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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT03201822
Other study ID # 429275
Secondary ID
Status Completed
Phase N/A
First received June 19, 2017
Last updated June 26, 2017
Start date April 1, 2013
Est. completion date May 25, 2013

Study information

Verified date June 2017
Source University of California, Davis
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

A randomized, double-masked and cross-over dietary intervention study in healthy young adult males to evaluate the concentration of F-derived metabolites in plasma and urine after single acute intakes of F-containing drinks on four different test days.


Description:

Flavanols (F) are plant-derived compounds commonly present in the human diet. Examples of F-containing foods and beverages are apples, chocolate, tea, wine, berries, pomegranate and nuts. The consumption of F-containing foods and beverages has been associated with improvements in cardiovascular health. In this context, there exists a great interest in describing the absorption, metabolism and excretion of F in humans, as it is thought that F-derived metabolites present in circulation are the mediators of F-beneficial effects in humans. Recently, we described a series of F-derived metabolites in circulation that are present after the consumption of a single acute intake amount of F in humans. A key question, however, is if the metabolites we observed after a single acute feeding are the same as those that occur in individuals who consume F-rich diets on a regular basis. Studies investigating the metabolism of numerous other xenobiotics have shown that the profile of metabolites can greatly vary over time, as well as with the amount of xenobiotic ingested. In this context, and considering that i) the amount of F-consumed from diet greatly varies among individuals, ii) recent epidemiology studies indicate that the vascular protective effects of F diets primarily occur when daily intake of F are relatively high; and iii) there is evidence of an intake amount-dependency on the vascular effects of F in dietary intervention studies; we submit it is important to assess whether or not there are F intake amount-dependent effects on the levels and profile of F-derived metabolites in humans. This study will provide new information concerning the F-derived metabolites that may be responsible for mediating F-beneficial effects in humans. We suggest the information that will be obtained from the outlined work will be particularly timely given ongoing discussion concerning the possible generation of dietary recommendations for F-rich foods.


Recruitment information / eligibility

Status Completed
Enrollment 14
Est. completion date May 25, 2013
Est. primary completion date May 25, 2013
Accepts healthy volunteers Accepts Healthy Volunteers
Gender Male
Age group 25 Years to 40 Years
Eligibility Inclusion Criteria:

- No prescription medications

- BMI 18.5 - 29.9 kg/m2

- Weight = 110 pounds

- previously consumed cocoa and peanut products, with no adverse reactions

Exclusion Criteria:

- Adults unable to consent

- Prisoners

- Non-English speaking*

- BMI = 30 kg/m2

- Allergies to nuts, cocoa and chocolate products

- Active avoidance of coffee and caffeinated soft drinks

- Under current medical supervision

- A history of cardiovascular disease, stroke, renal, hepatic, or thyroid disease

- History of clinically significant depression, anxiety or other psychiatric condition

- History of Raynaud's disease

- History of difficult blood draws

- Indications of substance or alcohol abuse within the last 3 years

- Current use of herbal, plant or botanical supplements (multi-vitamin/mineral supplements are allowed)

- Blood Pressure > 140/90 mm Hg

- GI tract disorders, previous GI surgery (except appendectomy)

- Self-reported malabsorption (e.g. difficulty digesting or absorbing nutrients from food, potentially leading to bloating, cramping or gas)

- Diarrhea within the last month, or antibiotic intake within the last month

- Vegetarian, Vegan, food faddists, individuals using non-traditional diets, on a weight loss diet or individual following diets with significant deviations from the average diet

- Metabolic panel results or complete blood counts that are outside of the normal reference range and are considered clinically relevant by the study physician

- Screening LDL = 190 mg/dl for those who have 0-1 major risk factors apart from LDL cholesterol (i.e. family history of premature coronary artery disease (male first degree relative < 55 years; CHD in female first degree relative < 65 years), cigarette smoker, HDL-C = 40 mg/dL)

- Screening LDL = 160 mg/dl for those who have 2 major risk factors apart from LDL cholesterol (i.e. family history of premature coronary artery disease (male first degree relative < 55 years; CHD in female first degree relative < 65 years), cigarette smoker, HDL-C = 40 mg/dL).

(using NCEP calculator http://hp2010.nhlbihin.net/atpiii/calculator.asp?usertype=prof)

- Screening LDL = 130 mg/dl for those who have 2 major risk factors apart from LDL cholesterol (i.e. family history of premature coronary artery disease (male first degree relative < 55 years; CHD in female first degree relative < 65 years), cigarette smoker, HDL-C = 40 mg/dL), and a Framingham 10-year Risk Score 10-20% (Framingham risk calculated using NCEP calculator http://hp2010.nhlbihin.net/atpiii/calculator.asp?usertype=prof)

- Cold, flu, or upper respiratory condition at screening

- Currently participating in a clinical or dietary intervention study

Study Design


Related Conditions & MeSH terms


Intervention

Other:
100 mg of Cocoa Flavanols/70 kg BW
Fruit-flavored non-dairy drink containing 100 cocoa flavanols/70kg BW.
200 mg of Cocoa Flavanols/70 kg BW
Fruit-flavored non-dairy drink containing 200 cocoa flavanols/70kg BW.
400 mg of Cocoa Flavanols/70 kg BW
Fruit-flavored non-dairy drink containing 400 cocoa flavanols/70kg BW.
1000 mg of Cocoa Flavanols/70 kg BW
Fruit-flavored non-dairy drink containing 1000 cocoa flavanols/70kg BW.

Locations

Country Name City State
United States UC Davis Davis California

Sponsors (2)

Lead Sponsor Collaborator
University of California, Davis Mars, Inc.

Country where clinical trial is conducted

United States, 

References & Publications (5)

Heiss C, Kleinbongard P, Dejam A, Perré S, Schroeter H, Sies H, Kelm M. Acute consumption of flavanol-rich cocoa and the reversal of endothelial dysfunction in smokers. J Am Coll Cardiol. 2005 Oct 4;46(7):1276-83. — View Citation

Koster H, Halsema I, Scholtens E, Knippers M, Mulder GJ. Dose-dependent shifts in the sulfation and glucuronidation of phenolic compounds in the rat in vivo and in isolated hepatocytes. The role of saturation of phenolsulfotransferase. Biochem Pharmacol. 1981 Sep 15;30(18):2569-75. — View Citation

McCullough ML, Chevaux K, Jackson L, Preston M, Martinez G, Schmitz HH, Coletti C, Campos H, Hollenberg NK. Hypertension, the Kuna, and the epidemiology of flavanols. J Cardiovasc Pharmacol. 2006;47 Suppl 2:S103-9; discussion 119-21. — View Citation

Ottaviani JI, Momma TY, Kuhnle GK, Keen CL, Schroeter H. Structurally related (-)-epicatechin metabolites in humans: assessment using de novo chemically synthesized authentic standards. Free Radic Biol Med. 2012 Apr 15;52(8):1403-12. doi: 10.1016/j.freeradbiomed.2011.12.010. Epub 2011 Dec 23. — View Citation

Schroeter H, Heiss C, Spencer JP, Keen CL, Lupton JR, Schmitz HH. Recommending flavanols and procyanidins for cardiovascular health: current knowledge and future needs. Mol Aspects Med. 2010 Dec;31(6):546-57. doi: 10.1016/j.mam.2010.09.008. Epub 2010 Sep 18. Review. — View Citation

Outcome

Type Measure Description Time frame Safety issue
Primary Change in levels of gut microbiome derived metabolites in urine Gut microbiome derived metabolites include conjugates of 5-(3',4'-dihydroxyphenyl)-g-valerolatone metabolites Urine collected 12h previous to intervention and up to 24 h after intervention
Primary Change in levels of gut microbiome derived metabolites in plasma Gut microbiome derived metabolites include conjugates of 5-(3',4'-dihydroxyphenyl)-g-valerolatone Plasma collected before (0h) and up to 6h post intervention
Primary Change in levels of structurally related epicatechin metabolites in urine Structurally related epicatechin metabolites include sulfated, glucuronidated and/or methylated metabolites of epicatechin Urine collected 12h previous to intervention and up to 24 h after intervention
Primary Change in levels of structurally related epicatechin metabolites in plasma Structurally related epicatechin metabolites include sulfated, glucuronidated and/or methylated metabolites of epicatechin Plasma collected before (0h) and up to 6h post intervention
Secondary Composite of pharmacokinetic (PK) parameters of metabolites Maximum Plasma Concentration (CMax) PK parameters: Cmax: maximum observed concentration in plasma; Before intervention (0h) and up to 24 h after intervention
Secondary Composite of pharmacokinetic (PK) parameters of metabolites Time to Maximum Plasma Concentration tmax: time to maximum concentration in plasma; Before intervention (0h) and up to 24 h after intervention
Secondary Composite of pharmacokinetic (PK) parameters of metabolites Area Under the Curve AUC0-t: area under the plasma concentration-time curve from hour 0 to the last measurable concentration in plasma; Before intervention (0h) and up to 24 h after intervention
Secondary Composite of pharmacokinetic (PK) parameters of metabolites Area Under the Curve extrapolated to infinity AUC0-8: area under the plasma concentration-time curve extrapolated to infinity; Before intervention (0h) and up to 24 h after intervention
Secondary Composite of pharmacokinetic (PK) parameters of metabolites Elimination Rate Constant ?Z: apparent terminal elimination rate constant in plasma; Before intervention (0h) and up to 24 h after intervention
Secondary Composite of pharmacokinetic (PK) parameters of metabolites Elimination Half-Life t1/2: apparent terminal elimination half-life in plasma; Before intervention (0h) and up to 24 h after intervention
Secondary Composite of pharmacokinetic (PK) parameters of metabolites Systemic Clearance CL/F: systemic clearance; Before intervention (0h) and up to 24 h after intervention
Secondary Composite of pharmacokinetic (PK) parameters of metabolites Renal Clearance CLR: renal clearance;sampling interval and the total interval examined; Before intervention (0h) and up to 24 h after intervention
Secondary Composite of pharmacokinetic (PK) parameters of metabolites cumulative Amount Excreted in Feces Aef(0-t): Cumulative amount excreted in the feces over each sampling interval and the total interval examined. Before intervention (0h) and up to 24 h after intervention
Secondary Composite of pharmacokinetic (PK) parameters of metabolites Volume of Distribution Vd/F: apparent volume of distribution; Before intervention (0h) and up to 24 h after intervention
Secondary Composite of pharmacokinetic (PK) parameters of metabolites cumulative Amount Excreted in Urine Aeu(0-t): cumulative amount excreted in the urine over each Before intervention (0h) and up to 24 h after intervention
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