My Dashboard
Courses
Articles Evidence Reviews Practice Updates Cases News Presentations
About Us
My Dashboard
Drug Monograph

Citalopram (Celexa)

citalopram hydrobromide

Selective Serotonin Reuptake Inhibitor (SSRI) · Oral
Pharmacokinetic Profile
Half-Life
~35 h
Metabolism
CYP3A4 & CYP2C19 (hepatic)
Protein Binding
~80%
Bioavailability
~80%
Volume of Distribution
~12 L/kg
Clinical Information
Drug Class
SSRI
Available Doses
10, 20 (scored), 40 mg (scored) tablets
Route
Oral
Renal Adjustment
No adjustment mild–moderate; caution in severe
Hepatic Adjustment
Yes — max 20 mg/day
Pregnancy
Risk of PPHN (3rd trimester); no established teratogenicity in human data
Lactation
Present in breast milk; monitor infant
Schedule / Legal Status
Prescription only (not scheduled)
Generic Available
Yes
Black Box Warning
Suicidal thoughts & behaviors in young adults
QT Prolongation
Dose-dependent; max 40 mg/day; max 20 mg/day in specific populations
Rx

Indications

IndicationApproved PopulationTherapy TypeStatus
Major Depressive Disorder (MDD)AdultsMonotherapyFDA Approved

Citalopram is FDA-approved solely for the treatment of major depressive disorder in adults. It is the racemic mixture of R- and S-citalopram; the S-enantiomer (escitalopram) is marketed separately as Lexapro. Despite its single approved indication, citalopram is one of the most commonly prescribed antidepressants globally and is included on the WHO Model List of Essential Medicines. It is not approved for paediatric use.

Off-Label Uses

Panic disorder: Effective in multiple RCTs at 20–40 mg/day. Evidence quality: High.

Obsessive-compulsive disorder (OCD): Used at doses of 20–40 mg/day; limited by QT ceiling. Evidence quality: Moderate (RCTs with racemic citalopram).

Generalized anxiety disorder (GAD): Studied at 10–40 mg/day with positive results. Evidence quality: Moderate.

Alcohol use disorder: Used as adjunct to reduce alcohol consumption. Evidence quality: Moderate (RCTs with mixed results).

Premenstrual dysphoric disorder (PMDD): Evidence quality: Moderate.

Vasomotor symptoms (menopause): Evidence quality: Low–Moderate.

Dose

Dosing

Adult Dosing by Clinical Scenario

Clinical ScenarioStarting DoseMaintenance DoseMaximum DoseNotes
Major depression — initial treatment20 mg once daily20–40 mg/day40 mg/dayAdminister once daily, with or without food. Increase after ≥1 week if needed
Doses >40 mg not recommended due to QT prolongation risk
Depression with comorbid anxiety10–20 mg once daily20–40 mg/day40 mg/dayLower starting dose if anxiety or panic features predominate to minimise early jitteriness
Screen for bipolar disorder before starting
Depression in patient on CYP2C19 inhibitor (e.g., omeprazole, cimetidine)20 mg once daily20 mg/day20 mg/dayCimetidine increased citalopram AUC by 43% and Cmax by 39%
Hard cap at 20 mg due to QT risk from elevated drug levels

Special Population Dosing

Clinical ScenarioStarting DoseMaintenance DoseMaximum DoseNotes
Patients >60 years of age20 mg once daily20 mg/day20 mg/dayAUC increased 23–30%, t½ increased 30–50% vs younger adults
Higher QT risk; higher hyponatraemia risk
Hepatic impairment20 mg once daily20 mg/day20 mg/dayOral clearance reduced 37%; t½ doubled
Hard cap at 20 mg due to QT risk
CYP2C19 poor metabolisers20 mg once daily20 mg/day20 mg/dayCmax +68%, AUC +107% compared to extensive metabolisers
Pharmacogenomic testing can identify these patients
Mild–moderate renal impairment20 mg once daily20–40 mg/day40 mg/dayOral clearance reduced by 17%; no dose adjustment required
Limited data in severe renal impairment (CrCl <20 mL/min); use with caution
Critical: QT Prolongation Dose Cap

Citalopram causes dose-dependent QTc prolongation. In a thorough QT study, the predicted QTcNi increase at 40 mg was 12.6 msec (upper bound 14.3 msec). At 60 mg (supratherapeutic), the increase was 18.5 msec (upper bound 21.0 msec). Cases of torsade de pointes, ventricular tachycardia, and sudden death have been reported in the postmarketing setting. Doses above 40 mg/day are not recommended for any patient. The maximum is further reduced to 20 mg/day in patients >60 years, those with hepatic impairment, CYP2C19 poor metabolisers, and those taking CYP2C19 inhibitors.

PK

Pharmacology

Mechanism of Action

Citalopram is a racemic SSRI that exerts its antidepressant effect by selectively inhibiting neuronal reuptake of serotonin (5-HT) in the central nervous system. It is considered the most selective SSRI, having no clinically meaningful affinity for 5-HT1A, 5-HT2A, dopamine D1/D2, adrenergic (α1, α2, β), histamine H1, GABA, muscarinic cholinergic, or benzodiazepine receptors. The S-enantiomer (escitalopram) is primarily responsible for serotonin reuptake inhibition, while the R-enantiomer is essentially inactive at SERT. Citalopram’s metabolites (demethylcitalopram and didemethylcitalopram) are at least 8 times less potent than the parent compound and do not meaningfully contribute to its clinical effect. Citalopram is a weak inhibitor of CYP2D6 and CYP1A2, with minimal impact on most co-administered drugs metabolised by these pathways.

ADME Profile

ParameterValueClinical Implication
AbsorptionBioavailability ~80%; Tmax ~4 h; absorption not affected by food; linear pharmacokinetics across 10–40 mgPredictable dose-exposure relationship; can be taken with or without food at any time of day
DistributionVd ~12 L/kg; plasma protein binding ~80% for citalopram and metabolitesModerate tissue distribution; lower protein binding than paroxetine or sertraline, reducing displacement interaction risk
MetabolismHepatic via CYP3A4 and CYP2C19 (primary N-demethylation); metabolites DCT (~50% parent levels at steady state), DDCT (~10%); metabolites ≥8× less potent; weak CYP2D6/CYP1A2 inhibitorCYP2C19 poor metabolisers have >2-fold exposure increase (dose cap 20 mg); CYP2C19 inhibitors (e.g., cimetidine, omeprazole) require dose reduction; CYP2D6 status has no significant impact
Eliminationt½ ~35 h; systemic clearance 330 mL/min (~20% renal); ~10% excreted in urine as parent, ~5% as DCT; steady state in ~1 week; accumulation factor ~2.5×Longer half-life than paroxetine or fluvoxamine — lower discontinuation syndrome risk; once-daily dosing; dose adjustment in hepatic impairment (clearance −37%, t½ doubled) and elderly (AUC +23–30%)
SE

Side Effects

≥10% Very Common
Adverse EffectIncidenceClinical Note
Nausea21% vs 14% placeboMost common GI complaint; usually transient; taking with food may help
Dry mouth20% vs 14% placeboDespite low muscarinic affinity; may persist; encourage oral hygiene
Somnolence18% vs 10% placeboDose-dependent; consider evening dosing if prominent
Insomnia15% vs 14% placeboOnly marginally above placebo; dose-dependent; morning dosing may help
Increased sweating11% vs 9% placeboDose-dependent; may persist with chronic use
1–10% Common
Adverse EffectIncidenceClinical Note
Tremor8% vs 6% placeboFine postural tremor; usually self-limiting
Diarrhoea8% vs 5% placeboSerotonergic GI effect; generally mild and transient
Ejaculation disorder (males)6.1% vs 1% placeboPrimarily ejaculatory delay; the only AE occurring at ≥5% and ≥2× placebo rate
Fatigue5% vs 3% placeboDose-dependent; usually improves with time
Dyspepsia5% vs 4% placeboGenerally mild; consider antacid if persistent
Upper respiratory tract infection5% vs 4% placeboLikely coincidental; comparable to placebo rate
Rhinitis5% vs 3% placeboGenerally self-limiting
Vomiting4% vs 3% placeboLess common than nausea; usually transient
Anxiety4% vs 3% placeboMore common early in treatment; may represent initial activation
Anorexia4% vs 2% placeboMean weight loss ~0.5 kg in controlled trials (vs no change for placebo)
Decreased libido (males)3.8% vs <1% placeboMay be underreported; enquire proactively
Agitation3% vs 1% placeboDistinguish from akathisia; consider dose reduction
Sinusitis3% vs <1% placeboMay be coincidental
Abdominal pain3% vs 2% placeboUsually self-limiting
Impotence (males)2.8% vs <1% placeboDose-dependent; discuss management strategies
Libido decreased (overall)2% vs <1% placeboFemales: decreased libido 1.3%, anorgasmia 1.1%
Yawning2% vs <1% placeboDose-dependent serotonergic effect; benign
Serious Serious Adverse Effects (Regardless of Frequency)
Adverse EffectEstimated FrequencyTypical OnsetRequired Action
QT prolongation / Torsade de PointesDose-dependent; 1.9% had QTcF >60 msec change; 0.5% >500 msecAny time; higher risk at doses >40 mg or in predisposed patientsECG if symptoms (syncope, palpitations); discontinue if QTc >500 msec; correct electrolytes; avoid QT-prolonging co-medications
Suicidal thoughts/behaviours14 per 1,000 (<18 y); 5 per 1,000 (18–24 y)First weeks to monthsClose monitoring at initiation and dose changes; weekly visits initially
Serotonin syndrome0.1% in premarketing trialsHours to days, especially with co-serotonergic drugsDiscontinue all serotonergic agents immediately; supportive care; hospital admission
Hyponatraemia (SIADH)Uncommon; Na <110 mmol/L reportedDays to weeks; higher risk in elderly, diuretic usersCheck sodium; discontinue citalopram; appropriate fluid management
Mania/hypomania activation0.1% (undiagnosed bipolar patients)Days to weeksDiscontinue antidepressant; psychiatric reassessment
Seizures0.3% (vs 0.5% placebo)Any timeUse caution in seizure disorders; evaluate if new seizure occurs
Abnormal bleedingUncommonAny time; risk increased with anticoagulants/NSAIDsAssess bleeding; monitor INR if on warfarin
Angle-closure glaucomaRare (postmarketing)Any timeEmergency ophthalmological referral; discontinue citalopram
Stevens-Johnson syndrome / TENVery rare (postmarketing)Days to weeksImmediate discontinuation; dermatology referral
Hepatic necrosisVery rare (postmarketing)VariableLFTs if symptomatic; discontinue if transaminases markedly elevated
Discontinuation Discontinuation Rates
Citalopram (MDD Trials)
16% vs 8% placebo
Top reasons: Nausea (4%), insomnia (3%), somnolence (2%), dizziness (2%), dry mouth (1%), vomiting (1%), asthenia (1%), agitation (1%)
Discontinuation Syndrome
Lower risk vs paroxetine / venlafaxine
Longer half-life (~35 h) provides a degree of self-tapering; symptoms include dizziness, paresthesia, nausea, irritability, insomnia. Gradual taper still recommended
Reason for DiscontinuationIncidenceContext
Nausea4% vs 0% placeboMost common reason; typically occurs in first 1–2 weeks
Insomnia3% vs 1% placeboDose-dependent; consider timing adjustment before discontinuing
Somnolence2% vs 1% placeboUsually transient
Dizziness2% vs <1% placeboUsually transient; rule out orthostatic component
Dry mouth1% vs <1% placeboRarely sole reason for discontinuation
Managing the QT Prolongation Risk

Citalopram is unique among SSRIs in having a formal FDA dose ceiling (40 mg/day) driven by cardiac safety data. Before prescribing, assess for risk factors: congenital long QT syndrome, bradycardia, hypokalaemia, hypomagnesaemia, recent MI, uncompensated heart failure, or co-administration of other QT-prolonging drugs. Obtain baseline electrolytes in at-risk patients and correct abnormalities before initiation. If symptoms suggestive of arrhythmia develop (syncope, palpitations, dizziness), obtain an ECG promptly. The dose cap effectively limits citalopram’s usefulness in conditions like OCD where higher SSRI doses are typically needed.

Int

Drug Interactions

Citalopram is metabolised primarily by CYP3A4 and CYP2C19, with CYP2C19 being the more clinically relevant pathway due to the QT-related dose ceiling. Unlike paroxetine or fluoxetine, citalopram is only a weak inhibitor of CYP2D6, resulting in fewer pharmacokinetic drug interactions with CYP2D6 substrates. The dominant interaction concern is pharmacodynamic: additive QT prolongation with other QT-prolonging drugs, and serotonin syndrome with other serotonergic agents.

MajorMAOIs (e.g., phenelzine, tranylcypromine, linezolid, IV methylene blue)
MechanismDual serotonergic enhancement
EffectRisk of serotonin syndrome (potentially fatal)
ManagementContraindicated. Allow ≥14 days washout in either direction
FDA PI
MajorPimozide
MechanismAdditive QT prolongation; citalopram co-administration increased QTc by ~10 msec vs pimozide alone
EffectRisk of torsade de pointes and ventricular arrhythmias
ManagementContraindicated. Do not co-prescribe
FDA PI
MajorQT-prolonging drugs (Class IA/III antiarrhythmics, thioridazine, chlorpromazine, moxifloxacin, methadone)
MechanismAdditive QTc interval prolongation
EffectIncreased risk of ventricular arrhythmias, torsade de pointes, sudden death
ManagementAvoid co-prescribing where possible; if unavoidable, ECG monitoring required, correct electrolytes, use lowest citalopram dose
FDA PI
MajorCYP2C19 inhibitors (cimetidine, omeprazole, esomeprazole, fluconazole)
MechanismCYP2C19 inhibition increases citalopram exposure; cimetidine increased AUC by 43%
EffectElevated citalopram levels increasing QT prolongation risk
ManagementMaximum citalopram dose is 20 mg/day when co-prescribed with any CYP2C19 inhibitor
FDA PI
ModerateOther serotonergic drugs (triptans, TCAs, SNRIs, tramadol, lithium, St. John’s Wort)
MechanismAdditive serotonergic activity
EffectIncreased risk of serotonin syndrome
ManagementMonitor for serotonin syndrome symptoms; discontinue if occurs
FDA PI
ModerateNSAIDs / Aspirin / Warfarin / Anticoagulants
MechanismSSRI-mediated serotonin depletion in platelets; warfarin prothrombin time increased by 5% with citalopram
EffectIncreased risk of GI and other bleeding
ManagementMonitor INR on warfarin; counsel on bleeding signs; consider PPI cover with NSAIDs
FDA PI
ModerateMetoprolol
MechanismCitalopram doubled metoprolol plasma levels (weak CYP2D6 inhibition)
EffectIncreased beta-blockade; potential for bradycardia and hypotension
ManagementMonitor heart rate and blood pressure; no clinically significant effects seen in formal study but caution warranted
FDA PI
ModerateImipramine / TCAs
MechanismWeak CYP2D6 inhibition; desipramine (imipramine metabolite) concentration increased ~50%
EffectPotential for TCA toxicity; additive QT risk with TCAs
ManagementMonitor TCA levels if combination used; ECG monitoring advisable
FDA PI
MinorCarbamazepine
MechanismEnzyme induction by carbamazepine may increase citalopram clearance (not seen in formal study at trough levels)
EffectPotential for reduced citalopram efficacy
ManagementMonitor clinical response; consider dose adjustment
FDA PI
MinorDigoxin / Lithium / Theophylline
MechanismNo significant PK interaction in formal studies
EffectNo clinically meaningful interaction expected; lithium has serotonin syndrome risk (pharmacodynamic)
ManagementStandard monitoring; lithium carries serotonin syndrome risk
FDA PI
Mon

Monitoring

  • Mood & Suicidality Weekly for 4 weeks, biweekly for 8 weeks, then per clinical judgement
    Routine     Assess for clinical worsening, suicidal ideation, unusual behavioural changes, especially in patients under 25. Use PHQ-9 or equivalent
  • ECG Baseline and after dose changes in at-risk patients
    Trigger-based     At-risk: cardiac disease, electrolyte abnormalities, co-prescribed QT-prolonging drugs, >60 years. Discontinue if QTc >500 msec. Obtain ECG promptly if syncope, palpitations, or dizziness
  • Electrolytes (K+, Mg2+) Baseline in at-risk patients; periodic monitoring
    Trigger-based     Correct hypokalaemia and hypomagnesaemia before initiation and periodically during treatment; these increase arrhythmia risk
  • Sodium (Na+) Baseline in at-risk; recheck 2–4 weeks
    Trigger-based     At-risk: elderly, diuretic users, volume-depleted. Check if confusion, falls, weakness, or seizures develop
  • Sexual Function Baseline, then each visit
    Routine     Enquire proactively; citalopram has moderate sexual side effect burden among SSRIs
  • Weight Baseline, then every 3–6 months
    Routine     Initial weight loss (~0.5 kg) may reverse with chronic use; monitor trends
  • Bleeding Signs Each visit if on anticoagulants/NSAIDs
    Trigger-based     Ask about bruising, epistaxis, GI bleeding. Monitor INR if on warfarin
CI

Contraindications & Cautions

Absolute Contraindications

  • Concurrent MAOI use or use within 14 days of stopping an MAOI (including linezolid and IV methylene blue) — serotonin syndrome risk
  • Concurrent pimozide — risk of additive QT prolongation and ventricular arrhythmias
  • Known hypersensitivity to citalopram or any excipient (angioedema, anaphylaxis reported)

Relative Contraindications (Specialist Input Recommended)

  • Congenital long QT syndrome — avoid unless benefits clearly outweigh risks; ECG monitoring essential
  • Recent acute myocardial infarction or uncompensated heart failure — increased arrhythmia susceptibility
  • Concurrent use of other QT-prolonging drugs — additive risk; use alternative SSRI if feasible
  • Uncorrected hypokalaemia or hypomagnesaemia — correct electrolytes before initiation
  • Undiagnosed bipolar disorder — risk of mania/hypomania; screen before starting

Use with Caution

  • Patients >60 years — max 20 mg/day; increased AUC, higher QT and hyponatraemia risk
  • Hepatic impairment — max 20 mg/day; clearance reduced 37%, t½ doubled
  • CYP2C19 poor metabolisers — max 20 mg/day; AUC more than doubled
  • Seizure disorders — seizures reported in 0.3% of treated patients; use cautiously
  • Anatomically narrow angles (untreated) — risk of angle-closure glaucoma
  • Late pregnancy — risk of neonatal poor adaptation syndrome and possible PPHN
  • Breastfeeding — present in breast milk (relative infant dose 0.7–9.4%); monitor infant for irritability, somnolence, poor feeding
  • Bradycardia — additive risk with QT prolongation; consider alternative SSRI
FDA Boxed Warning Suicidal Thoughts and Behaviours

Antidepressants increased the risk of suicidal thinking and behaviour in paediatric and young adult patients in short-term studies. The risk is highest in those under 18 (14 additional cases per 1,000 treated) and in the 18–24 age group (5 additional per 1,000). Citalopram is not approved for paediatric use. All patients initiated on antidepressant therapy should be closely monitored for clinical worsening and emergence of suicidal thoughts, especially during initial months and at dose changes.

FDA Safety Communication QT Prolongation and Dose Limitation

The FDA has issued safety communications regarding dose-dependent QT prolongation with citalopram. Doses above 40 mg/day are not recommended for any patient. The maximum is further reduced to 20 mg/day in patients over 60, those with hepatic impairment, CYP2C19 poor metabolisers, and patients taking concomitant CYP2C19 inhibitors. Torsade de pointes, ventricular tachycardia, and sudden death have been reported in the postmarketing setting.

Pt

Patient Counselling

Purpose of Therapy

Citalopram increases serotonin levels in the brain to help relieve symptoms of depression. Improvement may begin within 1 to 4 weeks, but full benefit can take longer. It is important to continue taking citalopram as prescribed even after feeling better, unless advised otherwise.

How to Take

Take citalopram once daily, with or without food. Swallow the tablet whole. Do not stop abruptly — discuss any dose changes with your prescriber.

Heart Rhythm (QT Prolongation)
Tell patientCitalopram can affect heart rhythm at higher doses. Never take more than prescribed. Tell all healthcare providers that you take citalopram before starting any new medications.
Call prescriberImmediately if you feel faint, lose consciousness, or notice your heart beating irregularly or unusually fast.
Nausea & Stomach Upset
Tell patientNausea affects about 1 in 5 patients and usually improves within the first 1–2 weeks. Taking the tablet with food may help.
Call prescriberIf nausea is severe, lasts beyond 2 weeks, or is accompanied by persistent vomiting.
Drowsiness or Insomnia
Tell patientSome patients feel sleepy, others have trouble sleeping. If drowsy, consider taking citalopram in the evening. If trouble sleeping, take it in the morning. These effects often improve over a few weeks.
Call prescriberIf sleep problems persist beyond 3–4 weeks or significantly affect daily life.
Sexual Side Effects
Tell patientDelayed ejaculation, reduced sex drive, or difficulty reaching orgasm can occur. These are common with antidepressants in this class and are worth discussing openly.
Call prescriberIf sexual side effects are distressing — dose adjustment or alternative medications can be considered.
Do Not Stop Suddenly
Tell patientAlthough citalopram has a lower discontinuation syndrome risk than some other antidepressants, stopping abruptly can still cause dizziness, tingling, nausea, and irritability. Always taper under medical supervision.
Call prescriberIf you accidentally miss several doses or experience withdrawal symptoms during a planned taper.
Mood Changes & Suicidality
Tell patientRarely, antidepressants may cause new or worsening thoughts of self-harm, especially early in treatment. Have a trusted person watch for mood changes.
Call prescriberImmediately if new or worsening suicidal thoughts, severe agitation, or unusual behavioural changes occur.
Ref

Sources

Regulatory (PI / SmPC)
  1. CELEXA (citalopram) tablets. Full Prescribing Information. AbbVie Inc. Revised October 2023. FDA Label Primary regulatory source for all dosing, adverse reaction incidence rates, contraindications, QT data, and pharmacokinetics used in this monograph.
  2. Citalopram capsules. Full Prescribing Information. Revised 2023. FDA Label (Capsules) Capsule formulation PI; confirms dosing and safety data consistent with tablet formulation.
  3. FDA Drug Safety Communication: Revised recommendations for Celexa (citalopram hydrobromide) related to a potential risk of abnormal heart rhythms with high doses. August 2012. FDA Safety Communication Key FDA communication establishing the 40 mg dose ceiling and 20 mg limits for specific populations based on QT prolongation data.
Key Clinical Trials
  1. Stahl SM. Placebo-controlled comparison of the selective serotonin reuptake inhibitors citalopram and sertraline. Biol Psychiatry. 2000;48(9):894–901. DOI Comparative efficacy trial supporting citalopram’s antidepressant effect in moderate-to-severe depression.
  2. Montgomery SA, Rasmussen JG, Tanghoj P. A 24-week study of 20 mg citalopram, 40 mg citalopram, and placebo in the prevention of relapse of major depression. Int Clin Psychopharmacol. 1993;8(3):181–188. DOI Long-term relapse prevention study showing continued citalopram treatment reduced relapse vs placebo; both 20 mg and 40 mg effective.
  3. Witchel HJ, Hancox JC, Nutt DJ. Psychotropic drugs, cardiac arrhythmia, and sudden death. J Clin Psychopharmacol. 2003;23(1):58–77. DOI Review of QT prolongation mechanisms with psychotropics; contextualises citalopram’s cardiac safety profile among SSRIs.
Guidelines
  1. American Psychiatric Association. Practice Guideline for the Treatment of Patients with Major Depressive Disorder. 3rd ed. Washington, DC: APA; 2010. APA APA guideline positioning SSRIs including citalopram as first-line treatment for MDD.
  2. National Institute for Health and Care Excellence (NICE). Depression in adults: treatment and management. NICE guideline NG222. 2022. NICE UK guideline on SSRI selection, monitoring, and discontinuation; considers citalopram a first-line option.
  3. Cipriani A, Furukawa TA, Salanti G, et al. Comparative efficacy and acceptability of 21 antidepressant drugs for the acute treatment of adults with major depressive disorder: a systematic review and network meta-analysis. Lancet. 2018;391(10128):1357–1366. DOI Landmark network meta-analysis comparing antidepressant efficacy and acceptability; citalopram used as the reference comparator.
Mechanistic / Basic Science
  1. Hyttel J. Citalopram — pharmacological profile of a specific serotonin uptake inhibitor with antidepressant activity. Prog Neuropsychopharmacol Biol Psychiatry. 1982;6(3):277–295. DOI Foundational pharmacological characterisation establishing citalopram’s selectivity for SERT over other monoamine transporters and receptors.
  2. Owens MJ, Knight DL, Nemeroff CB. Second-generation SSRIs: human monoamine transporter binding profile of escitalopram and R-fluoxetine. Biol Psychiatry. 2001;50(5):345–350. DOI Demonstrates that the S-enantiomer (escitalopram) is primarily responsible for serotonin transporter binding in racemic citalopram.
Pharmacokinetics / Special Populations
  1. Gutierrez MM, Abramowitz W. Steady-state pharmacokinetics of citalopram in young and elderly subjects. Pharmacotherapy. 2000;20(12):1441–1447. DOI Pharmacokinetic study in elderly demonstrating increased AUC and half-life, supporting the 20 mg dose cap in patients >60 years.
  2. Herrlin K, Yasui-Furukori N, Tybring G, et al. Metabolism of citalopram enantiomers in CYP2C19/CYP2D6 phenotyped panels of healthy Swedes. Br J Clin Pharmacol. 2003;56(4):415–421. DOI Demonstrates the role of CYP2C19 in citalopram metabolism and the pharmacogenomic basis for dose adjustment in poor metabolisers.
  3. Zivin K, Pfeiffer PN, Bohnert ASB, et al. Evaluation of the FDA warning against prescribing citalopram at doses exceeding 40 mg. Am J Psychiatry. 2013;170(6):642–650. DOI Population-level analysis assessing clinical impact of the FDA dose ceiling on citalopram prescribing and patient outcomes.