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Drug Monograph

Lemborexant

Brand: Dayvigo
Dual Orexin Receptor Antagonist (DORA) · Oral · Schedule IV (C-IV)
Pharmacokinetic Profile
Half-Life
17 h (5 mg); 19 h (10 mg)
Metabolism
Hepatic — CYP3A4 (major); CYP3A5 (minor)
Protein Binding
~94% (in vitro)
Tmax / Absorption
1–3 h fasted; delayed ~2 h with high-fat meal
Volume of Distribution
~1,970 L (extensive tissue distribution)
Clinical Information
Drug Class
Dual orexin receptor antagonist (OX1R / OX2R)
Available Doses
5 mg, 10 mg tablets
Route
Oral
Renal Adjustment
Not required; severe impairment ↑ AUC and somnolence risk
Hepatic Adjustment
Moderate: max 5 mg; severe: not recommended
Pregnancy
No human data; pregnancy registry available
Lactation
No human data; present in rat milk; monitor infants for sedation
Schedule / Legal
DEA Schedule IV (effective April 2020)
Generic Available
No (US); brand-only — patent protection through ~2035
Rx

Indications

IndicationApproved PopulationTherapy TypeStatus
Insomnia characterized by difficulties with sleep onset and/or sleep maintenanceAdultsMonotherapyFDA Approved

Lemborexant is the second dual orexin receptor antagonist (DORA) approved by the FDA, following suvorexant. Its mechanism — selective competitive antagonism at both the OX1R and OX2R orexin receptors — suppresses wake drive rather than augmenting GABA-mediated sedation, which is reflected in its broad indication covering both sleep onset and sleep maintenance. Lemborexant was approved in December 2019, after the publication of the 2017 American Academy of Sleep Medicine (AASM) clinical practice guideline; it is therefore not specifically addressed in that guideline. Cognitive behavioral therapy for insomnia (CBT-I) remains first-line in both AASM and ACP guidance, with pharmacotherapy reserved for patients in whom CBT-I is unavailable, has failed, or is needed as a temporary adjunct. The pivotal program comprised two phase 3 trials: SUNRISE 1 (Study 304, FDA Study 2; 1-month placebo- and zolpidem-controlled trial in older adults using polysomnographic latency to persistent sleep as the primary endpoint) and SUNRISE 2 (Study 303, FDA Study 1; 12-month placebo-controlled trial in adults ≥18 years using patient-reported sleep diary outcomes). Both demonstrated statistically significant superiority to placebo for sleep onset and sleep maintenance endpoints.

Off-Label & Investigational Uses

Irregular sleep–wake rhythm disorder in mild-to-moderate Alzheimer disease dementia — A phase 2 dose-finding RCT in 62 patients with ISWRD and AD-D (Moline 2021) used 4 weeks of treatment with lemborexant 2.5–15 mg. Outcomes were assessed by actigraphy and clinical scales; significant improvements versus placebo were reported in selected circadian rhythm parameters. Unlike suvorexant — whose label was updated to incorporate AD-population insomnia data — the lemborexant label does not include AD-specific findings. Evidence quality: low.

Delirium prevention in hospitalized older adults — Smaller observational and quasi-experimental studies; the evidence base is less mature than for suvorexant or ramelteon. Evidence quality: very low to low.

Dose

Dosing

The labeled approach is to use the lowest effective dose. Recommended starting dose is 5 mg taken immediately before going to bed, only when at least 7 hours of sleep opportunity remain before activities requiring full alertness. The 5 mg dose may be increased to a maximum of 10 mg once daily based on clinical response and tolerability. Concurrent CYP3A inhibitors and hepatic impairment dictate specific dose ceilings, and concurrent strong or moderate CYP3A inducers should be avoided altogether. There is no genuine 20 mg option — unlike suvorexant, lemborexant has only two strengths (5 and 10 mg).

Clinical ScenarioStarting DoseMaintenance DoseMaximum DoseNotes
Adult insomnia (sleep onset and/or maintenance) — primary indication5 mg PO5–10 mg nightly10 mg/dayTake immediately before bed; ≥7 h before planned awakening
Increase to 10 mg only if 5 mg is well tolerated but inadequate
Older adults (≥65 years)5 mg PO5–10 mg nightly10 mg/dayPer FDA label, exercise caution with doses >5 mg in patients ≥65
Somnolence at 10 mg: 9.8% in elderly vs 7.7% in younger adults
Mild hepatic impairment (Child-Pugh A)5 mg PO5–10 mg nightly10 mg/dayNo formal adjustment; AUC increased
Patients may experience increased somnolence
Moderate hepatic impairment (Child-Pugh B)5 mg PO5 mg nightly5 mg/dayMaximum 5 mg
AUC, Cmax, and terminal half-life all increased
Severe hepatic impairment (Child-Pugh C)Not recommendedNot studied; avoid use
Renal impairment (mild, moderate, severe)5 mg PO5–10 mg nightly10 mg/dayNo dose adjustment required
AUC increased in severe impairment; counsel on somnolence
Concomitant weak CYP3A inhibitor (e.g., chlorzoxazone, ranitidine)5 mg PO5 mg nightly5 mg/dayMaximum 5 mg
PBPK modelling predicts <2-fold AUC increase with weak inhibitors
Concomitant strong or moderate CYP3A inhibitor (e.g., itraconazole, clarithromycin, fluconazole, verapamil)AvoidUse alternative hypnotic
Substantial AUC increase expected
Concomitant strong or moderate CYP3A inducer (e.g., rifampin, carbamazepine, St. John’s wort, bosentan, efavirenz, etravirine, modafinil)AvoidChoose a non-CYP3A-dependent hypnotic
Efficacy substantially reduced
Pediatric (<18 years)Not establishedSafety and effectiveness not established
Clinical Pearl — The 7-Hour Rule

Lemborexant has a longer half-life than other hypnotics in routine use (~17 h at 5 mg, ~19 h at 10 mg), and steady-state accumulation is 1.5- to 3-fold. The FDA label is explicit that lemborexant should not be administered unless ≥7 hours remain before required awakening, and that the 10 mg dose carries a labeled caution regarding next-morning driving. CNS depressant effects may persist for several days after discontinuation. Patients who routinely cannot guarantee a full 7-hour sleep opportunity, on-call clinicians, and shift workers are not appropriate candidates.

Reassessment Trigger

If insomnia fails to remit after 7–10 days of treatment, the FDA label advises re-evaluation for an underlying psychiatric or medical disorder rather than continued empiric treatment.

PK

Pharmacology of Lemborexant

Mechanism of Action

Lemborexant is a competitive antagonist at the orexin OX1R and OX2R receptors with in vitro IC50 values of 6.1 nM and 2.6 nM, respectively. The orexin (hypocretin) signaling system originates in the lateral hypothalamus and projects to monoaminergic and cholinergic wake-promoting nuclei; orexin A and orexin B are the principal endogenous neuropeptides driving arousal. By blocking their binding at OX1R and OX2R, lemborexant suppresses wake drive rather than augmenting sleep drive. The major metabolite, M10, is pharmacologically active with comparable in vitro affinity to the parent compound (IC50 4.2 nM at OX1R and 2.9 nM at OX2R), and contributes to overall pharmacodynamic effect. The clinical signature of orexin antagonism is the labeled signal for narcolepsy-spectrum events — sleep paralysis, hypnagogic/hypnopompic hallucinations, and cataplexy-like leg weakness — which increase in incidence with dose; loss of orexin neurons is the pathological substrate of human narcolepsy with cataplexy, which is why narcolepsy is the only labeled contraindication.

ADME Profile

ParameterValueClinical Implication
AbsorptionTmax ~1–3 h fasted; less-than-proportional Cmax/AUC across 2.5–75 mg; high-fat meal decreases Cmax by 23%, increases AUC by 18%, and delays Tmax by ~2 hTake on an empty stomach for fastest sleep-onset effect; avoid taking immediately after a heavy meal
DistributionVd ~1,970 L (very large — extensive tissue distribution); plasma protein binding ~94% in vitro; blood-to-plasma ratio 0.65High-volume distribution explains long effective half-life; hemodialysis is not expected to remove drug in overdose
MetabolismHepatic; CYP3A4 is the major enzyme with minor contribution from CYP3A5; major circulating active metabolite is M10. M10 induces CYP3A and has weak inhibitory potential at CYP3A and inductive potential at CYP2B6CYP3A is the dominant determinant of drug interactions. Lemborexant decreases exposure of CYP2B6 substrates (e.g., bupropion, methadone)
Elimination~57% feces, ~29% urine (<1% unchanged); effective t½ 17 h (5 mg) and 19 h (10 mg); accumulation 1.5- to 3-fold; steady-state by ~7 daysLong half-life means CNS effects may persist for several days after discontinuation; clinically meaningful for transitions in care or surgery
SE

Side Effects

The pivotal lemborexant development program — comprising FDA Study 1 (also known as SUNRISE 2: 6-month placebo-controlled adult trial with 6-month extension) and FDA Study 2 (also known as SUNRISE 1: 1-month placebo- and zolpidem-controlled trial in older adults) — enrolled 1,418 adults with insomnia disorder. The most common adverse event was somnolence (combined preferred term: somnolence/lethargy/fatigue/sluggishness) at 6.9% on 5 mg and 9.6% on 10 mg, versus 1.3% on placebo. Most CNS adverse events show a clear dose response. The narcolepsy-spectrum events (sleep paralysis, hypnagogic/hypnopompic hallucinations, cataplexy-like leg weakness) — although uncommon — are mechanistically distinctive and dose-related. Lemborexant is a Schedule IV controlled substance, with abuse-liability profile in recreational sedative users statistically similar to zolpidem 30 mg and suvorexant 40 mg.

≥10% Very Common
Adverse EffectIncidenceClinical Note
None reported at this frequency in pivotal trials at the recommended dosesThe composite somnolence/fatigue endpoint at 10 mg approached this threshold (9.6%) but did not exceed it in pooled first-30-day data
1–10% Common — Pivotal Adult Insomnia Trials (First 30 Days, Pooled FDA Studies 1 + 2)
Adverse EffectIncidence (5 mg / 10 mg)Clinical Note
Somnolence / lethargy / fatigue / sluggishness (combined)6.9% / 9.6%Placebo 1.3%. Higher in elderly at the 10 mg dose (9.8% vs 7.7% in younger adults)
Headache5.9% / 4.5%Placebo 3.4%; usually mild and self-limiting
Nightmare or abnormal dreams0.9% / 2.2%Placebo 0.9%; clear dose-related signal at 10 mg; inquire on follow-up
Sleep paralysis1.3% / 1.6%Placebo 0%; counsel patients proactively about the nature of these events
No other adverse event was reported at ≥2% on lemborexant 5 or 10 mg at a higher rate than placebo in pooled first-30-day data.
Serious Regardless of Frequency
Adverse EffectEstimated FrequencyTypical OnsetRequired Action
Daytime impairment / impaired drivingDocumented in some subjects taking 10 mg in driving studiesMorning after dose; may persist for several days after discontinuationCounsel patients on 10 mg about next-morning driving; reduce dose or discontinue if daytime somnolence develops
Complex sleep behaviors (sleep-walking, sleep-driving, preparing/eating food, phone calls, sex with amnesia)2 events in pivotal trials, both on 10 mgAny time during therapy, including first doseDiscontinue immediately if any episode occurs; risk increased by alcohol and other CNS depressants
Worsening depression and emergence of suicidal ideationBy questionnaire: 0.4% (5 mg) and 0.3% (10 mg) vs 0.2% placeboVariableImmediately evaluate any new behavioral signs or suicidal ideation; prescribe smallest feasible quantity in patients with depression
Sleep paralysis (inability to move/speak during sleep–wake transitions)1.3% (5 mg) and 1.6% (10 mg); placebo 0%Sleep–wake transitionsReassure if isolated and brief; consider dose reduction or discontinuation if recurrent or distressing
Hypnagogic / hypnopompic hallucinations0.1% (5 mg) and 0.7% (10 mg); placebo 0%Falling asleep or wakingCounsel proactively about the nature of these events; consider dose reduction or discontinuation if recurrent
Cataplexy-like symptoms (transient leg weakness, day or night)Per labeled effect; not necessarily emotion-triggeredVariableConsider dose reduction or discontinuation; assess fall risk in older adults
Falls (related to drowsiness)Increased risk per label, particularly in elderlyAny timeAssess gait stability before dose escalation; lower dose in patients with prior falls
Respiratory depression in compromised patientsCannot be excluded in moderate-to-severe OSA or COPDVariableNot studied in moderate-to-severe OSA or COPD; consider risks before prescribing in these populations and in combination with opioids
Abuse and dependence (Schedule IV)Subjective abuse-liability similar to zolpidem 30 mg and suvorexant 40 mgVariableScreen substance-use history; monitor for misuse; prescribe limited quantities in at-risk patients. No physical dependence in clinical trials
Discontinuation Treatment-Emergent Withdrawal in Trials
First 30 Days (Pooled FDA Studies 1 + 2 = SUNRISE 2 + SUNRISE 1)
1.4% (5 mg) / 2.6% (10 mg) vs 1.5% placebo
Most common reasons: somnolence (1.0% / 0.7% vs 0.4%), nightmares (0.3% / 0.3% vs 0%).
6-Month Period (FDA Study 1 / SUNRISE 2)
4.1% (5 mg) / 8.3% (10 mg) vs 3.8% placebo
Most common reasons (10 mg): somnolence 2.9%, nightmares 1.3%, palpitations 0.6%.
Reason for Discontinuation (6-Month Period, FDA Study 1 / SUNRISE 2)Incidence (5 mg / 10 mg)Context
Somnolence1.0% / 2.9%Placebo 0.6%; the dominant dose-related discontinuation signal
Nightmares0.3% / 1.3%Placebo 0%; if mild, 5 mg dose may be tolerated
Palpitations0% / 0.6%Placebo 0%; class effect not described — investigate alternative cardiac causes
No evidence of withdrawal effects on the Tyrer Benzodiazepine Withdrawal Symptom Questionnaire after discontinuation in 1-month or 12-month trials. No rebound insomnia. Lemborexant remains a Schedule IV controlled substance based on abuse-liability data.
Management Pearl — Long Half-Life Considerations

Lemborexant’s effective half-life of 17–19 hours is materially longer than older hypnotics and longer than suvorexant. Per the FDA label, CNS depressant effects may persist for several days after discontinuation. This is clinically meaningful for patients undergoing surgery, sedation procedures, or transitions of care. When a patient stops lemborexant, schedule reassessment of mental status and driving capacity within the first week rather than assuming washout is complete after a single missed dose.

Int

Drug Interactions

Lemborexant is a CYP3A4 substrate (with minor CYP3A5 contribution), so CYP3A inhibitors and inducers dominate its pharmacokinetic interaction profile. The labeled interaction strategy is more restrictive than for suvorexant: even moderate CYP3A inhibitors should be avoided, and weak inhibitors require a dose ceiling of 5 mg. In addition, lemborexant is a CYP2B6 inducer that can reduce exposure of CYP2B6 substrates such as bupropion and methadone. Pharmacodynamic additivity with alcohol and other CNS depressants is the dominant non-PK concern.

Major Strong CYP3A inhibitors (itraconazole, clarithromycin, ketoconazole, posaconazole, ritonavir, nefazodone)
MechanismStrong CYP3A inhibition
EffectSubstantial increase in lemborexant AUC and Cmax
ManagementAvoid concomitant use. Choose an alternative anti-infective or non-CYP3A-dependent hypnotic
FDA PI
Major Moderate CYP3A inhibitors (fluconazole, verapamil, diltiazem, erythromycin)
MechanismModerate CYP3A inhibition
EffectClinically significant increase in lemborexant exposure
ManagementAvoid concomitant use per FDA label — note that this is more restrictive than for suvorexant, where moderate inhibitors only require dose reduction
FDA PI
Major Strong or moderate CYP3A inducers (rifampin, carbamazepine, phenytoin, St. John’s wort, bosentan, efavirenz, etravirine, modafinil)
MechanismCYP3A induction
EffectSubstantial decrease in lemborexant exposure with reduced efficacy
ManagementAvoid concomitant use per FDA label
FDA PI
Major Alcohol
MechanismPharmacodynamic — additive psychomotor impairment; alcohol also increases lemborexant Cmax and AUC
EffectGreater impairment of postural stability and memory than alcohol alone, near Tmax (~2 h post-dose)
ManagementCounsel patients not to consume alcohol on nights they take lemborexant
FDA PI
Major Other CNS depressants (opioids, benzodiazepines, tricyclic antidepressants, sedating antihistamines)
MechanismPharmacodynamic — additive CNS depression; respiratory depression with opioids
EffectIncreased risk of falls, daytime impairment, and complex sleep behaviors
ManagementAvoid combination with other hypnotics — the FDA label specifically states use of lemborexant with other insomnia drugs is not recommended. Use lowest effective opioid doses if co-prescribed
FDA PI
Moderate Weak CYP3A inhibitors (e.g., chlorzoxazone, ranitidine, cimetidine)
MechanismWeak CYP3A inhibition
EffectPBPK modeling predicts <2-fold AUC increase
ManagementMaximum recommended dose 5 mg per night while concurrent therapy continues
FDA PI
Moderate CYP2B6 substrates (bupropion, methadone, efavirenz)
MechanismLemborexant induces CYP2B6 via M10 metabolite
EffectDecreased AUC of CYP2B6 substrates with potential reduction in efficacy
ManagementMonitor patients for adequate clinical response to the CYP2B6 substrate; consider dose adjustment of the substrate if needed (e.g., methadone in opioid maintenance)
FDA PI
Difference from Suvorexant — More Restrictive CYP3A Strategy

Compared with suvorexant — where moderate CYP3A inhibitors require a dose reduction (5 mg, max 10 mg) — lemborexant takes a stricter position: moderate CYP3A inhibitors should be avoided altogether. Among commonly prescribed agents this is most likely to affect patients on diltiazem, verapamil, or fluconazole. Switching to a non-CYP3A inhibitor or selecting an alternative hypnotic is generally more practical than discontinuing the cardiovascular or antifungal therapy.

Mon

Monitoring

The FDA label does not specify routine laboratory monitoring for lemborexant. Clinical follow-up should focus on therapeutic response, daytime function, dose-related neuropsychiatric and narcolepsy-spectrum events, falls (especially in older adults), and — because lemborexant is a controlled substance — appropriate use and abuse-screening.

  • Sleep response Reassess at 7–10 days, then periodically
    Routine     Track sleep latency, wake after sleep onset, total sleep time, and daytime function. Per the FDA label, failure of insomnia to remit after 7–10 days should prompt re-evaluation for an underlying psychiatric or medical disorder.
  • Daytime somnolence and driving Each follow-up visit
    Routine     Specifically inquire about morning grogginess, near-misses while driving, and cognitive function. CNS depressant effects may persist for several days after discontinuation. Step down to 5 mg or discontinue if daytime impairment develops.
  • Falls and balance (older adults) Each follow-up visit
    Routine     Per FDA label, increased drowsiness raises fall risk, particularly in elderly. Assess gait stability and consider home safety review before increasing to 10 mg in patients ≥65.
  • Mood and suicidal ideation Each follow-up visit
    Routine     Suicidal ideation by questionnaire was higher with lemborexant than placebo (0.3–0.4% vs 0.2%). PHQ-9 with item 9 review or C-SSRS is appropriate, particularly in patients with prior depression.
  • Complex sleep behaviors Each follow-up visit
    Routine     Ask directly about sleep-walking, sleep-eating, sleep-driving, and unrecalled night-time activity. The label directs immediate discontinuation after any reported episode.
  • Narcolepsy-spectrum events Each follow-up visit
    Routine     Inquire specifically about sleep paralysis, vivid hallucinations on falling asleep or waking, and transient leg weakness. Sleep paralysis was reported in 1.3–1.6% in pivotal trials; dose reduction or discontinuation if recurrent.
  • Substance-use risk Baseline; ongoing as indicated
    Routine     Lemborexant is a Schedule IV controlled substance. Screen for prior alcohol or sedative misuse before initiation; monitor for early refill requests or self-escalation.
  • CYP2B6 substrate efficacy When co-administered
    Trigger-based     For patients on bupropion, methadone, or other CYP2B6 substrates, monitor for adequate clinical response to the substrate; consider dose adjustment if efficacy is reduced.
  • Respiratory status Baseline if compromised
    Trigger-based     Lemborexant has not been studied in moderate-to-severe OSA or COPD. Weigh hypnotic need against potential respiratory effects in compromised patients.
CI

Contraindications & Cautions

Absolute Contraindications (per FDA Label)

  • Narcolepsy — the only labeled contraindication. Orexin antagonism could exacerbate the underlying loss of orexin signaling that produces the disorder.

Not Recommended / Specialist Input Suggested

  • Concomitant strong or moderate CYP3A inhibitors — the FDA label directs avoidance of co-administration.
  • Concomitant strong or moderate CYP3A inducers — the FDA label directs avoidance of co-administration; efficacy is substantially reduced.
  • Severe hepatic impairment (Child-Pugh C) — not studied; the FDA label states lemborexant is not recommended.
  • Active major depression with suicidal ideation — a small dose-related signal in suicidal ideation by questionnaire was observed in pivotal trials. Prescribe the lowest feasible quantity per label.
  • Pediatric patients — safety and effectiveness have not been established.
  • Combination with other hypnotics — the FDA label specifically states use of lemborexant with other drugs to treat insomnia is not recommended.

Use with Caution

  • Older adults — exercise caution at doses above 5 mg per FDA label; falls and somnolence are more frequent.
  • Moderate hepatic impairment — maximum dose 5 mg.
  • Mild hepatic impairment or severe renal impairment — increased AUC and somnolence risk; consider lower dose.
  • Concomitant weak CYP3A inhibitor — maximum 5 mg.
  • Moderate or severe respiratory disease (OSA, COPD) — not studied; respiratory effects cannot be excluded.
  • History of substance use disorder — Schedule IV; abuse-liability comparable to zolpidem 30 mg in recreational users.
  • Patients who cannot guarantee 7 hours of sleep opportunity — risk of next-day impairment is materially increased.
  • Pregnancy and lactation — no human data are available. Animal teratogenicity occurred only at very high multiples of human exposure. The drug is present in rat milk; monitor breastfed infants for excessive sedation. A pregnancy exposure registry is available (1-888-274-2378).
FDA Class-Wide Regulatory Warning Complex Sleep Behaviors with Sedative-Hypnotics

In April 2019, the FDA required a Boxed Warning on eszopiclone, zaleplon, and zolpidem for rare but serious complex sleep behaviors (sleep-driving, sleep-walking, sleep-eating, and others) that have resulted in injuries and deaths. Lemborexant was approved in December 2019 — after the 2019 Boxed Warning — and is not included in it, but its FDA label states that complex sleep behaviors have been reported with lemborexant and directs immediate discontinuation if any patient experiences such an episode. Two complex sleep behavior events were reported in pivotal trials, both at the 10 mg dose. The risk is increased by alcohol and other CNS depressants. Counsel every patient on this risk before the first dose.

Pt

Patient Counselling

Purpose of Therapy

Lemborexant is approved for adults with insomnia involving difficulty falling asleep, staying asleep, or both. It works differently from older sleeping pills: rather than enhancing the brain’s sleep-promoting signals, it blocks the brain’s own wake-promoting signals (orexin). Lemborexant is a federally controlled substance because it can be misused; keep it in a secure place and do not share it. Cognitive behavioural therapy for insomnia (CBT-I) is the recommended first-line treatment for chronic insomnia and should ideally be offered or continued alongside any drug therapy.

How to Take It

Take one tablet immediately before going to bed, and only when you can stay in bed for at least 7 hours before being active again. The recommended starting dose is 5 mg; the maximum is 10 mg per night. Avoid taking it with or shortly after a heavy or fatty meal — food, especially a high-fat dinner, slows how quickly the medication starts working by about 2 hours. Do not drink alcohol on evenings you take lemborexant.

Next-Day Drowsiness & Driving
Tell patient You may feel drowsy or “foggy” the next morning, especially at the 10 mg dose. Do not drive or do anything that requires full alertness if you have had less than a full night of sleep, or if you took more than prescribed. Even after stopping the medication, the drowsiness can last for a few days because lemborexant stays in the body longer than older sleeping pills.
Call prescriber If you feel impaired enough that driving, work, or balance is affected the next day; if you have a near-miss while driving; if you have an unexplained fall.
7-Hour Rule & Timing
Tell patient Only take lemborexant when you can stay in bed at least 7 hours before being active. Take it immediately before going to bed. Avoid taking it right after a meal — particularly a heavy or fatty one — because food will delay how quickly it starts working.
Call prescriber If your work schedule or life routine means you cannot regularly get 7 hours of sleep — there may be a better option for your situation.
Complex Sleep Behaviours
Tell patient Rarely, sleep medications can cause people to do things while not fully awake — driving, eating, cooking, making phone calls, or having sex — with no memory of doing so. The risk is higher if combined with alcohol or other sedating medications.
Call prescriber Stop the medication and contact the clinic immediately if you (or a family member) notice any unrecalled night-time activity, even a single episode.
Sleep Paralysis & Vivid Dreams
Tell patient Some people experience brief, frightening episodes of being unable to move or speak as they fall asleep or wake up, vivid dream-like visions during these transitions, or transient leg weakness during the day or night. Nightmares are also somewhat more common at the 10 mg dose. These tend to be more likely at higher doses.
Call prescriber If these episodes are recurrent, distressing, or interfere with sleep — a lower dose or different medication may be appropriate.
Mood & Suicidal Thoughts
Tell patient Tell the prescriber if you have a history of depression or suicidal thinking. In studies, slightly more people on lemborexant reported suicidal thoughts than on placebo.
Call prescriber If you notice new or worsening depression, hopelessness, or any thoughts of self-harm, contact the clinic the same day. If you are in immediate crisis, call emergency services.
Drug Interactions
Tell patient Tell every clinician and pharmacist you take lemborexant. Do not drink alcohol on evenings you take it. Several common medications can interact: certain antibiotics (clarithromycin, erythromycin), antifungals (ketoconazole, itraconazole, fluconazole), heart drugs (diltiazem, verapamil), HIV medications, the antiseizure medications carbamazepine and phenytoin, and the herbal product St. John’s wort. Lemborexant can also lower the effectiveness of bupropion (used for depression and smoking cessation) and methadone.
Call prescriber Before starting any new medication — including over-the-counter sleep aids, antibiotics, antifungals, or herbal supplements such as St. John’s wort — check with the prescriber or pharmacist.
Controlled Substance & Storage
Tell patient Lemborexant is a federally controlled medication. Keep it in a safe place where others cannot access it. Do not share or sell it — that is illegal. Do not increase your dose on your own; contact the clinic if it does not seem to work.
Call prescriber If you find yourself wanting more than prescribed, taking it during the day, or using it in combination with alcohol or other sedatives.
Pregnancy & Breastfeeding
Tell patient Tell the prescriber if you are pregnant, planning to become pregnant, or breastfeeding. There is a pregnancy registry that collects information from women exposed to lemborexant during pregnancy (call 1-888-274-2378). It is not known whether lemborexant passes into human breast milk, but it does pass into the milk of lactating animals.
Call prescriber If you become pregnant while taking lemborexant, or if your breastfed baby seems unusually sleepy or feeds poorly.
Ref

Sources

Regulatory (PI / Safety Communications)
  1. U.S. Food and Drug Administration. Dayvigo (lemborexant) prescribing information — initial approval December 2019 (Reference ID 4538172). accessdata.fda.gov Initial approved US label — primary source for indications, dosing, contraindications, drug interactions, and incidence figures cited throughout this monograph.
  2. DailyMed (NIH). DAYVIGO (lemborexant) tablet, film coated — current label. dailymed.nlm.nih.gov Searchable, regularly updated mirror of the FDA-approved labeling, including current PLLR-format Pregnancy and Lactation sections.
  3. U.S. Drug Enforcement Administration. Schedules of Controlled Substances: Placement of Lemborexant in Schedule IV. Federal Register, April 7, 2020. federalregister.gov Final rule placing lemborexant in DEA Schedule IV, effective April 7, 2020.
  4. U.S. Food and Drug Administration. FDA Drug Safety Communication: FDA adds Boxed Warning for risk of serious injuries caused by sleepwalking with certain prescription insomnia medicines. April 30, 2019. fda.gov FDA communication clarifying that the 2019 Boxed Warning applies to eszopiclone, zaleplon, and zolpidem; lemborexant is not included.
Key Clinical Trials
  1. Rosenberg R, Murphy P, Zammit G, et al. Comparison of lemborexant with placebo and zolpidem tartrate extended release for the treatment of older adults with insomnia disorder: a phase 3 randomized clinical trial. JAMA Netw Open. 2019;2(12):e1918254. doi: 10.1001/jamanetworkopen.2019.18254 Pivotal SUNRISE 1 trial (Study 304, NCT02783729) in adults ≥55 years with insomnia disorder; 1-month, placebo- and zolpidem-controlled, with polysomnographic latency to persistent sleep as the primary endpoint. Corresponds to FDA Study 2.
  2. Kärppä M, Yardley J, Pinner K, et al. Long-term efficacy and tolerability of lemborexant compared with placebo in adults with insomnia disorder: results from the phase 3 randomized clinical trial SUNRISE 2. Sleep. 2020;43(9):zsaa123. doi: 10.1093/sleep/zsaa123 SUNRISE 2 trial (Study 303, NCT02952820), 6-month placebo-controlled period in 949 adults ≥18 years; corresponds to FDA Study 1. Patient-reported sleep diary outcomes; supports efficacy and the absence of rebound insomnia or withdrawal.
  3. Yardley J, Kärppä M, Inoue Y, et al. Long-term effectiveness and safety of lemborexant in adults with insomnia disorder: results from a phase 3 randomized clinical trial. Sleep Med. 2021;80:333–342. doi: 10.1016/j.sleep.2021.01.048 Full 12-month SUNRISE 2 outcomes including the 6-month active-treatment-only extension period; demonstrates sustained patient-reported efficacy across one year of treatment.
  4. Moline M, Thein S, Bsharat M, et al. Safety and efficacy of lemborexant in patients with irregular sleep–wake rhythm disorder and Alzheimer’s disease dementia: results from a phase 2 randomized clinical trial. J Prev Alzheimers Dis. 2021;8(1):7–18. doi: 10.14283/jpad.2020.69 Exploratory phase 2 dose-finding RCT (62 patients; 2.5/5/10/15 mg vs placebo) using actigraphy and clinical scales over 4 weeks of treatment in mild-to-moderate AD-D — supporting evidence for the off-label use of lemborexant in ISWRD with AD-D.
Guidelines
  1. Sateia MJ, Buysse DJ, Krystal AD, Neubauer DN, Heald JL. Clinical practice guideline for the pharmacologic treatment of chronic insomnia in adults: an American Academy of Sleep Medicine clinical practice guideline. J Clin Sleep Med. 2017;13(2):307–349. doi: 10.5664/jcsm.6470 AASM 2017 guideline; pre-dates lemborexant approval (December 2019) and therefore does not include a specific recommendation for lemborexant.
  2. Qaseem A, Kansagara D, Forciea MA, Cooke M, Denberg TD; Clinical Guidelines Committee of the American College of Physicians. Management of chronic insomnia disorder in adults: a clinical practice guideline from the American College of Physicians. Ann Intern Med. 2016;165(2):125–133. doi: 10.7326/M15-2175 ACP guideline emphasising CBT-I as first-line treatment for chronic insomnia, with pharmacotherapy reserved for patients in whom CBT-I is inadequate or unavailable.
Mechanistic / Basic Science
  1. Beuckmann CT, Suzuki M, Ueno T, Nagaoka K, Arai T, Higashiyama H. In vitro and in silico characterization of lemborexant (E2006), a novel dual orexin receptor antagonist. J Pharmacol Exp Ther. 2017;362(2):287–295. doi: 10.1124/jpet.117.241422 Receptor-binding and selectivity profile of lemborexant — establishes the OX1R/OX2R potency at low nanomolar concentrations and selectivity over 88 other receptors, transporters, and ion channels.
  2. Sakurai T. The neural circuit of orexin (hypocretin): maintaining sleep and wakefulness. Nat Rev Neurosci. 2007;8(3):171–181. Foundational review of orexin signalling and its role in arousal — the conceptual basis for orexin antagonism as a hypnotic strategy.
Pharmacokinetics, Special Populations & Driving
  1. Landry I, Aluri J, Hall N, et al. Effect of CYP3A inhibition and induction on the pharmacokinetics of lemborexant. Clin Pharmacokinet. 2021;60(4):539–552. Dedicated PK studies underpinning the CYP3A inhibitor and inducer interaction recommendations in the FDA label.
  2. Vermeeren A, Jongen S, Murphy P, et al. On-the-road driving performance the morning after bedtime administration of lemborexant in healthy adult and elderly volunteers. Sleep. 2019;42(4):zsy260. doi: 10.1093/sleep/zsy260 On-the-road driving study underpinning the FDA caution about next-morning driving impairment in some subjects taking the 10 mg dose.
  3. Murphy P, Moline M, Mayleben D, et al. Lemborexant, a dual orexin receptor antagonist (DORA) for the treatment of insomnia disorder: results from a Bayesian, adaptive, randomized, double-blind, placebo-controlled study. J Clin Sleep Med. 2017;13(11):1289–1299. Phase 2b dose-finding study supporting the registrational dosing strategy.