Targeted Precision Nutrition Strategy To Prevent Chronic Metabolic Diseases

NCT ID: NCT06923644

Last Updated: 2026-01-20

Basic Information

• Recruitment Status: RECRUITING
• Clinical Phase: NA
• Total Enrollment: 240 participants
• Study Classification: INTERVENTIONAL
• Study Start Date: 2025-04-23
• Study Completion Date: 2027-04-30

Brief Summary

Nutrition is very important to keep blood sugar levels balanced. If blood sugar levels are too high, it can lead to diseases such as cardiovascular disease and type 2 diabetes (T2DM). Therefore, adjusting what one eats, also called a diet or nutritional intervention, can help prevent these diseases. However, not everyone responds the same to a diet. In about 30% of people, a diet does not work as hoped. This can be due to various reasons, such as a person's metabolism, genetic predisposition, the composition of the food one eats, or the bacteria in the intestines. Everyday things like sleep, stress, and movement also play a role. The investigators used a computer model to classify people with overweight and obesity into groups based on these factors. The investigators call such a group a 'Metabolic Phenotype', or in short 'Metabotype'. Based on the Metabotype, a personalised diet was developed (personalised nutrition intervention) that may better suit each person's unique situation.

The investigators hypothesize that a precision nutrition intervention, tailored to Metabotypes identified through unsupervised clustering (using the aforementioned computer model) of predefined, accurate features related to cardiometabolic health-specifically, tissue-specific glucose and lipid metabolism and detailed body composition-will enhance blood glucose homeostasis, reduce cardiometabolic risk, and improve adherence to the intervention and mental well-being, compared to population-based dietary guidelines. The present project will contribute to targeted and efficient precision-based dietary strategies for individuals at increased risk of T2DM.

Detailed Description

Objective:

Our study aims to identify unique Metabotypes among individuals with overweight and obesity and assess their response to a 1-year precision dietary macronutrient modulation. The objective is to provide proof-of-concept that this approach improves glucose homeostasis, dietary adherence, and psychosocial well-being compared to population-based dietary guidelines.

Study design:

Two-centre dietary intervention study with a double-blind, randomised controlled parallel design, based on participants' Metabotype and hypothesized optimal diet. Participants' Metabotype and intervention arm will be blinded to the participants and researchers. Metabotypes were identified through hierarchical clustering of Principal Components (HCPC) using baseline data from The Maastricht Study (participant demographics, body composition, glucose- and insulin metabolism), whereafter clusters were cross-validated in independent cohorts. Based on a combination of post-hoc analyses of dietary intervention trials and literature, the optimal dietary macronutrient composition was determined for these Metabotypes.

Study population:

In total 240 men and women with overweight and obesity (age 40-75 years, BMI 25-40 kg/m2) will be included. Further details on in- and exclusion criteria will be described under ''Eligibility''. Following screening and baseline measurements, for each eligible participant, a classification algorithm will determine the participants' Metabotype cluster (one of three possible Metabotypes for each sex).

Intervention:

Following screening, baseline measurements, and determination of Metabotype, participants will be randomly assigned, using minimization, to either the Precision Nutrition (PN) group or the Control (CN) group. The PN group will receive a hypothesized optimal diet for their specific Metabotype, while the control group will be randomly assigned one of the diets optimized for a different Metabotype of the same sex. All participants will follow their assigned diets for 12 months, with each diet conforming to the Dutch healthy dietary guidelines. Participants will receive regular dietary consultation, and meal plans including variation lists to guide them with their dietary intake during the intervention.

Main study parameters/endpoints:

Extensive characterization will be done before, during, and after the intervention. Primary outcome measure is whole-body insulin sensitivity (Matsuda index) assessed by means of a 7-point oral glucose tolerance test (OGTT). Secondary outcomes include glycaemic variability, mean glucose levels, fasting lipid profiles, body composition, blood pressure, gene and protein expression of adipose tissue, microbial composition and functionality, metabolomics, physical activity, adherence to dietary recommendations, (mental) well-being, and quality of life.

Conditions

Obesity and Overweight; Pre-diabetic; Type 2 Diabetes Mellitus (T2DM)

Study Design

• Allocation Method: RANDOMIZED
• Intervention Model: PARALLEL
• Primary Study Purpose: PREVENTION
• Blinding Strategy: DOUBLE

Study Groups

Precision Nutrition Group (PN)

For a total duration of 12 months, participants in the Precision Nutrition (PN) Group will follow a diet tailored to their Metabotype, which is hypothesised to be optimal for them.

Group Type: EXPERIMENTAL

Optimal Metabotype-specific diet

Intervention Type: OTHER

Following screening, baseline measurements, and determination of Metabotype, participants will be randomly assigned, using minimisation, to either the Precision Nutrition (PN) group or the Control (CN) group. The PN group will receive a diet hypothesised to be optimal for their specific Metabotype. All participants will adhere to their assigned diets for 12 months. Each Metabotype-specific diet will align with the Dutch Healthy Dietary Guidelines, while varying in macronutrient composition and quality.

Control Group (CN)

For a total duration of 12 months, participants in the Control Group (CN) will be randomly assigned one of the diets optimised for a different Metabotype of the same sex, which is hypothesised to be suboptimal for them.

Group Type: EXPERIMENTAL

Sub-optimal diet

Intervention Type: OTHER

Participants randomised to the Control Group (CN), will be randomly assigned one of the two diets optimised for a different Metabotype of the same sex. The assigned CN Group diet will always have a macronutrient content and quality that is different than their hypothesised optimal diet. All diets will align with the Dutch Healthy Dietary Guidelines.

Interventions

Optimal Metabotype-specific diet

Following screening, baseline measurements, and determination of Metabotype, participants will be randomly assigned, using minimisation, to either the Precision Nutrition (PN) group or the Control (CN) group. The PN group will receive a diet hypothesised to be optimal for their specific Metabotype. All participants will adhere to their assigned diets for 12 months. Each Metabotype-specific diet will align with the Dutch Healthy Dietary Guidelines, while varying in macronutrient composition and quality.

Intervention Type: OTHER

Sub-optimal diet

Participants randomised to the Control Group (CN), will be randomly assigned one of the two diets optimised for a different Metabotype of the same sex. The assigned CN Group diet will always have a macronutrient content and quality that is different than their hypothesised optimal diet. All diets will align with the Dutch Healthy Dietary Guidelines.

Intervention Type: OTHER

Eligibility Criteria

Inclusion Criteria

• Men and women with a BMI ≥25 to <40 kg/m2
• Classification possible to one of the investigational metabolic phenotypes according to the classification algorithm.
• Weight stability for at least 3 months (+/- 3 kg)

Exclusion Criteria

Diseases

• (Pre-)diagnosis of type 1 or type 2 diabetes mellitus (i.e., FPG ≥ 7,0 mmol/L) and HbA1c ≥ 6,5% (48 mmol/mol)
• Renal or hepatic malfunctioning (pre-diagnosis or determined based on ALAT and creatinine values)
• Gastrointestinal diseases or abdominal surgery (allowed i.e.:

appendectomy, cholecystectomy)

• Food allergies, intolerances (including gluten/lactose intolerance) and/or eating disorders interfering with the study
• Cardiovascular diseases (e.g., heart failure) or cancer (e.g., noninvasive skin cancer allowed)
• High systolic blood pressure (untreated >160/100 mmHg, drug-regulated >140/90 mmHg)
• Diseases affecting glucose and/or lipid metabolism (e.g., pheochromocytoma, Cushing's syndrome, acromegaly)
• Diseases with a life expectation shorter than 5 years
• Major mental disorders
• Drug treated thyroid diseases (well substituted hypothyroidism is allowed inclusion)
• Other physical/mental conditions that may interfere with study outcomes

Medication

• Medication known to interfere with study outcomes (e.g., PPAR-α or PPAR-γ agonists (fibrates), sulfonylureas, biguanides, α-glucosidaseinhibitors, thiazolidinediones, repaglinide, nateglinide, insulin, and chronic use of NSAIDs)
• Use of certain anticoagulants other than acetylsalicylic acid
• Use of antidepressants (stable use ≥ 3 months prior to and during study allowed)
• Use of statins (stable use ≥ 3 months prior to and during study allowed)
• Chronic corticosteroids treatment (>7 consecutive days of treatment)
• Use of antibiotics within 3 months prior to the study

Lifestyle

• Participation in regular sports activities (moderate-to-vigorous physical exercise >4 hours per week)
• Having a restricted dietary pattern interfering with the study diets (e.g., vegetarian, vegan, Atkins diet and/or other special diets)
• Plans to lose or gain more than 5% body weight
• Abuse of alcohol (alcohol consumption >14 units/week) and/or drugs (cannabis included)
• Not willing to limit alcohol consumption to 7 drinks per week
• Regular smoking (including use of e-cigarettes and vapes)
• Use of strong vitamins or other dietary supplements (e.g., pre- or probiotics) expected to interfere with the study outcomes

Other

• Metabotype classification is not possible
• Pregnant or lactating women, or women who are planning to become pregnant
• Inability to comply with the study diet
• Blood donation within the last 3 months
• Participation in possibly interfering studies within the last 3 months
• Inability to understand study information and/or communicate with staff
• Unwillingness to be randomised or sign informed consent
• Unwillingness to save data for 15 years
• Deemed unsuitable for participation in the trial, for any reason, as judged by the research physician or principal investigator

• Minimum Eligible Age: 40 Years
• Maximum Eligible Age: 75 Years
• Eligible Sex: ALL
• Accepts Healthy Volunteers: Yes

Sponsors

Wageningen University and Research

OTHER

Sponsor Role: collaborator

Health Holland

OTHER

Sponsor Role: collaborator

TKI Agri & Food

UNKNOWN

Sponsor Role: collaborator

Nestle Health Science

INDUSTRY

Sponsor Role: collaborator

Beneo GmbH

INDUSTRY

Sponsor Role: collaborator

BARILLA G. e R. Fratelli S.p.A., Parma, Italy

UNKNOWN

Sponsor Role: collaborator

Maastricht University Medical Center

OTHER

Sponsor Role: lead

Responsible Party

Responsibility Role: SPONSOR

Principal Investigators

Ellen E Blaak, Prof. Dr. Ir.

Role: PRINCIPAL_INVESTIGATOR

Maastricht University Medical Center

Locations

Maastricht University Medical Center, Department of Human Biology, NUTRIM Institute of Nutrition and Translational Research in Metabolism

Maastricht, , Netherlands

Site Status: RECRUITING

Wageningen University and Research, Division of Human Nutrition

Wageningen, , Netherlands

Site Status: RECRUITING

Countries

Netherlands

Central Contacts

Ellen E Blaak, Prof. Dr. Ir.

Role: CONTACT

e.blaak@maastrichtuniversity.nl

+31433881503

Art Muijsenberg, MSc

Role: CONTACT

art.muijsenberg@maastrichtuniversity.nl

+31433882862

Facility Contacts

Ellen E Blaak, Prof. Dr. Ir.

Role: primary

e.blaak@maastrichtuniversity.nl

+31433881503

Art Muijsenberg, MSc

Role: backup

art.muijsenberg@maastrichtuniversity.nl

+31433882862

Lydia A Afman, Prof. Dr. Ir.

Role: primary

lydia.afman@wur.nl

+31(0)31 74 85789

Milena Banic, PhD

Role: backup

milena.banic@wur.nl

+31618713321

Other Identifiers

NL87817.068.24

Identifier Type: -

Identifier Source: org_study_id