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This will be a double-blind, placebo-controlled, parallel-group trial. Participants who are poor sleepers will be randomised to receive one of two investigational supplements, or a placebo control supplement, over a 28-day period. At baseline and following 28 days of consumption, sleep quality, gut microbiome profiles, cognitive performance, and mood will be assessed. Sleep outcome measures will also be assessed throughout the supplementation period to monitor the time course of any observed changes. A final data set of at least 66 participants is expected.
This will be a double-blind, placebo-controlled, parallel-group trial. Participants who are poor sleepers will be randomised to receive one of two investigational supplements, or a placebo control supplement, over a 28-day period. At baseline and following 28 days of consumption, sleep quality, gut microbiome profiles, cognitive performance, and mood will be assessed. Sleep outcome measures will also be assessed throughout the supplementation period to monitor the time course of any observed changes. A final data set of at least 66 participants is expected.
Interested participants will initially be scheduled to complete a screening telephone call with the researcher. Here, electronic informed consent will first be provided by the participant, by accessing a pre-emailed link to the Qualtrics survey platform, to an account which is hosted by Northumbria University. Once consent is obtained, the participant will confirm that they do not meet any of the study exclusion criteria, and will complete the SDS-CL checklist with the researcher, over the phone. If any clinical thresholds are met, participants will be invited to a separate clinical interview (again via phonecall) with Professor Jason Ellis, employing the International Classification of Sleep Disorders (ICSD-3) criteria, to determine elligibility.
If participants progress to enrolment, they will be invited to attend a lab-based training/screening session (protocol day -7) at Northumbria University. Here, hard and wet-signed (by both the participant and the researcher) consent forms will be completed and stored on site. Participants will then be familiarised with the study protocol and procedures. Participants will also be trained on the cognitive tasks. During the following 7 nights (Protocol days -7 to -1), participants will monitor their sleep and complete the daily Sleep Diary each morning. During this week, they will also drop off their pre-dose baseline stool sample at a remote drop-off location at Northumbria University.
Seven days following the lab-based screening visit (Supplement day 1, Protocol day 0), participants will attend the laboratory for their acute visit. Here, a pre-dose baseline sample of saliva and a single blood sample will be taken (for Alpha Amylase, Cortisol, Serotonin and Melatonin), and Blood Pressure, Heart Rate, Body Mass Index, and Waist-to-Hip Ratio will be measured. Participants will complete the Intake24 dietary assessment, and gastrointestinal symptoms questionnaires, as well as the Pittsburgh Sleep Quality Index (PSQI), State-Trait Anxiety Inventory (STAI), and Depression, Anxiety and Stress Scale - 21 Items (DASS-21). The cognitive task battery will additionally be completed.
After completing these measures, participants will receive instructions on the next phase of the trial. From that night, participants will consume their first dose of the investigational supplement (noting the time in their treatyment diary) 4 hours before their normal bed-time. They will monitor their sleep overnight. The following morning (supplementation day 2, protocol day 1), participants will complete their Sleep Diary. Participants will follow this procedure for the following 27 days. At some point during Protocol (Days 12-18), participants will return to Northumbria University to drop-off their interim stool sample.
On Protocol day 28, participants will return to the lab for the chronic testing visit. All of the outcome measures assessed during the acute lab visit (Protocol day 0) will be repeated here. At the end of the session, participants will be debriefed, and their participation payment arranged. At some point during Protocol (Days 27-33) participants will return to Northumbria University to drop-off their chronic stool sample.
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| Label | Type | Description | Intervention Names |
|---|---|---|---|
| Arm 1 | Experimental | Participants will be randomly allocated to consume investigational supplement (1 of 2 proprietary 'active' compositions) for 28 days. |
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| Arm 2 | Experimental | Participants will be randomly allocated to consume investigational supplement (1 of 2 proprietary 'active' compositions) for 28 days. |
|
| Control | Placebo Comparator | Participants will be randomly allocated to consume control supplement for 28 days. |
|
| Name | Type | Description | Arm Group Labels | Other Names |
|---|---|---|---|---|
| Proprietary 'active' composition 1 | Dietary Supplement | A proprietary orally administered dietary supplement consisting of standardized ingredients. |
|
| Measure | Description | Time Frame |
|---|---|---|
| Sleep Efficiency (SE) | Sleep efficiency (SE), commonly defined as the ratio of total sleep time (TST) to time in bed (TIB), will be reported as a percentage of time in bed. | Change from Baseline to end of supplementation period at 28 days |
| Measure | Description | Time Frame |
|---|---|---|
| Actigraphy - Sleep onset latency | recorded minutes taken from intention to sleep to sleep initiation | Change from baseline following 28 days of supplement consumption |
| Actigraphy - Sleep efficiency |
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INCLUSION CRITERIA
EXCLUSION CRITERIA
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| Name | Role | Phone | Extension | |
|---|---|---|---|---|
| Pamela Alfonso-Miller, MD | Contact | +44 01912274149 | pam.alfonso-miller@northumbria.ac.uk |
| Name | Affiliation | Role |
|---|---|---|
| Professor Jason Ellis, PhD | Northumbria University | Principal Investigator |
| Facility | Status | City | State | ZIP | Country | Contacts |
|---|---|---|---|---|---|---|
| Northumbria University- Northumbria Sleep center and NUTRAN | Newcastle upon Tyne | United Kingdom |
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| Proprietary 'active' composition 2 | Dietary Supplement | A proprietary orally administered dietary supplement consisting of standardized ingredients. |
|
| Inactive control supplement | Dietary Supplement | Flavored vehicle |
|
ratio of the total time spent asleep (total sleep time) in a night compared to the total amount of time spent in bed (percentage)
| Change from baseline following 28 days of supplement consumption |
| Actigraphy - Number of awakenings | recorded number of awakenings during entire sleep period | Change from baseline following 28 days of supplement consumption |
| Actigraphy - Wake after sleep onset (WASO) | recorded minutes awake during the entire sleep period following sleep onset | Change from baseline following 28 days of supplement consumption |
| COMPASS global performance measures | Speed of performance, and accuracy of performance measured by Computerised Mental Performance Assessment System (COMPASS, Northumbria University) | Change from baseline following 28 days of supplement consumption |
| Pittsburgh Sleep Quality Index (PSQI) | Pittsburgh Sleep Quality Index (PSQI): Total Score. The PSQI is a validated self-rating instrument assessing aspects of sleep quality.Minimum score 0 (better); maximum score 21 (worse) < or = 5 associated with good sleep quality; > 5 associated with poor sleep quality. | Change from baseline following 28 days of supplement consumption |
| Depression, Anxiety and Stress Scale - 21 Items (DASS-21) | A 21-item measure of mood over the previous week (each item is rated on scale from 0-3). Scoring creates 3 component scores: depression, anxiety and stress (each on a scale of 0-21) with higher scores indicating higher symptomology. Cut-off scores, according to each set of symptoms, are available (normal, mild, moderate, severe and extremely severe) or total scores can be derived by multiplying the sum of all three component scores by 2. | Change from baseline following 28 days of supplement consumption |
| State-Trait Anxiety Inventory (STAI) | A 40-item measure of current and general anxiety levels. Each item is rated on a scale from 1-4. Scoring creates two components: state anxiety (20 items) and trait anxiety (20 items), with a range for each between 20-80. Following transformation through reversed coding, higher scores indicate higher levels of anxiety | Change from baseline following 28 days of supplement consumption |
| Actigraphy - Total sleep time | recorded minutes asleep over entire sleep period | Change from baseline following 28 days of supplement consumption |
| Sleep Diary - Total sleep time | recorded minutes asleep over entire sleep period | Change from baseline following 28 days of supplement consumption |
| Sleep Diary - Sleep onset latency | logged minutes taken from intention to sleep to sleep initiation | Change from baseline following 28 days of supplement consumption |
| Sleep Diary - Sleep efficiency | ratio of the total time spent asleep (total sleep time) in a night compared to the total amount of time spent in bed (percentage) | Change from baseline following 28 days of supplement consumption |
| Sleep Diary - Number of awakenings | logged number of awakenings during entire sleep period | Change from baseline following 28 days of supplement consumption |
| Sleep Diary - Wake after sleep onset (WASO) | logged minutes awake during the entire sleep period following sleep onset | Change from baseline following 28 days of supplement consumption |