Daridorexant: Complete Drug Monograph & Prescribing Guide

Pharmacokinetic Profile

Half-Life

~8 h (no accumulation)

Metabolism

Hepatic — CYP3A4 (89%); other CYPs <3%

Protein Binding

99.7%

Bioavailability

~62% absolute

Volume of Distribution

~31 L

Clinical Information

Drug Class

Dual orexin receptor antagonist (OX1R / OX2R)

Available Doses

25 mg, 50 mg tablets

Route

Oral

Renal Adjustment

Not required (any severity, including severe; not studied on dialysis)

Hepatic Adjustment

Moderate: max 25 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 (C-IV)

Generic Available

No (US); brand-only — patent protection through ~December 2034

Indications

Indication	Approved Population	Therapy Type	Status
Insomnia characterized by difficulties with sleep onset and/or sleep maintenance	Adults	Monotherapy	FDA Approved

Daridorexant is the third dual orexin receptor antagonist (DORA) approved by the FDA, following suvorexant (2014) and lemborexant (2019). It was approved on January 7, 2022, and became commercially available in the US in May 2022 after DEA Schedule IV scheduling. Among the DORAs, daridorexant has the shortest effective half-life (~8 hours), a property selected during development to minimize next-day residual effects. The pivotal Phase 3 program (Studies 1 and 2, published as Mignot et al. Lancet Neurology 2022) was the first insomnia trial program to formally demonstrate that an insomnia drug improves patient-reported daytime functioning using the validated Insomnia Daytime Symptoms and Impacts Questionnaire (IDSIQ), in addition to objective polysomnographic improvements in latency to persistent sleep and wake after sleep onset.

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 2017 AASM clinical practice guideline pre-dates daridorexant approval and therefore does not contain a specific recommendation for it.

Off-Label & Investigational Uses

Insomnia in dementia populations — Unlike suvorexant (whose label was updated in 2020 to include findings from a phase 3 Alzheimer disease trial) and lemborexant (which has phase 2 data in irregular sleep–wake rhythm disorder with AD), daridorexant has not been studied in dedicated dementia-population trials. Use in mild cognitive impairment or early dementia is therefore extrapolation from the general insomnia population. Evidence quality: very low (extrapolation only).

Delirium prevention in hospitalized patients — Limited case series and small observational studies; the published evidence base is far less mature than for suvorexant or ramelteon. Evidence quality: very low.

Shift-work-related sleep disturbance and circadian rhythm disorders — Mechanistically plausible but not formally studied in registered trials. Evidence quality: very low.

Dose

Dosing

The recommended dosage range is 25 mg to 50 mg taken orally once per night within 30 minutes of going to bed, with at least 7 hours remaining before planned awakening. Unlike suvorexant and lemborexant, the FDA label provides a flexible dose range rather than a strict starting-dose-then-titrate algorithm; many prescribers begin at 25 mg in older or sensitive patients and 50 mg when substantial sleep maintenance impairment is the dominant complaint. Concomitant CYP3A4 inhibitors and hepatic impairment dictate specific dose ceilings, and concomitant strong or moderate CYP3A4 inducers must be avoided altogether.

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Dose	Notes
Adult insomnia (sleep onset and/or maintenance) — primary indication	25–50 mg PO	25–50 mg nightly	50 mg/day	Take within 30 min of bed; ≥7 h before planned awakening Choose dose based on relative weight of sleep onset vs maintenance complaint and patient sensitivity
Older adults (≥65 years)	25 mg PO	25–50 mg nightly	50 mg/day	No formal dose adjustment per label Likelihood of somnolence and fatigue increases with age; falls risk should be considered before escalation to 50 mg
Mild hepatic impairment (Child-Pugh A)	25–50 mg PO	25–50 mg nightly	50 mg/day	No dose adjustment required
Moderate hepatic impairment (Child-Pugh B, score 7–9)	25 mg PO	25 mg nightly	25 mg/day	Maximum 25 mg AUC and Cmax increased to a clinically relevant extent
Severe hepatic impairment (Child-Pugh C, score ≥10)	Not recommended	—	—	Not studied; avoid use
Renal impairment (mild, moderate, severe; not on dialysis)	25–50 mg PO	25–50 mg nightly	50 mg/day	No dose adjustment required (CrCl <30 mL/min not on dialysis was studied without clinically significant PK change)
Concomitant moderate CYP3A4 inhibitor (e.g., diltiazem, verapamil, fluconazole, erythromycin, ciprofloxacin)	25 mg PO	25 mg nightly	25 mg/day	Maximum 25 mg Diltiazem 240 mg increases daridorexant AUC ~2.4-fold
Concomitant strong CYP3A4 inhibitor (e.g., itraconazole, ketoconazole, clarithromycin, ritonavir, posaconazole, nefazodone)	Avoid			Use alternative hypnotic Itraconazole predicted to increase daridorexant AUC by >400% (PBPK modeling)
Concomitant strong or moderate CYP3A4 inducer (e.g., rifampin, carbamazepine, phenytoin, St. John’s wort, efavirenz, modafinil)	Avoid			Choose a non-CYP3A-dependent hypnotic Efavirenz reduces daridorexant AUC to ~0.4× (60% reduction); rifampin predicted >50% reduction
Pediatric (<18 years)	Not established	—	—	Safety and effectiveness not established

Clinical Pearl — Half-Life Positioning Within the DORA Class

Daridorexant’s effective half-life of approximately 8 hours and absence of accumulation with chronic dosing distinguish it from the other DORAs (suvorexant ~12 h; lemborexant 17–19 h). The 7-hour rule still applies — the FDA label is explicit that daridorexant should not be administered unless ≥7 hours remain before required awakening — but the shorter half-life is the design rationale behind its labeled improvement in daytime functioning, the first such demonstration for any insomnia drug. CNS depressant effects can still persist for several days after discontinuation in some patients, particularly older adults.

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.

Pharmacology of Daridorexant

Mechanism of Action

Daridorexant is a competitive antagonist at the orexin OX1R and OX2R receptors with high in vitro potency (Ki = 0.47 nM and 0.93 nM, respectively). The orexin (hypocretin) signaling system, originating in the lateral hypothalamus, drives wakefulness through projections to monoaminergic and cholinergic arousal nuclei; orexin A and orexin B are the principal endogenous neuropeptides. By blocking their binding at OX1R and OX2R, daridorexant suppresses wake drive rather than augmenting sleep drive — a mechanism that does not reproduce the GABAergic enhancement of benzodiazepine receptor agonists. The drug was selected from a pool of candidates specifically for an expected duration of effect of approximately 8 hours at therapeutic doses, with the aim of providing a full night of sleep coverage while minimising next-day residual sedation. As with the other DORAs, narcolepsy is the only labeled contraindication on mechanistic grounds, since the underlying pathology of human narcolepsy with cataplexy is loss of orexin signaling.

ADME Profile

Parameter	Value	Clinical Implication
Absorption	Tmax 1–2 h; absolute oral bioavailability ~62%; dose-proportional from 25 to 50 mg; high-fat meal delays Tmax by ~1.3 h and decreases Cmax by ~16% but does not affect AUC	Take on a relatively empty stomach for fastest sleep-onset effect; the AUC-preserving food effect means total exposure is unchanged
Distribution	Vd ~31 L; plasma protein binding 99.7%; blood-to-plasma ratio 0.64	Compact distribution volume; high protein binding means hemodialysis is not effective in overdose
Metabolism	Hepatic; CYP3A4 accounts for ~89% of metabolic clearance; other CYPs each contribute <3% individually	CYP3A4 dominates the interaction profile — strong inhibitors must be avoided, moderate inhibitors require dose reduction to 25 mg, and strong or moderate inducers must be avoided
Elimination	Terminal t½ ~8 h; ~57% feces, ~28% urine (both primarily as metabolites); trace parent drug in feces and urine; no accumulation with multiple-dose administration	Shortest half-life among the marketed DORAs; absence of accumulation simplifies long-term use; clinically meaningful next-day exposure is lower than with suvorexant or lemborexant

Side Effects

The pivotal program enrolled 1,854 adults with DSM-5 insomnia disorder across two 3-month placebo-controlled trials (Study 1, NCT03545191; Study 2, NCT03575104) and a 9-month extension (Study 3). A total of 1,232 patients received daridorexant in the safety population, with 576 treated for at least 6 months and 331 for at least 12 months. Approximately 40% of subjects were ≥65 years. The most common adverse reactions in the FDA Table 1 (≥2% on daridorexant and greater than placebo, Study 1) were headache and somnolence/fatigue, both at single-digit incidence rates and only modestly above placebo. Driving impairment was statistically significant compared to placebo after the first dose at 50 mg in healthy volunteers but was not statistically significant after 4 consecutive nights, although individual sensitivity was variable. The narcolepsy-spectrum events characteristic of the DORA class (sleep paralysis, hypnagogic/hypnopompic hallucinations, cataplexy-like leg weakness) are uncommon at recommended doses.

≥10% Very Common

Adverse Effect	Incidence	Clinical Note
None reported at this frequency in pivotal trials	—	No adverse event reached ≥10% incidence on daridorexant 25 mg or 50 mg in pivotal placebo-controlled trials

1–10% Common — FDA Table 1 (Study 1, ≥2% and Greater than Placebo)

Adverse Effect	Incidence (25 mg / 50 mg)	Clinical Note
Headache (incl. tension headache, migraine, head discomfort)	6% / 7%	Placebo 5%; usually mild and self-limiting
Somnolence or fatigue (incl. sedation, hypersomnia, lethargy)	6% / 5%	Placebo 4%; rate of somnolence/fatigue increases with patient age
Dizziness (incl. vertigo, labyrinthitis)	2% / 3%	Placebo 2%; counsel older adults about overnight ambulation
Nausea (incl. vomiting, procedural nausea)	0% / 3%	Placebo 2%; only at the 50 mg dose

No other adverse event was reported at ≥2% in Study 1 at a higher rate than placebo. Nightmares and abnormal dreams were not in Table 1 but have been identified in post-marketing experience.

Serious Regardless of Frequency

Adverse Effect	Estimated Frequency	Typical Onset	Required Action
Daytime impairment / impaired driving	Statistically significant after first dose at 50 mg in driving-simulator study; not statistically significant after 4 nights	Morning after dose; may persist for several days after discontinuation in some patients	Counsel against next-day driving; reduce to 25 mg or discontinue if daytime somnolence develops
Complex sleep behaviors (sleep-walking, sleep-driving, preparing/eating food, phone calls, sex with amnesia)	Reported with hypnotics including DORAs	Any time during therapy, including first dose	Discontinue immediately if any episode occurs; risk increased by alcohol and other CNS depressants
Worsening depression and emergence of suicidal ideation	Reported with hypnotics, particularly in primarily depressed patients	Variable	Use with caution in patients with depression; prescribe smallest feasible quantity to limit overdose risk; immediately evaluate any new behavioral signs or suicidal ideation
Sleep paralysis	0.5% (25 mg) and 0.3% (50 mg); placebo 0%	Sleep–wake transitions	Reassure if isolated and brief; consider dose reduction or discontinuation if recurrent or distressing
Hypnagogic / hypnopompic hallucinations	0.6% (25 mg); not reported at 50 mg or with placebo	Falling asleep or waking	Counsel proactively about the nature of these events; consider dose reduction or discontinuation if recurrent
Cataplexy-like symptoms (transient leg weakness, day or night)	Reported with orexin receptor antagonists; not necessarily emotion-triggered	Variable	Consider dose reduction or discontinuation; assess fall risk in older adults
Hypersensitivity reactions (post-marketing) — angioedema, rash, urticaria; angioedema with pharyngeal involvement reported	Frequency not established (post-marketing)	Any time	Permanently discontinue; treat as standard angioedema/anaphylaxis. Hypersensitivity to daridorexant is now a labeled contraindication (added October 2023)
Respiratory depression in compromised patients	Studied in mild–severe OSA and moderate COPD; clinically meaningful effects cannot be excluded	Variable	Consider risks before prescribing in OSA, COPD, or with concomitant opioids. Not studied in mild or severe COPD
Abuse and dependence (Schedule IV)	At 50 mg, “drug liking” significantly lower than zolpidem 30 mg or suvorexant 150 mg in recreational users; at supratherapeutic 100–150 mg doses, similar to comparators	Variable	Screen substance-use history; monitor for misuse. No physical dependence in clinical trials

Discontinuation Treatment-Emergent Withdrawal in Trials

Pivotal 3-Month Trials (Mignot 2022)

Comparable to placebo across treatment arms

In Study 1 and Study 2, the overall incidence of adverse events leading to discontinuation was similar across daridorexant 25 mg, 50 mg, and placebo arms. The FDA PI does not enumerate a discontinuation table at the level of individual reasons.

Long-Term Exposure (12 Months)

No physical dependence / no withdrawal on the Tyrer questionnaire

After 3 months of treatment, a 7-day placebo run-out period showed no withdrawal symptoms. Modest small increases in WASO and LPS in the days immediately following discontinuation were observed but did not constitute rebound insomnia.

Daytime Functioning — A Distinguishing Outcome

The pivotal Phase 3 program was the first insomnia drug program to demonstrate a statistically significant improvement in patient-reported daytime functioning (Insomnia Daytime Symptoms and Impacts Questionnaire — IDSIQ — sleepiness domain) at the 50 mg dose, alongside the conventional sleep onset and maintenance endpoints. This is the principal clinical positioning argument for choosing daridorexant within the DORA class — the trade-off is brand-only pricing and the absence of a US generic.

Int

Drug Interactions

Daridorexant is a CYP3A4 substrate, with ~89% of metabolic clearance attributable to that enzyme; CYP3A4 inhibitors and inducers therefore dominate the pharmacokinetic interaction profile. Daridorexant itself causes mild-to-moderate increases in exposure of CYP3A4 substrates and P-gp substrates with narrow therapeutic indices. Pharmacodynamic additivity with alcohol and other CNS depressants is the dominant non-PK concern. No clinically significant interaction has been observed with citalopram (an SSRI commonly co-prescribed with hypnotics).

Major Strong CYP3A4 inhibitors (itraconazole, ketoconazole, clarithromycin, posaconazole, ritonavir, nefazodone)

MechanismStrong CYP3A4 inhibition

EffectItraconazole predicted (PBPK) to increase daridorexant AUC by >400%

ManagementAvoid concomitant use. Choose alternative anti-infective or non-CYP3A-dependent hypnotic

FDA PI

Major Strong or moderate CYP3A4 inducers (rifampin, carbamazepine, phenytoin, St. John’s wort, efavirenz, modafinil, bosentan)

MechanismCYP3A4 induction

EffectEfavirenz reduces daridorexant AUC to ~0.4× (60% reduction); rifampin predicted to reduce AUC by >50%

ManagementAvoid concomitant use per FDA label

FDA PI

Major Alcohol

MechanismPharmacodynamic — additive psychomotor impairment; no clinically meaningful PK interaction

EffectAdditive impairment of postural stability and alertness near Tmax

ManagementCounsel patients not to consume alcohol on nights they take daridorexant

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

ManagementUse of daridorexant with other insomnia drugs is not recommended per label. Use lowest effective doses with necessary opioid co-prescribing; consider dose adjustment of either drug

FDA PI

Moderate Moderate CYP3A4 inhibitors (diltiazem, verapamil, fluconazole, erythromycin, ciprofloxacin, aprepitant, atazanavir)

MechanismModerate CYP3A4 inhibition

EffectDiltiazem 240 mg increases daridorexant AUC ~2.4-fold

ManagementReduce daridorexant to maximum 25 mg per night while concurrent therapy continues

FDA PI

Moderate CYP3A4 substrates with narrow therapeutic index (e.g., midazolam, alfentanil, certain immunosuppressants)

MechanismDaridorexant modestly inhibits CYP3A4

EffectSingle-dose daridorexant 50 mg increases midazolam AUC ~1.4-fold

ManagementUse with caution; monitor for substrate-specific toxicity

FDA PI

Moderate P-gp substrates with narrow therapeutic index (e.g., dabigatran, certain digoxin uses)

MechanismDaridorexant inhibits P-glycoprotein

EffectDaridorexant 50 mg increases dabigatran AUC ~1.4-fold

ManagementUse with caution; monitor anticoagulation parameters or substrate-specific endpoints

FDA PI

Minor Mild CYP3A4 inhibitors (e.g., ranitidine)

MechanismMild CYP3A4 inhibition

EffectPredicted daridorexant AUC increase ~1.5-fold

ManagementNo dose adjustment required per FDA label

FDA PI

Drugs Studied With No Clinically Meaningful Interaction

Per the FDA label, dedicated PK/PD studies showed no clinically meaningful interactions when daridorexant 50 mg was co-administered with citalopram 20 mg, warfarin (CYP2C9 substrate), rosuvastatin (BCRP/OATP substrate), or famotidine (gastric pH modifier). Daridorexant does not appear to affect alcohol concentrations.

Mon

Monitoring

The FDA label does not specify routine laboratory monitoring for daridorexant. Clinical follow-up should focus on therapeutic response, daytime function (the principal clinical positioning advantage), dose-related neuropsychiatric and narcolepsy-spectrum events, falls in older adults, and — because daridorexant is a controlled substance — appropriate use and abuse-screening. The October 2023 contraindication for hypersensitivity adds a specific requirement to assess and document any prior reaction.

Sleep response Reassess at 7–10 days, then periodically
Routine Track sleep latency, wake after sleep onset, total sleep time, and especially 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 function (IDSIQ-style review) Each follow-up visit
Routine Specifically inquire about sleepiness, alertness, mood, and cognition during the day — daridorexant is the only insomnia drug with a labeled daytime functioning improvement, so the absence of expected benefit should prompt reconsideration of dose, diagnosis, or therapy.
Daytime somnolence and driving Each follow-up visit
Routine Inquire about morning grogginess and near-misses while driving. Driving impairment was statistically significant after the first 50 mg dose in healthy volunteers; counsel new starters specifically about the first few mornings.
Falls and balance (older adults) Each follow-up visit
Routine The likelihood of somnolence increases with age; assess gait stability and consider home safety review before increasing to 50 mg in patients ≥65.
Mood and suicidal ideation Each follow-up visit
Routine Worsening of depression and suicidal thoughts have been reported with hypnotics. PHQ-9 with item 9 review or C-SSRS is appropriate, particularly in patients with prior depression. Prescribe the smallest feasible quantity in at-risk patients.
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 about sleep paralysis, vivid hallucinations on falling asleep or waking, and transient leg weakness. Dose reduction or discontinuation if recurrent or distressing.
Substance-use risk Baseline; ongoing as indicated
Routine Schedule IV controlled substance. Screen for prior alcohol or sedative misuse before initiation; monitor for early refill requests or self-escalation. Daridorexant 50 mg had lower “drug liking” than zolpidem or supratherapeutic suvorexant in the abuse-liability study, but supratherapeutic doses (100–150 mg) had similar profiles.
Hypersensitivity history Baseline; with any new reaction
Trigger-based Hypersensitivity to daridorexant, including angioedema with pharyngeal involvement, has been reported post-marketing and is now a labeled contraindication (added October 2023). Document any prior reaction; permanently discontinue after any episode.
Respiratory status Baseline if compromised
Trigger-based Daridorexant has been studied in mild–severe OSA (without CPAP) and moderate COPD, but not in mild or severe COPD. Clinically meaningful respiratory effects cannot be excluded.
Narrow-TI substrate effects When co-administered
Trigger-based For patients on midazolam, dabigatran, or other narrow-TI CYP3A4 / P-gp substrates, monitor for substrate-specific toxicity (e.g., bleeding, oversedation).

Contraindications & Cautions

Absolute Contraindications (per FDA Label)

Narcolepsy — orexin antagonism could exacerbate the underlying loss of orexin signaling that produces the disorder.
Hypersensitivity to daridorexant or any component of QUVIVIQ — added in October 2023 following post-marketing reports of angioedema with pharyngeal involvement. Patients with any prior reaction should not receive daridorexant.

Not Recommended / Specialist Input Suggested

Concomitant strong CYP3A4 inhibitors — the FDA label directs avoidance of co-administration.
Concomitant strong or moderate CYP3A4 inducers — the FDA label directs avoidance; efficacy is substantially reduced.
Severe hepatic impairment (Child-Pugh score ≥10) — not studied; the FDA label states daridorexant is not recommended.
Active major depression with suicidal ideation — worsening of depression and suicidal thoughts have been reported with hypnotics. Prescribe the smallest feasible quantity per label.
Pediatric patients — safety and effectiveness have not been established.
Combination with other hypnotics — the FDA label specifically states use of daridorexant with other drugs to treat insomnia is not recommended.

Use with Caution

Older adults — likelihood of somnolence and fatigue increases with age; falls risk should be considered before escalation to 50 mg.
Moderate hepatic impairment (Child-Pugh B, score 7–9) — maximum dose 25 mg.
Concomitant moderate CYP3A4 inhibitor — maximum 25 mg.
Compromised respiratory disease (OSA, COPD) — studied in mild–severe OSA (without CPAP) and moderate COPD; not studied in mild or severe COPD. Respiratory effects cannot be excluded.
History of substance use disorder — Schedule IV; abuse liability at supratherapeutic doses comparable to zolpidem and high-dose suvorexant.
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 reproduction studies showed no fetal toxicity at up to 8–10× MRHD. Daridorexant and metabolites are present in rat milk; monitor breastfed infants for excessive sedation. A pregnancy exposure registry is available (1-833-400-9611).

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. Daridorexant was approved in January 2022 — after the 2019 Boxed Warning — and is not included in it, but its FDA label states that complex sleep behaviors have been reported with hypnotics including DORAs and directs immediate discontinuation if any patient experiences such an episode. The risk is increased by alcohol and other CNS depressants. Counsel every patient on this risk before the first dose.

Patient Counselling

Purpose of Therapy

Daridorexant 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). Compared with the other drugs in the same class, daridorexant has a relatively short duration of action and was specifically designed to reduce next-day grogginess. It 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) remains 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 in the evening 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 dose is either 25 mg or 50 mg, chosen by your prescriber. 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 1–2 hours, although the total amount of medication absorbed is unchanged. Do not drink alcohol on evenings you take daridorexant.

Next-Day Drowsiness & Driving

Tell patient Although daridorexant has a shorter duration of action than older sleeping pills, you may still feel drowsy or “foggy” the next morning, especially after the first few doses or if you took the 50 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.

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 daridorexant when you can stay in bed at least 7 hours before being active. Take it within 30 minutes of going to bed. Avoid taking it right after a heavy or fatty meal — food will delay how quickly it starts working by 1–2 hours.

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 or unusually vivid dreams have also been reported. These tend to be brief and self-limiting.

Call prescriber If these episodes are recurrent, distressing, or interfere with sleep — a lower dose or a different medication may be appropriate.

Allergic Reactions

Tell patient Rare cases of allergic reactions including hives, rash, and swelling of the face, throat, or tongue (angioedema) have been reported with daridorexant after it was approved. If you have ever had an allergic reaction to daridorexant, you should not take it again.

Call prescriber Stop the medication and seek emergency care immediately if you develop swelling of the face, lips, tongue, or throat; difficulty breathing or swallowing; or a widespread rash with hives.

Mood & Suicidal Thoughts

Tell patient Tell the prescriber if you have a history of depression or suicidal thinking. Sleep medications, including daridorexant, can in rare cases worsen depression or suicidal thoughts.

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 daridorexant. Do not drink alcohol on evenings you take it. Several common medications can interact: certain antibiotics (clarithromycin, erythromycin, ciprofloxacin), antifungals (itraconazole, ketoconazole, fluconazole), heart drugs (diltiazem, verapamil), HIV medications, the antiseizure medications carbamazepine and phenytoin, and the herbal product St. John’s wort. Daridorexant can also affect the level of certain blood thinners (dabigatran).

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 Daridorexant 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 daridorexant during pregnancy (call 1-833-400-9611). It is not known whether daridorexant passes into human breast milk, but it does pass into the milk of lactating animals.

Call prescriber If you become pregnant while taking daridorexant, or if your breastfed baby seems unusually sleepy or feeds poorly.

Ref

Sources

Regulatory (PI / Safety Communications)

U.S. Food and Drug Administration. Quviviq (daridorexant) prescribing information — current label revised September 2024 (Reference ID 5454933; supplement s011); initial approval January 2022 (Reference ID 4901828). accessdata.fda.gov Authoritative US label — primary source for indications, dosing, contraindications, drug interactions, and incidence figures cited throughout this monograph. Includes hypersensitivity contraindication added October 2023 and updated respiratory function section September 2024.
DailyMed (NIH). QUVIVIQ (daridorexant) 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.
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; daridorexant — approved in 2022 — is not included.

Key Clinical Trials

Mignot E, Mayleben D, Fietze I, et al. Safety and efficacy of daridorexant in patients with insomnia disorder: results from two multicentre, randomised, double-blind, placebo-controlled, phase 3 trials. Lancet Neurol. 2022;21(2):125–139. doi: 10.1016/S1474-4422(21)00436-1 Pivotal Phase 3 program (Studies 1 and 2; 1,854 adults across 156 sites in 17 countries) demonstrating efficacy on objective polysomnographic LPS and WASO and — uniquely among insomnia drugs — patient-reported daytime functioning at the 50 mg dose using the IDSIQ.
Zammit G, Dauvilliers Y, Pain S, et al. Daridorexant, a new dual orexin receptor antagonist, in elderly subjects with insomnia disorder. Neurology. 2020;94(21):e2222–e2232. doi: 10.1212/WNL.0000000000009475 Phase 2 dose-finding study in elderly patients with insomnia, supporting the 25 mg and 50 mg doses chosen for the Phase 3 program.
Kunz D, Dauvilliers Y, Benes H, et al. Long-term safety and tolerability of daridorexant in patients with insomnia disorder. CNS Drugs. 2023;37(1):93–106. doi: 10.1007/s40263-022-00980-8 Long-term (9-month) extension trial (Study 3) following Studies 1 and 2; supports 12-month tolerability with no evidence of physical dependence or rebound insomnia.
Fietze I, Bassetti CLA, Mayleben DW, et al. Efficacy and safety of daridorexant in older and younger adults with insomnia disorder: a secondary analysis of a randomised placebo-controlled trial. Drugs Aging. 2022;39(10):795–810. doi: 10.1007/s40266-022-00977-4 Pre-specified subgroup analysis of the pivotal trials in patients ≥65 years; supports preserved efficacy and tolerability in older adults at recommended doses.

Guidelines

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 daridorexant approval (January 2022) and therefore does not include a specific recommendation for it.
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.
Riemann D, Baglioni C, Bassetti C, et al. European guideline for the diagnosis and treatment of insomnia. J Sleep Res. 2017;26(6):675–700. doi: 10.1111/jsr.12594 European Sleep Research Society guideline; concordant with US recommendations on CBT-I as first-line therapy.

Mechanistic / Basic Science

Treiber A, de Kanter R, Roch C, et al. The use of physiology-based pharmacokinetic and pharmacodynamic modeling in the discovery of the dual orexin receptor antagonist ACT-541468. J Pharmacol Exp Ther. 2017;362(3):489–503. doi: 10.1124/jpet.117.241596 Discovery and PK/PD modelling paper for daridorexant (originally ACT-541468) — explains the rational selection of an ~8-hour half-life to minimise next-day residual effects.
Sakurai T. The neural circuit of orexin (hypocretin): maintaining sleep and wakefulness. Nat Rev Neurosci. 2007;8(3):171–181. doi: 10.1038/nrn2092 Foundational review of orexin signalling and its role in arousal — the conceptual basis for orexin antagonism as a hypnotic strategy.

Pharmacokinetics & Special Populations

Markham A. Daridorexant: first approval. Drugs. 2022;82(5):601–607. doi: 10.1007/s40265-022-01699-y Adis review summarising the regulatory development, pharmacology, and key clinical data supporting the 2022 FDA approval.
Muehlan C, Boehler M, Brooks S, Zuiker R, van Gerven J, Dingemanse J. Clinical pharmacology of the dual orexin receptor antagonist ACT-541468 in elderly subjects: exploration of pharmacokinetics, pharmacodynamics and tolerability following single-dose morning and repeated-dose evening administration. J Psychopharmacol. 2020;34(3):326–335. doi: 10.1177/0269881119882854 Phase 1 study characterising daridorexant pharmacokinetics, pharmacodynamics, and tolerability in healthy elderly subjects — informs the lack of formal dose adjustment for older adults in the current label.