Sleep requirements change across the lifespan and quality of sleep declines as we age^{(Reference Madrid-Valero, Martínez-Selva and Couto1)}. Poor sleep across adulthood has been associated with ramifications on subjective health, quality of life^{(Reference Magee, Caputi and Iverson2)} and advancement of cognitive decline and dementia^{(Reference Hudon, Escudier and De Roy3)}. Among the modifiable factors that are posited to contribute to sleep quality, diet and nocturnal metabolism are thought to be strong predictors of sleep quality^{(Reference St-Onge, Mikic and Pietrolungo4)}.

The aim of the current study was to evaluate the effectiveness of nutritional formulation (delivered in a powdered- based drink) containing 0.75 g Mulberry Leaf Extract (0.75g) and a natural source of Tryptophan (120mg) consumed concurrently with an evening-meal (Glycemic load of 55 ± 10%) to promote better sleep and next-day mood and cognitive performance in healthy adult poor sleepers.

The clinical trial was a double-blind, controlled, randomized, 2-arm, sequential groups cross-over design (ClinicalTrials.gov Identifier: NCT05372900). Adult (aged 25–50), self-identified poor sleepers (confirmed by Pittsburg Sleep Quality Index >5 and <85% mean sleep efficiency over 14-days at screening) received standardized meals and concurrent daily intake of the nutritional formulation or placebo approximately 4 hours before bedtime. Intervention phases lasted 14-days with a 28- to 42-day washout period in-between. Primary outcomes were Sleep Efficiency (SE) and Sleep Onset Latency (SOL) measured by actigraphy. Secondary outcomes included inter alia: mood (Brief Mood Introspection Scale), sleep quality (Karolinska Sleepiness Scale) and objective cognitive performance measures (Psychomotor Vigilance Task, 2-back task, NASA Task Load Index) taken at breakfast, lunch and dinner time (1–1.5- hours, 6- and 12-hours post-wake respectively).

Linear mixed model analysis was conducted with intention-to-treat, adjusting for baseline and treatment order for sleep, mood, and cognitive outcomes. Consumption of the active treatment resulted a significant improvement in SOL (actigraphy= -3.48 mins, p = .026; self- report =−16.7mins, p = .031) compared to control. There was no significant effect on SE (p = .230). Sleep and mood self-report measures showed that participants felt significantly less sleepy (p = .041) and more aroused (p = .026) the next morning. Interestingly, cognitive performance was improved on several tests throughout the next day at breakfast, lunch and dinner assessment points: For psychomotor vigilance, reaction time (p = .598, p = .051, p= .024 respectively) and number of lapses, where lapses are characterized as those made within 698 ms (2x median reaction time for the cohort) showed significant improvement (p = .027, p = .005, p = .004 respectively). Participants also reported actively feeling these performance improvements (performance dimension of NASA TLX) following treatment compared to control conditions (p = .014, p = .063, p = .010, respectively).Our findings demonstrate that sleep onset, quality and next day cognitive performance can be ameliorated by a daily dinner time supplemental nutritional intervention and may represent a convenient strategy to support the betterment of sleep and mood and cognitive benefits in adult populations.