Introduction

This article reviews interesting and important findings published since 2013 relevant to the treatment of circadian rhythm sleep-wake disorders. The recent update to the clinical practice guideline for the treatment of intrinsic circadian rhythm sleep-wake disorders is first summarized, followed by a review of recent treatment studies published since then. These include studies assessing treatments for delayed sleep-wake phase disorder, non-24-hour sleep-wake disorder, irregular sleep-wake disorder, and shift work. New approaches to estimate circadian timing are then reviewed, including home saliva collection to directly measure the dim light melatonin onset, and the use of circadian questionnaires to estimate the dim light melatonin onset. General rules to guide light and exogenous melatonin treatments are also presented. New developments in light treatment are also discussed, including light flashes during sleep and wearable light devices. Substances such as caffeine and alcohol, and devices such as electronic tablets are also considered, for their potential to inadvertently shift circadian timing in an unwanted direction. Lastly, an update on melatonin supplements in the USA is discussed, along with the controversy surrounding the use of melatonin supplements in patients with prediabetes or diabetes.

Update to Clinical Practice Guideline for the Treatment of Intrinsic Circadian Rhythm Sleep-Wake Disorders

In 2012, the American Academy of Sleep Medicine (AASM) formed a task force to update the practice parameters for the intrinsic circadian rhythm sleep-wake disorders (CRSWDs). Search terms were agreed upon, and a literature search was conducted of relevant articles published since the last practice parameters were issued in 2007. The task force then developed PICO (patient, population, or problem; intervention; comparison; and outcomes; see Table 1 in [1••]) questions that were used in the assessment of the literature. As part of this process, the critical outcomes and the degree of change considered clinically relevant were defined. The task force then chose articles from the literature search for inclusion, and the relevant data were extracted (including study methodology and type, subject population, intervention(s), relevant outcome measures, harms, and limitations). The extracted data were classified by CRSWD, outcome measure, PICO question addressed, study design, and assessment method. Meta-analyses were conducted when possible. Finally, the GRADE (Grading of Recommendations Assessment, Development, and Evaluation) system was used to evaluate the data and arrive at treatment recommendations by taking into account the quality of the evidence, an assessment of risks and benefits, and patient values and preferences.

The use of the more rigorous GRADE system resulted in truly novel CRSWD practice guidelines that were notable for a lack of any recommendation for the majority of disorders and interventions assessed. The recommendations that were made were further notable for the general weakness of recommendation (see Table 5 in [1••]). For those interventions without a recommendation, an accompanying editorial made clear that the task force was not indicating that these interventions should not be used by clinicians [2]; rather, the available evidence was insufficient to make a recommendation for or against such interventions. In brief, the practice parameters issued a weak recommendation for the use of light therapy in advanced sleep-wake phase disorder (ASWPD) and irregular sleep-wake rhythm disorder (ISWRD), and a strong recommendation against the use of sleep-promoting medications in ISWRD. There was also a weak recommendation for timed melatonin or melatonin agonists in delayed sleep-wake phase disorder (DSWPD), non-24-hour sleep-wake rhythm disorder (N24SWD), and ISWRD in children/adolescents with neurological disorders, but a weak recommendation against melatonin in elderly demented populations. In terms of combination treatments, there was a weak recommendation for the use of light and behavioral interventions in children/adolescents with DSWPD, and a weak recommendation against the use of melatonin and light in elderly demented individuals with ISWRD. A pictorial summary of the recommendations for treatment is shown in Fig. 1. The general weakness of these practice parameters reflects the deficits in the evidence base and highlights the need for clinical trials for CRSWD interventions [2].

Fig. 1
figure 1

A pictorial representation of the most recent clinical practice guideline recommendations for treatment of intrinsic circadian rhythm sleep-wake disorders. From top down is advanced sleep-wake phase disorder, delayed sleep-wake phase disorder, non-24-hour sleep-wake disorder in the blind with circadian period >24 h, non-24-hour sleep-wake disorder in the blind with circadian period <24 h, irregular sleep-wake disorder for the elderly, and irregular sleep-wake disorder for children. The times in red indicate the range in typical fall asleep or wake times seen in patients prior to treatment, and the red arrow represents the direction of desired phase shifts. The light bulb symbol represents light therapy. The circles represent melatonin pills with doses suggested by the authors to either minimize or maximize melatonin’s soporific effect as needed

Following the publication of the AASM practice parameters, we published a practical review aimed at helping clinicians treat patients with a CRSWD or those suspected of having some degree of circadian misalignment that impacted disease signs and/or symptoms [3]. Updates to the practice guidelines for the treatment of extrinsic CRSWDs (shift work and jet lag disorders) should be forthcoming from the AASM in the next few years.

More Recent Studies on Circadian Rhythm Sleep-Wake Disorders

We searched for studies of intrinsic circadian rhythm sleep-wake disorders published from 2014 onwards, to identify any studies published after the literature search for the update in clinical practice guideline. We found no new studies of advanced sleep-wake phase disorder. There was one new study of delayed sleep-wake phase disorder. In this study, Saxvig et al. [4] randomized 40 adolescents diagnosed with DSWPD to one of four 2-week treatments: dim morning light plus placebo capsules, bright morning light plus placebo capsules, dim morning light plus melatonin capsules, and bright morning light plus melatonin capsules. All the treatments included the gradual advancement in wake times and capsule and light administration times by 1 h per day (such prescribed sleep-wake scheduling would have classified even the light- or melatonin-only interventions as combination treatments in the AASM CRSWD practice guidelines). Light (“approximately 10,000 lx” versus 400 lx of “dim red” light) was administered for 30–45 min upon awakening while capsules (3 mg melatonin or placebo) were administered 12 h after waking (but not before 8 pm). Outcomes included sleep diaries, wrist actigraphy, and salivary dim light melatonin onset (DLMO). No differences were found across the four groups with an approximate 2 h advance seen in the DLMO and rise time and a 1 h advance in bedtime. Therefore, none of the interventions either alone or in combination were any more effective than the advancement of wake times alone. The study also included a subsequent 3-month open label trial of melatonin and bright light versus no intervention and found that only the former maintained the shift in sleep to an earlier time.

There were two new publications concerning blind individuals with N24SWD. Most important was Lockley et al.’s study [5•] of the drug tasimelteon in this population which became the first medication approved by the FDA for the treatment of any CRSWD. The study was a randomized, placebo controlled study in 84 individuals with N24SWD comparing 20 mg of tasimelteon and placebo administered 1 h before a target bedtime. Tasimelteon was found to safely and effectively treat individuals with N24SWD: entrainment (synchronization to the 24-h day) occurred in 20 % (8 of 40) of patients receiving the drug compared with 3 % (1 of 38) receiving placebo. As noted in the AASM CRSWD practice guideline [1••], the entrainment rate was lower than the 67 % entrainment rate (12 of 18 patients) found in the meta-analysis of melatonin treatment in N24SWD. However, as noted by the authors themselves, this may have been because entrainment was assessed after just 1 month of treatment. Such a theory is borne out by the higher rates of entrainment found during the longer, open label treatment with tasimelteon. The tasimelteon study also demonstrated improvements (increases and decreases, respectively) in nighttime and daytime sleep (as measured by the worst quartiles of treatment days compared to baseline). Of note, the tasimelteon study could also be considered to include a component of prescribed sleep/wake scheduling as subjects were instructed to maintain self-selected 9-h sleep opportunities with bedtimes within a 4-h range (21:00 to 01:00). The second new publication in N24SWD was a small placebo controlled study by St. Hilaire and Lockley [6] looking at the effects of caffeine on entrainment in three blind individuals with the disorder. Caffeine (150 mg at 10 am) failed to entrain the subjects although it did improve daytime alertness in the setting of circadian misalignment.

A single new study of light therapy in elderly patients with dementia and irregular sleep-wake rhythm disorder (ISWRD) was published by Figueiro et al. [7]. The study looked at 4 weeks of “bluish-white” light in 14 individuals with dementia living in a skilled nursing facility using custom built “luminaires” in the patient’s rooms (on from approximately 6–8 am to approximately 6 pm). Light and activity were measured with a Daysimeter device placed on the wrist, and improvements with light therapy were seen in sleep efficiency and total sleep time as well as an increase in “phasor magnitude” (a quantification of the relationship between the timing and amplitude of the rest-activity rhythm and light-dark timing) that the authors suggested represented an increase in “circadian entrainment.” As noted above, AASM practice parameters included a weak recommendation for light therapy in this particular patient population with ISWRD, and the results of this study are consistent with this recommendation.

We also searched for recent studies of shift work and jet lag from 2013 onwards, deemed relevant to treatment. One study reported on the effects of aligning work schedules to individual shift worker’s chronotype and found significant improvements in the workers’ sleep [8]. Specifically, in an industrial factory, over a 5-month period, Vetter and colleagues abolished morning shifts for late chronotypes and night shifts for early chronotypes, while intermediate chronotypes continued to work morning, evening, and night shifts in a rotating forward shift schedule. In response, they observed in the late and early chronotypes, a significant increase in self-reported sleep duration on work days (24–28 min) along with improvements in sleep quality and wellbeing. This study highlights the importance of considering chronotype when assigning work schedules for shift workers.

New Approaches for Measuring Circadian Timing in Patients

The most reliable marker of circadian timing in humans is the dim light melatonin onset (DLMO) [9], which is the time when endogenous melatonin levels begin to rise in dim light, on average about 2–3 h before habitual bedtime [10, 11]. Melatonin must be measured in dim light because light can suppress melatonin secretion [12]. As highlighted by others, the measurement of the DLMO in patients can assist both with the diagnosis of most circadian rhythm sleep-wake disorders, and also with optimizing the timing of bright light and/or exogenous melatonin treatment [13, 14]. However, the DLMO is not yet commonly measured in the clinic. As a proof of concept study, we recently tested a home kit and procedure with objective measures of compliance to the requirement for dim light levels and scheduled times for saliva samples. In 32 healthy controls, we found that the home DLMOs compared favorably to the standard laboratory-based DLMOs (r = 0.91, p < 0.001), and only 8 % of home DLMOs were confounded by light or sampling errors [15•]. In a second study of 32 patients with DSWPD, we also found that the home DLMOs compared favorably to the standard laboratory-based DLMOs (r = 0.93, p < 0.001) [16•]. Compliance to the home procedures was also good in these patients, but light and sampling errors occurred more frequently around the time of the DLMO, resulting in greater data loss (17 % of the home DLMOs were invalid) [16•]. Overall, these studies demonstrate that accurate DLMOs can be assessed in the home, and we hope that in the future home-based assessment of the DLMO for the diagnosis and treatment of CRSWD becomes the norm [17].

However, when measuring the DLMO is not feasible, one approach to estimating circadian phase could be to use circadian questionnaires that ask people about the timing of their behavior, such as their sleep. Two commonly used questionnaires include the Morningness-Eveningness Questionnaire (MEQ) [18] from which a MEQ chronotype score can be derived and the Munich ChronoType Questionnaire [19] from which a midpoint of sleep on work-free days, sleep corrected (MSFsc) chronotype value can be derived. In 2014, Kitamura and colleagues [20] reported results from the first study to assess the MEQ score, MSFsc, and DLMO in the same sample of subjects (n = 44). They found the DLMO was significantly correlated with the MEQ score (r = -0.40, p = 0.055) and MSFsc (r = 0.54, p < 0.001). Recently, in a larger sample (n = 60) with a larger range in chronotype and DLMO, we found stronger correlations between DLMO, MEQ score, and MSFsc [21•]. In this case, both MEQ score and MSFsc were essentially similarly correlated with the DLMO (MEQ score r = -0.70, p < 0.001; MSFsc r = 0.68, p < 0.001). However, we noted a range of about 4 h in the DLMO around each chronotype score, suggesting these measures of chronotype are too variable to be used to time circadian-based treatments, as this could result in the mistiming of treatments relative to the DLMO, potentially worsening the circadian misalignment [21•]. It remains to be determined how closely phase shifts in the DLMO can be reflected in changes in these chronotype scores.

Currently, instead of estimating the DLMO from chronotype scores, we use rough rules of thumb to guide light and melatonin treatment when measuring the DLMO is not feasible [3, 22]. For example, for phase advancing light treatments, we tend to avoid starting the light treatment more than 1 h earlier than spontaneous wake time to avoid accidental phase delays. Phase delaying light can extend into the first 3 h or so of the habitual sleep episode. For melatonin treatments, we tend to estimate the DLMO about 2–3 h before bedtime, such that melatonin is taken about 5 h before habitual bedtime to phase advance and around habitual wake time to phase delay. We typically instruct patients to take low doses (≤0.5 mg) when they need to minimize the soporific effect of exogenous melatonin, and high doses (3 mg) when falling asleep (a dark pulse) would assist in the desired phase shift (Fig. 1). Ultimately, however, the treatment of CRSWD will be optimized once the direct assessment of the DLMO in the clinic or in people’s homes becomes more commonly available.

New Methods of Light Administration

The main burden typically associated with light treatment is the time commitment, such as a 30-min to 1-h treatment per day, and/or the usual requirement to be seated close to a light box in order to receive light of sufficient intensity [3]. To avoid the daily time commitment during wakefulness, there has been much interest in applying light treatment during sleep, when the circadian system is usually very sensitive to light. Recently, a 1-h interval of millisecond flashes of bright light from a flash bulb placed above people’s heads while they slept was found to significantly phase delay the DLMO by about 30 min [23•]. The 1-h interval of light flashes was timed to occur during the third hour of the habitual sleep episode. The bright light was of sufficient intensity to still reach the retina after passing through closed eyelids, without major disruption to sleep [23•]. Indeed, such light flashes may sometimes produce larger phase delays than seen with continuous light [24]. Others have recently reported on a light mask worn during sleep that can also phase delay circadian timing, up to 30 min after a 60-min light exposure window during the first 2 h of the habitual sleep episode [25]. While these recent findings are promising, to our knowledge, no such light at night systems or light masks are currently commercially available.

The requirement to be seated close to a light box for 30 min to 1 h per day likely contributes to adherence issues in home treatments. Two wearable light devices are now available commercially. The Luminette 2 device (Myluminette.com) resembles a visor, with the light source positioned above the eyes. The Re-timer device (Re-timer.com) is more similar to glasses, and the light source is positioned below the eyes. Both devices are lightweight, very portable, and easily charged; have good battery life; have adjustable light intensity to accommodate patient preference; and importantly permit the patient to be ambulatory during light treatment. In our opinion, these wearable devices are likely to improve compliance to light treatment. While there is evidence that an earlier prototype of the Re-timer could shift circadian timing [26], we await publications that conclusively demonstrate that these devices can shift circadian timing.

Substances and Devices That May Alter Circadian Timing

As noted above, caffeine failed to result in entrainment in a small placebo controlled study in blind individuals with N24SWD [6] who would have required daily phase advances to effectively treat their disorder (shifts in the timing of the circadian pacemaker to an earlier time). However, another study recently demonstrated that caffeine is capable of causing phase delays in the timing of the circadian pacemaker raising the possibility that caffeine could be used as a true chronobiotic. Burke et al. [27•] administered 2.9 mg/kg of caffeine 3 h before habitual bedtime in a double-blind, placebo controlled fashion in five healthy individuals and found that caffeine caused a phase delay that was approximately 40 min longer than the dim light placebo control. In comparison, the response to a 3-h exposure of ∼3000 lx beginning at habitual bedtime was about 85 min longer than the dim light placebo. Therefore, caffeine might have potential as a phase delaying agent in ASWPD or in N24SWD patients with circadian periods that are less than 24 h and therefore require corrective phase delays to achieve entrainment. However, first, it would have to be determined whether the direct alerting effects of caffeine would negate any circadian resetting benefits in these disorders and whether the dose-response and phase-response curves for caffeine are favorable for its use in CRSWDs.

A single dose of alcohol can alter phase shifts to light in rodents, presumably due to the alcohol directly altering levels of GABA and glutamate in the suprachiasmatic nuclei, the location of the central circadian pacemaker [28, 29]. We recently conducted two placebo controlled, within subject design studies to determine for the first time if a single dose of alcohol (0.6–0.8 g/kg, approximating 2–3 standard drinks) can alter phase shifts to light in humans [30•]. In one study, 14 healthy subjects consumed alcohol (vs. placebo) in the late evening immediately before a 2-h bright light treatment, to test the effect of alcohol on phase delays to light. In the other study, ten healthy subjects consumed alcohol (vs. placebo) in the early morning, immediately before a 2-h bright light treatment, to test the effect of alcohol on phase advances to light. In both studies, there was not a consistent response, with alcohol increasing phase shifts to light in some individuals, but decreasing phase shifts to light in other individuals. Additionally, the differences in phase shifts between alcohol and placebo were on average always less than 30 min, indicating the changes in phase shifts were not meaningful. It remains to be determined if chronic alcohol consumption can alter phase shifts to light.

Finally, the use of light-emitting devices must be considered both as potential interventions in CRSWDs and, more likely, as precipitators or perpetuators of these disorders. Chang et al. [31] demonstrated in a randomized cross-over laboratory study that exposure to a light-emitting electronic book (e-Book) for approximately 4 h prior to bedtime over five evenings caused a phase delay compared to reading a printed book for the same period (the DLMO occurred ∼1.5 h later in the e-Book condition). This study was criticized as lacking generalizability due to the daytime light levels (∼90 lx); the subjects were exposed to in the laboratory—the contention being that most individuals experience brighter light conditions during their waking day outside the laboratory and that such relatively dim light might have caused increased sensitivity of the circadian system to the resetting effects of the e-Books [32]. However, this study and others [33] highlight the impact of industrial lighting conditions on biological timing. Specifically, they are consistent with the hypothesis that a significant delay in the timing of the biological clock occurs under conditions of artificial light exposure. To what extent the exposure to industrial lighting conditions contributes to the development of some CRSWDs remains to be demonstrated as does the potential impact, in CRSWDs, of countermeasures targeting this same exposure [34].

Update on Exogenous Melatonin

The development of several melatonin agonists (including tasimelteon noted above) has brought to the fore the question of whether exogenous melatonin itself or melatonin agonists are most appropriate for the treatment of CRSWDs. Melatonin was given a weak recommendation for the treatment of DSWPD, N24SWD, and children and adolescents with neurological disorders and ISWRD in the AASM practice parameters. As we have noted previously, melatonin is classified as a dietary supplement by the FDA and therefore is not regulated like pharmaceuticals. This has led to questions regarding both the purity and the dose accuracy of various melatonin preparations. However, choosing a melatonin preparation from a supplier that participates in the USP verified program for dietary supplements might address these issues. Indeed, in 2015, a melatonin USP-certified product was added to the national formulary of the Veterans Health Administration (http://www.pbm.va.gov/clinicalguidance/drugmonographs.asp) which is the largest integrated health care system in the USA (www.va.gov/health). The specific indications included DSWPD and N24SWD.

The potential contraindications to melatonin use have included excessive sedation with ingestion, pregnancy or nursing, seizure disorders, and warfarin therapy. More recently, the question of the potential effects of exogenous melatonin on glucose tolerance has been raised despite the fact that lower endogenous levels of melatonin have been found to be associated with increased risk of type II diabetes [35]. Rubio-Sastre et al. demonstrated that 5 mg of exogenous melatonin acutely impaired glucose tolerance [36]. The same group has recently also showed that a common genetic variant that is associated with increased type II diabetes risk is also associated with worse glucose tolerance in response to exogenous melatonin [37]. As the potential metabolic consequences of melatonin administration become clearer, they will have to be weighed against the possible metabolic consequences of circadian misalignment associated with the CRSWDs themselves [38, 39].

Conclusions

This review provided an update on recent findings and developments that are relevant to the treatment of CRSWD. These new findings ranged from the new update to the clinical practice guideline for the treatment of intrinsic CRSWD, to recent treatment studies published since then. New approaches to estimate circadian timing, new developments in light treatment, and consideration of substances and devices that may inadvertently shift circadian timing were also reviewed. Lastly, recent developments regarding melatonin supplements were discussed. It is clear that large randomized clinical trials testing combination treatments in patients with carefully defined CRSWD are sorely needed [2]. Field-based studies are also required, as laboratory settings often lead to an artificial restriction in activities and movement, that can for example, artificially reduce the high variability in light exposure people often receive in their homes [40].