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Drug Monograph

Remeron (Mirtazapine)

mirtazapine tablets and orally disintegrating tablets (SolTab)

Noradrenergic and Specific Serotonergic Antidepressant (NaSSA) · Oral
Pharmacokinetic Profile
Half-Life
20–40 h (females longer than males)
Metabolism
CYP2D6, CYP3A4, CYP1A2
Protein Binding
85%
Bioavailability
~50%
Volume of Distribution
Widely distributed
Clinical Information
Drug Class
NaSSA (tetracyclic)
Available Doses
Tablets: 7.5, 15, 30, 45 mg | SolTab: 15, 30, 45 mg
Route
Oral
Renal Adjustment
May be needed (mod-severe)
Hepatic Adjustment
May be needed
Pregnancy
Use only if clearly needed
Lactation
Present in breast milk; exercise caution
Schedule
Not a controlled substance
Generic Available
Yes
Black Box Warning
Suicidality in youth
Rx

Indications

IndicationApproved PopulationTherapy TypeStatus
Major Depressive Disorder (MDD)AdultsMonotherapyFDA Approved

Mirtazapine is an atypical tetracyclic antidepressant and the first noradrenergic and specific serotonergic antidepressant (NaSSA) to reach market. FDA-approved in 1996, its efficacy for MDD was established in four 6-week controlled trials of adult outpatients dosed between 5 and 60 mg/day, and a longer-term relapse prevention study of up to 40 weeks. Mirtazapine is not approved for pediatric use. Its unique receptor pharmacology produces a distinctive clinical profile: potent sedation, appetite stimulation, antiemetic effects, and anxiolysis, with minimal sexual dysfunction. Clinicians frequently select mirtazapine for patients with depression complicated by insomnia, poor appetite, low body weight, or prominent anxiety, as well as those who have not tolerated SSRIs or SNRIs.

Off-Label Uses

Insomnia: Widely used at low doses (7.5–15 mg) for its potent H1-mediated sedation. Sedation is paradoxically greater at lower doses. Evidence quality: Moderate.

Appetite stimulation (cancer, HIV, elderly): Used to counteract cachexia and anorexia; 5-HT2C and H1 antagonism drive weight gain and appetite. Evidence quality: Moderate.

Nausea/vomiting (antiemetic): 5-HT3 antagonism provides ondansetron-like antiemetic properties; used in palliative care and chemotherapy-associated nausea. Evidence quality: Low-Moderate.

PTSD, generalized anxiety, social anxiety: Anxiolytic properties from 5-HT2A and H1 antagonism; some guideline recommendations. Evidence quality: Low.

Pruritus: H1 antagonism may relieve itch in cholestatic and uremic conditions. Evidence quality: Low.

Dose

Dosing

Adult Dosing by Clinical Scenario

Clinical ScenarioStarting DoseMaintenance DoseMaximum DoseNotes
MDD — standard adult15 mg once daily at bedtime15–45 mg once daily45 mg/dayDose changes at intervals ≥1–2 weeks (long half-life)
Administer in the evening before sleep due to sedative effects
MDD — insomnia-predominant7.5–15 mg at bedtime15–30 mg at bedtime45 mg/dayLower doses are paradoxically more sedating due to dominant H1 effects
Increasing dose may actually reduce sedation as NE activation counterbalances H1
MDD — anorexia / weight loss-predominant15 mg at bedtime30–45 mg at bedtime45 mg/dayAppetite stimulation and weight gain are dose-related; 7.5% had ≥7% body weight gain vs 0% placebo
MDD — elderly (≥65 years)7.5–15 mg at bedtime15–45 mg at bedtime45 mg/dayReduced clearance (40% lower in elderly males, 10% lower in elderly females)
Increased hyponatremia and over-sedation risk; start low
MDD — renal impairment (moderate: CrCl 11–39)15 mg at bedtimeDose decrease may be neededClearance reduced ~30%; monitor for adverse effects
Severe impairment (CrCl <10): clearance reduced ~50%
MDD — hepatic impairment15 mg at bedtimeDose decrease may be neededClearance reduced ~30% in hepatic impairment; ALT elevations ≥3× ULN occurred in 2% vs 0.3% placebo
MDD — with strong CYP3A4 inhibitorDose decrease may be neededKetoconazole increases Cmax ~40% and AUC ~50%; also applies to clarithromycin, HIV protease inhibitors
MDD — with strong CYP3A inducerDose increase may be neededCarbamazepine decreases mirtazapine levels by ~60%; also phenytoin, rifampin
MDD — with cimetidineDose decrease may be neededCimetidine increases mirtazapine levels by ~50%
MDD — discontinuation / taperingGradual dose reduction recommendedDiscontinuation syndrome reported: dizziness, paresthesia, anxiety, nausea, sweating, abnormal dreams
Clinical Pearl: Paradoxical dose-dependent sedation

Mirtazapine’s sedative effect is paradoxically greater at lower doses (7.5–15 mg) than at higher doses (30–45 mg). This occurs because at low doses, the potent H1 histamine receptor antagonism dominates, producing marked drowsiness. At higher doses, increased noradrenergic and serotonergic neurotransmission through α2-adrenergic blockade provides an activating effect that partially counterbalances the H1-mediated sedation. Clinicians can leverage this by using lower doses for insomnia-predominant depression and titrating upward if excessive daytime sedation limits function. Patients should be counselled that increasing the dose may paradoxically improve daytime alertness.

PK

Pharmacology

Mechanism of Action

Mirtazapine is classified as a noradrenergic and specific serotonergic antidepressant (NaSSA). Unlike SSRIs and SNRIs, it does not inhibit the reuptake of serotonin or norepinephrine. Instead, mirtazapine enhances central noradrenergic and serotonergic neurotransmission through antagonism of central presynaptic α2-adrenergic autoreceptors and heteroreceptors, which removes the inhibitory brake on NE and 5-HT release. It selectively blocks postsynaptic 5-HT2A, 5-HT2C, and 5-HT3 receptors, channelling enhanced serotonergic activity specifically through 5-HT1A receptors, which mediate antidepressant and anxiolytic effects. Its potent H1 histamine receptor antagonism accounts for its pronounced sedative and appetite-stimulating properties. Mirtazapine has negligible affinity for muscarinic cholinergic receptors, which distinguishes it from tricyclic antidepressants.

ADME Profile

ParameterValueClinical Implication
AbsorptionRapidly absorbed; Tmax ~2 h; bioavailability ~50% (first-pass metabolism); food has minor effect on rate but not extentCan be given with or without food; administer at bedtime for optimal sleep benefit; steady state in 4–6 days
DistributionProtein binding 85% (non-specific, reversible); widely distributed into tissuesCrosses blood-brain barrier; moderate protein binding unlikely to produce displacement interactions
MetabolismHepatic via CYP2D6 and CYP3A4 (both major pathways), with CYP1A2 contributing; N-demethylation (to active desmethylmirtazapine, ~3–10% of activity), hydroxylation, and conjugationSusceptible to CYP3A inducers (carbamazepine reduces levels ~60%) and inhibitors (ketoconazole increases AUC ~50%); CYP2D6 inhibitors cause only modest increases (~17–32%); does not significantly inhibit CYP enzymes itself
Eliminationt½: 20–40 h (gender-dependent; females longer); 75% urine, 15% feces; ~100% excreted within 4 daysLong half-life supports once-daily dosing; dose changes ≥1–2 weeks apart; reduced clearance in elderly (especially males: 40% lower), renal impairment (~30–50%), and hepatic impairment (~30%)
SE

Side Effects

≥10%Very Common (US 6-week placebo-controlled trials)
Adverse EffectIncidenceClinical Note
Somnolence54% (placebo 18%)Most common adverse effect; dose-dependent paradox: more sedating at lower doses; resulted in 10.4% discontinuation rate (vs 2.2% placebo)
Dry mouth25% (placebo 15%)Encourage hydration, sugar-free gum, and good oral hygiene
Increased appetite17% (placebo 2%)Mediated by 5-HT2C and H1 antagonism; clinically useful in anorexic or cachectic patients
Constipation13% (placebo 7%)Increase fibre and fluid intake; osmotic laxative if persistent
Weight gain12% (placebo 2%)7.5% had ≥7% body weight gain vs 0% placebo; 8% of premarketing patients discontinued for weight gain
1–10%Common
Adverse EffectIncidenceClinical Note
Asthenia / fatigue8% (placebo 5%)Related to H1 antagonism; may improve with dose adjustment
Dizziness7% (placebo 3%)Likely related to orthostatic effects and sedation; rise slowly from sitting/lying position
Flu-like syndrome5% (placebo 3%)Monitor for actual infection signs, especially given agranulocytosis risk
Abnormal dreams4% (placebo 1%)Vivid or disturbing dreams; 5-HT2A antagonism alters sleep architecture
Thinking abnormal3% (placebo 1%)Usually mild cognitive effects related to sedation
Tremor2% (placebo 1%)Less common than with SSRIs or SNRIs
Confusion2% (placebo 0%)More common in elderly; monitor and consider dose reduction
Peripheral edema2% (placebo 1%)Monitor fluid status
Urinary frequency2% (placebo 1%)Usually mild and self-limiting
SeriousSerious (Regardless of Frequency)
Adverse EffectEstimated FrequencyTypical OnsetRequired Action
Agranulocytosis / severe neutropeniaRare (~0.1%; 3/2796 in premarketing trials)Days 9–61 of treatmentDiscontinue immediately if sore throat, fever, stomatitis, or infection signs develop with low WBC; closely monitor patient; all 3 cases recovered after discontinuation
Serotonin syndromeRareHours to days after initiation or dose increaseDiscontinue mirtazapine and all serotonergic agents; supportive care; can occur alone or with concomitant serotonergic drugs
QTc prolongation / Torsades de PointesRare (mostly in overdose or with QT-prolonging drugs)VariableCaution in patients with cardiovascular disease, family history of QT prolongation, or concurrent QTc-prolonging drugs; ECG if indicated
Suicidal ideation (age <25)UncommonFirst weeks or dose changesClose monitoring; FDA Black Box Warning; not approved for pediatric use
Hyponatremia / SIADHRareWeeks to monthsMonitor serum sodium if symptoms develop (confusion, weakness, falls); discontinue if symptomatic; elderly and diuretic users at higher risk
Severe skin reactions (SJS, TEN)Very rareVariableDiscontinue immediately; emergency care; permanent contraindication to rechallenge
Elevated cholesterol / triglycerides15% cholesterol ≥20% above ULN; 6% triglycerides ≥500Weeks to monthsMonitor lipid panel; weigh cardiovascular risk; consider lipid-lowering therapy or alternative antidepressant
Transaminase elevations (≥3× ULN)2.0% (vs 0.3% placebo)VariableMonitor LFTs if symptoms develop; some cases resolved despite continued treatment; use with caution in hepatic impairment
Mania / hypomania activation0.2%First weeksScreen for bipolar before initiation; discontinue; initiate mood stabilizer
DiscontinuationTreatment Discontinuation Rates
Mirtazapine (n=453)
16% vs 7% placebo
Top reasons: Somnolence (10.4% vs 2.2% placebo), nausea (1.5% vs 0%)
Weight Gain (premarketing)
8%
Discontinued specifically for weight gain during open-label and long-term treatment
Weight Gain Management

Weight gain is the most clinically limiting metabolic side effect of mirtazapine. In controlled trials, 7.5% of patients gained ≥7% of body weight compared to 0% on placebo. In pediatric trials (not an approved population), the figure was 49%. Counsel patients about dietary management from the outset. Consider baseline weight and metabolic parameters (lipids, glucose) before starting treatment. If clinically significant weight gain develops that is not desirable, reassess the risk-benefit of continued treatment and consider alternative antidepressants.

Int

Drug Interactions

Mirtazapine is metabolized by CYP2D6, CYP3A4, and CYP1A2 but does not significantly inhibit any CYP enzymes itself, giving it a relatively clean outbound interaction profile. The main interactions are inbound: drugs that inhibit or induce CYP3A4 significantly alter mirtazapine exposure. Additionally, its serotonergic properties create a risk of serotonin syndrome with other serotonergic agents, and its sedative properties are additive with CNS depressants.

MajorMAOIs (phenelzine, tranylcypromine, isocarboxazid, linezolid, IV methylene blue)
MechanismAdditive serotonergic effects with impaired serotonin degradation
EffectSerotonin syndrome (agitation, hyperthermia, rigidity, myoclonus, autonomic instability)
ManagementContraindicated. Allow 14 days between MAOI and mirtazapine in BOTH directions
FDA PI
MajorOther serotonergic drugs (SSRIs, SNRIs, triptans, TCAs, fentanyl, lithium, tramadol, tryptophan, St. John’s Wort)
MechanismAdditive serotonergic activity
EffectIncreased risk of serotonin syndrome
ManagementMonitor for serotonin syndrome symptoms; consider discontinuation if occurs. Note: mirtazapine + SSRI/SNRI combination (“California rocket fuel”) is used clinically but requires vigilant monitoring
FDA PI
ModerateStrong CYP3A4 inducers (carbamazepine, phenytoin, rifampin)
MechanismCYP3A4 induction increases mirtazapine metabolism
EffectCarbamazepine decreases mirtazapine levels by ~60%; potential loss of efficacy
ManagementIncrease mirtazapine dose as needed; decrease again if inducer is discontinued
FDA PI
ModerateStrong CYP3A4 inhibitors (ketoconazole, clarithromycin, HIV protease inhibitors)
MechanismCYP3A4 inhibition decreases mirtazapine clearance
EffectKetoconazole increases Cmax by ~40% and AUC by ~50%
ManagementDecrease mirtazapine dose as needed; increase again if inhibitor is discontinued
FDA PI
ModerateCimetidine
MechanismNon-specific inhibition of mirtazapine metabolism (multiple CYP pathways)
EffectIncreases mirtazapine levels by ~50%
ManagementDecrease mirtazapine dose as needed; increase again if cimetidine is discontinued
FDA PI
ModerateWarfarin
MechanismMechanism not fully characterized; modest INR increase observed
EffectIncreased anticoagulant effect
ManagementMonitor INR when starting or stopping mirtazapine in warfarin-treated patients
FDA PI
ModerateAlcohol and benzodiazepines
MechanismAdditive CNS depressant effects with H1 antagonist-mediated sedation
EffectImpaired cognitive and motor performance; excessive sedation
ManagementAvoid alcohol; use benzodiazepines cautiously; warn patients about additive sedation
FDA PI
MinorCYP2D6 inhibitors (paroxetine, fluoxetine)
MechanismCYP2D6 inhibition modestly increases mirtazapine levels (paroxetine: ~17%; fluoxetine: ~32%)
EffectModest increase in exposure without clinically relevant consequences in most patients
ManagementNo routine dose adjustment needed; monitor for enhanced sedation or other adverse effects
FDA PI
Mon

Monitoring

  • Complete Blood CountIf infection signs develop
    Trigger-based    Agranulocytosis (ANC <500/mm³) occurred in 2/2796 premarketing patients (+ 1 severe neutropenia). If sore throat, fever, stomatitis, mucous membrane ulceration, or flu-like symptoms develop, obtain CBC with differential immediately. Discontinue if WBC is low.
  • Weight & BMIBaseline, then each visit
    Routine    7.5% of patients gained ≥7% body weight (vs 0% placebo). Monitor appetite and weight at every follow-up. Counsel on dietary measures from initiation.
  • Lipid PanelBaseline, then periodically
    Routine    Nonfasting cholesterol ≥20% above ULN in 15% (vs 7% placebo); triglycerides ≥500 mg/dL in 6% (vs 3% placebo). Check fasting lipids at baseline and at 3–6 months.
  • Suicidality AssessmentWeekly for first 4 weeks, then at each visit
    Routine    Especially important in patients under 25. Monitor for clinical worsening, agitation, irritability, and suicidal ideation.
  • Hepatic FunctionBaseline; as indicated
    Trigger-based    ALT ≥3× ULN occurred in 2.0% vs 0.3% placebo. Monitor LFTs if symptoms of hepatotoxicity develop. Use with caution in hepatic impairment (clearance reduced ~30%).
  • Serum SodiumAs indicated
    Trigger-based    Hyponatremia (SIADH) reported; check if confusion, weakness, unsteadiness, or falls develop. Elderly and diuretic users at highest risk.
  • Sedation LevelEach visit, especially early
    Routine    54% experience somnolence. Assess impact on driving and daily function. Consider dose adjustment (paradoxically, increasing dose may reduce sedation).
  • Renal FunctionBaseline
    Routine    75% renally excreted. Clearance reduced ~30% (moderate) to ~50% (severe impairment). Dose reduction may be needed.
CI

Contraindications & Cautions

Absolute Contraindications

  • Concurrent MAOI use or use within 14 days of MAOI discontinuation in either direction (serotonin syndrome risk)
  • Concurrent linezolid or IV methylene blue (reversible MAO inhibition)
  • Known hypersensitivity to mirtazapine or any excipient (SJS, bullous dermatitis, erythema multiforme, TEN reported)

Relative Contraindications (Specialist Input Recommended)

  • Severe hepatic impairment: Clearance significantly reduced; dose decrease needed; ALT elevations occur more frequently
  • Severe renal impairment (CrCl <10): Clearance reduced ~50%; dose decrease needed
  • Known cardiovascular disease or QT prolongation risk: Post-marketing TdP reports; exercise caution and consider ECG monitoring
  • Phenylketonuria (SolTab only): Contains phenylalanine (2.6 mg per 15 mg tablet, 5.2 mg per 30 mg, 7.8 mg per 45 mg)

Use with Caution

  • Bipolar disorder: Screen before initiation; mania/hypomania activation reported in 0.2%
  • Seizure disorders: 1 seizure in 2796 premarketing patients; prescribe with caution
  • Elderly patients: Reduced clearance, increased sedation risk, increased hyponatremia risk, increased fall risk
  • Patients receiving concomitant serotonergic drugs: Serotonin syndrome risk
  • Cardiovascular disease or hypotension risk: Orthostatic hypotension observed in early volunteer trials
FDA Boxed Warning Suicidality in Pediatric and Young Adult Patients

Antidepressants increased the risk of suicidal thoughts and behaviors in pediatric and young adult patients in short-term studies. Closely monitor all antidepressant-treated patients for clinical worsening and emergence of suicidal thoughts and behaviors. Mirtazapine is not approved for use in pediatric patients. In an 8-week pediatric trial, 49% of mirtazapine-treated patients gained ≥7% body weight (vs 5.7% placebo), highlighting the unfavorable benefit-risk profile in this population.

Pt

Patient Counselling

Purpose of Therapy

Mirtazapine is prescribed to treat depression. Unlike many other antidepressants, it works by increasing the release of both serotonin and norepinephrine in the brain through a unique mechanism. It also helps with sleep and appetite, which are often disrupted in depression. Improvement in sleep may begin within the first few days, while improvement in mood typically takes 2 to 4 weeks. Continue taking the medication as prescribed even after you feel better.

How to Take

Take mirtazapine once daily, preferably in the evening before bedtime, as it causes drowsiness. Tablets can be taken with or without food. If using the orally disintegrating tablet (SolTab), open the blister pack with dry hands, place the tablet on your tongue, and let it dissolve in your saliva without chewing or crushing. It does not need water. Do not stop this medication suddenly; talk to your prescriber about tapering gradually.

Drowsiness & Sedation
Tell patientDrowsiness is the most common side effect, affecting about half of patients. It is most noticeable in the first few weeks. Taking the medication at bedtime helps. Counterintuitively, increasing the dose may actually reduce daytime drowsiness. Do not drive or operate machinery until you know how this medication affects you.
Call prescriberIf excessive daytime drowsiness persists beyond 2–3 weeks and affects daily function; dose adjustment may help.
Weight Gain & Increased Appetite
Tell patientThis medication commonly increases appetite and may cause weight gain. Monitor your weight regularly. Focus on balanced eating, portion control, and regular physical activity from the start. For some patients, this appetite increase is a benefit, particularly if depression has caused significant weight loss.
Call prescriberIf weight gain is rapid or exceeds what you are comfortable with; alternative treatments can be discussed.
Signs of Infection (Agranulocytosis Warning)
Tell patientRarely, mirtazapine can lower white blood cell counts, making you more susceptible to infection. This is uncommon but requires urgent attention. Be aware of signs like sore throat, fever, mouth sores, or flu-like symptoms that seem unusual or severe.
Call prescriberImmediately if you develop fever, sore throat, mouth ulcers, or any signs of infection. A blood test will be needed promptly.
Alcohol & Sedating Substances
Tell patientAvoid alcohol while taking mirtazapine. The combination significantly increases drowsiness and impairs coordination and judgment. Similarly, be cautious with other sedating medications, including over-the-counter antihistamines and sleep aids.
Call prescriberIf you are prescribed any new medication, including benzodiazepines or opioids, while on mirtazapine.
Do Not Stop Abruptly
Tell patientStopping mirtazapine suddenly can cause withdrawal symptoms including dizziness, nausea, anxiety, tingling sensations, and disturbed sleep. Always taper gradually under your prescriber’s guidance.
Call prescriberIf you accidentally miss several doses or want to discontinue; withdrawal symptoms can usually be managed by reinstating and slowly tapering.
Ref

Sources

Regulatory (PI / SmPC)
  1. REMERON (mirtazapine) Tablets / REMERONSolTab (mirtazapine) Orally Disintegrating Tablets. Full Prescribing Information. Merck Sharp & Dohme Corp. Revised March 2020. accessdata.fda.govPrimary source for all dosing, adverse reaction Table 3 and 4 data, contraindications, warnings, pharmacokinetic parameters, and drug interactions cited in this monograph.
  2. REMERON (mirtazapine) Tablets. Full Prescribing Information. Revised 2021. accessdata.fda.govUpdated label with QTc prolongation data from thorough QT study, post-marketing TdP and sudden death reports.
Key Clinical Trials
  1. Wheatley DP, van Moffaert M, Timmerman L, Slooff CJ. Mirtazapine: efficacy and tolerability in comparison with fluoxetine in patients with moderate to severe major depressive disorder. J Clin Psychiatry. 1998;59(6):306-312. doi:10.4088/JCP.v59n0606Randomized controlled trial demonstrating comparable efficacy of mirtazapine versus fluoxetine in moderate-severe MDD with faster onset of effect on anxiety and sleep symptoms.
  2. Fawcett J, Barkin RL. A meta-analysis of eight randomized, double-blind, controlled clinical trials of mirtazapine for the treatment of patients with major depression and symptoms of anxiety. J Clin Psychiatry. 1998;59(3):123-127. doi:10.4088/JCP.v59n0306Meta-analysis confirming mirtazapine efficacy with particular benefit in depression with anxiety symptoms.
  3. Thase ME, Nierenberg AA, Keller MB, Panagides J; Relapse Prevention Study Group. Efficacy of mirtazapine for prevention of depressive relapse: a placebo-controlled double-blind trial of recently remitted high-risk patients. J Clin Psychiatry. 2001;62(10):782-788. doi:10.4088/JCP.v62n1006Relapse prevention trial establishing long-term maintenance efficacy at 15–45 mg/day for up to 40 weeks.
Guidelines
  1. Lam RW, Kennedy SH, Adams C, et al. Canadian Network for Mood and Anxiety Treatments (CANMAT) 2023 Update on Clinical Guidelines for Management of Major Depressive Disorder in Adults. Can J Psychiatry. 2024;69(9):641-687. doi:10.1177/07067437241245384Current Canadian guideline listing mirtazapine as a first-line antidepressant, particularly suitable for depression with insomnia, anxiety, or appetite loss.
  2. Qaseem A, Owens DK, Etxeandia-Ikobaltzeta I, et al. Nonpharmacologic and pharmacologic treatments of adults in the acute phase of major depressive disorder: a living clinical guideline from the American College of Physicians. Ann Intern Med. 2023;176(2):239-252. doi:10.7326/M22-1693ACP guideline including mirtazapine among recommended second-generation antidepressants for acute MDD treatment.
Mechanistic / Basic Science
  1. de Boer T. The pharmacologic profile of mirtazapine. J Clin Psychiatry. 1996;57 Suppl 4:19-25.Foundational paper describing the NaSSA mechanism: α2-adrenergic antagonism, 5-HT2/5-HT3 antagonism, and H1 antagonism.
  2. Anttila SAK, Leinonen EVJ. A review of the pharmacological and clinical profile of mirtazapine. CNS Drug Rev. 2001;7(3):249-264. doi:10.1111/j.1527-3458.2001.tb00198.xComprehensive review of mirtazapine receptor pharmacology, clinical efficacy data, and the paradoxical dose-dependent sedation profile.
Pharmacokinetics / Special Populations
  1. Timmer CJ, Sitsen JM, Delbressine LP. Clinical pharmacokinetics of mirtazapine. Clin Pharmacokinet. 2000;38(6):461-474. doi:10.2165/00003088-200038060-00001Definitive PK review: bioavailability ~50%, t½ 20–40 h, gender/age effects, CYP enzyme contributions, and renal/hepatic impairment data.
  2. Mirtazapine. In: StatPearls [Internet]. Treasure Island (FL): StatPearls Publishing; 2024. ncbi.nlm.nih.govCurrent comprehensive review of mechanism, dosing, clinical applications, adverse effects, and toxicity across all clinical scenarios.
  3. Hassanein EHM, Althagafy HS, Baraka MA, Abd-alhameed EK, Ibrahim IM. Pharmacological update of mirtazapine: a narrative literature review. Naunyn Schmiedebergs Arch Pharmacol. 2024;397:4097-4116. doi:10.1007/s00210-023-02880-wRecent narrative review covering updated pharmacological understanding, off-label uses, and special population considerations.