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The SIMBA Project - The Effect of a Prebiotic Supplement on Glucose Metabolism and Gut Microbiota in Obese Adults

Not Applicable
Conditions
Metabolic Syndrome
Gut Microbiota
Glucose Metabolism
Interventions
Dietary Supplement: Fermented canola-seaweed
Other: Placebo
Registration Number
NCT04120051
Lead Sponsor
University of Copenhagen
Brief Summary

Modulation of the gut microbiota via administration of pro- and prebiotics have been proposed to contribute to weight loss and reduce plasma glucose and serum lipid levels, improving the inflammatory state and decreasing the incidence of type 2 diabetes and cardiovascular disease. This study will test a fermented canola-seaweed (FCS) product, high in glucosinolates and putatively prebiotic oligosaccharides, in human subjects with obesity.

Detailed Description

The overall objective of this study is to investigate a fermented canola-seaweed (FCS) product in obese human subjects with increased risk of metabolic syndrome (MS). We will study the effects of the FCS on glucose handling and related cardiometabolic traits such as dyslipidemia and low-grade systemic inflammation. Finally, we will examine the gut microbiota and the metabolic phenotype of the subjects to explore molecular mechanisms related to the potential improvements.

It is hypothesized that the FCS product will improve postprandial glucose handling, blood lipids and low-grade inflammation in obese subjects with increased risk of MS. Furthermore, it is hypothesized that this effect is modified through gut microbiota compositional and functionality changes

Methods:

This study will be conducted as a randomized, controlled, investigator and participant blinded intervention trial. The participants will be randomized to the FCS supplement or control and are expected to consume one sachet of either every day for 6 weeks.

Randomization, blinding and allocation concealment:

After having given oral and written consent, randomization will be performed separately for each participant in blocks of variable size to ensure equal randomization throughout the enrolment phase of the study. The randomization sequence will be done by an investigator without contact to the participants. The personnel conducting the study will allocate participants to the sequence of intervention using a list of participant identification numbers matched with allocated sequences. The participants will be blinded to the intervention and blinding of the allocation sequence will be present for investigators during sample analysis and initial data analysis.

Examinations:

Participants will arrive for clinical examination after an overnight fast of at least 8 hours. Lifestyle questionnaires and questionnaires about medication use will be performed for baseline characterization of the participants. Blood pressure and anthropometric measurements are performed including measurements of body weight, height, waist and hip circumference, and bio-impedance measurements for assessing body fat mass. A fasting blood sample is obtained and an oral glucose tolerance test (OGTT) is performed with collection of blood samples after 0, 30 and 120 min. Samples will be analyzed with standard clinical procedures for glycaemic variability markers, including glucose, insulin, c-peptide, and HbA1c, as well as plasma lipids. Furthermore, fecal samples will be collected at both examination visits and kept stored for future microbiota analyses, using untargeted shotgun sequencing.

Samples in biobank will be stored for further analyses, which could include gastrointestinal hormones, gut microbiota metabolites, blood, and fecal metabolome and low-grade inflammation markers. In addition, a subgroup of participants (10 in each group) will be equipped with a 24-h continuous glucose monitoring device for 14 days at the start of the intervention period. Both examination days consists of similar examinations and data collections and are estimated to last approximately 2½ hours.

Recruitment & Eligibility

Status
UNKNOWN
Sex
All
Target Recruitment
100
Inclusion Criteria
  • Participants who have provided written informed consent
  • Age between 30 and 65 years
  • Body mass index ≥31 kg/m^2
Exclusion Criteria
  • Body mass index <31 kg/m^2
  • Diagnosis of diabetes (HbA1c ≥ 6,5% (48 mmol/mol)) or pharmacological treatment of diabetes
  • Use of peroral glucocorticoids
  • Lack of compliance with the procedures (ingestion of sachets) in the study protocol, judged by Investigator
  • Ingestion of pre- or probiotic supplements during the study and 14 days prior to study start
  • Use of systemic antibiotics 1 month prior to study start
  • Use of cholesterol lowering drugs
  • Have had an obesity or abdominal surgery
  • Chronic inflammation disorders (excluding obesity)
  • Diagnosed psychiatric disorder including depression requiring treatment
  • Gastro intestinal and liver disorders
  • Gluten intolerance
  • Maltodextrin intolerance
  • Intensive physical training/ elite athlete (>10 hours of strenuous physical activity per week)
  • Pregnant or lactating
  • High intake of alcohol (>14 drinks/week for women and >21 drinks/week for men)
  • Simultaneous blood donation for other purpose than this study
  • Simultaneous participation in other clinical intervention studies
  • Inability, physically or mentally, to comply with the procedures required by the study protocol as evaluated by the principal investigator or clinical responsible.

Study & Design

Study Type
INTERVENTIONAL
Study Design
PARALLEL
Arm && Interventions
GroupInterventionDescription
Fermented canola-seaweed supplementFermented canola-seaweedIngredients: Canola meal, seaweed, wheat, glucose, Vitamin D and lactic acid bacteria
PlaceboPlaceboIngredients: Rye flour, water, iodized salt, brown sugar
Primary Outcome Measures
NameTimeMethod
changes in 2-h post-OGTT glucose in blood between baseline and endpointWeek 0 and Week 6

2 hour post oral glucose tolerance test glucose measurement in blood (mmol/L)

Secondary Outcome Measures
NameTimeMethod
Changes in blood lipids between baseline and endpointWeek 0 and Week 6

Measurements of total and HDL cholesterol (mmol/L) and triglycerides (mmol/L)

Changes in body composition between baseline and endpointWeek 0 and Week 6

Measured using a Tanita body composition analyser. Fat free mass and Body fat mass in kilograms used to calculate body fat percentage.

Changes in Hba1c between baseline and endpointWeek 0 and Week 6

fasting measurement of blood glycated hemoglobin (%)

Changes in small metabolites between baseline and endpointWeek 0 and Week 6

Measured using blood metabolomic measurements of amino acids, lipids, and other small metabolites (umol/L)

Changes in Liver function markersWeek 0 and week 6

Alanine transaminase (ALAT) (U/L), Aspartate transaminase (ASAT) (U/L)

Changes in circulating endotoxin/lipopolysaccharide (LPS) concentrationsWeek 0 and Week 6

LPS (pg/ml)

Changes in fasting blood glucose between baseline and endpointWeek 0 and Week 6

Fasting measurement of blood glucose (mmol/L)

Changes in 30 min post OGTT between baseline and endpointWeek 0 and Week 6

Measurement of blood glucose 30 min after OGTT (mmol/L)

Changes in Interleukin-6 between baseline and endpointWeek 0 and Week 6

Blood measurements of Interleukin-6 (pg/mL)

Changes in weight between baseline and endpointWeek 0 and Week 6

Measured using a Tanita body composition analyser. Body weight in kilograms

Changes in blood pressure (BP) between baseline and endpointWeek 0 and Week 6

Systolic BP (mmHG) Diastolic BP (mmHG)

Changes in waist circumference between baseline and endpointWeek 0 and Week 6

Measured using measurement tape

Continuous glucose monitoringWeek 0

Continuous glucose monitor from Abbott is worn for 14 days in each period providing glucose measurements continuously (mmol/L)

Changes in gut microbiota compositionWeek 0 and Week 6

Measured on fecal samples

Insulin sensitivity and secretionWeek 0 and Week 6

Measured as part of the OGTT. Plasma glucose (mmol/l). Plasma insulin - fasting (pmol/l)

Changes in C-Reactive Protein between baseline and endpointWeek 0 and Week 6

Blood measurements of C-Reactive Protein (mg/L)

Trial Locations

Locations (1)

University of Copenhagen

🇩🇰

Frederiksberg, Danmark, Denmark

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