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Drug Monograph

Suvorexant

Brand: Belsomra
Dual Orexin Receptor Antagonist (DORA) · Oral · Schedule IV (C-IV)
Pharmacokinetic Profile
Half-Life
~12 h (95% CI 12–13)
Metabolism
Hepatic — CYP3A (major); CYP2C19 (minor)
Protein Binding
>99% (albumin and α1-acid glycoprotein)
Bioavailability
~82% (10 mg)
Volume of Distribution
~49 L
Clinical Information
Drug Class
Dual orexin receptor antagonist (OX1R / OX2R)
Available Doses
5, 10, 15, 20 mg tablets
Route
Oral
Renal Adjustment
Not required (any severity)
Hepatic Adjustment
No adjustment in mild/moderate; not recommended in severe
Pregnancy
Postmarketing data insufficient to establish risk; animal fetal weight reduction at high doses
Lactation
Present in human milk at low concentrations (RID <1%); monitor infants for somnolence
Schedule / Legal
DEA Schedule IV (C-IV)
Generic Available
No (US); patent protection through ~2029–2033
Rx

Indications

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

Suvorexant is the first-in-class dual orexin receptor antagonist (DORA) approved by the FDA for insomnia. Unlike the benzodiazepine receptor agonists (Z-drugs and benzodiazepines), it does not enhance GABA neurotransmission; instead, it blocks the wake-promoting orexin signaling system, which is consistent with its broader labeled indication covering both sleep onset and sleep maintenance. The 2017 American Academy of Sleep Medicine clinical practice guideline gives suvorexant a conditional (weak) recommendation specifically for sleep maintenance insomnia in adults. 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.

Labeled Population — Mild-to-Moderate Alzheimer Disease

In February 2020 the FDA approved a label update incorporating findings from a phase 3 polysomnography trial of suvorexant in 285 patients with mild-to-moderate Alzheimer disease and insomnia (Herring 2020). Suvorexant produced statistically significant improvements in total sleep time and wake-after-sleep-onset versus placebo. The labeled indication wording is unchanged (“insomnia characterized by difficulties with sleep onset and/or sleep maintenance”); use in this population is therefore on-label and supported by PI-incorporated evidence. Adverse-event rates in this trial are reflected in the Side Effects section.

Off-Label & Investigational Uses

Delirium prevention in hospitalized older adults — Several Japanese RCTs and observational analyses suggest a reduction in delirium incidence when suvorexant is used prophylactically in at-risk inpatients (Hatta 2020). Findings in mixed and ICU populations have been more variable. Evidence quality: low to moderate.

Insomnia in substance-use recovery — Small early-phase studies in opioid and alcohol use disorder; not established. Evidence quality: very low.

Dose

Dosing

The labeled approach is to use the lowest effective dose. Recommended starting dose is 10 mg taken within 30 minutes of going to bed, only when at least 7 hours of sleep opportunity remain before activities requiring full alertness. The 10 mg dose may be increased to a maximum of 20 mg once daily if 10 mg is well tolerated but ineffective. Because suvorexant exposure is higher in women and in patients with high BMI, dose escalation should be especially conservative in obese women. Concurrent CYP3A inhibitors materially change the exposure–effect relationship and dictate specific dose ceilings.

Clinical ScenarioStarting DoseMaintenance DoseMaximum DoseNotes
Adult insomnia (sleep onset and/or maintenance) — primary indication10 mg PO10–20 mg nightly20 mg/dayTake within 30 min of bed; ≥7 h before planned awakening
May increase to 20 mg if 10 mg well tolerated but ineffective
Older adults (≥65 years)10 mg PO10–20 mg nightly20 mg/daySame recommended dosing as younger adults
15 mg was the dose used in pivotal elderly trial arms; counsel on falls and next-day driving
Mild-to-moderate Alzheimer disease (labeled population)10 mg PO10–20 mg nightly20 mg/daySame recommended dosing
In the AD trial, 77% of patients were uptitrated from 10 mg to 20 mg after 2 weeks
Obese women (BMI ≥30)10 mg PO10 mg nightly10–20 mg/dayCautious escalation
AUC ~46% and Cmax ~25% higher than non-obese women
Concomitant moderate CYP3A inhibitor (e.g., diltiazem, verapamil, erythromycin, fluconazole, ciprofloxacin)5 mg PO5–10 mg nightly10 mg/dayMay increase to 10 mg only if needed
Avoid grapefruit juice on dosing nights
Concomitant strong CYP3A inhibitor (e.g., ketoconazole, itraconazole, clarithromycin, ritonavir, nefazodone)Not recommendedUse alternative hypnotic
Substantial increase in exposure expected
Concomitant strong CYP3A inducer (e.g., rifampin, carbamazepine, phenytoin)Efficacy may be reducedChoose a non-CYP3A-dependent hypnotic if appropriate
Mild–moderate hepatic impairment (Child-Pugh A–B)10 mg PO10 mg nightly20 mg/dayNo formal dose adjustment
Apparent terminal t½ ~19 h in moderate impairment vs ~15 h healthy
Severe hepatic impairment (Child-Pugh C)Not recommendedNot studied; avoid use
Renal impairment (any severity, including severe)10 mg PO10–20 mg nightly20 mg/dayNo dose adjustment required
Pediatric (<18 years)Not establishedSafety and effectiveness not established
Clinical Pearl — The 7-Hour Rule

Suvorexant has a half-life of approximately 12 hours, longer than most short-acting hypnotics. The FDA label is explicit that suvorexant should not be administered unless ≥7 hours remain before required awakening, and that the 20 mg dose carries a labeled caution against next-day driving. Patients waking earlier than planned, 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 Suvorexant

Mechanism of Action

Suvorexant is a highly selective antagonist at both orexin receptor subtypes, OX1R and OX2R. The orexin (hypocretin) system, with peptidergic neurons in the lateral hypothalamus projecting widely to monoaminergic and cholinergic wake-promoting nuclei, is a key driver of arousal and wakefulness. By blocking the binding of orexin A and orexin B at OX1R and OX2R, suvorexant suppresses wake drive rather than augmenting sleep drive — a fundamentally different mechanism from GABAergic hypnotics. The clinical signature of this mechanism is the labeled signal for narcolepsy-spectrum events (sleep paralysis, hypnagogic/hypnopompic hallucinations, and cataplexy-like leg weakness) in some patients. 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
AbsorptionMedian Tmax ~2 h fasted (range 0.5–6 h); absolute oral bioavailability ~82% at 10 mg; less-than-proportional exposure increase across 10–80 mg due to reduced absorption at higher dosesTime to effect delayed if taken with or soon after a meal (Tmax delayed ~1.5 h with high-fat meal); take on an empty stomach for fastest onset
DistributionVd ~49 L; protein binding >99% (albumin and α1-acid glycoprotein); not preferentially distributed to red blood cellsHigh protein binding; clinically meaningful displacement interactions are unlikely. Hemodialysis is not expected to remove drug in overdose
MetabolismHepatic; CYP3A is the major enzyme, with minor contribution from CYP2C19. Major circulating metabolite (hydroxy-suvorexant) is not pharmacologically activeCYP3A is the dominant determinant of drug interactions — strong CYP3A inhibitors are not recommended; moderate inhibitors require dose reduction
Elimination~66% feces, ~23% urine (as metabolites); steady-state by day 3; t½ ~12 h; accumulation 1- to 2-fold with daily dosingHalf-life is meaningfully longer than older hypnotics — adequate sleep opportunity (≥7 h) is essential. No renal dose adjustment
SE

Side Effects

The most common adverse event in pivotal trials of suvorexant 15 mg or 20 mg was somnolence (7% vs 3% on placebo). Other common events including headache, dizziness, dry mouth, abnormal dreams, and cough occurred at incidences within 1–2 percentage points of placebo. Most CNS adverse events show a clear dose response, and the labeled narcolepsy-spectrum events (sleep paralysis, hypnagogic/hypnopompic hallucinations, cataplexy-like leg weakness) — although uncommon — are mechanistically distinctive and increase with dose. Suvorexant is a Schedule IV controlled substance, and abuse-liability studies in recreational polydrug users showed subjective ratings comparable to zolpidem.

≥10% Very Common
Adverse EffectIncidenceClinical Note
None reported at this frequencyNo adverse event reached ≥10% incidence on suvorexant 15 mg or 20 mg in pivotal placebo-controlled trials
1–10% Common — Pivotal Adult Insomnia Trials (Suvorexant 15 or 20 mg, n=493 vs Placebo n=767)
Adverse EffectIncidenceClinical Note
Somnolence (next-day)7%Placebo 3%; dose-related (2% at 10 mg → 5% at 20 mg → 12% at 40 mg). Higher in women (8%) than men (3%)
Headache7%Placebo 6%; usually mild and self-limiting
Dizziness3%Placebo 2%; counsel older adults to rise slowly if waking overnight
Diarrhea2%Placebo 1%
Dry mouth2%Placebo 1%
Upper respiratory tract infection2%Placebo 1%; clinical significance unclear
Abnormal dreams2%Placebo 1%; usually not bothersome but warrant inquiry on follow-up
Cough2%Placebo 1%
No other adverse event was reported at ≥2% on suvorexant 15 mg or 20 mg at a higher rate than placebo in pivotal trials.
1–10% Common — Mild-to-Moderate Alzheimer Disease Trial (Suvorexant 10–20 mg, n=142 vs Placebo n=143)
Adverse EffectIncidenceClinical Note
Somnolence4%Placebo 1%; lower absolute rate than non-AD trials, possibly reflecting shorter exposure
Dry mouth2%Placebo 1%
Falls2%Placebo 0%; assess gait stability and fall risk before dose escalation in dementia
Serious Regardless of Frequency
Adverse EffectEstimated FrequencyTypical OnsetRequired Action
Daytime impairment / impaired drivingDose-related; documented at 20 mg in healthy non-elderly volunteersMorning after doseCounsel against next-day driving at 20 mg dose; reduce dose or discontinue if daytime somnolence develops
Complex sleep behaviors (sleep-driving, sleep-eating, phone calls, sex with amnesia)Reported with hypnotics including suvorexantAny time during therapyStrongly consider permanent discontinuation after any episode; risk increased by alcohol and other CNS depressants
Worsening depression and emergence of suicidal ideationDose-dependent increase in suicidal ideation by questionnaire in trialsVariableImmediately 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)Uncommon; dose-relatedSleep–wake transitionsReassure if isolated and brief; consider dose reduction or discontinuation if recurrent or distressing
Hypnagogic / hypnopompic hallucinationsUncommon; dose-relatedFalling 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)Uncommon; dose-related; not necessarily emotion-triggeredVariableConsider dose reduction or discontinuation; assess fall risk in older adults and patients with dementia
Respiratory depression in compromised patientsCannot be excluded in OSA or COPD per PIVariableNot studied in severe OSA or severe COPD; consider risks before prescribing in these populations and in combination with opioids
Abuse and dependence (Schedule IV)Subjective effects similar to zolpidem in recreational drug usersVariableScreen substance-use history; monitor for misuse; prescribe limited quantities in at-risk patients
Discontinuation Treatment-Emergent Withdrawal in Trials
Pivotal 3-Month Trials (Suvorexant 15 / 20 mg vs placebo)
3% vs 5% placebo
Per the FDA label, no individual adverse reaction led to discontinuation at an incidence ≥1%.
Long-term Exposure
No physical dependence / no withdrawal in completed trials
No clear evidence of withdrawal symptoms or rebound insomnia after abrupt discontinuation. Suvorexant is nonetheless a Schedule IV controlled substance based on abuse-liability data.
Management Pearl — Driving and Daytime Function

Driving studies in healthy adults documented impaired Standard Deviation of Lane Position with the 20 mg dose, with a small minority of subjects (4 non-elderly women) prematurely terminating the driving test due to somnolence. The FDA label specifically cautions patients on the 20 mg dose against next-day driving and other activities requiring full mental alertness. Counsel every patient — including those on 10 mg — to allow at least 8 hours between dose and driving and to discontinue or step down if morning impairment develops.

Int

Drug Interactions

Suvorexant is a CYP3A substrate, and CYP3A inhibitor / inducer interactions are the dominant pharmacokinetic concerns. Suvorexant itself is a weak intestinal P-glycoprotein inhibitor with a small effect on digoxin exposure. Pharmacodynamic additivity with alcohol and other CNS depressants is the dominant non-PK concern. Paroxetine showed no clinically meaningful PK or PD interaction in a dedicated study.

Major Strong CYP3A inhibitors (ketoconazole, itraconazole, posaconazole, clarithromycin, nefazodone, ritonavir, indinavir, saquinavir, nelfinavir, boceprevir, telaprevir, telithromycin, conivaptan)
MechanismStrong CYP3A inhibition
EffectSubstantial increase in suvorexant exposure with concomitant excess sedation and impairment
ManagementConcomitant use is not recommended. Choose an alternative antifungal/antibiotic/antiviral, or a non-CYP3A-dependent hypnotic
FDA PI
Major Alcohol
MechanismPharmacodynamic — additive psychomotor impairment; no clinically meaningful PK change
EffectIncreased CNS depression and risk of complex sleep behaviors
ManagementCounsel patients not to consume alcohol on nights they take suvorexant
FDA PI
Major Other CNS depressants (opioids, benzodiazepines, tricyclic antidepressants, sedating antihistamines)
MechanismPharmacodynamic — additive CNS depression and respiratory depression with opioids
EffectIncreased risk of falls, daytime impairment, complex sleep behaviors, and respiratory depression
ManagementAvoid combination with other hypnotics. With necessary opioid co-use, use lowest effective doses and counsel on driving and machinery
FDA PI
Moderate Moderate CYP3A inhibitors (diltiazem, verapamil, erythromycin, fluconazole, ciprofloxacin, aprepitant, atazanavir, fosamprenavir, amprenavir, imatinib, grapefruit juice)
MechanismModerate CYP3A inhibition
EffectSignificant increase in suvorexant exposure
ManagementReduce starting dose to 5 mg; max 10 mg if needed for efficacy. Avoid grapefruit juice on dosing nights
FDA PI
Moderate Strong CYP3A inducers (rifampin, carbamazepine, phenytoin)
MechanismInduction of CYP3A
EffectSubstantial decrease in suvorexant exposure with reduced efficacy
ManagementChoose a non-CYP3A-dependent hypnotic during enzyme-inducer therapy
FDA PI
Minor Digoxin
MechanismSuvorexant inhibits intestinal P-glycoprotein
EffectSlight increase in digoxin levels
ManagementMonitor digoxin concentrations as clinically indicated
FDA PI
Drugs Studied With No Clinically Meaningful Interaction

Per the FDA label, dedicated PK/PD studies showed no clinically meaningful interactions when suvorexant was co-administered with paroxetine, midazolam (CYP3A substrate), warfarin, or oral contraceptives. Suvorexant is unlikely to cause clinically significant inhibition of CYP1A2, CYP2B6, CYP2C8, CYP2C9, CYP2C19, or CYP2D6.

Mon

Monitoring

The FDA label does not specify routine laboratory monitoring for suvorexant. Clinical follow-up should focus on therapeutic response, daytime function, dose-related neuropsychiatric and narcolepsy-spectrum events, and — because suvorexant 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 difficulty concentrating. Reduce to 10 mg or discontinue if daytime impairment develops.
  • Mood and suicidal ideation Each follow-up visit
    Routine     A dose-dependent increase in suicidal ideation by questionnaire was observed in trials. 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. Strongly consider permanent discontinuation after any 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. Dose reduction or discontinuation if recurrent.
  • Falls and balance (older adults, dementia) Each follow-up visit
    Routine     Falls were reported in 2% of suvorexant-treated patients in the AD trial vs 0% on placebo. Assess gait stability, especially before dose escalation in dementia or frail older adults.
  • Substance-use risk Baseline; ongoing as indicated
    Routine     Suvorexant is a Schedule IV controlled substance. Screen for prior alcohol or sedative misuse before initiation; monitor for early refill requests or dose escalation.
  • Respiratory status Baseline if compromised
    Trigger-based     In patients with OSA or COPD, weigh hypnotic need against potential respiratory effects. Suvorexant has not been studied in severe OSA or severe COPD.
  • Digoxin levels When co-administered
    Trigger-based     Per the FDA label, monitor digoxin concentrations when co-administered with suvorexant.
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 CYP3A inhibitors — co-administration is not recommended due to substantial increase in suvorexant exposure.
  • Severe hepatic impairment (Child-Pugh C) — not studied; the FDA label states suvorexant is not recommended.
  • Active major depression with suicidal ideation — a dose-dependent increase in suicidal ideation was observed in pivotal trials. Prescribe the lowest feasible quantity per label.
  • Pediatric patients — safety and effectiveness have not been established.

Use with Caution

  • Severe obstructive sleep apnea or severe COPD — not studied in these populations; respiratory effects cannot be excluded. Weigh risk–benefit individually.
  • Mild-to-moderate respiratory disease — clinically meaningful respiratory effects cannot be excluded.
  • Older adults — falls and confusion are more clinically meaningful; the 15 mg dose was used in pivotal elderly trial arms.
  • Mild-to-moderate Alzheimer disease — labeled population data exist; falls were reported in 2% (vs 0% placebo). Assess gait and supervision needs.
  • Obese patients, particularly obese women — exposure is meaningfully higher; cautious dose escalation. AUC is approximately 46% higher in obese women vs non-obese women.
  • Concomitant moderate CYP3A inhibitors — start at 5 mg, max 10 mg.
  • History of substance use disorder — Schedule IV; abuse-liability comparable to zolpidem in recreational users.
  • Patients who cannot guarantee 7 hours of sleep opportunity — risk of next-day impairment is materially increased.
  • Pregnancy and lactation — postmarketing data are insufficient to establish drug-associated risk; animal studies show decreased fetal weight at high doses. Suvorexant and its metabolite are present in human breast milk at low concentrations (relative infant dose <1%); monitor breastfed infants for somnolence and feeding problems.
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. Suvorexant was not included in the 2019 Boxed Warning, but its FDA label states that complex sleep behaviors have been reported with suvorexant and that discontinuation should be strongly considered for any patient who reports such an episode. 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

Suvorexant 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). Suvorexant 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 within 30 minutes of 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 10 mg; the maximum is 20 mg per night. Take it on an empty stomach for fastest effect — taking it with or shortly after a meal will delay how quickly it begins working. Do not drink alcohol on evenings you take suvorexant.

Next-Day Drowsiness & Driving
Tell patient You may feel drowsy or “foggy” the next morning, especially at the 20 mg dose. Do not drive or do anything that requires full alertness within 8 hours of taking your dose, and do not drive at all the day after a 20 mg dose if you feel impaired.
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 suvorexant when you can stay in bed at least 7 hours before being active. Take it within 30 minutes of going to bed. Take it on an empty stomach if possible — meals will delay how quickly it works.
Call prescriber If you regularly cannot get 7 hours of sleep — there may be a better option for your schedule.
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 & Hallucinations
Tell patient Some people experience brief, frightening episodes of being unable to move or speak as they fall asleep or wake up, or vivid dream-like visions during these transitions. Mild leg weakness during the day or at night has also been reported. 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, more people on suvorexant reported suicidal thoughts than on placebo, especially at higher doses.
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 suvorexant. Do not drink alcohol on evenings you take it. Avoid grapefruit juice. Several common medications — certain antibiotics (clarithromycin, erythromycin, ciprofloxacin), antifungals (ketoconazole, fluconazole), heart drugs (diltiazem, verapamil), and HIV medications — can change the level of suvorexant in your blood.
Call prescriber Before starting any new medication — including over-the-counter sleep aids, antibiotics, antifungals, or supplements — check with the prescriber or pharmacist.
Controlled Substance & Storage
Tell patient Suvorexant 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. Effects on the human fetus are not fully characterised. Suvorexant does pass into breast milk in small amounts; if you breastfeed, the prescriber may suggest watching the baby for unusual sleepiness or feeding difficulty.
Call prescriber If you become pregnant while on suvorexant, or if your breastfed baby seems unusually sleepy or feeds poorly.
Ref

Sources

Regulatory (PI / Safety Communications)
  1. U.S. Food and Drug Administration. Belsomra (suvorexant) prescribing information — supplement s006 (February 2020 label update incorporating Alzheimer disease findings; initial approval August 2014). accessdata.fda.gov Authoritative US label — primary source for indications, dosing, contraindications, interactions, and incidence figures cited throughout this monograph.
  2. DailyMed (NIH). BELSOMRA (suvorexant) tablet, film coated — current label. dailymed.nlm.nih.gov Searchable, regularly updated mirror of the FDA-approved labeling, including the PLLR-format Pregnancy and Lactation sections.
  3. 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; suvorexant is not included.
  4. Merck. FDA approves BELSOMRA (suvorexant) C-IV label update to include findings from study of insomnia in patients with mild-to-moderate Alzheimer’s disease (press release, February 3, 2020). merck.com Source for the 2020 label update incorporating Alzheimer disease trial findings into the prescribing information.
Key Clinical Trials
  1. Herring WJ, Snyder E, Budd K, et al. Orexin receptor antagonism for treatment of insomnia: a randomized clinical trial of suvorexant. Neurology. 2012;79(23):2265–2274. Phase IIb randomized trial establishing dose-response and the basis for the registrational program.
  2. Herring WJ, Connor KM, Ivgy-May N, et al. Suvorexant in patients with insomnia: results from two 3-month randomized controlled clinical trials. Biol Psychiatry. 2016;79(2):136–148. Pivotal Phase III trials (Studies 1 and 2) supporting the FDA approval; source for efficacy data on sleep latency and sleep maintenance.
  3. Michelson D, Snyder E, Paradis E, et al. Safety and efficacy of suvorexant during 1-year treatment of insomnia with subsequent abrupt treatment discontinuation: a phase 3 randomised, double-blind, placebo-controlled trial. Lancet Neurol. 2014;13(5):461–471. 12-month efficacy and safety data; supports absence of physical dependence and rebound insomnia after abrupt discontinuation.
  4. Herring WJ, Ceesay P, Snyder E, et al. Polysomnographic assessment of suvorexant in patients with probable Alzheimer’s disease dementia and insomnia: a randomized trial. Alzheimers Dement. 2020;16(3):541–551. Randomized trial of 285 patients with mild-to-moderate Alzheimer disease; basis for the February 2020 FDA label update incorporating AD findings into the prescribing information.
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 that gives suvorexant a conditional (weak) recommendation for sleep maintenance insomnia in adults.
  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. Cox CD, Breslin MJ, Whitman DB, et al. Discovery of the dual orexin receptor antagonist [(7R)-4-(5-chloro-1,3-benzoxazol-2-yl)-7-methyl-1,4-diazepan-1-yl][5-methyl-2-(2H-1,2,3-triazol-2-yl)phenyl]methanone (MK-4305) for the treatment of insomnia. J Med Chem. 2010;53(14):5320–5332. Discovery and characterisation of suvorexant (MK-4305) — establishes the OX1R/OX2R selectivity profile.
  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. Sun H, Kennedy WP, Wilbraham D, et al. Effects of suvorexant, an orexin receptor antagonist, on sleep parameters as measured by polysomnography in healthy men. Sleep. 2013;36(2):259–267. Polysomnographic characterisation of suvorexant pharmacodynamics in healthy adults.
  2. Vermeeren A, Sun H, Vuurman EFPM, et al. On-the-road driving performance the morning after bedtime use of suvorexant 20 and 40 mg: a study in non-elderly healthy volunteers. Sleep. 2015;38(11):1803–1813. On-the-road driving study underpinning the FDA caution against next-day driving at the 20 mg dose.
  3. Hatta K, Kishi Y, Wada K, et al. Real-world effectiveness of ramelteon and suvorexant for delirium prevention in 948 patients with delirium risk factors. J Clin Psychiatry. 2020;81(1):19m12865. Largest real-world cohort supporting the off-label use of suvorexant for delirium prevention in at-risk inpatients.