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Clinical Trial Details — Status: Recruiting

Administrative data

NCT number NCT06061042
Other study ID # NL79197.018.21
Secondary ID
Status Recruiting
Phase N/A
First received
Last updated
Start date October 2023
Est. completion date December 2027

Study information

Verified date February 2023
Source Academisch Medisch Centrum - Universiteit van Amsterdam (AMC-UvA)
Contact Jur Kroon, BSc
Phone +31 683238752
Email jur.kroon@amsterdamumc.nl
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

We aim to determine the effect of combined isocaloric time restricted eating and meal timing on metabolic health, liver fat, functional brain networks, inflammation, and sleep pattern/quality in subjects with obesity and insulin resistance.


Description:

Obesity is an alarming global health issue, with increasing prevalence. Obesity leads to a vast array of disorders, including dyslipidemia, the accumulation of intrahepatic triglycerides (IHTG), multiorgan insulin resistance and type 2 diabetes mellitus. In addition, disruption of the circadian rhythm (circadian misalignment), which is associated with irregular eating schedules, is an important risk factor for the development of obesity, IHTG and type 2 diabetes mellitus. Time restricted eating (TRE) is a form of intermittent fasting, in which the daily eating period is restricted. The beneficial effect of this type of diet might relate to adequate synchronization of food intake and fasting to the internal rhythm of the circadian tissue clocks, improving metabolic handling of nutrients and metabolic flexibility.


Recruitment information / eligibility

Status Recruiting
Enrollment 30
Est. completion date December 2027
Est. primary completion date December 2027
Accepts healthy volunteers Accepts Healthy Volunteers
Gender All
Age group 50 Years to 75 Years
Eligibility Inclusion Criteria: - Ability to provide informed consent; - BMI > 30kg/m^2; - Insulin resistance, as defined by fasting plasma insulin > 62 pmol/L and/or prediabetes, as defined by fasting plasma glucose > 5.3 and < 7.0 mmol/L; - Stable weight for 3 months prior to study inclusion - For women, 1 year after last menstrual cycle Exclusion Criteria: - Use of any medication, except for those related to treatment of metabolic syndrome; - Any medical condition interfering with study outcomes or design; - History of any psychiatric disorder, including eating disorders; - Performing shift work - Performing intensive sports (>3 hours/week); - Smoking; - Drugs abuse or alcohol abuse (>3 units/day); - Contraindication for MRI; - Known lactose/gluten intolerance; - Known soy, egg, milk or peanut allergy; - Childhood onset of obesity

Study Design


Related Conditions & MeSH terms


Intervention

Behavioral:
Early time restricted eating
Subjects will follow an isocaloric diet, designed by a dietician. The eating window for the early-TRE group is between 7 AM - 5 PM
Late time restricted eating
Subjects will follow an isocaloric diet, designed by a dietician. The eating window for the late-TRE group is between 10 AM - 8 PM

Locations

Country Name City State
Netherlands Amsterdam UMC, location AMC Amsterdam Noord-Holland

Sponsors (2)

Lead Sponsor Collaborator
Academisch Medisch Centrum - Universiteit van Amsterdam (AMC-UvA) Diabetesfonds

Country where clinical trial is conducted

Netherlands, 

Outcome

Type Measure Description Time frame Safety issue
Primary Insulin Sensitivity We will use the Oral Minimal Model Method in conjunction with a Mixed Meal Tolerance Test (MMTT) to quantitatively evaluate insulin sensitivity. Concentrations of insulin, glucose, and C-peptide will be measured during the course of the MMTT to serve as the requisite inputs for the model. The output is in dl/kg/min/uU/ml. Baseline 1 and week 4 for intervention 1; Baseline 2 and week 12 for intervention 2
Secondary Change in plasma insulin Fasted and stimulated insulin (pmol/L) will be measured during MMTT Baseline 1 and week 4 for intervention 1; Baseline 2 and week 12 for intervention 2
Secondary Change in plasma glucose Fasted and stimulated glucose (mmol/L) will be measured during MMTT Baseline 1 and week 4 for intervention 1; Baseline 2 and week 12 for intervention 2
Secondary Change in intrahepatic fat To quantify the intrahepatic fat content, a single voxel 1H-MRS (magnetic resonance spectroscopy) will be used. Relative fat content will be expressed as the ratio of the fat peak over the cumulative fat and water peak. This will also be corrected for T2 relaxation. Baseline 1 and week 4 for intervention 1; Baseline 2 and week 12 for intervention 2
Secondary Change in beta cell function (C-peptide) Fasted and stimulated C-peptide (nmol/L) will be measured during MMTT Baseline 1 and week 4 for intervention 1; Baseline 2 and week 12 for intervention 2
Secondary Change in insulin aignaling Biopsies will be taken from skeletal muscle and subcutaneous fat to measure key proteins in the insulin signalling pathway (Western blots) Baseline 1 and week 4 for intervention 1; Baseline 2 and week 12 for intervention 2
Secondary Change in glucose variability In our study, we will deploy Continuous Glucose Monitors (CGMs) to acquire an in-depth understanding of glucose variability in participants throughout the course of the intervention. These monitors gauge glucose concentrations in the interstitial fluid (mmol/L), serving as a reliable proxy for blood glucose levels. This approach will enable us to assess key metrics such as mean, minimum and maximum glucose levels. Baseline 1 to week 4 for intervention 1, Baseline 2 to week 12 for intervention 2
Secondary De novo lipogenesis Fasted and stimulated de novo lipogenesis (DNL) will be measured during the MMT as 2H incorporation into fatty acids following deuterated water (2H2O) administration Baseline 1 and week 4 for intervention 1; Baseline 2 and week 12 for intervention 2
Secondary Immunological markers We will conduct immune cell phenotyping on whole blood samples to identify and categorize various immune cell types. Additionally, we will assess immune cell function and metabolism in isolated peripheral blood mononuclear cells (PBMCs). Inflammatory markers will also be assessed in serum samples to provide a comprehensive overview of immune and inflammatory status. Baseline 1 and week 4 for intervention 1; Baseline 2 and week 12 for intervention 2
Secondary Physical activity Physical activity will be assessed via accelerometry. Accelerometry represents the magnitude of acceleration in any direction, over a predefined epoch. Baseline 1 to week 4 for intervention 1, Baseline 2 to week 12 for intervention 2
Secondary Functional brain activity Brain activation maps and functional connectivity will be assessed by blood oxygen dependent signals in the resting state and after visual food cues using functional magnetic resonance imaging (fMRI). Baseline 1 and week 4 for intervention 1; Baseline 2 and week 12 for intervention 2
Secondary Psychological factor - Food Craving We will use the General Food Cravings Questionnaire (G-FCQ) to evaluate the frequency and intensity of food cravings among participants. The scoring for the G-FCQ ranges between 21 and 105, with higher scores indicative of more pronounced food craving tendencies. Baseline 1 and week 4 for intervention 1; Baseline 2 and week 12 for intervention 2
Secondary Psychological factor - Eating behaviour We will utilize the Dutch Eating Behavior Questionnaire (NVE) to assess and categorize the eating behaviors and tendencies of our participants. The NVE discerns three distinct eating styles: emotional eating, external eating, and restrained eating. A higher score within a specific style suggests a predominant inclination towards that particular eating behavior. Baseline 1 and week 4 for intervention 1; Baseline 2 and week 12 for intervention 2
Secondary Psychological factor - Hunger scale We will employ a nine-question visual analogue scale (VAS) to assess hunger. Each question will be scored 0-100. Baseline 1 and week 4 for intervention 1; Baseline 2 and week 12 for intervention 2
Secondary Psychological factor - Food addiction We will use the Yale Food Addiction Scale 2.0 (YFAS 2.0) to assess addictive behaviours. The YFAS 2.0 is designed in accordance with the DSM-5 criteria, and its scoring system mirrors the number of DSM-5 criteria fulfilled indicative of addiction. Baseline 1 and week 4 for intervention 1; Baseline 2 and week 12 for intervention 2
Secondary Psychological factor - Impulsiveness We will use the Barratt Impulsiveness Scale (BIS) to scale impulsiveness towards food. This will help us understand how impulsivity might influence dietary behaviour. The score ranges from 30-120 and a higher score leans towards greater impulsivity. Baseline 1 and week 4 for intervention 1; Baseline 2 and week 12 for intervention 2
Secondary Psychological factor - Chronotype To determine natural sleep-wake patterns, we will use the Munich Chronotype Questionnaire (MCTQ). This tool offers a comprehensive understanding of sleep behaviors, revealing a chronotype. Baseline 1 and week 4 for intervention 1; Baseline 2 and week 12 for intervention 2
Secondary Subject experience with intervention We will employ a semi-structured oral interview as part of our qualitative approach to understand our participants' experience and adherence to the intervention. Baseline 1 and week 4 for intervention 1; Baseline 2 and week 12 for intervention 2
Secondary Delay discounting computational task The delay discounting task aids in understanding the decision-making processes that might contribute to overeating and poor food choices. In this task, we will be able to measure the ability of each individual to delay immediate gratification for a greater future reward. Baseline 1 and week 4 for intervention 1; Baseline 2 and week 12 for intervention 2
Secondary Iowa gambling computational task We use the Iowa gambling task to assess decision-making and risk-reward sensitivity. Participants choose cards from four decks, each with different reward and punishment rates, aiming to maximize their winnings. We use this task to study risk taking and impulsive behaviour. Baseline 1 and week 4 for intervention 1; Baseline 2 and week 12 for intervention 2
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