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Drug Monograph

Fetzima (Levomilnacipran)

levomilnacipran hydrochloride extended-release capsules

Serotonin-Norepinephrine Reuptake Inhibitor (SNRI) · Oral
Pharmacokinetic Profile
Half-Life
~12 hours
Metabolism
CYP3A4 (primary); minor CYP2C8, 2C19, 2D6, 2J2
Protein Binding
22%
Bioavailability
92%
Volume of Distribution
387–473 L
Clinical Information
Drug Class
SNRI (norepinephrine-preferential)
Available Doses
20 mg, 40 mg, 80 mg, 120 mg ER capsules
Route
Oral
Renal Adjustment
Required (moderate-severe)
Hepatic Adjustment
Not required
Pregnancy
Risk in third trimester
Lactation
Unknown in human milk; milnacipran present in milk (milk/plasma ratio 1.85)
Schedule
Not a controlled substance
Generic Available
Limited
Black Box Warning
Suicidality in youth
Rx

Indications

IndicationApproved PopulationTherapy TypeStatus
Major Depressive Disorder (MDD)Adults (18+)MonotherapyFDA Approved

Levomilnacipran is the active 1S,2R-enantiomer of milnacipran and was approved by the FDA in July 2013 for the treatment of MDD in adults. Its efficacy was established in three 8-week, randomized, double-blind, placebo-controlled studies (two fixed-dose and one flexible-dose) at doses of 40 to 120 mg once daily. The drug is explicitly not approved for fibromyalgia management, despite its parent compound milnacipran holding that indication. Levomilnacipran is distinguished from other SNRIs by its preferential norepinephrine reuptake inhibition (NE:5-HT selectivity ratio of approximately 2:1), which may confer benefits for fatigue and motivational symptoms in depression.

Off-Label Uses

Fibromyalgia: Despite milnacipran’s approval for fibromyalgia, levomilnacipran has not been studied for this indication, and the FDA PI explicitly states it is not approved for fibromyalgia. Evidence quality: Very low.

Fatigue-predominant depression: Mechanism-based rationale from its noradrenergic profile; limited direct clinical evidence beyond post-hoc analyses of pivotal MDD trials. Evidence quality: Low.

Anxiety disorders: No dedicated trials; limited evidence from pooled analyses of anxious depression subgroups. Evidence quality: Very low.

Dose

Dosing

Adult Dosing by Clinical Scenario

Clinical ScenarioStarting DoseMaintenance DoseMaximum DoseNotes
MDD — new diagnosis, standard patient20 mg daily × 2 days, then 40 mg daily40–120 mg once daily120 mg/dayTitrate in 40 mg increments every ≥2 days based on response and tolerability
Titration pack available: two 20 mg + twenty-six 40 mg capsules
MDD — moderate renal impairment (CrCl 30–59 mL/min)20 mg daily × 2 days, then 40 mg daily40–80 mg once daily80 mg/dayDo not exceed 80 mg/day
MDD — severe renal impairment (CrCl 15–29 mL/min)20 mg daily × 2 days, then 40 mg daily40 mg once daily40 mg/dayDo not exceed 40 mg/day
Half-life prolonged to ~27.7 h in severe impairment
MDD — end-stage renal disease (ESRD)Not recommendedDialysis unlikely to reduce plasma concentrations due to large Vd
MDD — hepatic impairment (any severity)20 mg daily × 2 days, then 40 mg daily40–120 mg once daily120 mg/dayNo dose adjustment needed; hepatic elimination is low
Applies to mild, moderate, and severe hepatic impairment (Child-Pugh 1–13)
MDD — concurrent strong CYP3A4 inhibitor20 mg daily × 2 days, then 40 mg daily40–80 mg once daily80 mg/dayDo not exceed 80 mg/day with ketoconazole, itraconazole, clarithromycin, etc.
Ketoconazole increases levomilnacipran AUC by ~57%
MDD — elderly (65+)20 mg daily × 2 days, then 40 mg daily40–120 mg once daily120 mg/dayNo age-based adjustment; modestly higher exposure (Cmax +24%, AUC +26%)
Monitor for hyponatremia; limited data (<3% of trial patients were 65+)
MDD — discontinuation / taperingGradual dose reduction recommendedNo specific taper schedule in PI; reduce dose gradually whenever possible to minimize discontinuation symptoms
Clinical Pearl: Titration schedule and noradrenergic advantage

Unlike desvenlafaxine (which starts at target dose), levomilnacipran requires a 2-day lead-in at 20 mg followed by titration. The therapeutic range is 40–120 mg, offering dose flexibility. Its preferential norepinephrine reuptake inhibition across all therapeutic doses distinguishes it from venlafaxine and duloxetine, which achieve meaningful noradrenergic activity only at higher doses. This makes levomilnacipran particularly worth considering for patients whose depression features prominent fatigue, low energy, or psychomotor slowing. Capsules must be swallowed whole and must not be opened, chewed, or crushed.

Alcohol Interaction Warning

Alcohol disrupts the extended-release mechanism of levomilnacipran capsules. In vitro data show that 40% alcohol causes nearly complete drug release within 4 hours, creating a dose-dumping risk. Patients must be counselled to avoid alcohol while taking levomilnacipran. This interaction is unique to levomilnacipran among the SNRIs.

PK

Pharmacology

Mechanism of Action

Levomilnacipran is the more pharmacologically active 1S,2R-enantiomer of the racemic SNRI milnacipran. It inhibits both serotonin (SERT) and norepinephrine (NET) reuptake transporters, but with a distinctive selectivity profile: levomilnacipran is approximately 2-fold more potent at inhibiting norepinephrine reuptake than serotonin reuptake. This contrasts sharply with other marketed SNRIs (venlafaxine, desvenlafaxine, duloxetine), all of which preferentially inhibit serotonin reuptake. Importantly, levomilnacipran achieves simultaneous serotonin and norepinephrine reuptake inhibition across its full dose range (40–120 mg), unlike venlafaxine, which requires higher doses to engage the norepinephrine transporter. Levomilnacipran has no clinically meaningful affinity for muscarinic, histaminergic, or adrenergic receptors, which accounts for its relatively clean side-effect profile outside of its expected monoaminergic effects.

ADME Profile

ParameterValueClinical Implication
Absorption92% bioavailability (ER capsule vs solution); Tmax 6–8 h; food does not significantly affect concentrationCan be given with or without food; steady state within ~3 days at once-daily dosing; no interconversion between enantiomers
DistributionVd = 387–473 L; protein binding 22% (non-saturable, 10–1000 ng/mL)Very wide tissue distribution; dialysis ineffective for overdose; low protein binding minimizes displacement interactions
MetabolismPrimary: CYP3A4 (desethylation to N-desethyl levomilnacipran); minor: CYP2C8, 2C19, 2D6, 2J2; also UGT glucuronidationStrong CYP3A4 inhibitors require dose cap at 80 mg/day; does not significantly inhibit or induce CYP enzymes; weak P-gp substrate
Eliminationt½ ~12 h; clearance 21–29 L/h; 58% unchanged in urine; 18% as N-desethyl metabolite; all metabolites inactivePrimarily renal elimination of parent drug; dose reduction in moderate and severe renal impairment; not recommended in ESRD
SE

Side Effects

≥10%Very Common
Adverse EffectIncidence (40–120 mg)Clinical Note
Nausea17% (placebo 6%)Most common adverse effect; tends to occur early and is often transient; only cause of discontinuation in ≥1% of patients (1.5%)
1–10%Common
Adverse EffectIncidence (40–120 mg)Clinical Note
Constipation9% (placebo 3%)Likely noradrenergic effect; increase fiber, fluids; osmotic laxative if persistent
Hyperhidrosis9% (placebo 2%)Related to noradrenergic activation; breathable clothing, clinical antiperspirants
Heart rate increased6% (placebo 1%)Noradrenergic class effect; mean increase ~7 bpm; monitor in patients with cardiac disease
Tachycardia6% (placebo 2%)Includes sinus tachycardia and postural orthostatic tachycardia syndrome
Erectile dysfunction (men)6% (placebo 1%)Dose-related: 6% at 40 mg, 8% at 80 mg, 10% at 120 mg; inquire proactively
Ejaculation disorder (men)5% (placebo <1%)Includes delayed ejaculation, ejaculation failure, and premature ejaculation
Palpitations5% (placebo 1%)Noradrenergic effect; often benign but evaluate if persistent or symptomatic
Vomiting5% (placebo 1%)Usually early and self-limiting; taking with food may help
Urinary hesitation4% (placebo 0%)Dose-related: 4%/5%/6% at 40/80/120 mg; more prominent in males; evaluate for urinary retention
Testicular pain (men)4% (placebo <1%)Includes epididymitis and seminal vesiculitis; unique among SNRIs
Hot flush3% (placebo 1%)Noradrenergic mediated vasomotor effect
Blood pressure increased3% (placebo 1%)Includes systolic, diastolic, and orthostatic BP increases; control hypertension before starting
Hypertension3% (placebo 1%)Includes labile hypertension; regular monitoring essential
Hypotension3% (placebo 1%)Includes orthostatic hypotension and postural dizziness; advise rising slowly
Decreased appetite3% (placebo 1%)Weight-neutral in short-term and long-term studies
Rash2% (placebo 0%)Includes generalized, maculopapular, erythematous, and macular rash
SeriousSerious (Regardless of Frequency)
Adverse EffectEstimated FrequencyTypical OnsetRequired Action
Suicidal ideation (age <25)UncommonFirst weeks or dose changesClose monitoring; consider discontinuation if worsening; FDA Black Box Warning
Serotonin syndromeRareHours to days after dose increase or serotonergic co-medicationImmediate discontinuation; supportive care; cyproheptadine if severe
Sustained hypertensionUncommonWeeks to monthsRegular BP monitoring; control pre-existing hypertension before initiation; consider dose reduction or discontinuation
Urinary retentionUncommonVariable; dose-relatedDiscontinue or reduce dose; evaluate for BPH; may require catheterization in acute cases
Hyponatremia / SIADHRareFirst weeks; higher risk in elderlyCheck serum sodium; discontinue if symptomatic; fluid restriction
Mania / hypomania activationRareFirst weeksDiscontinue; evaluate for bipolar disorder; initiate mood stabilizer
Abnormal bleedingUncommonAny time, especially with concurrent anticoagulants/NSAIDsMonitor for bruising, GI bleeding; adjust anticoagulation as needed
SeizuresRareAny timeDiscontinue; use cautiously in patients with seizure disorders
Angle-closure glaucomaRareAny timeAvoid in untreated anatomically narrow angles; urgent ophthalmology referral if acute symptoms
Takotsubo cardiomyopathyVery rare (post-marketing)VariableDiscontinue; cardiology referral; supportive care
DiscontinuationTreatment Discontinuation Rates
Adults (40–120 mg, all doses)
9% vs 3% placebo
Top reason: Nausea (1.5% vs 0.4% placebo); no other single adverse event caused ≥1% discontinuation
Serious adverse events
0.7% vs 1.3% placebo
No deaths occurred during clinical trials; serious adverse event rate was lower than placebo
Managing Cardiovascular Effects

The noradrenergic potency of levomilnacipran produces clinically significant cardiovascular effects more prominently than other SNRIs. Heart rate increases (mean ~7 bpm), tachycardia, palpitations, and blood pressure elevation are all more common than with placebo. Pre-existing hypertension must be controlled before initiation. Routine heart rate and blood pressure monitoring throughout treatment is essential. These effects may limit levomilnacipran’s suitability for patients with significant cardiovascular disease, tachyarrhythmias, or uncontrolled hypertension.

Int

Drug Interactions

Levomilnacipran is primarily metabolized by CYP3A4, making strong CYP3A4 inhibitors the main pharmacokinetic interaction concern. Unlike desvenlafaxine (UGT-metabolized) and duloxetine (CYP1A2/2D6-metabolized), levomilnacipran does not significantly inhibit or induce any CYP enzymes. Its low protein binding (22%) further reduces displacement interaction risk. The most important interactions are pharmacodynamic: serotonergic combinations and the unique alcohol-induced dose-dumping effect on the extended-release formulation.

MajorMAOIs (phenelzine, tranylcypromine, isocarboxazid)
MechanismAdditive serotonin accumulation from reuptake inhibition plus impaired degradation
EffectLife-threatening serotonin syndrome risk
ManagementContraindicated. Allow 14 days after stopping MAOI before starting levomilnacipran; 7 days after stopping levomilnacipran before starting MAOI
FDA PI
MajorLinezolid / IV methylene blue
MechanismMAO-A inhibition combined with SNRI activity
EffectSerotonin syndrome risk
ManagementContraindicated. If urgent treatment needed, stop levomilnacipran and monitor for 7 days or 24 h after last dose of linezolid/methylene blue
FDA PI
MajorOther serotonergic agents (triptans, tramadol, fentanyl, lithium, buspirone, SSRIs/SNRIs, TCAs, St. John’s Wort)
MechanismAdditive serotonergic effects via multiple pathways
EffectIncreased risk of serotonin syndrome
ManagementMonitor closely if combination is clinically warranted; discontinue immediately if signs of serotonin syndrome develop
FDA PI
MajorAlcohol (ethanol)
MechanismAlcohol disrupts ER capsule beads causing accelerated drug release (dose dumping); 40% alcohol causes nearly complete release in 4 hours in vitro
EffectRapid, uncontrolled increase in levomilnacipran plasma concentrations; risk of acute toxicity
ManagementAvoid concomitant use; counsel all patients about this risk
FDA PI
ModerateStrong CYP3A4 inhibitors (ketoconazole, itraconazole, clarithromycin)
MechanismCYP3A4 is the primary metabolic pathway; potent inhibition increases levomilnacipran AUC by ~57%
EffectClinically meaningful increase in levomilnacipran exposure
ManagementCap levomilnacipran dose at 80 mg/day
FDA PI
ModerateAnticoagulants / Antiplatelet agents (warfarin, aspirin, NSAIDs)
MechanismSNRI-mediated impairment of platelet aggregation via serotonin depletion; additive bleeding risk
EffectIncreased risk of GI and other bleeding events
ManagementMonitor for bleeding; carefully monitor INR when initiating or discontinuing levomilnacipran in warfarin-treated patients
FDA PI
MinorCYP3A4 inducers (carbamazepine) and substrates (alprazolam)
MechanismIn vivo studies showed no clinically meaningful change in levomilnacipran exposure with carbamazepine or alprazolam
EffectNo clinically significant interaction
ManagementNo dose adjustment needed for CYP3A4 inducers or substrates
FDA PI
MinorDrugs metabolized by CYP1A2, 2B6, 2C8, 2C9, 2C19, 2D6, 2E1, 3A
MechanismLevomilnacipran does not significantly inhibit or induce these enzymes in vitro
EffectNo clinically significant interaction expected
ManagementNo dose adjustment needed; low DDI potential is a clinical advantage
FDA PI
Mon

Monitoring

  • Blood PressureBaseline, then regularly
    Routine    Control pre-existing hypertension before initiation. Monitor for sustained BP increases. Noradrenergic potency of levomilnacipran makes this particularly important compared to serotonin-preferential SNRIs.
  • Heart RateBaseline, then regularly
    Routine    Mean increase ~7 bpm; monitor for tachycardia (6% incidence) and palpitations (5%). Pre-existing tachyarrhythmias and other cardiac disease should be treated before initiation.
  • 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.
  • Urinary FunctionEach visit
    Routine    Inquire about urinary hesitation or difficulty voiding at each follow-up; dose-related (4–6%). Particularly relevant in males and patients with prostatic hypertrophy. Discontinue if urinary retention develops.
  • Sexual FunctionBaseline, then periodically
    Routine    Inquire proactively; erectile dysfunction (6%, dose-related up to 10% at 120 mg), ejaculation disorder (5%), and testicular pain (4%) are notable. Female sexual dysfunction was <2% in trials.
  • Serum SodiumAs indicated
    Trigger-based    Check if symptoms of hyponatremia develop. Elderly patients and those on diuretics are at highest risk.
  • Renal FunctionBaseline
    Routine    Creatinine clearance determines dosing caps. 58% of drug excreted renally unchanged.
  • Intraocular PressureBaseline in at-risk patients
    Trigger-based    Mydriasis from SNRIs may trigger angle-closure glaucoma in patients with untreated anatomically narrow angles.
CI

Contraindications & Cautions

Absolute Contraindications

  • Hypersensitivity to levomilnacipran, milnacipran HCl, or any excipient in the formulation
  • Concurrent MAOI use or use within 14 days of MAOI discontinuation
  • Initiation in patients receiving linezolid or IV methylene blue

Relative Contraindications (Specialist Input Recommended)

  • Uncontrolled hypertension: Blood pressure must be adequately managed before starting levomilnacipran; noradrenergic potency amplifies BP effects
  • Significant cardiac disease or tachyarrhythmias: Pre-existing cardiac conditions should be treated before initiation; heart rate increases of ~7 bpm are expected
  • Urinary obstruction or severe BPH: Dose-dependent urinary hesitation and retention risk; alternative antidepressant may be preferable
  • Untreated narrow-angle glaucoma: Mydriasis may precipitate acute angle-closure attack
  • End-stage renal disease: Not recommended; drug accumulates and dialysis is ineffective

Use with Caution

  • Seizure disorders: Seizures have been reported rarely
  • Moderate-severe renal impairment: Dose cap required (80 mg or 40 mg depending on severity)
  • Bipolar disorder: Screen before initiation; risk of mania/hypomania activation
  • Elderly patients (65+): Increased hyponatremia risk; limited clinical trial data in this age group
  • Patients at bleeding risk: Concurrent anticoagulant or NSAID use increases bleeding risk
  • Third trimester pregnancy: Neonatal adaptation syndrome reported with SNRI exposure
FDA Boxed Warning Suicidality in Children, Adolescents, and Young Adults

Antidepressants increased the risk of suicidal thinking and behavior in pediatric and young adult patients in short-term studies. Closely monitor all patients for clinical worsening and emergence of suicidal thoughts and behaviors. Levomilnacipran is not approved for use in pediatric patients. Two randomized, placebo- and active-controlled 8-week trials in pediatric patients (7–17 years) with MDD did not establish efficacy, and an increased risk of blood pressure elevation was observed in this population.

Pt

Patient Counselling

Purpose of Therapy

Levomilnacipran is prescribed to treat major depression by increasing the availability of both serotonin and norepinephrine in the brain. Improvement in mood and energy levels typically begins within 2 to 4 weeks, with full therapeutic benefit developing over 6 to 8 weeks. It is important to continue taking the medication as prescribed even after symptoms improve, to prevent relapse.

How to Take

Take one capsule at approximately the same time each day, with or without food. Swallow the capsule whole; do not open, chew, or crush it, as this will damage the extended-release mechanism. The starting dose is 20 mg for the first 2 days, after which your prescriber will increase and adjust the dose based on how you respond.

Avoid Alcohol Completely
Tell patientAlcohol can break down the extended-release coating of the capsule, causing the entire dose to be released at once. This can lead to dangerously high drug levels. Do not drink any alcohol while taking levomilnacipran.
Call prescriberIf you consumed alcohol after taking levomilnacipran and experience rapid heartbeat, nausea, dizziness, or unusual symptoms.
Heart Rate & Blood Pressure Changes
Tell patientThis medication may increase your heart rate and blood pressure. You may feel your heart beating faster than usual, or experience palpitations. These effects are expected and usually mild, but your prescriber will monitor them regularly.
Call prescriberIf you experience rapid or pounding heartbeat that is persistent or concerning, chest pain, severe headache, or blurred vision suggesting dangerously high blood pressure.
Urinary Difficulties
Tell patientSome patients, particularly men, notice difficulty starting urination or a weak urine stream. This is a recognized side effect and tends to be dose-related.
Call prescriberImmediately if you are unable to urinate at all, experience painful urination, or notice significant difficulty voiding. These may indicate urinary retention requiring medical intervention.
Nausea
Tell patientNausea is the most common side effect, affecting about 1 in 6 patients. It usually occurs early in treatment and often improves within the first 1–2 weeks. Taking the medication with food may help.
Call prescriberIf nausea is severe, persistent beyond 2–3 weeks, or associated with significant vomiting or inability to keep the medication down.
Sexual Side Effects
Tell patientChanges in sexual function including difficulty with erections, delayed ejaculation, or testicular discomfort may occur, particularly in men. Women may experience decreased libido. Do not feel embarrassed to discuss these, as management options are available.
Call prescriberIf sexual side effects are bothering you; dose adjustment or alternative treatment strategies can be discussed.
Do Not Stop Abruptly
Tell patientStopping levomilnacipran suddenly can cause withdrawal symptoms such as dizziness, nausea, headache, irritability, and sensory disturbances. Always taper under medical guidance.
Call prescriberIf you accidentally miss several doses or stop taking the medication; if withdrawal symptoms are severe despite gradual tapering.
Ref

Sources

Regulatory (PI / SmPC)
  1. Fetzima (levomilnacipran) Extended-Release Capsules. Full Prescribing Information. AbbVie Inc. Revised April 2024. dailymed.nlm.nih.govPrimary source for all dosing, contraindications, adverse reaction incidence rates, and pharmacokinetic parameters cited in this monograph.
  2. Fetzima (levomilnacipran) FDA label. August 2023 revision (Warnings and Precautions update). accessdata.fda.govMost current FDA label PDF including 2023 warnings updates on serotonin syndrome and bleeding risk.
Key Clinical Trials
  1. Asnis GM, Bose A, Gommoll CP, Chen C, Greenberg WM. Efficacy and safety of levomilnacipran sustained release 40 mg, 80 mg, or 120 mg in major depressive disorder: a phase 3, randomized, double-blind, placebo-controlled study. J Clin Psychiatry. 2013;74(3):242-248. doi:10.4088/JCP.12m08197Pivotal fixed-dose Study 1 establishing efficacy of levomilnacipran 40, 80, and 120 mg for MDD.
  2. Bakish D, Bose A, Gommoll C, et al. Levomilnacipran ER 40 mg and 80 mg in patients with major depressive disorder: a phase III, randomized, double-blind, fixed-dose, placebo-controlled study. J Psychiatry Neurosci. 2014;39(1):40-49. doi:10.1503/jpn.130040Fixed-dose Study 2 confirming efficacy of 40 mg and 80 mg doses with MADRS primary endpoint.
  3. Sambunaris A, Bose A, Gommoll CP, et al. A phase III, double-blind, placebo-controlled, flexible-dose study of levomilnacipran extended-release in patients with major depressive disorder. J Clin Psychopharmacol. 2014;34(1):47-56. doi:10.1097/JCP.0000000000000060Flexible-dose Study 3 (40–120 mg) supporting clinical flexibility in dosing.
  4. Shiovitz T, Greenberg WM, Chen C, Forero G, Gommoll CP. A randomized, double-blind, placebo-controlled trial of the efficacy and safety of levomilnacipran ER 40-120 mg/day for prevention of relapse in patients with major depressive disorder. Innov Clin Neurosci. 2014;11(1-2):10-22.Relapse prevention trial establishing longer-term efficacy of levomilnacipran for MDD maintenance treatment.
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 levomilnacipran as a first-line antidepressant option for MDD.
Mechanistic / Basic Science
  1. Auclair AL, Bhardwaj SK, Bhougal A, et al. Levomilnacipran (F2695), a norepinephrine-preferring SNRI: profile in vitro and in neurochemical and behavioral models of antidepressant activity. Neuropharmacology. 2013;70:338-347. doi:10.1016/j.neuropharm.2013.02.024Characterizes the preferential noradrenergic selectivity profile of levomilnacipran (NE:5-HT ~2:1).
  2. Stahl SM, Grady MM, Moret C, Briley M. SNRIs: their pharmacology, clinical efficacy, and tolerability in comparison with other classes of antidepressants. CNS Spectr. 2005;10(9):732-747. doi:10.1017/S1092852900019726Comparative review of SNRI pharmacology placing milnacipran/levomilnacipran in the context of the SNRI class.
Pharmacokinetics / Special Populations
  1. Brunner E, Gommoll C, Engel C, et al. Disposition and metabolism of [14C]-levomilnacipran, a serotonin and norepinephrine reuptake inhibitor, in humans, monkeys, and rats. Drug Des Devel Ther. 2015;9:3199-3215. doi:10.2147/DDDT.S82505Comprehensive mass-balance and metabolite identification study establishing renal excretion of 58% unchanged drug and CYP3A4-mediated desethylation pathway.
  2. Asnis GM, Henderson MA. Levomilnacipran for the treatment of major depressive disorder: a review. Neuropsychiatr Dis Treat. 2015;11:125-135. doi:10.2147/NDT.S54710Comprehensive review of efficacy, safety, tolerability, and PK profile from pivotal and long-term studies.
  3. Gautam M, Kaur M, Jagtap P, Krayem B. Levomilnacipran: more of the same? Prim Care Companion CNS Disord. 2019;21(5):27423. doi:10.4088/PCC.19nr02521Narrative review analyzing the unique noradrenergic profile of levomilnacipran and its potential for fatigue-predominant depression.