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Hypnotic

From Wikipedia, the free encyclopedia
Drug whose use induces sleep
This article is about the class of prescription medicines. For the state of mind, seeHypnosis. For other uses, seeHypnotic (disambiguation).
"Sleeping pills" redirects here. For the 2003 film, seeSleeping Pills (film).
Hypnotic
Drug class
Zolpidem tablets, a common but potent hypnotic used for insomnia.
Class identifiers
SynonymsSedative; Somnifacient; Soporific; Sleeping pill; Sleep aid; Sedative–hypnotic; Hypnotica
UseInsomnia,hypersomnia,narcolepsy
Mechanism of actionVarious
Biological targetVarious
Chemical classVarious
Legal status
Legal status
  • Variable
In Wikidata

Ahypnotic (fromGreekHypnos, sleep[1]), also known as asomnifacient orsoporific, and commonly known assleeping pills, are a class ofpsychoactive drugs whose primary function is toinduce sleep[2] and to treatinsomnia (sleeplessness). Some hypnotics are also used to treatnarcolepsy andhypersomnia by improving sleep at night and thereby reducingdaytime sleepiness.[3][4] Certain hypnotics can be used to treatnon-restorative sleep and associated symptoms in conditions likefibromyalgia as well.[5][4][6][7]

This group of drugs is related tosedatives.Whereas the term sedative describes drugs that serve to calm orrelieve anxiety, the term hypnotic generally describes drugs whose main purpose is to initiate, sustain, or lengthen sleep. Because these two functions frequently overlap, and because drugs in this class generally produce dose-dependent effects (ranging fromanxiolysis toloss of consciousness), they are often referred to collectively assedative–hypnotic drugs.[8]

Hypnotic drugs are regularly prescribed for insomnia and other sleep disorders, with over 95% of insomnia patients being prescribed hypnotics in some countries.[9] Many hypnotic drugs are habit-forming and—due to many factors known to disturb the human sleep pattern—a physician may instead recommend changes in the environment before and during sleep, bettersleep hygiene, the avoidance of caffeine andalcohol or other stimulating substances, or behavioral interventions such ascognitive behavioral therapy for insomnia (CBT-I), before prescribing medication for sleep. When prescribed, hypnotic medication should be used for the shortest period of time necessary.[10]

Among individuals with sleep disorders, 13.7% are taking or prescribednonbenzodiazepines (Z-drugs), while 10.8% are takingbenzodiazepines, as of 2010, in the USA.[11] Early classes of drugs, such asbarbiturates, have fallen out of use in most practices but are still prescribed for some patients. In children, prescribing hypnotics is not currently acceptable—unless used to treatnight terrors orsleepwalking.[12] Elderly people are more sensitive to potential side effects of daytime fatigue andcognitive impairment, and ameta-analysis found that the risks generally outweigh any marginal benefits of hypnotics in the elderly.[13] A review of the literature regarding benzodiazepine hypnotics and Z-drugs concluded that these drugs have adverse effects, such asdependence and accidents, and that optimal treatment uses the lowest effective dose for the shortest therapeutic time, with gradual discontinuation to improve health without worsening of sleep.[14]

Falling outside the above-mentioned categories, the neurohormonemelatonin and its analogues (e.g.,ramelteon) serve a hypnotic function.[15]

Types

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GABAA receptor positive allosteric modulators

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Main article:GABAA receptor positive allosteric modulator

Benzodiazepines

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Main article:Benzodiazepine § Insomnia

Benzodiazepines can be useful for short-term treatment of insomnia. Their use beyond 2 to 4 weeks is not recommended due to the risk of dependence. It is preferred that benzodiazepines be taken intermittently and at the lowest effective dose. They improve sleep-related problems by shortening the time spent in bed before falling asleep, prolonging sleep time, and reducing wakefulness.[16][17] Likealcohol, benzodiazepines are commonly used to treat insomnia in the short-term (both prescribed and self-medicated), but worsen sleep in the long-term. While benzodiazepines can put people to sleep (i.e., inhibit NREM stage 1 and 2 sleep), while asleep, the drugs disruptsleep architecture by decreasing sleep time, delaying time to REM sleep, and decreasing deepslow-wave sleep (the most restorative part of sleep for both energy and mood).[18][19][20]

Other drawbacks of hypnotics, including benzodiazepines, are possibletolerance to their effects,rebound insomnia, and reduced slow-wave sleep and a withdrawal period typified by rebound insomnia and a prolonged period of anxiety and agitation.[21][22] The list of benzodiazepines approved for the treatment of insomnia is similar among most countries, but which benzodiazepines are officially designated as first-line hypnotics prescribed for the treatment of insomnia can vary distinctly between countries.[17] Longer-acting benzodiazepines, such asnitrazepam anddiazepam, have residual effects that may persist into the next day and are, in general, not recommended.[16]

It is not clear whether the newernonbenzodiazepine (Z-drug) hypnotics are better than the short-acting benzodiazepines. The efficacy of these two groups of medications is similar.[16][22] According to the USAgency for Healthcare Research and Quality, indirect comparison indicates that side effects from benzodiazepines may be about twice as frequent as from nonbenzodiazepines.[22] Some experts suggest using nonbenzodiazepines preferentially as a first-line long-term treatment of insomnia.[17] However, the UKNational Institute for Health and Clinical Excellence (NICE) did not find any convincing evidence in favor of Z-drugs. A NICE review pointed out that short-acting Z-drugs were inappropriately compared in clinical trials with long-acting benzodiazepines. There have been no trials comparing short-acting Z-drugs with appropriate doses of short-acting benzodiazepines. Based on this, NICE recommended choosing the hypnotic based on cost and the patient's preference.[16]

Older adults should not use benzodiazepines to treat insomnia unless other treatments have failed to be effective.[23] When benzodiazepines are used, patients, their caretakers, and their physician should discuss the increased risk of harms, including evidence which shows twice the incidence oftraffic collisions among driving patients, as well as falls and hip fracture for all older patients.[9][23]

Theirmechanism of action is primarily atGABAA receptors.[24]

Nonbenzodiazepines

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Main article:Nonbenzodiazepine

Nonbenzodiazepines (Z-drugs) are a class ofpsychoactive drugs that are "benzodiazepine-like" in nature. Nonbenzodiazepinepharmacodynamics are almost entirely the same as benzodiazepine drugs, and therefore entail similar benefits, side effects, and risks. Nonbenzodiazepines, however, have dissimilar or different chemical structures, and are unrelated to benzodiazepines on a molecular level.[25][26]

Examples includezopiclone (Imovane),eszopiclone (Lunesta),zaleplon (Sonata), andzolpidem (Ambien). Since the generic names of all drugs of this type start withZ, they are often referred to asZ-drugs.[27]

Research on nonbenzodiazepines is new and conflicting. A review by a team of researchers suggests the use of these drugs for people who have trouble falling asleep (but not staying asleep),[note 1] as next-day impairments were minimal.[28] The team noted that the safety of these drugs had been established, but called for more research into their long-term effectiveness in treating insomnia. Other evidence suggests thattolerance to nonbenzodiazepines may be slower to develop than with benzodiazepines.[failed verification] A different team was more skeptical, finding little benefit over benzodiazepines.[29]

Barbiturates

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Main article:Barbiturate

Barbiturates are drugs that act ascentral nervous systemdepressants, and can therefore produce a broad spectrum of effects, from mildsedation to totalanesthesia. They are also effective asanxiolytics, hypnotics, andanticonvulsant effects; however, these effects are somewhat weak, preventing barbiturates from being used insurgery in the absence of other analgesics. They have dependence liability, bothphysical andpsychological. Barbiturates have now largely been replaced bybenzodiazepines in routine medical practice – such as in the treatment of anxiety and insomnia – mainly because benzodiazepines are significantly less dangerous inoverdose. However, barbiturates are still used in general anesthesia, forepilepsy, and forassisted suicide. The principalmechanism of action of barbiturates is believed to bepositive allosteric modulation ofGABAA receptors.[30] Barbiturates are derivatives ofbarbituric acid. Examples includeamobarbital,pentobarbital,phenobarbital,secobarbital, andsodium thiopental.

Quinazolinones

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Main articles:Quinazolinone andMethaqualone

Quinazolinones are also a class of drugs that function as hypnotics/sedatives that contain a 4-quinazolinone core. Examples of quinazolinones includecloroqualone,diproqualone,etaqualone (Aolan, Athinazone, Ethinazone),mebroqualone,afloqualone (Arofuto),mecloqualone (Nubarene, Casfen), andmethaqualone (Quaalude). This class of drugs has been largely discontinued and is no longer used clinically.

Neurosteroids

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Main article:Neurosteroid

Oralprogesterone (Prometrium)metabolizes intoneurosteroids includingallopregnanolone andpregnanolone which act aspotent GABAA receptor positive allosteric modulators.[31][32][33] As a result, oral progesterone candose-dependently produceside effects includingdizziness,drowsiness,sedation,somnolence,fatigue,anxiety reduction,euphoria, andcognitive impairment.[34][35][36] For this reason, oral progesterone is often taken at night before bed.[37] Oral progesterone taken before bed has been found to improve multiple sleep outcomes in clinical studies.[38][39]Zuranolone is asyntheticanalogue of allopregnanolone that likewise acts as a GABAA receptor positive allosteric modulator but isorally active.[40] It is under development for the treatment of insomnia and is inphase 3clinical trials for this indication as of September 2025.[41][42]

Others

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See also:Sleep induction § Alcohol

Other GABAA receptor positive allosteric modulators with hypnotic effects includealcohol (ethanol),chloral hydrate,urethane (ethyl carbamate),isoflurane,allopregnanolone (brexanolone), andpropofol, among others.[43][44]

GABAA receptor agonists

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Main article:GABAA receptor agonist

TheGABAA receptoragonistgaboxadol (THIP; LU-2-030), asyntheticderivative of theneurotransmitterγ-aminobutyric acid (GABA) and ananalogue of thealkaloidmuscimol, underwent formal clinical development for the treatment ofinsomnia and reachedphase 3clinical trials for this indication in the 1990s and 2000s.[45][46][47] It was found to effectively improvesleep onset andduration in people withinsomnia.[45] In addition, and unlike other hypnotics likebenzodiazepines, gaboxadol improvedslow wave sleep, preservedsleep architecture, and did not suppressREM sleep.[45] Moreover, in contrast tobenzodiazepines,tolerance did not appear to develop to gaboxadol's hypnotic effects.[45]

The development of gaboxadol was discontinued in 2007.[47][48][49] This was due to high rates ofpsychiatric andhallucinogenic effects indrug users at supratherapeutic doses, failure of a 3-month efficacy trial, and other cited reasons.[47][48][50] Moreover, there was tension concerning hypnotics in thepharmaceutical industry at the time owing to bizarre reports ofzolpidem (Ambien)-induceddelirium that emerged in the media in 2006, which may have made the developer of gaboxadol more concerned about potential liability issues.[47] According to journalistHamilton Morris, the discontinuation of gaboxadol's late-stage development may have deprived people with insomnia access to an effective, safe, and non-addictive treatment.[47] There has been some further study of gaboxadol as a hypnotic byDavid Nutt and colleagues following the discontinuation of its development.[51][52]

Muscimol, the compound from which gaboxadol was derived, is anaturally occurring constituent ofAmanita mushrooms such asAmanita muscaria (fly agaric) and is apotent GABAA receptor agonist similarly.[53][54] However, muscimol is lessselective, moretoxic, and far less-researched than gaboxadol.[53][55][54][56] Muscimol is reported to inducesleep in humans in addition to its well-known hallucinogenic effects that occur at sufficiently high doses.[53][57] The drug shows similar effects on sleep in rodents as gaboxadol.[58][54][45] By the mid-2020s,microdosing of muscimol andAmanita mushrooms for claimed therapeutic benefits, the most prominently cited of which is improved sleep, has become increasingly prominent.[53][59][60]

GABAB receptor agonists

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TheGABAB receptoragonistsodium oxybate (SXB; Xyrem), also known asγ-hydroxybutyrate (GHB), has hypnotic and sleep-improving effects.[3][61][5] It robustly increasesslow wave sleep (deep sleep), decreasessleep fragmentation, and improvesrapid eye movement (REM) sleep consolidation, all whilst preserving physiologicalsleep architecture.[3][61][5][62] The drug is approved and clinically used in the treatment ofnarcolepsy andexcessive daytime sleepiness (EDS).[3][4] Narcolepsy is associated with poor sleep, and sodium oxybate improvessleep quality and stability in the condition, in turn reducing symptoms likedaytime sleepiness andcataplexy.[3][62] The robust enhancement of slow wave sleep by sodium oxybate is unusual and potentially advantageous relative to other hypnotics.[63][6][64] In addition, unlike the case of many other hypnotics,tolerance does not appear to develop to the hypnotic effects of sodium oxybate.[65][4]

Sodium oxybate also completed formal clinical development forfibromyalgia.[5][66] This condition has very high rates ofnon-restorative sleep (unrefreshing sleep) that may be directly involved in its symptoms.[67][68][6][69] Sodium oxybate improved sleep in fibromyalgia and showed moderate effectiveness in treating multiple symptoms across the condition includingpain andfatigue.[5] However, despite its effectiveness, sodium oxybate was ultimately not approved for treatment of fibromyalgia owing mostly to concerns about possiblemisuse.[5] Sodium oxybate has also been investigated and been of interest to improve sleep and associated symptoms in other conditions with sleep disruption, such asmyalgic encephalomyelitis/chronic fatigue syndrome (ME/CFS) andlong COVID, which also have high rates of non-restorative sleep.[4][69][67][70] In addition, sodium oxybate was limitedly studied to improveinsomnia in people withdepression orbipolar disorder.[4] However, it was reported to paradoxically disrupt sleep and induce narcolepsy-like changes in these individuals.[4] Moreover, concerns about misuse have limited use of sodium oxybate for other medical conditions.[71] GHB has also garnered a reputation as adate-rape drug, although the actual prevalence of this appears to be much lower than popular perception.[72]

The GABAB receptor agonistbaclofen has also been more limitedly investigated for improvement of sleep and has been found to be effective in enhancing sleep similarly to sodium oxybate.[69][73][74] However, in people with narcolepsy, baclofen and sodium oxybate both improved sleep but only sodium oxybate reduced daytime sleepiness.[74] In any case, research in this area is limited, and there remains significant interest in baclofen in the potential treatment of sleeping problems.[73][69] Unlike sodium oxybate, baclofen is not acontrolled substance and has much less or nomisuse potential.[74][75] Baclofen and sodium oxybate have been found to activate the GABAB receptor differently, which is thought to underlie the differences in their effects.[74] Another difference between baclofen and sodium oxybate is that baclofen has a much longerelimination half-life andduration of action in comparison (half-life 3–4 hours versus 0.5–1.0 hours, respectively).[73][76][75]

GABA reuptake inhibitors

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Main article:GABA reuptake inhibitor

TheGABA transporter 1 (GAT-1) andGABA reuptake inhibitortiagabine (Gabitril) is approved and clinically used as ananticonvulsant.[77] It has also been usedoff-label in the treatment ofanxiety disorders and other conditions.[78] The drug increasesγ-aminobutyric acid (GABA) levels in the brain and has been found to improve sleep, including by increasingslow wave sleep (deep sleep).[77][64] In addition, tiagabine has been reported to make sleep feel more restorative and to improve several cognitive outcomes.[77][64] The drug has anelimination half-life of 5 to 8 hours.[79]

Melatonin receptor agonists

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Main article:Melatonin receptor agonist

Melatonin, the hormone produced in thepineal gland in the brain and secreted in dim light and darkness, among its other functions, promotes sleep indiurnal mammals.[80] It activates themelatoninMT1 andMT2 receptors to produce beneficial effects on sleep, therefore being used exogenously for mild insomnia.[81] A small improvement in sleep onset and total sleep time by using melatonin has been shown in recent systematic reviews.[82]Syntheticanalogues of melatonin, ormelatonin receptor agonists, have also been made. Among these,ramelteon andtasimelteon are used for sleep disorders.Agomelatine is an antidepressant of this class, with some studies also reporting an effect on sleep.[83]

Histamine H1 receptor antagonists

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Main article:H1 antagonist

Antihistamines, also known ashistamineH1 receptorantagonists, are a class of drugs that inhibit action at histamine H1 receptors. They are clinically used to alleviate allergic reactions includingallergic rhinitis,allergic conjunctivitis, andurticaria, which are mediated byhistamine.[citation needed]First-generation antihistamines, such asdoxylamine (Unisom) anddiphenhydramine (Benadryl), often cause sedation as a side effect, which can be utilized to treat insomnia. Some antihistamines, such as doxylamine, are available for purchaseover-the-counter (OTC) in some countries and can be used for the occasional relief of insomnia.[84] Many sedating antihistamines also haveanticholinergic activity that can produceside effects likecognitive impairment.[85][86] Low-dosedoxepin (Silenor) is approved by the FDA for the treatment of insomnia.[87]Non-selective hypnotics that possess histamine H1 receptor antagonism include theantidepressantsamitriptyline, high-dosedoxepin,trazodone, andtrimipramine; theantipsychoticsolanzapine andquetiapine; and the antihistamineshydroxyzine,promethazine, andcyproheptadine, among others.[85][88][89][90]Second-generation antihistamines such ascetirizine andloratadine produce much less if any sedation due to a greatly reduced capacity to cross theblood–brain barrier.[91]

Orexin receptor antagonists

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Main article:Orexin antagonist

Orexin receptor antagonists are drugs that block theorexinOX1 and/orOX2 receptors, hence reducing thewakefulness-promoting effects of theorexin system and inducing sleep.[92]Non-selective orexin receptor antagonists includingsuvorexant,lemborexant, anddaridorexant andselective orexin OX2 receptor antagonists likeseltorexant have been shown inclinical studies to improvesleep onset,sleep duration, andsleep quality.[93][94][95]

Serotonin 5-HT2A receptor antagonists

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Serotonin5-HT2A receptorantagonists such asritanserin,ketanserin,eplivanserin,volinanserin,nelotanserin, andpimavanserin have been studied and developed to improve sleep.[96][97] They do not improvesleep onset, but have been found to increaseslow wave sleep (deep sleep) and reducenighttime awakenings.[96][97] Conversely, improvement in subjective sleep ratings have been more mixed.[96] Ultimately noselective serotonin 5-HT2A receptor antagonists have been approved for treatment ofinsomnia.[96] The only selective serotonin 5-HT2A receptor antagonist to be approved for any indication is pimavanserin for treatment ofParkinson's diseasepsychosis.[97] Besides selective serotonin 5-HT2A receptor antagonists however, many non-selective agents used as hypnotics show serotonin 5-HT2A receptor antagonism, for instanceantidepressants liketrazodone,mirtazapine, andamitriptyline,antipsychotics likequetiapine andolanzapine, andantihistamines likehydroxyzine andcyproheptadine.[98][99][100][88][86]

Gabapentinoids

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Main article:Gabapentinoid

Gabapentinoids, also known asα2δ subunit-containingvoltage-gated calcium channelligands, include drugs likegabapentin,pregabalin, andgabapentin enacarbil.[101] They have been found to increaseslow wave sleep (deep sleep) in people withinsomnia and healthy individuals.[102][99] However, they do not appear to improvesleep onset.[102] The gabapentinoidatagabalin (PD-0200390) was under formal development for treatment of insomnia, but development was discontinued following unsatisfactory clinical trial results.[102]PD-0299685 is another gabapentinoid that was under development for the treatment of insomnia, specifically that related tomenopausal symptoms, but its development was discontinued similarly.[103][104]

Cannabinoids

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Main articles:Cannabinoid andCannabis (drug)

Cannabinoids, orcannabinoid receptoragonists, such as theδ9-tetrahydrocannabinol (THC) found incannabis, have been found to be effective in improving sleep in healthy people and in people withinsomnia.[105][106] They have been found to improvesleep onset,sleep duration, andsleep quality.[105][106]Cannabidiol (CBD), which acts differently than other cannabinoids like THC, is not effective in improving sleep on the other hand.[105]Zenivol is acannabis extract which is approved for the treatment of insomnia inGermany.[107][106]

α1- and β-adrenergic receptor antagonists

[edit]
Main articles:Alpha-1 blocker andBeta blocker

Theα1-adrenergic receptorantagonistprazosin is usedoff-label to treatinsomnia,nightmares, and poorsleep quality in people withpost-traumatic stress disorder (PTSD).[108][109][110][111] It is clinically effective for this purpose.[109][110][111] However, the drug is also anantihypertensive agent and can lowerblood pressure, thereby producingside effects likedizziness andorthostatic hypotension.[108] Certainnon-selective hypnotics such astrazodone andtricyclic antidepressants (TCAs) likeamitriptyline andtrimipramine are also α1-adrenergic receptor antagonists.[102][112][113] The combination of prazosin and thecentrally-penetrantbeta blocker (β-adrenergic receptor antagonist)timolol has been found to be synergistic in producing sedative and hypnotic effects in animals.[102][114] Conversely, timolol alone produced no such effects.[102][114] Centrally active beta blockers likepropranolol andmetoprolol on their own are not effective or clinically used as hypnotics and have actually been associated with insomnia as a side effect.[115][116][117] Certain beta blockers likelabetalol andcarvedilol also block the α1-adrenergic receptor to varying extents and have been associated withsomnolence as a side effect.[88][118][119] However, these two beta blockers have also been associated with insomnia similarly to selective beta blockers.[88]

α2-Adrenergic receptor agonists

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α2-Adrenergic receptoragonists likeclonidine can improve sleep and may be useful in the treatment of insomnia.[102][120][121] An example of this is in the treatment of insomnia in children and adolescents withattention deficit hyperactivity disorder (ADHD), for instance duestimulant therapy.[120][121][122] Similarly to clonidine, the α2-adrenergic receptor agonistdexmedetomidine has sedative and hypnotic effects and is used to producesedation in hospital settings.[123] The sleep induced by dexmedetomidine is said to closely resemble natural sleep.[123][124][125] Theselectiveα2A-adrenergic receptor agonisttasipimidine (ODM-105) is under development for the treatment of insomnia and is inphase 2clinical trials for this indication as of October 2024.[126][127] α2-Adrenergic receptor agonists can producehypotension andbradycardia asside effects, which has limited their use.[128][123] Activation of the α2A-adrenergic receptor is thought to be responsible for most of the physiological effects of the α2-adrenergic receptors, including hypotension.[126] On the other hand, the preferential α2A-adrenergic receptor agonistguanfacine appears to show less sedation and hypotension than clonidine.[129]

Serotonin precursors

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Theserotonin precursorstryptophan and5-hydroxytryptophan (5-HTP; oxitriptan) are available asover-the-countersupplements.[130][131] They are often used to producesleepiness and treatinsomnia.[130][131] However, little to no clinical data exist to support their use or effectiveness.[130]

Multiple mechanisms

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Antidepressants

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Someantidepressants have hypnotic and/or sedative effects.[102] These include theserotonin antagonist and reuptake inhibitor (SARI)trazodone,[132]tricyclic antidepressants (TCAs) such asamitriptyline,[133]doxepin,[134] andtrimipramine,[135] andtetracyclic antidepressants (TeCAs) likemirtazapine[136][137] andmianserin.[138][102] These agents produce their hypnotic and sedative effects via multiplemechanisms of action that may includehistamineH1 receptorantagonism,serotonin5-HT2A receptor antagonism, andα1-adrenergic receptor antagonism.[102] Some hypnotic antidepressants, such as trazodone and mirtazapine, have been shown to enhanceslow wave sleep, which may be due to serotonin 5-HT2A receptor antagonism.[77]

Antipsychotics

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Certaintypical antipsychotics (first-generation) likechlorpromazine andatypical antipsychotics (second-generation) includingclozapine,olanzapine,quetiapine,risperidone,ziprasidone, andzotepine may have sedative and/or hypnotic effects and have been used in the treatment of insomnia.[139][140] However, the most commonly used agents for insomnia are quetiapine and olanzapine.[102][141] They are thought to produce these effects via multiplemechanisms of action, includinghistamineH1 receptorantagonism,serotonin5-HT2A receptor antagonism,α1-adrenergic receptor antagonism, and/ordopamineD2 receptor antagonism.[102][139] While some of these drugs are frequently prescribed for insomnia, such use is not recommended unless the insomnia is due to an underlying mental health condition treatable byantipsychotics as the risks frequently outweigh the benefits.[142][143] Some of the more serious adverse effects have been observed to occur at the low doses used for this off-label prescribing, such asdyslipidemia andneutropenia,[144][145][146][147] and a recent network meta-analysis of 154 double-blind, randomized controlled trials of drug therapies vs. placebo for insomnia in adults found that quetiapine had not demonstrated any short-term benefits in sleep quality.[148]

Herbal supplements

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Someherbalsupplements, includingvalerian,kava,chamomile,lavender,passion flower, andhops among others, are purported to have hypnotic effects and are used to treat sleeping problems, but little to no clinical data are available to support their use.[149][150][151][130][152]

Other drugs

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Various other types of drugs have also been found to produce hypnotic-type effects inscientific research.[102] Examples includehistamineH3 receptoragonists likeα-methylhistamine,BP 2.94,GT-2203 (VUF-5296), andSCH-50971,[153]adenosineA1 andA2A receptor agonists likeadenosine andYZG-331,[154][102][155] anddopamineD1 receptorreceptor antagonists likeNNC 01-0687 (ADX-10061, CEE-03-310, NNC-687).[156][157]

Comparative effectiveness

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A majorsystematic review andnetwork meta-analysis of medications for the treatment ofinsomnia was published in 2022.[94] It found a widely varying range ofeffect sizes (standardized mean difference or SMD) in terms ofclinical effectiveness for insomnia.[94] The assessed medications and their effect sizes includedbenzodiazepines (e.g.,temazepam,triazolam, many others) (SMDs 0.58 to 0.83),Z-drugs (eszopiclone,zaleplon,zolpidem,zopiclone) (SMDs 0.03 to 0.63), sedativeantidepressants andantihistamines (doxepin,doxylamine,trazodone,trimipramine) (SMDs 0.30 to 0.55), theantipsychoticquetiapine (SMD 0.07),orexin receptor antagonists (daridorexant,lemborexant,seltorexant,suvorexant) (SMDs 0.23 to 0.44), andmelatonin receptor agonists (melatonin,ramelteon) (SMDs 0.00 to 0.13).[94] Thecertainty of evidence varied and ranged from high to very low depending on the medication.[94] Certain medications often used as hypnotics, including the antihistaminesdiphenhydramine,hydroxyzine, andpromethazine and the antidepressantsamitriptyline andmirtazapine among others, were not included in analyses due to insufficient data.[94]

Risks

[edit]

The use of sedative medications in older people generally should be avoided. These medications are associated with poorer health outcomes, includingcognitive decline,fall, andbone fractures.[158] Sedatives and hypnotics should also be avoided in people withdementia, according to the clinical guidelines known as theMedication Appropriateness Tool for Comorbid Health Conditions in Dementia (MATCH-D).[159] The use of these medications can further impede cognitive function for people with dementia, who are also more sensitive to side effects of medications.[citation needed] Some hypnotics, such as low-dosedoxepin,melatonin receptor agonists, andorexin receptor antagonists, may be safer and more appropriate in older adults however.[160]

History

[edit]
Le VieuxSéducteur byCharles Motte [fr].
(A corrupt old man tries to seduce a woman by urging her to take a hypnotic draught in her drink)

Hypnotica was a class of somniferous drugs and substances tested in medicine of the 1890s and later. These includeurethan,acetal,methylal,sulfonal,paraldehyde,amylenhydrate,hypnon, chloralurethan, ohloralamid, or chloralimid.[161]

Research about using medications to treat insomnia evolved throughout the last half of the 20th century. Treatment for insomnia in psychiatry dates back to 1869, whenchloral hydrate was first used as a soporific.[162]Barbiturates emerged as the first class of drugs in the early 1900s,[163] after which chemical substitution allowed derivative compounds. Although they were the best drug family at the time (with less toxicity and fewer side effects), they were dangerous inoverdose and tended to cause physical and psychological dependence.[164][165][166]

During the 1970s,quinazolinones[167] andbenzodiazepines were introduced as safer alternatives to replace barbiturates; by the late 1970s, benzodiazepines emerged as the safer drug.[162]

Benzodiazepines are not without their drawbacks;substance dependence is possible, and deaths from overdoses sometimes occur, especially in combination withalcohol or otherdepressants. Questions have been raised as to whether they disturb sleep architecture.[168]

Nonbenzodiazepines or Z-drugs likezolpidem were introduced in the 1990s and 2000s. Although it is clear that they are less toxic than barbiturates, their predecessors, comparative efficacy over benzodiazepines has not been established. Such efficacy is hard to determine withoutlongitudinal studies. However, some psychiatrists recommend these drugs, citing research suggesting they are equally potent with less potential for abuse.[25]

Orexin receptor antagonists likesuvorexant were introduced in the 2010s and 2020s.[169]

See also

[edit]

Notes

[edit]
  1. ^Because the drugs have a shorterelimination half life they are metabolized more quickly: nonbenzodiazepines zaleplon and zolpidem have a half-life of 1 and 2 hours (respectively); for comparison, the benzodiazepine clonazepam has a half-life of about 30 hours. This makes the drug suitable for sleep-onset difficulty, but the team noted sustained sleep efficacy was unclear.

References

[edit]
  1. ^"Definition of HYPNOTIC".www.merriam-webster.com. Retrieved2021-09-27.
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Look uphypnotic in Wiktionary, the free dictionary.
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