Abstract
Parasomnias are abnormal behaviors and/or experiences emanating from or associated with sleep typically manifesting as motor movements of varying semiology. We discuss mainly nonrapid eye movement sleep and related parasomnias in this article. Sleepwalking (SW), sleep terrors (ST), confusional arousals, and related disorders result from an incomplete dissociation of wakefulness from nonrapid eye movement (NREM) sleep. Conditions that provoke repeated cortical arousals, and/or promote sleep inertia, lead to NREM parasomnias by impairing normal arousal mechanisms. Changes in the cyclic alternating pattern, a biomarker of arousal instability in NREM sleep, are noted in sleepwalking disorders. Sleep-related eating disorder (SRED) is characterized by a disruption of the nocturnal fast with episodes of feeding after arousal from sleep. SRED is often associated with the use of sedative–hypnotic medications, in particular the widely prescribed benzodiazepine receptor agonists. Compelling evidence suggests that nocturnal eating may in some cases be another nonmotor manifestation of Restless Legs Syndrome (RLS). Initial management should focus upon decreasing the potential for sleep-related injury followed by treating comorbid sleep disorders and eliminating incriminating drugs. Sexsomnia is a subtype of disorders of arousal, where sexual behavior emerges from partial arousal from nonREM sleep. Overlap parasomnia disorders consist of abnormal sleep-related behavior both in nonREM and REM sleep. Status dissociatus is referred to as a breakdown of the sleep architecture where an admixture of various sleep state markers is seen without any specific demarcation. Benzodiazepine therapy can be effective in controlling SW, ST, and sexsomnia, but not SRED. Paroxetine has been reported to provide benefit in some cases of ST. Topiramate, pramipexole, and sertraline can be effective in SRED. Pharmacotherapy for other parasomnias continues to be less certain, necessitating further investigation. NREM parasomnias may resolve spontaneously but require a review of priming and predisposing factors.
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Classification of parasomnias
Parasomnias are typically classified by the sleep state out of which they arise, nonrapid eye movement sleep (NREM) and rapid eye movement sleep (REM). We will focus mainly on NREM and related parasomnias in our discussion. (see Table 1) [1].
NREM parasomnias include disorders of arousal: confusional arousals, sleepwalking, and sleep terrors. These behaviors emerge when the cortex incompletely arouses from deep NREM sleep often due to comorbid conditions that provoke repeated arousal and/or promote sleep inertia. Changes in the cyclic alternating pattern, a biomarker of arousal instability in NREM sleep, are noted in sleepwalking and related disorders [2].
Sleep-related eating disorder, currently classified in the International Classification of Sleep Disorders 3nd revision (ICSD-3) under nonREM parasomnia [1], is considered a subtype of SW.
Parasomnia overlap disorder, a combination of disorders of arousal and RBD, and status dissociatus, which are less commonly encountered among the parasomnia patient population, are currently classified as variants of RBD [1].
NREM Parasomnias
Disorders of Arousal
NREM sleep parasomnias are characterized by abnormal nocturnal behavior, impaired consciousness, and autonomic nervous system activation due to impaired arousal. This group of parasomnias, which is comprised of confusional arousal, sleepwalking, and sleep terror, is characterized by similar familial patterns and pathophysiological mechanisms. They typically arise from slow-wave (N3) NREM sleep [1]. Distinguishing features include duration, complexity, and type of behavior as well as degree of amnesia. Precipitating factors include conditions that result in either sleep fragmentation (noise), increased homeostatic sleep pressure (sedatives, sleep deprivations), or both (obstructive sleep apnea) (see Table 2) [1].
General criteria of disorders of arousal are listed in Table 3.
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1.
Confusional arousals (CoA) are characterized by disoriented behavior during arousal from NREM sleep, often with vocalizations and poor recall of events the following day. While typically lasting less than 5 min, episodes can occasionally last up to an hour. These prolonged episodes most commonly occur in the setting of polyneuropharmacy, in particular sedative–hypnotics. The behavior is typically benign however occasionally the patient can become aggressive and violent [1]. Diagnostic criteria are listed in Table 4.
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2.
Sleepwalking (SW) is the combination of ambulation with the persistence of impaired consciousness following arousal from sleep. Patients typically have amnesia and the behaviors are inappropriate, such as placing car keys in the refrigerator or rearranging furniture to nonfunctional locations. Attempting to arouse the patient is often difficult and may paradoxically worsen confusion and disorientation [1]. Table 5 enumerates the diagnostic criteria.
SW can become prolonged and/or dangerous. Alarming reports have described leaving the house, automobile driving, and sometimes discharge of loaded firearms. Similar to CoA, prolonged SW behaviors have been associated with sedative–hypnotic medications, in particular the benzodiazepine receptor agonists; however, unlike CoA, SW frequently occurs in the setting of Restless Legs Syndrome (see pathophysiology below).
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3.
Sleep terrors (ST) are episodes of intense fear initiated by a sudden cry or loud scream accompanied by increased autonomic nervous system activity. Most commonly, ST occur in preadolescent children. Parents often describe the patient as being inconsolable during events. In adults, ST can involve impulsively bolting out of bed without proper judgment in response to an imminent threatening image or dream fragment [1]. In such a clinical scenario, they likely also constitute SW. Severe injury or even death may result from leaping out of bed or jumping through a window. ST can last for greater than 5 min and attempts to abort an episode frequently result in even greater agitation. The criteria for ST are listed in Table 6.
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4.
Sexsomnia, considered a subtype of confusional arousal, is characterized by recurrent amnestic sexual behavior ranging from masturbation to sexual intercourse [3, 4]. This category was formally described in 2007 with further updates and exploration in 2015 [5, 6]. The abnormal sexual activity occurs in slow-wave sleep or N3 akin to other NREM parasomnias. Studies have demonstrated male gender predilection. Evidence of treatment is limited in the literature, but clonazepam has shown benefit with some mixed results due to difficulty tolerating the drug [7]. Fluoxetine and trimipramine also provided relief in few cases [7]. The cases with coexistent OSA responded to treatment with CPAP or mandibular advancement device. The amnestic sexual behavior can result in relationship strife with potential forensic consequences (for extensive review, see [3–5].
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5.
Another variation is sleep-related eating disorder (see below), manifesting with dysfunctional nocturnal eating often leading to weight gain. Interestingly, nocturnal eating is a common nonmotor manifestation of RLS [8, 9] and the misdiagnosis and treatment of RLS as insomnia (with sedative–hypnotics) frequently leads to amnestic sleep-related eating disorder [8]. Diagnostic criteria are listed in Table 7.
Clinical Presentation
Although NREM parasomnias peak in childhood, they are not uncommon in adults with a prevalence range between 1 and 4% [1, 10]. NREM parasomnia behaviors occur on a spectrum in terms of duration, autonomic activity, and impaired arousal. CoA are frequently of shorter duration compared to SW or ST. Prolonged (> 60 min) episodes have been associated with sedative–hypnotic medications [11]. Regarding autonomic function, CoA and SW have less autonomic activation compared to ST, which are characterized by increased HR, tachypnea, diaphoresis, and facial flushing. While all of the NREM parasomnias have impaired arousal, attempts to wake a patient from a ST often result in a paradoxical increase in agitation. NREM parasomnia patients are at least partially amnestic for nocturnal behaviors. Children with ST will not recall the dramatic events often to the bewilderment of concerned parents who witness the experiences [1]. Some of the clinical features are listed in Table 8.
Obstructive sleep apnea (OSA) and RLS are the most commonly identified precipitating factors in patients with SW [11, 12]. Other conditions that are associated with NREM parasomnias are also characterized by sleep fragmentation and/or increased homeostatic sleep pressure including the following: shift work, sedatives, environmental sleep disruption, and Periodic Limb Movements (PLMs) [13, 14].
Parasomnias are notoriously common in patients on sedative–hypnotic medications. One group of investigators noted a high frequency of SW and other amnestic complex behaviors among psychiatric patients who took benzodiazepine receptor agonist (BRA) medication [15]. These findings are consistent with other reports of abnormal nocturnal behavior induced by BRAs, in particular zolpidem [11, 16, 17]. In the setting of BRA induced parasomnias, the behaviors are often prolonged and can include amnestic nocturnal eating (SRED), sexual activity (sexsomnia), and sleep driving. These complex amnestic behaviors frequently occurred in the setting of CNS polypharmacy or supratherapeutic doses. Not unexpectedly there has been an increase in sleep-associated amnestic complex behavior in parallel to the contemporary rise in use of sedative–hypnotic medication [11] which ultimately led to inclusion of a black box warning by FDA in 2019 for careful monitoring and discontinuation of these agents in patients who experience a parasomnia after taking them.
Intriguingly many cases of BRA induced SW are noted to have comorbid RLS which could be easily misdiagnosed and treated as insomnia [8, 11]. Then, not surprisingly, BRAs, whose mechanism of action, with suppression of memory along with executive function, unleashes prolonged amnestic ambulating events by disinhibiting hippocampal and frontal lobe function [8, 11].
SW has also been associated with a variety of other medications and medical conditions. Implicated agents have included: central nervous system depressant sodium oxybate [18], antidepressants amitriptyline [19], buproprion [20], paroxetine [21], and mirtazapine [22], the mood stabilizer lithium [23], antipsychotics quetiapine [24], and olanzapine [25, 26], the antihypertensive agent metoprolol [27], the antiseizure agent topiramate [28], and the antibiotic fluoroquinolone [29]. Medical conditions associated with NREM parasomnias include: migraine [30], febrile illness [31], vitiligo [32], hyperthyroidism [33], as well as encephalitis and Stroke [1]. These diverse conditions and medications likely induce NREM parasomnias through a final common pathway. The exact mechanism of that pathway has not yet been determined. One interesting possible explanation, i.e. the serotonin hypothesis, will be described later.
Pathophysiology
SW and related disorders occur when there is an incomplete dissociation of NREM sleep into wakefulness. Two pathological processes may lead to this sleep–wake boundary dysfunction (see Table 2). First, phenomena that deepen sleep and enhance sleep inertia promote NREM parasomnias by impairing otherwise normal arousal mechanisms. Second, conditions that cause repeated cortical arousals lead to NREM parasomnias through sleep fragmentation. These abnormal arousals are often associated with the normal alternating arousal microstructure of NREM sleep, the cyclic alternating pattern (CAP) [2]. The complex amnestic behaviors that characterize these conditions are related to central pattern generators [34]. The isolated activation of these functional groups of motor neurons with a relative paucity of activity in brain regions that control executive function and memory account for the poor judgment and amnesia that characterize NREM parasomnias.
In the normal transition from light NREM sleep to wakefulness, consciousness emerges quickly, typically within seconds. The duration of normal arousal depends upon an intricate combination of variables including the following: duration of prior wakefulness, current sleep duration, depth of NREM sleep, circadian rhythm phase, effects of sedating or stimulating medications, as well as multiple genetic and environmental factors. Stimuli of endogenous and exogenous origins activate neurons in the brainstem and the basal forebrain. These regions subsequently promote wakefulness through both direct activation of the cerebral cortex and by inhibiting thalamic reticular neurons, thus blocking spindle oscillations. These alerting phenomena lead to suppression of slow wave activity (SWA) and more predominant fast cortical activity appears compatible with wakefulness [35].
The speed of the conversion from NREM sleep to wakefulness depends upon the intensity of SWA. Most arousals into wakefulness arise from lighter stages (N1 or N2) of sleep with minimal SWA. The threshold for which stimulation is required to produce an awakening during light sleep is low. By comparison, the threshold for an awakening from deep NREM sleep (N3), characterized by nearly continuous SWA, is high and awakenings are typically prolonged [36]. Subsequently, sleep inertia during N3 sleep arousals is strong (subjectively referred to as “sleep drunkenness”) and promotes a return to somnolence.
In NREM parasomnias, impaired arousal mechanisms and the persistence of sleep drive result in a failure of the brain to fully transition into wakefulness. Indeed, most SW and related disorders arise out of N3 sleep. Thus, sleep-promoting conditions such as sleep deprivation and sedative–hypnotic medication will lead to NREM parasomnias.
Conversely, disorders that lead to fragmented NREM sleep precipitate SW and other disorders of arousal by increasing arousal frequency. OSA, noise, and orexin dysfunction (cause of sleep instability in narcolepsy) all promote parasomnias by fragmenting NREM sleep. In fact, CoA can be precipitated in the sleep laboratory through sleep deprivation (which promotes SWA) combined with a sudden loud noise (see management below) [14].
The chronic intermittent airway collapse in patients with OSA leads to NREM parasomnias through parallel mechanisms, sleep fragmentation as well as increased homeostatic sleep drive [2, 12, 33, 37].
Combinations of predisposing and precipitating factors frequently lead to SW. For example, CNS polypharmacy is often the setting for dangerous behavior such as sleep driving [33, 38]. Other examples include patients with OSA, who are prescribed sedative–hypnotic medication to assist with continuous positive airway pressure (CPAP) compliance. A similar situation often in patients with RLS misdiagnosed as having insomnia and subsequently treated with a BRA. As patients with RLS have a strong subconscious drive to ambulate, it is not unexpected that agents which suppress memory and executive function would lead to amnestic sleepwalking behaviors [8, 33].
A genetic component has also been suggested, supported by studies demonstrating high prevalence. of human leukocyte antigen (HLA) DQB1*05:01 and HLA DQB1*04 alleles in various nonREM parasomnias [13].
Sleep Microarchitecture in NREM Parasomnias and the Cyclic Alternating Pattern
In patients with nonREM parasomnia, evaluation of sleep demonstrated either normal distribution of NREM sleep and its individual sleep stages [39, 40] or slightly decreased N2 and higher N3 (slow wave) sleep [41] .
However, the microstructure of sleep in patients with NREM parasomnias often demonstrates several interesting findings. Commonly there is an increase in arousals, either related to PLMs, respiratory events or spontaneously [41, 42]. Autonomic activation, as measured by heart rate variability, precedes cortical and behavioral arousals [43]. Further, the density of slow-wave activity (SWA) during the early sleep cycles is relatively decreased compared to controls [2, 44]. However, immediately preceding a confusional arousal, there is frequently an increase in SWA, commonly referred to as hypersynchronous delta (HSD) [41, 45]. The cyclic alternating pattern (CAP), a marker of NREM instability provides insight into these phenomena [46] (see below). Immediately after arousal, there is typically a persistent slowing of brain activity as measured by surface EEG [40, 47].
The CAP is an intrinsic oscillation throughout NREM sleep between periods of cortical arousal and quiescence throughout NREM sleep. This oscillation typically occurs every 20 to 40 s and provides the scaffolding for normal (such as K complexes and delta bursts) as well as pathological NREM phenomena (CA and SW events) [46]. SW/ST patients have an increased number of CAP cycles and a higher CAP rate, which is a measure of NREM instability [2, 39, 48]. Further, a subtype of cortical arousal in the CAP (phase A1) is characterized by hypersynchronous delta activity (HSD) and the majority of reports indicate SW, ST, and CoA are often preceded by a phase A1 run of HSD, indicating that these events are linked to the CAP [41, 45]. Finally, it has been proposed that the CAP may be used as a biomarker for treatment response. In particular, resolution of CAP abnormalities in patients who are being treated for sleep disordered breathing is associated with a resolution of SW behaviors [46].
The increase in CAP activity noted in parasomnias (increased type A1 arousals and increased CAP rate) indicates underlying NREM instability. Thus, abnormal CAP activity is likely not the cause of parasomnias but rather a marker of a sleep destabilizing process. Candidate processes include neuropsychiatric disease, medications, subtle respiratory events, as well as innate genetic factors. In fact PLM’s are also plausibly not directly causal to sleep instability but instead are a manifestation of unstable CAP [34]. These insights suggest that treatment of NREM parasomnias should be directed at resolving underlying sleep destabilizing processes and that the CAP changes (decrease in CAP rate and number of A1 events) may be used as a marker of treatment response.
Intracranial monitoring and neuroimaging in NREM parasomnia patients have indicated that the slowing of cortical activity after arousal is not diffusely distributed and that certain regions may become more activated/wake-like and coexist with regions that are in slow/NREM sleep-like activity. One report captured confusional arousal in a 20-year-old male who was undergoing intracerebral EEG monitoring for refractory epilepsy. The cingulate and motor cortices demonstrated an arousal followed by brain waves consistent with wakefulness while in parallel the fronto-parietal associative cortices had increased delta activity consistent with deep NREM sleep [49]. These findings were very similar to a SW event that was captured in a 16 yo male with cranial single photon emission computed tomography. In this case, the parasomnia was characterized by activation (increased regional cerebral blood flow) of motor coordination pathways with a relative paucity of activation in the frontal lobe [50].
Central Pattern Generators and their Role in Parasomnias
The behaviors that characterize parasomnias span a broad range from inaudible vocalizations to complex behaviors. It has been noted that these automatisms often resemble stereotyped behavior noted in other primates as well as more genetically distant mammalian and reptilian species [51]. In fact nocturnal subconscious behavior frequently resembles “primitive” activity such as: defensive postures, violent gestures, and sexual movement [34, 52]. The presence of similar behaviors among animal groups with distant common ancestors suggests that they arise from shared brain structures, in particular subcortical regions, including the brainstem and spinal cord.
A unifying concept, the central pattern generators (CPG’s), explains this spectrum of activity. CPGs are functional groups of neurons that give rise to subconscious patterns of motor activity.
CPGs require a certain amount of activation or disinhibition to generate stereotyped or quasi-stereotyped motor activity. This has been elegantly described as the facilitation of a “kinetic melody” [34]. During NREM parasomnias, intrinsic activation of an encoded motor plan occurs during the cortical arousal phase of the CAP (see above) [34]. Thus, any process, such as sleep apnea, that leads to NREM instability promotes more frequent CPG behavioral activation. External stimuli, such as a sudden noise can also promote activation of CPGs and in fact this technique is used to clinically induce SW and CoA (see management below).
Furthermore, during NREM parasomnias CPGs are activated in isolation from other brain structures that are important for normal wakeful behavior. In particular, imaging studies have revealed a paucity of activation in the dorsal lateral frontal cortex and hippocampal structures during NREM sleep [53]. Thus, with sudden arousals, the motor activity of SW (an expression of CPG activation) occurs in parallel with poor executive function and amnesia.
Importantly, by further impairing frontal lobe function, CPG behaviors are amplified in the setting of sedative–hypnotic medication. This occurs through enhancement of GABAa activity and is related to dose and binding affinity [33]. By hindering cortical arousal, sedative–hypnotics impede the conscious, executive, “brake” on CPG behavior. Thus, elaborate inappropriate behaviors emerge as brain regions that encode motor behaviors are activated in parallel to frontal lobe inhibition. This is particularly relevant in the setting of pathological predisposed behaviors, such as the urge to ambulate in patients with RLS.
Serotonin Theory of Parasomnias
While the molecular pathophysiology of NREM parasomnias is poorly understood there is evidence that serotonergic pathways may be implicated [54]. First, serotonergic agents have been known to induce SW [23, 31] but conversely, these agents can also effectively treat other parasomnias, most notably ST [55]. Second, serotonin provides activation to motor neurons [56, 57]. Third, this motor activity may be dissociated from consciousness [54]. Fourth, serotonin activity is a plausible link between sleep disordered breathing and parasomnias as serotonin neurons are activated by hypercapnic acidosis [54, 57]. Fifth, disorders associated with SW such as migraine [30] and fever [31], are characterized by surges of serotonin [54]. It has thus been suggested that serotonergic neurons, activated by nocturnal respiratory events, may pathologically trigger CPG’s resulting in sleep-related motor activity [54]. This is an intriguing hypothesis; however, further research is needed and any explanation should account for the discrepancy in the treatment between parasomnias.
Alternative Theory of Sleep Terrors
ST, while superficially similar to CoA and SW (in regard to abrupt arousal from SWS), may nevertheless originate in part from a distinctive neurophysiologic mechanism. In particular, it has been suggested that instead of an overlap between NREM and wakefulness as implicated in other NREM parasomnias, ST may represent a disorder of transition between deep NREM sleep (N3) and REM sleep. This theory would explain several unique features of ST: the high autonomic activity and the apparent vivid mentation (both from REM) combined with difficult arousability (from N3). Further, REM–NREM overlap may also explain the striking preponderance of ST in childhood as children have a greater proportion of both N3 and REM sleep. Intriguingly, the antidepressant medication paroxetine, an agent that can both induce SW [21] and treat ST [55], is a potent REM suppressor. Thus, if ST were due to pathological REM/NREM overlap, it would be expected that paroxetine would block these phenomena. Conversely, paroxetine would not be expected to have a therapeutic effect on SW, a wake/NREM phenomena. However, based on paroxetine’s serotonergic effects it would be expected to potentially worsen SW [54] (see serotonin theory of parasomnias above).
Sleep-Related Eating Disorder
Under normal human physiological conditions, nighttime is characterized by a prolonged period of fasting associated with sleep. Energy homeostasis is maintained through the sleep period by alterations in metabolism and appetite modulation. This stands in contrast to fasting during sedentary wakefulness which demonstrates progressive hypoglycemia over 12 h. The sleep-related fast is disrupted in SRED, characterized by recurrent episodes of nocturnal eating after arousal with adverse consequences. The episodes are described as occurring in an involuntary, compulsive, or “out of control manner”. Often, patients describe an inability to return to sleep without eating and in this regard resemble other nocturnal compulsions that interfere with sleep such as restless legs syndrome (RLS). Amnestic SRED, like SW, is often related to sedative–hypnotic medication use, most commonly zolpidem. These cases are often characterized by prolonged episodes with elaborate and sometimes dangerous food preparation [16, 33, 58, 59].
Clinical Presentation
SRED is common (4–5% prevalence) particularly among patients with other sleep disorders [8, 44, 60]. The most striking relationship is between SRED and RLS where both eating and motor symptoms frequently coexist and fluctuate in parallel. In a survey of 88 RLS patients who presented to a sleep disorder center, 61% had frequent nocturnal eating (NE) and 36% had SRED [8]. These findings are similar to a survey of 100 RLS patients who demonstrated a 33% prevalence of SRED [44]. Further, the mistreatment of RLS with benzodiazepine receptor agonists frequently induces amnestic SRED [40]. In contrast, dopaminergic therapy resolves NE and SRED in parallel with motor restlessness [6, 44] (see the relationship between SRED and RLS below).
At night SRED patients consume foods higher in carbohydrates and fats than typical daytime ingestion [61]. Weight gain is commonly reported [1, 62]. The majority of patients describe chronic unrelenting daily symptoms that may persist for decades prior to pursuing treatment [62]. Nearly a quarter of SRED patients will experience greater than 5 episodes of nocturnal food ingestion [61]. The majority (60–83%) of reported SRED cases are female and frequently coexists with daytime eating disorders [60–62].
Amnestic SRED, although common in many SRED cases, is especially common in the setting of sedative–hypnotic medications, in particular the benzodiazepine receptor agonists [8, 15, 16, 62]. These unconscious episodes may include nonfood ingestions such as cigarettes, coffee grounds, or eggshells. Other patients will ingest substances they would otherwise avoid, such as patients with food allergies, diabetes, hyperlipidemia, or undergoing general anesthesia the next day [46, 63]. Patients may fall asleep with an oral bolus of food, which combined with the circadian decline in salivation places the patient at high risk of dental caries [46]. Finally, food preparation can include using the stove and/or oven in a haphazard manner increasing the risk for fires [46, 63].
SRED is usually associated with SW. Three series have reported comorbid SW in 48 to 65% of patients with SRED. SW without eating may precede SRED and then once nocturnal eating develops, it may become the predominant SW behavior [15, 62].
Pathophysiology
SRED and Benzodiazepine Receptor Agonists
Several early reports noted that amnestic nocturnal eating was associated with sedating psychotropic medications. A 1981 case report described amnestic nocturnal eating after initiating a combination of chlorpromazine, amitriptyline, and methyprylon [64]. Subsequently, SRED has been reportedly induced with triazolam, lithium, olanzapine, risperidone, zopiclone, and zaleplon [25, 46, 65, 66] as well as zolpidem extended-release formulation [67].
The majority of drug cases are related to zolpidem, a benzodiazepine receptor agonist. The first series of zolpidem associated SRED described five middle-aged patients, two of whom already had intermittent episodes of conscious nocturnal eating prior to starting zolpidem. Interestingly all 5 had a history of RLS. Soon after initiating zolpidem, each patient described amnestic nocturnal eating that stopped with discontinuation [16].
Further reports have strengthened the relationship between zolpidem and SRED. In a series of 1235 patients at an outpatient psychiatry clinic, the combination of zolpidem and antidepressants posed the greatest risk for SRED [15]. In another report of 29 sleepwalkers with frequent BRA use, approximately 2/3 of patients described sleep-related eating behavior [68]. The vast majority of reports note improvement if not outright resolution once the agents were discontinued [16, 68].
SRED frequently occurs when, in a desperate attempt to initiate sleep, patients take supratherapeutic doses of zolpidem [58, 69].
BRAs enhance GABA activity at central GABA A receptors resulting in hypnotic phenomena [33]. As these agents suppress executive function it may be that zolpidem by itself, does not activate SRED but instead disinhibits the behavior in a patient population at risk for nocturnal feeding. Patients with RLS who are not on sedatives demonstrate a greater tendency towards wakeful, nonpathological nocturnal eating [8, 44]. Conversely, when on sedatives, particularly BRAs, patients with RLS frequently demonstrated amnestic SRED [8, 16, 67, 70]. (see section on RLS and SRED).
Medication-Induced Amnesia
Impaired consciousness, as a defining criterion for SRED, has evolved since complete or at least partial unawareness was necessary for diagnosis. In the original series of 32 SRED patients, 84% claimed an impaired recall [71]. Conversely, a subsequent report noted full awareness in all 26 patients after episodes of nocturnal eating in a sleep laboratory [61].
The Relationship Between SRED and RLS
In many cases of SRED, nocturnal food ingestion is best characterized as restless eating, i.e., in order to facilitate sleep. In this regard, nocturnal feeding behaviors bear a striking similarity to the motor symptoms of RLS. In fact, reports have described that nocturnal eating is pervasive among RLS patients including the original description by Ekbom in 1960 [8, 69, 70]. “They often have to get up and walk, “like a caged bear,” to quote one of my patients, or they go into the kitchen and get something to eat” [72]. Further similarities in epidemiology, polysomnographic phenomena, clinical course, and treatment response are reviewed here and suggest an intimate relationship between nocturnal food ingestion and RLS.
RLS is a disorder affecting approximately 8 to 10% of the population and thus a common cause of sleep initiation and maintenance failure [1, 73, 74]. Further, while RLS is distinct from, it is commonly confused with psychophysiological insomnia (PI). Thus, it may be expected that many patients with RLS will be mistakenly treated with therapies designed to treat PI, agents such as BRAs.
Like SRED, RLS has a higher prevalence in women [1, 73]. Further, medication-induced SRED is more common in women [58, 69].
Similar to RLS [75], several features of SRED suggest an underlying dopamine dysfunction. First, dopamine mediates impulsive behaviors such as motor restlessness, smoking, and binge eating [75]. Second, a polysomnography (PSG) study of 35 SRED patients demonstrated that 77% had PSG confirmation of wakeful RLS and periodic limb movement during sleep [61]. Third, rhythmic masticatory muscle activity (RMMA) and bruxism, dopaminergic phenomena [56, 76] associated with RLS, are commonly seen in SRED [46, 61]. In the original SRED case series, prominent RMMA was described during NREM sleep and after arousals [46]. Recently, RMMA was found in 29 of 35 patients diagnosed with SRED during their PSG evaluations [61].
Recently, two investigations demonstrated a high prevalence of both SRED and nondysfunctional nocturnal eating in patients with RLS. A community survey of 100 RLS patients reveals a high prevalence of SRED in RLS (33%) compared to normal population controls (1%) [70]. The authors pondered whether the compulsive nocturnal eating was related to underlying RLS brain pathology or whether nocturnal eating was merely “killing time” as previously suggested. This question was addressed in another study of 130 patients with either RLS or PI who presented to a sleep disorders center. This report noted that 61% of RLS patients described either nondysfunctional NE (25%) or SRED (36%). Conversely, only 12% of patients with PI described NE and no patients met criteria for SRED. This study suggests that nocturnal eating in RLS is not merely “killing time” as PI patients were more likely to have prolonged (> 5 min) nightly awakenings (93%) compared to patients with RLS (64%) [8].
Intriguingly, the nocturnal feeding behavior of SRED closely resembles the motor activity of RLS. RLS is characterized by an underlying feeling (often poorly described) of discomfort in the lower extremities that compels the patient to move. Movement relieves the discomfort and sleep is unable to be reinitiated until this urge is addressed [77]. In SRED, patients state that after awakening from sleep, they have a compulsion to eat (often without hunger) that interferes with sleep maintenance. Subsequently, once food is ingested, the feeling abates and sleep may be reinitiated [1, 46, 70].
Compulsive nocturnal eating is not unexpected as RLS patients often describe other nonmotor nocturnal urges [78]. Recently, 6 cases of nocturnal eating and nocturnal smoking were reported. 5 of the 6 cases either presented with or were noted to have RLS. Patients claimed that they would wake up and be unable to return to sleep without eating and/or smoking. In a follow-up study that investigated the prevalence of sleep-related smoking, RLS patients demonstrated an increased prevalence (12%) compared to matched controls (2%). Interestingly, among RLS patients with nocturnal smoking, SRED was common (83%) and both phenomena often began simultaneously [78].
It has been debated whether SRED in RLS may be caused by dopaminergic drugs as these agents are known to trigger daytime impulsive behaviors such as gambling [79–81]. However, the preponderance of evidence suggests that dopamine agents are not the cause of SRED. First, dopamine agents suppress feeding behavior in animal models [82]. Second, a review of the original SRED series noted that dopaminergic therapy resolved the dysfunctional eating in 7 of 8 patients in whom the treatment was attempted [46]. Later, two cases of SRED were noted to resolve with levodopa (in combination with buproprion and trazodone) [83]. Third, in a separate survey of patients with both SRED and RLS, 10 patients reported that nocturnal eating emerged prior to or concomitant with motor restlessness and none reported that nocturnal eating emerged after the start of dopaminergic therapy. Also, RLS patients with SRED were not significantly more likely to use dopaminergic drugs compared to RLS patients without SRED. In fact, subjects whose nocturnal eating symptoms were under control were more likely to be on these agents than subjects who continued to have nocturnal eating [70]. Fourth, a double-blind treatment trial of pramipexole for SRED demonstrated improved sleep and reduced nighttime activity and further did not result in increased feeding activity [84]. Another series monitored therapy outcomes in 44 RLS patients previously unexposed to dopaminergics. In this population, the frequency of both NE and SRED diminished by half with dopaminergics. Further, only one patient reported an exacerbation of NE after dopamine agents were initiated and there were no cases of dopaminergics inducing de novo NE. Consistent with other reports, nocturnal eating symptoms demonstrated a clinical response in parallel to motor RLS symptoms [8]. Finally, treatment with dopaminergic agents appears to improve other nonmotor manifestations of RLS that frequently coexist with SRED. In particular, all patients who reported a remission of nocturnal smoking had been treated with dopaminergic agents [84].
Conceptually, as RLS patients are predisposed to NE, greater than 60% in one survey [8], then amnestic SRED would be the expected result when RLS patients are treated with agents that suppress memory as well as executive function. Thus, it is not a surprise that 80% of RLS patients exposed to sedative–hypnotics had subsequent amnestic SRED or sleepwalking behavior [8].
While RLS is a condition distinct from PI, it can be easily misdiagnosed and thus mistreated as insomnia related to cognitive hypervigilance. In 2002, the first case series of 5 patients with zolpidem-induced amnestic SRED was reported. Incidentally, all 5 patients were noted to have RLS [16]. Others have commented that RLS appears to be ubiquitous in the setting of zolpidem induced SRED [85].
Zolpidem-induced SRED among patients with PI is rare. Among 25 PI patients treated with either a benzodiazepine or BRA, only two reported amnestic behavior, and in neither case did the events persist [8]. These findings are consistent with previous reports where SRED and SW are rare (1% or less) in zolpidem treated insomnia patients when RLS has been carefully excluded [86]. Thus, one can conclude that in the absence of motor restlessness, sedative–hypnotics are safe agents and there is minimal risk of SW/SRED behaviors.
Management of Disorders of Arousal
Evaluation
The first steps of parasomnia management include the following: a severity assessment, identification and treatment of comorbid sleep disorders, elimination of presumed inducing agents, and ensuring environmental safety. Most CoA and many SW episodes are benign and limited in duration. In these cases, patients may be given reassurance and advised to avoid sleep deprivation and sedating agents. Situations that deserve more thorough investigation include the following: violent/potentially injurious behavior, nonviolent dangerous behavior (such as leaving the house), high-frequency episodes, or if the parasomnia is associated with symptoms suggestive of another sleep disorder or neuropsychiatric condition [87].
Correctly diagnosing a parasomnia requires a detailed review of the sleep–wake complaints followed by a neuropsychiatric history and examination. A report from a bed partner is particularly helpful as many patients are unable to properly recall the nocturnal events by the time they are discussed with a clinician.
In SW, there is often a lifelong history, beginning in childhood, of prolonged, complex, nonviolent activities emanating from the first half of the sleep period with residual confusion [1]. However, in a series of 54 adult patients with injurious SW (and/or ST), one-third developed their persistent SW after the age of 16 years [88].
Polysomnography
The primary role in the polysomnographic evaluation of parasomnias is to rule out conditions such as sleep disordered breathing as a cause of nocturnal behaviors. The sleep fragmentation of OSA during REM or NREM sleep can lead to DEB or CoA/SW, respectively.
PSG with video monitoring is often helpful in the evaluation of parasomnias even if abnormal behaviors do not arise during the sleep study [89]. Under routine conditions, PSG does not typically demonstrate CoA/SW or DEB. This is due to the intermittent nature of parasomnias as well as the laboratory effect (foreign environment) decreasing N3 sleep compared to the home sleeping environment [89, 90]. However, even without abnormal behaviors, PSG facilitates diagnosis as CoA/SW patients often demonstrate NREM sleep instability.
Sleep deprivation combined with forced awakening increases the likelihood of triggering a NREM parasomnia event during laboratory testing and thus helps facilitate diagnosis. In particular, one protocol recommends 25 h of sleep deprivation leading up to a PSG combined with an alarm awakening during SWS. Using these methods, somnambulistic events were induced in 100% of patients with a history of SW compared to only 30% of patients if sleep deprivation is not used. Importantly, no control subject without a history of SW demonstrated somnambulistic events using this combined method of sleep deprivation and forced arousals (a 100% sensitivity) [14].
In addition to NREM instability, CoA/SW PSG recordings often reveal a 10-s-long buildup of hypersynchronous delta waves immediately preceding a parasomnia event (see discussion on CAP above). Subsequently, postarousal EEG shows a persistence of slowed cortical activity, that either evolves into wakeful EEG activity or returns to NREM sleep [40].
Polysomnography (PSG) is used to characterize SRED with commonly consumed nocturnal food made available at bedside in order to facilitate eating behavior. Similar to SW, SRED arises out of NREM sleep. One study documented that 44 of 45 feeding episodes in 26 patients arose from NREM sleep [56].
Table 9 enlists various PSG findings in NREM parasomnia.
Conservative Strategies
Environmental Safety
Environmental modification is a critical component in treating parasomnia cases with potential for sleep-related injury. The patient should be advised to remove any bedside object or furniture that could be injurious either to them or to a bed partner. Firearms and other weapons should be removed from the bedroom and windows locked with curtains drawn to prevent lacerations. Bedroom door alarms are helpful ways to signal others that a sleepwalker is wandering, however loud auditory stimuli could paradoxically worsen NREM parasomnias [14].
Treatment of Comorbid Conditions/Aggravating Factors
Reversing comorbid conditions characterized by frequent cortical arousal in sleepwalkers often dramatically diminishes nocturnal behaviors. Sixty SW patients were studied with PSG and followed for a year. A high number (n = 53) were diagnosed as having sleep disordered breathing. The majority of patients had only a mild burden of disease, often not reaching criteria for OSA, but instead upper airway resistance syndrome. However, the results were striking. Only 3 patients dropped out of the study while of the remaining 50 all reported resolution of SW after treatment (42 reported CPAP, 8 upper airway surgeries). These dramatic results suggest that treatment of even mild, asymptomatic SDB may result in resolution of SW [42].
When SW is associated with sedative–hypnotics, it is of particular importance to reconsider the diagnosis for which the medication was originally prescribed. In these cases, patients may not have insomnia (for which the sedating agent was prescribed) but rather another disorder of sleep initiation such as RLS or a delayed circadian rhythm [8, 14, 33, 46, 67]. Discontinuing offending agents will typically resolve the parasomnia particularly if another underlying condition is identified and treated [8, 33, 46]. Treatments include the following: dopamine agonists in RLS [91] and evening melatonin/morning light therapy in a delayed circadian rhythm [92]. Conversely, in the setting of carefully diagnosed insomnia patients, those in whom other disorders are excluded, BRAs are well tolerated and SW rarely induced [8]. Patients with insomnia can also be successfully treated with cognitive behavioral therapy [93, 94]. Treatment of NREM parasomnias is summarized in Table 10.
Behavioral Therapy
Some behavioral and cognitive strategies demonstrating some degree of benefit are discussed below.
-
I.
Hypnotherapy:
There is some literature showing benefit of clinical hypnosis improving DOA. In 1991, a case series of 27 patients (8 with SW,15 with SW and ST, and 4 with ST) showed that hypnotherapy was helpful with lasting improvement in 74% of the patients. It was noted that 20 out of 23 (87%) SW patients who underwent self-hypnosis training described significant improvement after greater than 6 months of follow-up [100]. Another later study demonstrated that 7 of 11 (67%) sleepwalkers treated with physician-administered hypnosis described significant improvement which persisted after 5 years [101].
-
II.
Anticipatory awakening:
It is a commonly used method in childhood NREM parasomnias [84] especially in cases where the occurrence of nocturnal events is highly predictable. This technique involves purposefully arousing the parasomniac 15 to 20 min prior to the anticipated onset of a typical episode for a duration of roughly 1 to 4 weeks. Sustained positive results in children have been reported; however, there is negligible data in adults [101, 102]. This method appears to be a relatively low-risk therapy.
Other behavioral interventions include psychotherapy and relaxation therapy which have shown improvement in anecdotal cases [93, 95, 103].
Pharmacotherapy
If NREM parasomnia behaviors persist despite resolution of exacerbating disorders and removal of inducing agents, pharmacological interventions may be considered. The most commonly prescribed agents include benzodiazepines and to a lesser extent antidepressant medication. Efficacy depends upon which parasomnia is being treated. Antidepressants have some efficacy in the treatment of ST, whereas these agents may exacerbate SW.
It is important to recognize that the evidence for all therapies is currently based on a small number of studies, typically case reports and case series. Only rarely have there been controlled clinical investigations and sample size was typically small. Furthermore, as described below, much of the evidence is contradictory [104].
Benzodiazepines
Clonazepem is commonly used as first-line pharmacotherapy; however, studies show conflicting results. In 1996, a series of 170 patients with mixed sleep disorders (69 with SW/ST) were treated with benzodiazepines, primarily clonazepam (n = 136), and followed for clinical response [96]. The vast majority of patients (86%) reported good control after an average follow-up of 3.5 years. The authors reported that clonazepam efficacy was sustained with low risk of dosage escalation, with any significant dose increase, by paired t test, after a mean 3.3 years of nightly therapy, and with low risk of side effects. A separate clinical case series reported on 6 SW patients, who were initiated on clonazepam. SW was suppressed in 5 of 6 patients [105]. Conversely, a later report claims that clonazepam failed to demonstrate sustained efficacy in 5 SW patients. This investigation carefully excluded even subtle sleep disordered breathing. After 1 year, all patients treated with clonazepam dropped out of the study and reported a persistence of SW [42].
Antidepressant Medication
Agents with strong serotonergic actions are occasionally effective in the treatment of some NREM parasomnia patients, most commonly ST (see serotonin hypothesis above). One report described two patients with a history of ST combined with SW, both of whom failed diazepam therapy but responded well to imipramine (a tricyclic antidepressant) [96]. Later, a 7-year-old girl with ST failed to respond to imipramine; however, she had a compelling therapeutic response to trazadone (a phenylpiperazine antidepressant) [97]. In contrast to these successful ST cases, a series of SW patients included 8 patients who were treated with various serotonergic agents and/or benzodiazepine. After 1 year of follow-up, all 8 patients described a persistence of SW [42].
Paroxetine appears to be particularly effective in the treatment of ST. In one report, 6 patients had a significant reduction if not outright elimination of ST events. The authors suggested that SSRIs may be uniquely effective for ST through serotonin effects on terror centers in the midbrain periaqueductal gray matter [55]. Conversely, there has been a report of paroxetine inducing SW [21]. Moreover, these findings are in contrast to a dramatic elimination of SW behavior in patients who are effectively treated for sleep disordered breathing [42].
Sleep-Related Eating Disorder Treatment
Treatment of Comorbid Conditions
The first goal in treating SRED is to eliminate implicated medications and correct comorbid sleep disorders, especially RLS. The majority of patients with drug-induced SRED notice improvement after inducing agents are discontinued [16, 58, 67, 68]. It can often be controlled outright by treating comorbid RLS [8]. In cases of SRED associated with obstructive sleep apnea, continuous positive airway pressure may eliminate both the sleep disordered breathing and the nocturnal eating [106].
Pharmacotherapy
In cases without comorbid sleep disorders (or at least unrecognized comorbid sleep disorders) two classes of pharmacotherapies have been studied and appear to be potentially effective, antiseizure medication topiramate and dopaminergic agents. The original SRED case series noted that either bedtime levodopa or bromocriptine was effective in eliminating nocturnal eating in 8 patients [107]. Pramipexole, a dopamine agonist, was investigated in a small double-blind, placebo-controlled crossover trial. It was well tolerated and subjects noted improved sleep and reduced nighttime activity was documented with actigraphy [84]. An open-label trial of topiramate in four patients with nocturnal eating demonstrated positive results. The agent was well tolerated, reports of nocturnal eating were diminished, and weight loss (mean of 11.1 kg) was noted in all four individuals over 8.5 months [108]. Finally, a study of 25 SRED patients on topiramate reported that 17 (68%) of SRED patients were treatment responders. Adverse events were high however and over 12 months 41% of patients discontinued the medication [109]. Recently, a double-blind randomized control trial has demonstrated significant efficacy, supporting the use of topiramate in SRED. The symptoms were significantly reduced with topiramate (74.7 to 33.2% nights/week) compared to placebo (77.0 to 57.4%) [99]. Use of SSRIs such as low dose sertraline at 25 mg has also been noted to improved SRED demonstrated in two recent case reports [110].
Parasomnia Overlap Disorder
Parasomnia overlap disorder (POD) is a condition characterized by coexistence of REM sleep behavior disorder (RBD) and either a disorder of arousal, SRED, sexsomnia, or rhythmic movement disorder [1]. It is either idiopathic or sometimes can be associated with neurological conditions such as narcolepsy, multiple sclerosis, structural lesions in the brain, psychiatric disorders, substance abuse, and withdrawal states [1]. Even though it is considered a variant of of RBD according to ICSD-3 classification, association with phenoconversion into a neurodegenerative disease has not been established [111]. In fact, it has also been proposed that it represents a distinct parasomnia category owing to younger age of onset, more prominent features of DOA, and lack of proven association with synuclein disorders [112].
Status Dissociatus
Status dissociatus is a condition where disintegration of various stages of being, wakefulness, and NREM and REM sleep occurs, characterized by lack of orchestration of behavioral, neurophysiological, and autonomic markers defining different sleep stage boundaries. It is considered a subtype of RBD according to ICSD-3 [1] and was initially described in 1991 in 6 cases where multiple, ambiguous, and intermixed variable oscillations in sleep state-dependent variables were noted [113]. The PSG demonstrated admixtures of various markers of different sleep stages occurring simultaneously, suggesting breakdown of the boundaries between distinct sleep states. Clinically patient appeared to be asleep but would demonstrate complex motor behavior suggestive of dream enactment [114]. This phenomenon has been noted in conditions such as alcohol withdrawal state, narcolepsy, autoimmune encephalititis, Iglon-5 parasomnia, fatal familial insomnia, and alpha synuclein disorders [90, 115]. The pathophysiological mechanism is considered to be Gamma-butyric acid (GABA)-mediated thalamocortical dysfunction.
Agrypnia excitata is the extreme form of status dissociatus with compete disintegration of sleep state boundaries. Behaviorally it is manifested as continuous motor and autonomic hyperactivity with the patient clinically in a hallucinatory state with seemingly semi purposeful movements termed as “oneiric behavior”[1, 113].
Summary
Parasomnias represent abnormal behaviors and experiences that arise from sleep. They range from subclinical events only noticed by a wakeful bed partner to complex and also violent, potentially life-threatening motoric behaviors. DOA share the same pathophysiological mechanism, and hence, conservative management comprises of environment modification and safety assurance. NREM parasomnias are treated by identifying and reversing conditions that enhance homeostatic sleep drive and/or fragment sleep. Correcting RLS may help diminish sleepwalking behaviors in amnestic SRED. Sexsomnia is a subtype of DOA, which shares similar pathophysiological mechanism. If behavioral management is unsuccessful, pharmacotherapy with limited evidence can be utilized in potentially injurious NREM parasomnia cases.
POD and status dissociatus are lesser known variants of RBD, which are mentioned in this article, as they intrude upon the NREM stage of sleep.
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Irfan, M., Schenck, C.H. & Howell, M.J. NonREM Disorders of Arousal and Related Parasomnias: an Updated Review. Neurotherapeutics 18, 124–139 (2021). https://doi.org/10.1007/s13311-021-01011-y
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DOI: https://doi.org/10.1007/s13311-021-01011-y