FTGO: FIT to Grow Old - Functionality of the Immune System and Healthy Aging

Sponsor

Wageningen University (Other)

Overall Status

Active, not recruiting

CT.gov ID

NCT05940337

Collaborator

Top Consortium for Knowledge and Innovation (TKI) Argi & Food (Other), Mead Johnson Nutrition (Industry), Hycult Biotech (Other)

156

Enrollment

Location

31.6

Anticipated Duration (Months)

4.9

Patients Per Site Per Month

Study Details

Study Description

Brief Summary

Aging is commonly associated with reduced functionality of the immune system, resulting in a higher prevalence of infectious disease, auto-immune disease, cancer, and lower efficiency of vaccination. Nutritional strategies are increasingly recognized as a method to improve immune functionality, as several nutrients are shown to exert immunomodulatory properties. However, the large variation between individuals with regard to immune responses asks for more personalized approaches. Therefore, this field of research would benefit from a selection of those individuals with immune dysfunction. It is recently shown that immune functionality is largely dependent on intracellular metabolism, leading to the introduction of the new term 'immune cell fitness' which combines the metabolic and functional status of an immune cell. Within this study, we will determine the immune cell fitness of monocytes from healthy young adults and elderly subjects by measuring and integrating a broad range of metabolic and functional immune parameters into an immune cell fitness score. We aim to identify those individuals with immune dysfunction, the unfit. Furthermore, to identify potential nutritional strategies to improve immune cell fitness, we will study the effects of metabolites and nutrients on the immune cell fitness status of monocytes from elderly subjects.

Condition or Disease	Intervention/Treatment	Phase
Aging

Detailed Description

Rationale: Aging is commonly associated with reduced functionality of the immune system, resulting in a higher prevalence of infectious disease, auto-immune disease, cancer, and low-er efficiency of vaccination. The reduction in immune functionality is called 'immunosenes-cence' and is often observed in addition to a chronic state of systemic inflammation, referred to as 'inflammaging'. It is commonly believed that strategies improving immune functionality can be applied to improve healthy aging. Nutritional strategies, in particular, receive increasing attention, as several foods and nutrients are shown to exert immunomodulatory properties. Nutritional strategies focussing on the intake of polyunsaturated fatty acids have indeed shown improvements in cytokine profiles and inflammatory gene expression, but suffer from large inter-individual variation, which might be caused by differences in immune functionality. Recent studies within the field of immunometabolism have shown that immune functionality is largely dependent on intracellular metabolism, leading to the introduction of the new term ' immune cell fitness' which combines the metabolic and functional status of an immune cell. To improve the efficiency of immunomodulatory nutritional intervention strategies and work towards personalized approaches to support healthy aging, the identification of individuals with reduced immune cell fitness will be crucial.

Objective: The primary aim of this study is to extensively characterize immune cell fitness in the elderly population in order to distinguish immunologically fit elderly from the unfit. Since immune cell fitness is a new concept, we will define a good immune cell fitness state using a young adult study population. Using a follow-up visit, we will evaluate whether our measure of immune cell fitness is robust and stable over time. Furthermore, to identify potential nutritional strategies to improve immune cell fitness and work towards personalized approaches, we will study the effects of metabolites and nutrients on their ability to improve immune cell fitness in monocytes from the elderly.

Study design: The study will be a cross-sectional study in which we will compare the immune cell fitness state of elderly people using young adult people to define an 'immune fit' status. Immune cell fit-ness will be measured in monocytes, which will be obtained from blood samples. Subjects will be given a standardized meal which they consume in the evening before the study visit at latest 8.00 pm. After consumption of the meal, subjects are not allowed to eat or drink anything but water.

On the study day, before the start of blood sampling, a small blood sample via a finger prick is collected to measure CRP levels. CRP levels of ≥10.0 mg/L are considered to indicate severe infection and will consequently exclude the subject from participating on that specific day. The relevant subjects are asked to make a new appointment. If CRP levels are < 10 mg/L, blood sampling will continue.

Blood sampling and anthropometric measurements including body weight, waist and hip circumference and a DEXA scan will be performed in each subject, after which the subjects will receive breakfast. Subjects will fill in an FFQ to gain insights into regular dietary intake. In addition, subjects will fill in questionnaires on sleep quality and general health.

Elderly subjects will be contacted for a follow-up visit at least 6 months and the latest 18 months after the study visit. The study-design of the follow-up visit will be similar to the first study visit, including the standardized meal the evening before, overnight fast, blood sampling, anthropometric measurements (except for the DEXA-scan, this will only be performed as a link between immune cell fitness and fat distribution is found in the first part of the study), and questionnaires. The freshly collected blood sample will be used for our secondary aims, namely 1) to study the effects of nutrients and metabolites on immune cell fitness, and 2) to test whether our measure of immune cell fitness is robust and stable over time.

Study Design

Study Type:

Observational

Actual Enrollment :

156 participants

Observational Model:

Cohort

Time Perspective:

Cross-Sectional

Official Title:

FIT to Grow Old - Functionality of the Immune System and Healthy Aging

Actual Study Start Date :

Nov 11, 2020

Anticipated Primary Completion Date :

Jul 1, 2023

Anticipated Study Completion Date :

Jul 1, 2023

Arms and Interventions

Arm	Intervention/Treatment
Elderly
Young adults

Outcome Measures

Primary Outcome Measures

Lactate production [1 day]
Lactate excretion by monocytes after ex-vivo exposure to inflammatory stimuli
Cytokine production [1 day]
Cytokine excretion by monocytes after ex-vivo exposure to inflammatory stimuli. Measured using ELISA for IL-6, IL-1b. IL-1RA, IL-8, TNFalpha.

Secondary Outcome Measures

Phagocytosis [1 day]
Phagocytic capacity of monocytes. Measured using absorbed fluorescent beads and flow cytometry.
Glycolytic and oxidative capacity [1 day]
Glycolytic and oxidative capacity of monocytes. Measured using Seahorse Assays (Agilent).

Other Outcome Measures

Circulating immune mediators [1 day]
Circulating cytokines and other immune related markers in plasma
Glucose levels [1 day]
circulating glucose concentration in plasma
Lipid profile [1 day]
Circulating lipids (Triglycerides, HDL and LDL)
Anthropometric measures - body weight [1 day]
Bodyweight in kg
Anthropometric measures - body height [1 day]
bodyheight in cm
Anthropometric measures - WHR [1 day]
waist- and hip-circumference in cm
Anthropometric measures - DEXA [1 day]
Dual Energy Xray absorptiometry to measure fat distribution in percentages of total mass, total body
C-reactive protein [1 day]
Concentrations in whole blood and plasma
Questionnaires - FFQ [1 day]
Food frequency questionnaire. Results are expressed as the average amount of portions consumed weekly for each food group (e.g. bread, spread, snacks, cold meal, warm meal).
Questionnaires - general health [1 day]
General health questionnaires. Questionnaires are translated into Dutch and therefore not validated. Answers will be coded and used for analysis. Some questions include a score from 1 to 5 or 10, where low scores represent bad outcomes or not frequent, and high scores represent good outcomes or frequent.
Questionnaires - sleep quality [1 day]
Sleep quality questionnaires. Questionnaires are translated into Dutch and therefore not validated. Answers will be coded and used for analysis. Some questions include a score from 1 to 5 or 10, where low scores represent bad outcomes or not frequent, and high scores represent good outcomes or frequent.
Gene expression [1 day]
expression of metabolic and inflammatory genes in monocytes and macrophages at baseline and after stimulation with pro-inflammatory mediators. Measured using qPCR and RNAsequencing.

Eligibility Criteria

Criteria

Ages Eligible for Study:

20 Years to 75 Years

Sexes Eligible for Study:

All

Inclusion Criteria:

Age 20 - 30y and 60 - 75y
BMI 18.5 - 25 kg/m2 (young adults); 20 - 30 kg/m2 (elderly)
Willing to fast overnight for 12 hours
Willing to give a blood sample
Having a general practitioner
Signed informed consent

Exclusion Criteria:

Diagnosed with metabolic and/or inflammatory disease (e.g. diabetes, cardiovascular disease (with the exception of hypertension), arthritis, arthrosis, glycogen storage dis-orders and auto-immune diseases)
Current diagnosis of cancer
Regular use of medication that interferes with immune function (e.g. corticosteroids, cytokine blockers)
Regular use of medication that may interfere with metabolism (e.g. metabolic inhibitors or activators)
Use of medication that interferes with immune function and metabolism in at least one week preceding the study visit (e.g. NSAID, anti-histamines, corticosteroids)
More than 4kg weight gain or weight loss over the last 4 months
Vaccination within 3 months preceding the study visit (e.g. immunization against influ-enza, pneumonia, and travel-related infections)
Donated blood within 2 months preceding the study visit
Pregnant, lactating or wishing to become pregnant in the period between the screening and study visit (self-reported)
Regular use of hard drugs and soft drugs (i.e. weekly use) and at least no use within 2 months preceding the study visit
Excessive alcohol use (i.e. >14 units per week)
Use of cigarettes and other tobacco products
Participation in another study that involves an intervention 2 months preceding the study visit
Members of the research team
Working, or doing an internship or thesis at the division "Human Nutrition and Health", Wageningen University

Contacts and Locations

Locations

	Site	City	State	Country	Postal Code
1	Department of Human Nutrition & Health, Wageningen University	Wageningen	Gelderland	Netherlands	6708WE

Sponsors and Collaborators

Wageningen University
Top Consortium for Knowledge and Innovation (TKI) Argi & Food
Mead Johnson Nutrition
Hycult Biotech

Investigators

Principal Investigator: Lydia Afman, Wageningen University
Principal Investigator: Rinke Stienstra, Wageningen University

Study Documents (Full-Text)

None provided.

More Information

Publications

None provided.

Responsible Party:

Lydia A. Afman, Associate professor, Wageningen University

ClinicalTrials.gov Identifier:

NCT05940337

Other Study ID Numbers:

NL70696.081.19

First Posted:

Jul 11, 2023

Last Update Posted:

Jul 11, 2023

Last Verified:

Jul 1, 2023

Individual Participant Data (IPD) Sharing Statement:

Plan to Share IPD:

Studies a U.S. FDA-regulated Drug Product:

Studies a U.S. FDA-regulated Device Product:

Keywords provided by Lydia A. Afman, Associate professor, Wageningen University

Study Results

No Results Posted as of Jul 11, 2023