0002 24-hour Variation in Metabolic Responses to a 6.5-Hour Meal Window in Humans

Authors

Leilah Grant, Brigham and Women's Hospital
Kritika Vashishtha, Brigham and Women's Hospital
Shauni Omond, Brigham and Women's Hospital, Harvard Medical School
Lauren McKenzie, Brigham and Women's Hospital
Melissa St. Hilaire, Merrimack CollegeFollow
Steven W. Lockley, Brigham and Women's Hospital
Shadab A. Rahman, Harvard Medical School

Document Type

Conference Proceeding

Publication Title

SLEEP

Publication Date

5-2025

Meeting Name

39th Annual Meeting of the Associated Professional Sleep Societies

Meeting Date

June 7-11

Meeting Location

Seattle

Abstract/ Summary

Introduction

Meal timing influences human health. For example, compared to eating during the day, eating identical meals at night acutely elevates levels of glucose and triglycerides. While most studies have compared single meals given at two distinct (often opposite) times of day, the timecourse of the 24-hour variation in metabolic responses to meals is unknown. The aim of this study was to examine systematically how the timing of meals across the 24-hour circadian cycle influences daily exposure to triglycerides, triglyceride-rich lipoproteins [remnant cholesterol (remnant-C)] and glucose.

Methods

Ten healthy adults (6 female) aged 22-35 years were randomized to a 16-hour intervention ‘day’ in dim light (< 3 lux) between two 8-h sleep episodes in darkness, with a 6.5-hour meal window in the center of the day scheduled at one of 16 stimulus times distributed every 90-minutes (~22.5 degrees) across the 24-hour day between participants. A 26–48.5-h constant routine (CR) with hourly identical meals preceded the intervention day. Blood samples collected every 20-60 minutes throughout the CR and intervention day were assayed for triglyceride, remnant-C and glucose. The 24-h area under the curve (AUC) of the intervention day was calculated and expressed relative to the first 24-h AUC of the CR to control for interindividual differences in metabolic analyte levels. Mealtime response curves were generated by analyzing the relative AUC by the clock time of meal onset using a single-harmonic sinusoidal regression.

Results

Significant mealtime response curves were generated for triglycerides (p< 0.05), remnant-C (p< 0.01) and glucose (p< 0.001). The fitted curve for the 24-h AUC showed that daily levels were lowest when eating during daytime hours for triglyceride and remnant -C, which were lowest when eating at ~7pm, and glucose, which was lowest at ~9am.

Conclusion

The timing of meals across the 24-hour day alters daily exposure to triglycerides, triglyceride-rich lipoproteins, and glucose, with generally worse metabolic responses when the eating window started at night compared to the day. These mealtime response curves can inform practical advice on timing diet-based interventions to reduce cardiometabolic health risks, particularly in shift workers and others who eat at night.