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NCT05463861 Clinical Trial

Lemborexant in Delayed Sleep Phase Syndrome

Delayed Sleep Phase Syndrome Clinical Trial

Official title:
Lemborexant in Delayed Sleep Phase Syndrome

Clinical Trial Details — Status: Recruiting

Administrative data
NCT number NCT05463861
Other study ID # 59441
Secondary ID
Status Recruiting
Phase Phase 4
First received
Last updated
Start date February 1, 2022
Est. completion date May 30, 2025

Study information
Verified date May 2023
Source Stanford University
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

The purpose of the study is to evaluate whether Lemborexant is more effective than placebo in shortening sleep onset latency in patients with delayed sleep phase syndrome (both type 1 and type 2). This will be tracked using sleep logs as well as actigraphy. In this 2-year study, we will examine if Lemborexant administered 5-10 mg nightly taken at desired bedtime (at least 2 hours prior to self-reported sleep onset habitual time) can improve the symptoms of Delayed Sleep Phase Syndrome.

Description:

Delayed sleep phase syndrome (DSPS) is a disorder in which a person's sleep is delayed by two hours or more beyond what is considered an acceptable or conventional bedtime. The delayed sleep then causes difficulty in being able to wake up at the desired time. In DSPS, bedtime is shifted later than the general population such that individuals have difficulty getting enough sleep to meet their sleep needs before they have to get up for their daytime obligations (work, school, childcare, etc.). As a result, patients experience daytime impairment, including daytime sleepiness and cognitive impairment. DSPS, if maintained in adulthood, is associated with numerous deleterious health effects, although causality is not well established. Two phenotypes of DSPS are recognized depending on the phase of entrainment: one with a late phase and normal phase angle (non-circadian) and other with a late phase and abnormal phase angle (circadian). The differentiation of these two phenotypes is theoretical: a mixed situation may be involved in some cases and the exact pathophysiology of each subtype is still controversial. In theory, however, separating the sample into these two subtypes is likely important to predict short- and long-term responses to orexin antagonists in DSPS. Lemborexant is one of the dual orexin receptor antagonists on the US market. The purpose of this study is to examine if lemborexant administered 5 to 10 mg nightly, taken at desired bedtime (at least 2 hours prior to self-reported sleep onset time), can improve the symptoms of Delayed Sleep Phase Syndrome both in the circadian and non-circadian phenotypes. The phenotypes will be recruited in 1:1 proportion.The effect of lemborexant will be analyzed based on the collection of information from actigraphy watches, sleep diaries, and sleep scales. The total participation time involved in this study will be approximately 6 weeks (2 weeks of baseline assessment followed by 2-weeks of treatment/placebo, and 2 weeks post-treatment).

Recruitment information / eligibility
Status Recruiting
Enrollment 60
Est. completion date May 30, 2025
Est. primary completion date May 13, 2025
Accepts healthy volunteers No
Gender All
Age group 18 Years and older
Eligibility Inclusion Criteria: 1. 18 years of age or older. 2. Diagnosed with delayed sleep phase syndrome (DSPS) meaning that: 1. Sleep is delayed by two hours or more beyond what is considered an acceptable or conventional bedtime for the subject (their desired bedtime). 2. Subjects not able to fall asleep if trying to sleep before the later bedtime; 3. This is interfering with their wishes/having social impact. 3. Concomitant medications will be allowed, though dosages will be required to remain fixed throughout participation in the study. 4. The participant also needs to be willing and able to comply with all aspects of the protocol. Exclusion Criteria: 1. Clinically significant depression (PHQ-9 score of 10 or more), anxiety disorder (GAD-7 score of 10 or more), substance use disorder, any other sleep disorder (assessed by the Alliance Sleep Questionnaire- ASQ), or any medical disorder/therapy that could interfere with the trial (this will be verified through interview and analysis of the ASQ). 2. Use of medications with significant effects on sleep-wake function (insomnia therapies, stimulants)- unless they are discontinued at least 5 half-lives prior to study participation. Non-sedative antidepressants or SSRI will be allowed if at a stable dose in the absence of concomitant severe depression or severe anxiety. 3. Use of CYP3A inhibitors and CYP3A inducers, at least 1 week (or five half-lives, whichever is longer) prior to the first day of the baseline phase. 4. Pregnancy (verified by urine pregnancy test on visits 1, 2, and 3) or plan to become pregnant in the next 3 months or currently breastfeeding. 5. Shift workers or subjects working unusual hours. 6. Any risk of suicide within 6 months of screening period or throughout the trial (accessed by the Investigator and by the C-SSRS questionnaire). 7. Transmeridian travel across more than 3 time zones 4 weeks prior to the screening phase. 8. Transmeridian travel across more than 2 time zones during this trial (including the screening phase). 9. Having a positive drug test or being unwilling to refrain from using illegal drugs or marijuana during this trial. 10. Any clinically abnormal symptom or organ impairment found by medical history at Screening or Baseline and physical examinations, vital signs, ECG findings, or laboratory test results that require medical treatment. 11. Impaired liver function (values for enzymes aspartate transaminase (AST) and alanine transaminase (ALT) > 1.5 times the Upper Limit of Normal). 12. Known to be human immunodeficiency virus positive. 13. Has a QT interval corrected using Fridericia's formula interval (QTcF interval) >450 ms demonstrated on repeated ECGs (repeated only if initial ECG showed corrected QT interval (QTc) >450 ms) at Screening or Baseline.

Study Design

Related Conditions & MeSH terms

Intervention

Drug:
Lemborexant
Lemborexant tablet administered orally once daily.
Placebo
Placebo to match Lemborexant tablet administered orally once daily.

Locations
Country Name City State
United States Stanford Univeristy Redwood City California

Sponsors (2)
Lead Sponsor Collaborator
Stanford University University of California, San Francisco

Country where clinical trial is conducted

United States, 

Outcome
Type Measure Description Time frame Safety issue
Primary Change in actigraphy sleep latency onset Sleep latency is the time from laying down until falling asleep. Actigraphy data obtained using Axivity- AX6. From 2 weeks prior to randomization to 4 weeks post randomization
Secondary Change in Epworth Sleepiness Scale (ESS) This is a scale to evaluate daytime sleepiness. Range from 0 to 24 points (higher scores mean more sleepiness). From randomization to 4 weeks post randomization
Secondary Change in Karolinska Sleepiness Scale (KSS) Self-report for daytime sleepiness with 1 being extremely alert and 10 being extremely sleepy, can't keep awake. From randomization to 4 weeks post randomization
Secondary Change in sleep diary derived sleep onset latency Sleep latency is the time from laying down until falling asleep as estimated by patient in dairy. From 2 weeks prior to randomization to 4 weeks post randomization
Secondary Sleep Regularity Index Sleep Regularity Index is defined as the percentage probability of a person being asleep (or awake) at any two time points 24 hours apart. Actigraphy data obtained using Axivity- AX6. From 2 weeks prior to randomization to 4 weeks post randomization
Secondary Change in actigraphy derived total sleep time Actigraphy data obtained using Axivity- AX6. From 2 weeks prior to randomization to 4 weeks post randomization
Secondary Change in sleep diary derived total sleep time. Estimated by patient in dairy. From 2 weeks prior to randomization to 4 weeks post randomization
Secondary Change in mean actigraphy derived wake time Wake time is total time awake over night after sleep onset. Actigraphy data obtained using Axivity- AX6. From 2 weeks prior to randomization to 4 weeks post randomization
Secondary Change in mean sleep diary derived wake time Wake time is total time awake over night after sleep onset as estimated by patient in dairy. From 2 weeks prior to randomization to 4 weeks post randomization
See also
  Status Clinical Trial Phase
Completed NCT00834886 - Randomized Controlled Trial on the Treatment Effects of Melatonin and Light Therapy on Delayed Sleep Phase Syndrome Phase 4
Not yet recruiting NCT02962037 - Are Patients Suffering From DSPS Show Compromising in Everyday Functions and Abilities Before Handling the Disorder? Phase 4
Recruiting NCT04690504 - Validation of Circadian Biomarkers in Patients With Sleep Disorders
Recruiting NCT04792697 - Experimental Manipulation of Sleep and Circadian Rhythms and the Role Played on Reward Function in Teens N/A
Recruiting NCT03956745 - Biomarkers for Circadian Timing in Healthy Adults
Active, not recruiting NCT03980340 - Breath Biomarkers for Sleep Loss and Circadian Timing
Completed NCT03715465 - The Clinical Utility of Measuring the Circadian Clock in Treatment of Delayed Sleep-Wake Phase Disorder Phase 3
Completed NCT01419938 - Does Cognitive Behaviour Therapy (CBT) Improve the Effect of Light Therapy N/A
Recruiting NCT00282061 - Synchronization and Desynchronization Between Circadian Rhythms in Patients With Delayed Sleep Phase Syndrome (DSPS) Phase 1