MedPath

Resveratrol and the Metabolic Syndrome

Not Applicable
Completed
Conditions
Insulin Resistance
Metabolic Syndrome
Obesity
Interventions
Dietary Supplement: Resveratrol
Dietary Supplement: Placebo
Registration Number
NCT01714102
Lead Sponsor
Rockefeller University
Brief Summary

Metabolic syndrome is a serious health condition that affects about 35 percent of adults and places them at higher risk of cardiovascular disease, diabetes, stroke and diseases related to fatty buildups in artery walls. The underlying causes of metabolic syndrome are obesity, being overweight, physical inactivity and genetic factors. In recent decades, the prevalence has increased dramatically in the United States. Lifestyle interventions including dietary modification, physical activity and weight loss form the basis of treatment for these patients. However, research has shown that even when people are able to incorporate these changes, they often revert back to their usual lifestyle resulting in weight gain and continued risk for diabetes and heart disease.

Resveratrol, a natural plant derived compound found in grapes, peanuts and red wine, has been found to reverse some of the features of the metabolic syndrome (insulin resistance, high triglycerides, high blood pressure) in rodents. These improvements occurred without weight loss, and were proven to be a direct result of resveratrol ingestion. Other studies reveal improvement in cardiovascular health, tumor suppression, and longevity. However, there are few studies investigating these beneficial effects in humans. Investigators propose to prove that resveratrol, administered to subjects with the metabolic syndrome, under controlled conditions of weight stability, common diet, and strict compliance with the study drug, will improve the symptoms of the metabolic syndrome, thereby decreasing the chance of developing diabetes or heart disease.

Detailed Description

The metabolic syndrome is a serious health condition that affects about 35 percent of adults and places them at higher risk of cardiovascular disease, diabetes, stroke and diseases related to fatty buildups in artery walls. The underlying causes of metabolic syndrome are obesity, being overweight, physical inactivity and genetic factors. In recent decades, the prevalence has increased dramatically in the United States. Lifestyle interventions including dietary modification, physical activity and weight loss form the basis of treatment for these patients. However, research has shown that even when people are able to incorporate these changes, they often revert back to their usual lifestyle resulting in weight gain and continued risk for diabetes and heart disease.

Resveratrol, a natural plant derived compound found in grapes, peanuts and red wine, has been found to reverse some of the features of the metabolic syndrome (insulin resistance, high triglycerides, high blood pressure) in rodents. These improvements occurred without weight loss, and were proven to be a direct result of resveratrol ingestion. Other studies reveal improvement in cardiovascular health, tumor suppression, and longevity. However, there are few studies investigating these beneficial effects in humans. In a systematic review of resveratrol research, the authors conclude that "in contrast to the lacking data of resveratrol in humans, the animal data are promising and indicate the need for further human clinical trials." Of the small clinical studies that have been done, the results are encouraging. Improvement in triglycerides, blood pressure and insulin resistance were noted. Resveratrol was well tolerated without serious side effects. These studies, however, did not recruit subjects with the metabolic syndrome, nor were they tightly controlled.

The investigators propose to prove that resveratrol, administered to subjects with the metabolic syndrome, under controlled conditions of weight stability, common diet, and strict compliance with the study drug, will improve the symptoms of the metabolic syndrome, thereby decreasing the chance of developing diabetes or heart disease.

Recruitment & Eligibility

Status
COMPLETED
Sex
Male
Target Recruitment
28
Inclusion Criteria

  • Age 30 - 60 year old men

  • Willingness to be randomized to resveratrol or placebo.

  • BMI 30-40

  • Evidence of insulin resistance with one of the following:

    2 hr oral glucose tolerance result =/>120mg/dl at 2hrs acanthosis nigricans, or HgA1C 5.7 - 7.9%, or FBS >/= 100 mg/dl AND at least 2 of the following: waist circumference > 102 cm triglycerides > 150 but < 500 mg/dL HDL < 40 mg/dL Pre- hypertension or hypertension: BP>120/80 mmHg but <150/90 mmHg

  • Willingness to consume only study food and drink during the in-pt phases

  • Willingness to avoid the use of over-the-counter medications, herbs, or supplements within the last 30 days.

  • Willingness to avoid NSAIDS (advil, aleve, motrin, etc.) and aspirin for the entire study

  • Willingness to avoid ingestion of any foods containing peanuts, bilberries, blueberries, cranberries, strawberries, raspberries, grapes, grape juice, cocoa powder, dark chocolate, and red wine throughout the entire study, including run-in period.

  • Willingness to maintain weight for the duration of the study.

  • Willingness not to start an exercise regime during study participation

Exclusion Criteria
  • Tobacco smoker any time within the last 3 months
  • Bleeding disorder by history or by Bleeding Questionnaire results
  • History, physical or EKG findings suggestive of CV disease including angina, MI, hx of med/surg tx of atherosclerotic heart disease, or congestive heart disease
  • BP > 145/90 after 10 minutes of rest on 2 or more screening visits
  • Fasting glucose > 165 mg/dL at screening
  • HbA1C > 8.0 at screening
  • Current use of oral hypoglycemic agents
  • Chronic glucocorticosteroid use or use of oral glucocorticosteroids for 5 days within the last year (inhaled glucocorticosteroid use may be acceptable; this will be determined by the PI)
  • Current use of over the counter or prescription weight loss medication
  • Current use or within the last 30 days, any cholesterol lowering medications (statins, fibrates, red yeast rice, niacin).
  • Hyperthyroidism or untreated hypothyroidism
  • Obstructive sleep apnea, or significant symptoms suggestive of this condition.
  • Current use of anticoagulants
  • Known history of chronic hepatitis or liver enzymes (ALT or AST > 2.5 times the normal upper limit)
  • Known HIV infection or confirmed positive test for HIV antibodies at screening
  • Inflammatory bowel disease
  • Active cancer (currently under treatment)
  • Other medical condition that may cause significant weight loss or gain
  • Chronic or acute renal disease
  • Seizure disorder
  • History of any psychiatric hospital admission within the last 2 years
  • History of schizophrenia, psychosis, or bipolar disease
  • History, physical, social or lab findings suggestive of any medical or psychological condition that would, in the opinion of the PI, impact the subject's ability to successfully participate in the study.
  • Alcohol or drug abuse within the last 2 years
  • Any medications metabolized by cytochrome p450 3A4 (CYPA3A4) (see attachment of these medications as an appendix)
  • Any autoimmune disease (ie rheumatoid arthritis, systemic lupus erythematosis, psoriasis)
  • Physical condition requiring special diet (ie celiac disease)

Study & Design

Study Type
INTERVENTIONAL
Study Design
PARALLEL
Arm && Interventions
GroupInterventionDescription
PlaceboResveratrolPlacebo for 30 days
ResveratrolPlacebo1000 mg PO BID for 30 days
Primary Outcome Measures
NameTimeMethod
Reduction in Insulin resistanceDays 4-8 and Days 31-35

Investigators anticipate resveratrol will have positive effect (ie reduction) on Insulin resistance as determined by Euglycemic hyperinsulinemic clamp

Secondary Outcome Measures
NameTimeMethod
Reduction lipid valuesDays 4-8 and Days 31-35

Lipid values to be reviewed: cholesterol, LDL, HDL, TG

Changes in HOMA-IRDays 4-8 and Days 31-35

Changes in 2 hr oral glucose tolerance test HOMA-IR

Reduction in blood pressure measurementsDays 4-8 and Days 31-35

24 hour systolic blood pressure measurements

Changes in gene expression in adipose tissueDays 4-8 and Days 31-35

Changes in RNA sequencing of adipose tissue

Reduction in serum cytokines/chemokinesDays 4-8 and Days 31-35

Investigators anticipate resveratrol will have positive effect (ie reduction) on Serum cytokines/chemokines: IL6, IL10, TNFalpha, hsCRP, leukocytes, PAI-1, fibrinogen, adiponectin, MCP-1,GLP-1, leptin, insulin, serum endotoxins

Reduction in crown like structures and adipose tissue massDays 4-8 and Days 31-35

Crown like structures in adipose tissue, and adipose tissue mass

Changes in gene expression in stoolDays 4-8 and Days 31-35

Changes in microbiome and RNA gene expression in stool samples

Trial Locations

Locations (1)

The Rockefeller University

🇺🇸

New York, New York, United States

Related Trials

Resveratrol in Type2 Diabetes and Obesity

TerminatedNot Applicable
University at Buffalo
Posted 7/8/2010
Updated 11/9/2022

Resveratrol and Type 2 Diabetes

Unknown StatusNot Applicable
Maastricht University Medical Center
Posted 7/12/2012
Updated 9/4/2014

Diet and Health in Adults with Metabolic Syndrome

Active, Not RecruitingNot Applicable
University of Arkansas, Fayetteville
Posted 5/2/2019
Updated 11/13/2024
© Copyright 2025. All Rights Reserved by MedPath
HomeTerms & ConditionsPrivacy Policy