Alleviation Of Metabolic Endotoxemia In Adults With Metabolic Syndrome With Milk Fat Globule Membrane

Not Applicable

Completed

• Conditions: Metabolic Syndrome; Metabolic Endotoxemia
• Interventions: Dietary Supplement: MFGM-enriched full-fat dairy milk; Dietary Supplement: Soy phospholipid/lecithin milk

• Registration Number: NCT03860584
• Lead Sponsor: Ohio State University

Brief Summary

Metabolic syndrome (MetS) adults (n = 24; 18-65 y) will be enrolled to complete a 2-arm, double-blind, randomized controlled, crossover trial. They will be randomized in 4-unit blocks to receive, for 14 d, a controlled diet with dairy milk (3.5% fat; 3 servings/d) enriched with milk fat globule membrane (MFGM, MEB) or a matched dairy milk that instead contains soy lecithin/phospholipid (control, COMP). All foods during each study period will be provided to ensure weight maintenance and to increase homogeneity of gut and host responses. Anthropometrics and blood pressure will be assessed at days 0, 7, and 14. Prior to (day 0) and after each 2-wk arm (day 14), a fasting blood sample will be collected to assess serum endotoxin and metabolic chemistries (glucose, lipids, insulin), and Toll-like receptor 4 /nuclear factor kappaB (TLR4/NFκB)-dependent genes from whole blood. A breath sample will be collected to assess the correlation analysis of plasma metabolic biomarkers. After the 2-week intervention, from fecal samples collected on day 13, the investigators will assess microbiota composition and function, short chain fatty acids (SCFA), and intestinal inflammatory markers (calprotectin, myeloperoxidase). On d 14, participants in the fasted state will receive a high-fat/high-glucose meal challenge to induce gut-derived endotoxin translocation. At 30-minute intervals for 3-hour, the investigators will evaluate circulating endotoxin, glucose, and insulin; TLR4/NFκB-dependent genes will be assessed from whole blood at 0 hour and 3-hour. Gut permeability probes will be co-administered with the test meal challenge, and 24-hour urine will be collected to assess gut barrier integrity. Participants will then undergo a 2-week washout prior to receiving the alternative treatment and completing all procedures in an identical manner.

Detailed Description

Background and hypothesis:

Our preclinical evidence shows that phospholipid-rich milk fat globule membrane (MFGM) attenuates lipopolysaccharide-induced increases in gut permeability and pro-inflammatory cytokines. MFGM also attenuates inflammation in association with a prebiotic and/or antimicrobial activity that modulates microbiota composition. Our central hypothesis is that MFGM-enriched dairy milk compared with a matched milk beverage containing soy lecithin (control) decreases metabolic endotoxemia and improves glucose tolerance in metabolic syndrome (MetS) adults by increasing gut barrier integrity in association with alleviating gut dysbiosis and inflammation.

Study Design:

The investigators will enroll male and female MetS adults (n = 24; 18-65 y) to complete a 2-arm, double-blind, randomized controlled, crossover trial. They will be randomized in 4-unit blocks to receive, for 14 days, a controlled diet with dairy milk (3.5% fat; 3 servings/d) enriched with MFGM-derived phospholipid or a matched dairy milk that instead contains coconut and palm oil (control). The investigators will provide all foods during each study period to ensure weight maintenance and to increase homogeneity of gut and host responses.

Subjects:

Participants will be recruited from Columbus, OH area. Participants having no history of liver or cardiovascular disease or cancer will be enrolled. They will have ≥3 established criteria for MetS: i) glucose (100-126 mg/dL), ii) waist circumference (\>89 or \>102 cm for F/M), iii) HDL-C (\<50 or \<40 mg/dL in F/M), iv) TG \>150 mg/dL, and iv) blood pressure \>130/85 mmHg. Major exclusion criteria include: unstable body mass (±2 kg over prior 3-mo) vegetarian; food allergies or lactose intolerance; user of dietary supplements or probiotics (within past 1-mo); pregnancy, lactation, changes in birth control (within 6-month); any gastrointestinal disorders; chronic diarrhea; smoker; excess alcohol (\>2 drinks/day); excess aerobic exercise (\>7 h/week); recent antibiotic or anti-inflammatory agent use; blood pressure \>140/90 mmHg.

Dietary Control:

The intervention will be performed in the Human Nutrition Metabolic Kitchen under the auspice of a registered dietitian (PI Bruno). In each 2-wk intervention, participants' diet will be rigorously controlled. All foods will be prepared, packaged, and provided every 3-4 days to supply a weight maintenance (i.e. eucaloric) diet. To assess compliance, participants will return MFGM/coconut/palm oil milk bottles for counting and any uneaten food portions for weighed measurement. Milk beverages will also be formulated to contain para-aminobenzoic acid (PABA; 80 mg/milk serving). Spot urine samples will be collected 4 times during each study arm coinciding when participants pick up test foods. Urinary PABA will be measured by spectrophotometry. Separate from this, participants will also keep food logs to document any dietary deviation. Diets will be standardized at 50-60% of energy from carbohydrate with low fiber intakes (\~15 g/day) similar to Americans' diets to prevent potential masking of the benefits of MFGM, 15-20% from protein, and 25-30% from fat. Importantly, other than test beverages provided as part of the eucaloric diet, diets will be otherwise devoid of significant amounts of dairy foods, fermented products, and probiotics to prevent confounding effects.

Measurements:

Anthropometrics and blood pressure will be assessed at days 0, 7, and 14. Prior to (day 0), at day 7 and after each 2-wk arm (day 14), a fasting blood sample will be collected to assess serum endotoxin and metabolic chemistries (glucose, insulin, lipids (triglyceride, total and HDL cholesterol), and TLR4/NFκB-dependent genes from whole blood. A breath sample will be collected to assess the correlation analysis of plasma metabolic biomarkers. After the 2-week intervention, from fecal samples collected on day 13, the investigators will assess microbiota composition and function, SCFAs, and intestinal inflammatory markers (calprotectin, myeloperoxidase). During this period, participants will also record daily stool characteristics using a 7-point Bristol Stool scale. On days 14, participants in the fasted state will receive a high-fat/high-glucose meal challenge to induce gut-derived endotoxin translocation. At 30-minute intervals for 3 hours, the investigators will evaluate circulating endotoxin, glucose, and insulin; TLR4/NFκB-dependent genes will be assessed from whole blood at 0 hour and 3-hour. Gut permeability probes will be co-administered with the test meal challenge, and 24-hour urine will be collected to assess gut barrier integrity. Participants will then undergo a 2-week washout prior to receiving the alternative treatment and completing all procedures in an identical manner.

Basic Information
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Recruitment & Eligibility
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Study & Design
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Trial Locations

Study Timeline

• Study First Submitted: 2019-02-28
• Study First Submitted QC: 2019-02-28
• Study First Posted: 2019-03-04
• Study Start: 2019-07-01
• Primary Completion: 2020-12-20
• Study Completion: 2020-12-20
• Status Verified: 2023-06
• Last Update Submitted: 2023-06-18
• Last Update Posted: 2023-06-22

Recruitment & Eligibility

• Status: COMPLETED
• Sex: All
• Target Recruitment: 24

Inclusion Criteria

• Serum Glucose 100-126 mg/dl
• Waist C >89/102 cm; F/M
• Serum HDL-C: <50/40 mg/dl; F/M
• Serum TG: >150 mg/dl
• BP >130/85 mmHg
• Serum Endotoxin >25 EU/ml

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Exclusion Criteria

• Unstable body mass (±2 kg over prior 3-mo)
• Vegetarian
• Food allergies or lactose intolerance
• User of dietary supplements or probiotics (within past 1-mo)
• Pregnancy, lactation, changes in birth control (within 6-mo)
• Any gastrointestinal disorders
• Chronic diarrhea
• Smoker
• Excess alcohol (>2 drinks/d)
• Excess aerobic exercise (>5 h/wk)
• Recent antibiotic or anti-inflammatory agent use
• BP >140/90 mmHg

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Study & Design

• Study Type: INTERVENTIONAL
• Study Design: CROSSOVER

Arm && Interventions

Group	Intervention	Description
MFGM-enriched full-fat dairy milk	MFGM-enriched full-fat dairy milk	Participants in this arm will receive MFGM-enriched full-fat dairy milk (3 servings/d) that contains MFGM at 10% phospholipid (relative to total lipid content) delivering MFGM at \~10-times that in full-fat dairy milk.
Soy phospholipid/lecithin milk	Soy phospholipid/lecithin milk	Participants in this arm will receive a matched dairy milk that instead contains soy phospholipid/lecithin.

Primary Outcome Measures

Name	Time	Method
Plasma Glucose	day 14 (0, 30, 60, 90, 120, 150, 180 minutes post-meal challenge)	Between-treatment difference in the area under the curve of plasma glucose (0-3 hours) on day 14
Serum Endotoxin (LPS)	day 14 (0, 30, 60, 90, 120, 150, 180 minutes post-meal challenge)	Between-treatment difference in the area under the curve of serum endotoxin (0-3 hours) on day 14

Secondary Outcome Measures

Name	Time	Method
Plasma glucagon-like peptide-1	day 14	Between-treatment change in plasma glucagon-like peptide-1 (fasting) on day 14 relative to day 0
Circulating TNFa mRNA	day 14 (0, 3 hour post-meal challenge)	Between-treatment change in circulating TNFa mRNA post meal challenge (0-3 h) on day 14
Circulating Toll-like receptor 4 mRNA	day 14 (0, 3 hour post-meal challenge)	Between-treatment change in circulating Toll-like receptor 4 mRNA post meal challenge (0-3 h) on day 14
Plasma Total Cholesterol	day 14	Between-treatment change in plasma total cholesterol (fasting) on day 14 relative to day 0
Urine erythritol	day 14	Between-treatment difference in 24 hour urinal excretion of erythritol post-meal challenge on day 14
Fecal Acetate	day 13	Between-treatment difference in fecal acetate on day 13
Plasma HDL-C	day 14	Between-treatment change in plasma HDL-C (fasting) on day 14 relative to day 0
Plasma Triglyceride	day 14	Between-treatment change in plasma triglyceride (fasting) on day 14 relative to day 0
Urine Lactulose	day 14	Between-treatment difference in 24 hour urinal excretion of lactulose post-meal challenge on day 14
Fecal bacterial abundance and composition	day 13	Between-treatment difference in fecal bacterial abundance and composition on day 13
Fecal Butyrate	day 13	Between-treatment difference in fecal butyrate on day 13
Fecal Propionate	day 13	Between-treatment difference in fecal propionate on day 13
Plasma Insulin	day 14 (0, 30, 60, 90, 120, 150, 180 minutes post-meal challenge)	Between-treatment difference in the area under the curve of plasma insulin (0-3 hours) on day 14
Urine sucralose	day 14	Between-treatment difference in 24 hour urinal excretion of sucralose post-meal challenge on day 14
Urine mannitol	day 14	Between-treatment difference in 24 hour urinal excretion of mannitol post-meal challenge on day 14
Fecal Myeloperoxidase	day 13	Between-treatment difference in fecal myeloperoxidase on day 13
Plasma gastric inhibitory polypeptide (GIP)	day 14	Between-treatment change in plasma gastric inhibitory polypeptide (GIP) (fasting) on day 14 relative to day 0
Fecal Calprotectin	day 13	Between-treatment difference in fecal calprotectin on day 13
Circulating IL-6 mRNA	day 14 (0, 3 hour post-meal challenge)	Between-treatment change in circulating IL-6 mRNA post meal challenge (0-3 h) on day 14

Trial Locations

Locations (1)

The Ohio State University; 🇺🇸 Columbus, Ohio, United States