/mL

Clinical Pearl: Nonlinear Pharmacokinetics Above 150 mg/day

Clomipramine and its active metabolite desmethylclomipramine exhibit capacity-limited (saturable) metabolism. Above 150 mg/day, plasma levels may rise disproportionately, prolonging half-lives and increasing seizure risk. Therapeutic drug monitoring is strongly recommended when doses exceed 150 mg/day or when CYP2D6 inhibitors are co-prescribed. Steady state takes 2–3 weeks at a given dose.

Clomipramine Pharmacology

Mechanism of Action

Clomipramine is the most serotonin-selective of the tricyclic antidepressants. The parent compound potently inhibits the serotonin transporter (SERT), which is believed to underlie its anti-obsessional efficacy. Its principal metabolite, desmethylclomipramine (DCMI), preferentially inhibits norepinephrine reuptake, adding dual-action antidepressant properties but also increasing anticholinergic and cardiovascular side effects. Additionally, clomipramine blocks histamine H1 receptors (contributing to sedation and weight gain), muscarinic acetylcholine receptors (responsible for anticholinergic effects), and alpha-1 adrenergic receptors (causing orthostatic hypotension). Like other TCAs, it also blocks cardiac sodium channels, which creates a narrow therapeutic-toxic window in overdose. The serotonergic selectivity of the parent compound is what distinguishes clomipramine from other TCAs in OCD treatment.

ADME Profile

Parameter	Value	Clinical Implication
Absorption	Well absorbed; bioavailability ~50%; Tmax 2–6 h (mean 4.7 h); food does not significantly affect absorption	Can be taken with or without food; divided dosing with meals during titration reduces GI side effects
Distribution	Extensive distribution into brain and CSF; protein binding ~97% (albumin); DMI CSF/plasma ratio 2.6	High protein binding means potential displacement interactions with other highly bound drugs; CNS penetration supports central efficacy
Metabolism	Hepatic: CYP2D6 and CYP3A4 (demethylation to DCMI); CYP1A2, CYP2C19 also involved; DCMI is pharmacologically active (t½ ~69 h)	Nonlinear pharmacokinetics above 150 mg/day; CYP2D6 PMs accumulate drug; smoking induces CYP1A2 and lowers CMI levels
Elimination	t½ CMI: 19–37 h (mean 32 h); t½ DCMI: 54–77 h (mean 69 h); 60% urine, 32% faeces; <1% unchanged in urine	Long metabolite half-life means steady state takes 2–3 weeks; dose changes should be separated by at least 2 weeks

Side Effects

Clomipramine has a high side-effect burden compared with SSRIs. The incidence data below are from placebo-controlled OCD trials (adults N=322, placebo N=319) from the Anafranil PI.

≥10% Very Common

Adverse Effect	Incidence (CMI)	Placebo	Clinical Note
Dry mouth	84%	17%	Anticholinergic; encourage oral hygiene, sugar-free gum
Somnolence	54%	16%	Dose-related; consolidate dose at bedtime once tolerated
Tremor	54%	2%	Fine postural tremor; may respond to dose reduction or propranolol
Dizziness	54%	14%	Orthostatic component; advise slow position changes
Headache	52%	41%	High placebo rate suggests only partly drug-attributable; treat symptomatically
Constipation	47%	11%	Anticholinergic; increase fibre and fluids
Ejaculation failure (males)	42%	2%	Serotonergic effect; therapeutic for premature ejaculation but distressing for others
Fatigue	39%	18%	Often improves over weeks; bedtime dosing helps
Nausea	33%	14%	Serotonergic; take with food; usually attenuates over 2 weeks
Increased sweating	29%	3%	Noradrenergic/serotonergic; may persist long-term
Insomnia	25%	15%	Paradoxical; consider dose timing adjustment
Dyspepsia	22%	10%	Take with meals during titration phase
Libido change	21%	3%	Serotonergic; significant impact on adherence
Impotence (males)	20%	3%	May require dose reduction or switching
Weight gain	18%	1%	Antihistaminic effect; monitor weight regularly
Abnormal vision	18%	4%	Anticholinergic mydriasis; rule out angle closure if eye pain
Nervousness	18%	2%	Serotonergic activation; usually transient
Micturition disorder	14%	2%	Anticholinergic urinary hesitancy; caution in BPH
Myoclonus	13%	<1%	Serotonergic; nocturnal jerks common; assess for serotonin syndrome at high doses
Anorexia	12%	<1%	May coexist with weight gain (appetite vs metabolic effects diverge)
Increased appetite	11%	2%	Antihistaminic; dietary counselling recommended

1–10% Common

Adverse Effect	Incidence	Clinical Note
Paresthesia	9%	Peripheral neuropathic sensation; usually benign
Memory impairment	9%	Anticholinergic cognitive burden; problematic in elderly
Taste perversion	8%	Metallic taste; usually transient
Rash	8%	Assess for DRESS if systemic symptoms present
Flushing	8%	Vasomotor instability
Vomiting	7%	Serotonergic; take with food
Tinnitus	6%	Monitor; may indicate ototoxicity at high levels
Postural hypotension	6%	Alpha-1 blockade; falls risk in elderly
Tachycardia	4%	Anticholinergic; obtain ECG if symptomatic
Palpitations	4%	Usually benign; ECG if persistent

Serious Serious (regardless of frequency)

Adverse Effect	Estimated Frequency	Typical Onset	Required Action
Seizures	~1.5% cumulative at 1 year	Dose- and duration-dependent	Limit dose to ≤250 mg/day; discontinue if seizure occurs; avoid in patients with seizure history
Suicidal ideation / behaviour	Uncommon (age-dependent)	First weeks to months	Close monitoring especially <25 years; consider stopping if emergent suicidality
Serotonin syndrome	Rare	Hours to days after adding serotonergic drug	Discontinue all serotonergic agents; supportive care; cyproheptadine
Cardiac arrhythmia / QRS prolongation	ECG abnormalities in 1.5%	Any time; higher risk in overdose	Baseline ECG; monitor QRS; discontinue if >120 ms; cardiology consult
DRESS (Drug Rash with Eosinophilia & Systemic Symptoms)	Rare (postmarketing)	2–8 weeks	Discontinue immediately; dermatology/allergy consult
Hepatotoxicity	SGOT ≥3×ULN in ~1%; SGPT ≥3×ULN in ~3%	Weeks to months	Monitor LFTs; discontinue if significant elevation or jaundice
Mania / hypomania	Uncommon	First weeks	Discontinue; screen for bipolar disorder; initiate mood stabiliser
Hyponatraemia (SIADH)	Rare	Weeks	Check sodium; elderly at higher risk; fluid restriction

Discontinuation Discontinuation Rates

Overall Discontinuation

~20%

Of 3,616 patients in US premarketing trials. Half had multiple complaints; 9% of total could not identify a single primary reason.

Primary Reasons

5.4% CNS complaints

Somnolence was the single most common reason. GI complaints (nausea/vomiting) accounted for 1.3%.

Reason for Discontinuation	Incidence	Context
Somnolence / sedation	Primary CNS reason (5.4% total CNS)	Most common identifiable cause; bedtime dosing may mitigate
Nausea / vomiting	Primary GI reason (1.3% total GI)	Usually improves with food and gradual titration
Sexual dysfunction	Significant contributor	Ejaculatory failure and libido change commonly cited; dose-related

Managing Sexual Dysfunction

Sexual side effects occur in 30–40% of patients and are one of the leading causes of non-adherence. Strategies include dose reduction to the minimum effective dose, timing the dose after sexual activity, or adding a PDE-5 inhibitor for erectile dysfunction. For ejaculatory delay that is therapeutically desired (premature ejaculation), the same mechanism becomes the indication rather than the side effect.

Int

Drug Interactions

Clomipramine is metabolised primarily by CYP2D6 (to DCMI) and CYP3A4, with contributions from CYP1A2 and CYP2C19. It does not induce drug-metabolising enzymes. Its very high protein binding (~97%) creates a theoretical risk of displacement interactions.

MajorMAO Inhibitors

MechanismCombined serotonergic and noradrenergic excess

EffectLife-threatening serotonin syndrome and hypertensive crisis

ManagementContraindicated: 14-day washout required in both directions; includes linezolid and IV methylene blue

FDA PI

MajorSSRIs (fluoxetine, fluvoxamine, paroxetine, sertraline)

MechanismAdditive serotonergic activity + CYP2D6 inhibition (fluoxetine/paroxetine) and CYP1A2 inhibition (fluvoxamine)

EffectSerotonin syndrome risk; markedly elevated CMI plasma levels

ManagementIf combination necessary (e.g., OCD augmentation), use low CMI doses with TDM; allow 5-week washout after fluoxetine

FDA PI

MajorQTc-Prolonging Agents

MechanismAdditive cardiac conduction delay

EffectRisk of ventricular arrhythmias including torsades de pointes

ManagementAvoid combination; obtain ECG; correct electrolytes

Medscape

ModerateHaloperidol

MechanismCYP2D6 inhibition by haloperidol

EffectIncreased clomipramine plasma concentrations

ManagementMonitor CMI levels; adjust dose accordingly

FDA PI

ModerateCarbamazepine & other CYP inducers

MechanismCYP1A2 and CYP3A4 induction accelerating CMI clearance

EffectReduced clomipramine levels, potentially subtherapeutic

ManagementMonitor levels; dose increase may be needed; also note: CMI increases phenobarbital levels

FDA PI

ModerateAlcohol & CNS Depressants

MechanismAdditive CNS depression

EffectPotentiated sedation and psychomotor impairment

ManagementAvoid alcohol; reduce dose of sedative agents as tolerated

FDA PI

ModerateHighly Protein-Bound Drugs (warfarin, digoxin)

MechanismPotential displacement from albumin binding sites (97% bound)

EffectIncreased free fraction of either drug

ManagementMonitor INR if on warfarin; monitor digoxin levels

FDA PI

MinorAnticholinergic Agents

MechanismAdditive muscarinic blockade

EffectWorsened dry mouth, constipation, urinary retention, delirium

ManagementReview anticholinergic burden; minimise polypharmacy in elderly

Lexicomp

Mon

Monitoring

ECG Baseline; repeat at therapeutic dose and if dose >150 mg/day
Routine Assess QRS, QTc, and conduction intervals. ECG abnormalities developed in 1.5% of patients in premarketing trials. QRS >100 ms warrants caution; >120 ms requires dose reduction or discontinuation.
TDM (Plasma Levels) After 3–4 weeks on stable dose; and with any dose change
Routine Measure trough combined CMI + DCMI levels. Target range 150–300 ng/mL. Mandatory when dose >150 mg/day, when co-prescribed with CYP2D6/1A2 inhibitors, or if toxicity suspected. Nonlinear kinetics make TDM essential.
Blood Pressure Baseline; during titration
Routine Orthostatic hypotension in ~20% of patients (often asymptomatic). Lying and standing measurements recommended, especially in elderly.
Liver Function Baseline; periodically during treatment
Routine Transaminase elevations (SGOT ~1%, SGPT ~3% ≥3×ULN) reported in premarketing trials. Rare postmarketing reports of severe hepatic injury. Discontinue if jaundice or significant elevation.
Weight & BMI Baseline, then every 3 months
Routine Weight gain in 18% of patients. Early dietary and exercise counselling recommended.
Mental State Every visit for first 3 months
Routine Monitor for suicidality (especially <25 years), manic switching, and psychosis activation. Y-BOCS scores to track OCD response.
Sodium If confusion, nausea, headache in elderly
Trigger-Based SIADH-related hyponatraemia reported; elderly at greater risk.

Contraindications & Cautions

Absolute Contraindications

Hypersensitivity to clomipramine or other tricyclic antidepressants (cross-reactivity within dibenzazepine class)
Concurrent MAOI use or use within 14 days of stopping an MAOI (including linezolid and IV methylene blue)
Acute recovery period after myocardial infarction

Relative Contraindications (Specialist Input Recommended)

Severe cardiovascular disease — conduction abnormalities, heart failure, recent arrhythmias; TCA cardiotoxicity risk
Seizure disorder or history of seizures — clomipramine lowers seizure threshold dose-dependently; cumulative seizure rate ~1.5% at 1 year
Untreated narrow-angle glaucoma — anticholinergic mydriasis may trigger angle closure
Severe hepatic impairment — extensive hepatic metabolism; rare fatal hepatotoxicity reported postmarketing
Bipolar disorder (unscreened) — risk of manic switching; screen before initiation

Use with Caution

Urinary retention / prostatic hypertrophy — anticholinergic effects worsen obstructive symptoms
Elderly patients — higher sensitivity to anticholinergic, cardiovascular, and sedative effects; hyponatraemia risk
Patients at risk of suicide — prescribe smallest feasible quantity; TCA overdose has a narrow toxic-to-therapeutic ratio
CYP2D6 poor metabolisers — increased exposure; TDM advised
Smokers — smoking induces CYP1A2; smoking cessation may raise clomipramine levels significantly

FDA Boxed Warning Suicidal Thoughts and Behaviours

Antidepressants, including clomipramine, increase the risk of suicidal thinking and behaviour in children, adolescents, and young adults (<25 years) in short-term studies. In pooled analyses of over 4,400 paediatric and 77,000 adult patients, 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. All patients should be monitored for clinical worsening and emergence of suicidal thoughts, especially during the initial months of therapy and at dose changes. Clomipramine is not approved for paediatric use except for OCD in patients ≥10 years.

Patient Counselling

Purpose of Therapy

Clomipramine works by adjusting the balance of serotonin in the brain, which helps reduce obsessive thoughts and compulsive behaviours. It typically takes 6 to 12 weeks for the full anti-OCD effect to become apparent. Patients should understand that improvement is gradual and should not stop the medication abruptly even if they feel it is not working in the first few weeks.

How to Take

During the first weeks, clomipramine should be taken in divided doses with meals to reduce nausea. Once a stable dose is reached, the full daily dose can be taken at bedtime to take advantage of its sedating effects and reduce daytime drowsiness. Capsules can be opened and mixed with soft food for patients who have difficulty swallowing.

Drowsiness & Sedation

Tell patientDrowsiness affects over half of patients and is most pronounced in the first weeks. Taking the full dose at bedtime helps. Avoid driving or operating machinery until you know how the medication affects you.

Call prescriberIf daytime sedation persists beyond 3–4 weeks or causes significant functional impairment.

Dry Mouth & Constipation

Tell patientDry mouth is very common (affects most patients). Sip water frequently, use sugar-free gum, and maintain dental hygiene to prevent cavities. For constipation, increase fibre and fluid intake.

Call prescriberIf constipation is severe, accompanied by abdominal pain, or if you develop difficulty urinating.

Sexual Side Effects

Tell patientDelayed orgasm, reduced libido, or erectile difficulty affects a large proportion of patients. These effects are dose-related and often manageable. Do not feel embarrassed to report them, as strategies exist to help.

Call prescriberIf sexual side effects are intolerable or are causing you to consider stopping the medication.

Seizure Risk

Tell patientAt the doses used for OCD, there is a small risk of seizures (about 1 in 70 patients over a year). Do not exceed the prescribed dose. Discuss with your prescriber before engaging in activities where sudden loss of consciousness could be dangerous (swimming, climbing, driving heavy machinery).

Call prescriberImmediately if you experience a seizure or any episode of unexplained loss of consciousness.

Mood Changes & Suicidality

Tell patientRarely, some patients — particularly those under 25 — may experience worsening mood, agitation, or new thoughts of self-harm in the early weeks. Family members should also be alert to these changes.

Call prescriberImmediately if you or your family notice worsening depression, agitation, or any thoughts of self-harm.

Stopping Treatment

Tell patientDo not stop clomipramine abruptly. Withdrawal symptoms including dizziness, nausea, headache, irritability, and sleep disturbance can occur. Your prescriber will plan a gradual dose reduction if stopping is appropriate.

Call prescriberIf you wish to stop the medication or if you experience withdrawal symptoms despite gradual tapering.

Ref

Sources

Regulatory (PI / SmPC)

Anafranil (clomipramine hydrochloride) Capsules USP — Full Prescribing Information. SpecGx LLC (Mallinckrodt). Revised September 2024. DailyMed Primary source for FDA-approved indication, dosing, pharmacokinetics, adverse reactions, contraindications, and drug interactions.

Key Clinical Trials

Clomipramine Collaborative Study Group. Clomipramine in the treatment of patients with obsessive-compulsive disorder. Arch Gen Psychiatry. 1991;48(8):730–738. DOI Landmark multicenter placebo-controlled trial establishing clomipramine efficacy in OCD in adults.
DeVeaugh-Geiss J, Moroz G, Biederman J, et al. Clomipramine hydrochloride in childhood and adolescent obsessive-compulsive disorder — a multicenter trial. J Am Acad Child Adolesc Psychiatry. 1992;31(1):45–49. DOI Pivotal paediatric OCD trial supporting FDA approval for ages 10–17.
Ackerman DL, Greenland S. Multivariate meta-analysis of controlled drug studies for obsessive-compulsive disorder. J Clin Psychopharmacol. 2002;22(3):309–317. DOI Meta-analysis comparing clomipramine with SSRIs in OCD, showing clomipramine retains a significant efficacy advantage.
Soomro GM, Altman DG, Rajagopal S, Oakley Browne M. Selective serotonin re-uptake inhibitors (SSRIs) versus placebo for obsessive compulsive disorder (OCD). Cochrane Database Syst Rev. 2008;(1):CD001765. DOI Cochrane review of SSRIs in OCD, providing context for clomipramine’s place relative to SSRI monotherapy.

Guidelines

American Psychiatric Association. Practice guideline for the treatment of patients with obsessive-compulsive disorder. Am J Psychiatry. 2007;164(7 Suppl):5–53. DOI APA guideline recommending clomipramine as a second-line pharmacological option after SSRI failure in OCD.
National Institute for Health and Care Excellence (NICE). Obsessive-compulsive disorder and body dysmorphic disorder: treatment. Clinical guideline CG31 (updated 2005). NICE UK guideline positioning clomipramine as an alternative to SSRIs when response is inadequate.

Mechanistic / Basic Science

Gillman PK. Tricyclic antidepressant pharmacology and therapeutic drug interactions updated. Br J Pharmacol. 2007;151(6):737–748. DOI Comprehensive review of TCA receptor pharmacology including clomipramine’s serotonin transporter selectivity.
Hyttel J. Pharmacological characterization of selective serotonin reuptake inhibitors (SSRIs). Int Clin Psychopharmacol. 1994;9(Suppl 1):19–26. DOI Provides comparative in-vitro serotonin transporter binding data for clomipramine versus SSRIs.

Pharmacokinetics / Special Populations

Hiemke C, Bergemann N, Clement HW, et al. Consensus guidelines for therapeutic drug monitoring in neuropsychopharmacology: update 2017. Pharmacopsychiatry. 2018;51(1–02):9–62. DOI AGNP consensus establishing therapeutic reference range for combined CMI + DCMI (150–300 ng/mL) and TDM recommendations.
Gex-Fabry M, Eap CB, Oneda B, et al. CYP2D6 and CYP2C19 genetic polymorphisms and steady-state plasma concentrations of clomipramine and its metabolites. Ther Drug Monit. 2008;30(5):559–569. DOI Pharmacogenomic study demonstrating the impact of CYP2D6 and CYP2C19 polymorphisms on clomipramine plasma levels.
Vandel S, Bertschy G, Baumann P, et al. Fluvoxamine and fluoxetine: interaction studies with amitriptyline, clomipramine and neuroleptics in phenotyped patients. Pharmacol Res. 1995;31(6):347–353. DOI Documents the pharmacokinetic interaction between SSRIs and clomipramine via CYP inhibition in phenotyped patients.
Patel P, Abdijadid S. Clomipramine. In: StatPearls [Internet]. Treasure Island, FL: StatPearls Publishing; updated August 16, 2024. NCBI Bookshelf Peer-reviewed clinical summary covering indications, dosing, PK, adverse effects, and interprofessional management.