MedPath

Effect of Oleactiv® on LDL Oxidability

Not Applicable
Completed
Conditions
Hypercholesterolemia
Interventions
Dietary Supplement: Maltodextrin
Dietary Supplement: Plant food supplement
Registration Number
NCT05221346
Lead Sponsor
Institut Pasteur de Lille
Brief Summary

Oleactiv® have previously demonstrated beneficial effects in an animal model of diet-induced atherosclerosis. After a 12-week supplementation, a substantial reduction of aortic fatty streak area has been observed. Also, Oleactiv®-supplemented hamsters displayed significant decrease of both non-HDL-cholesterol and triglycerides levels. Also, phenolic compounds from Oleactiv® demonstrated that increase of cholesterol efflux capacity (CEC) is one of the mechanisms that may explain preventive effect on atheroma development.

These effects observed in animals will thus be investigated in human. The main hypothesis of the present study is that phenolic compounds from Oleactiv® may improve LDL oxidability in volunteers with moderate hypercholesterolemia after 3 weeks of consumption.

Detailed Description

Not available

Recruitment & Eligibility

Status
COMPLETED
Sex
Male
Target Recruitment
26
Inclusion Criteria
  • Male aged between 40 and 70 years (limits included),
  • BMI between 20 and 30 kg / m² (limits included)
  • Weight over 65kg (to respect volume blood collection reglementation)
  • Fasting plasma LDL cholesterol between 1.16 g / L and 1.9 g / L (limits included) if the cardiovascular risk is low OR Fasting plasma LDL cholesterol between 1.0 g / L and 1.9 g / L (limits included) if the cardiovascular risk is moderate (SCORE calculated according to the European Society of Cardiology 2019)
  • Able and willing to participate to the study by complying with the protocol procedures as evidenced by his dated and signed informed consent form,
  • Affiliated with a social security scheme.
Exclusion Criteria

  • Dyslipidemia or hyperlipidemia:

    • Fasting total cholesterol ≥ 3.0 g / L
    • Fasting triglycerides> 2 g / L
    • with heterozygous familial hypercholesterolemia

  • Hypertensive-treated

  • Diabetes treated or not with medication

  • Taking drugs known to have an impact on lipid metabolism (statin, ezetimibe, colestyramine, fibrate, etc.) in the month preceding inclusion and / or likely to consume them during the test

  • Consuming food supplements or functional foods known to have an influence on cholesterolemia (phytosterol, phytostanol, red rice yeast, policosanols, beta-glucans at a dose greater than 3 g / d) in the month preceding the inclusion and / or likely to take during the test

  • Consuming probiotics in the form of a food supplement in the month preceding inclusion and / or likely to take them during the test

  • Following or having followed a hypocaloric diet (energy intake <1,500 kCal / day) in the month preceding inclusion and / or likely to undertake this diet during the test

  • Who donated blood in the 3 months preceding inclusion

  • Diagnosed eating disorders (bulimia, anorexia nervosa, vomiting)

  • High level athlete (physical activity for 1 hour per day)

  • Smoking more than 5 cigarettes per day

  • Bariatric surgery or who has a gastroplasty ring

  • Consuming more than 3 standard drinks of alcoholic beverage daily,

  • Consuming drugs,

  • Suffering from serious illnesses such as cancer, recent myocardial infarction, serious digestive pathologies or others diseases found to be inconsistent with the conduct of the study by the investigator,

  • Taking part in another clinical trial or being in the exclusion period of a previous clinical trial,

  • Under legal protection (guardianship, wardship) or deprived from his rights following administrative or judicial decision,

  • Presenting a psychological or linguistic incapability to sign the informed consent,

  • Any other condition which in the investigator's opinion may adversely affect the subject's ability to complete the study or its measures or which may pose significant risk to the subject.

  • Known allergy to one of the component of the supplement (Grape, olive, artichoke, blackcurrant or pomegranate) or to corn.

Study & Design

Study Type
INTERVENTIONAL
Study Design
CROSSOVER
Arm && Interventions
GroupInterventionDescription
MaltodextrinMaltodextrin* Dietary supplements in capsule form * 1 capsule per day at breakfast
Plant food supplementPlant food supplement* Dietary supplements in capsule form * 1 capsule per day at breakfast
Primary Outcome Measures
NameTimeMethod
Change from baseline of LDL oxidability after 3 weeks of food supplement consumption compared to placebo group3 months

LDL oxidability

Secondary Outcome Measures
NameTimeMethod
Change from baseline of arterial stiffness after 3 weeks of food supplement consumption compared to placebo group3 months

Arterial stiffness via the Sphygmocor® measuring device

Change from baseline of lipid metabolism after 3 weeks of food supplement consumption compared to placebo group3 months

Total cholesterol, HDL, LDL, Triglycerides,

Change from baseline of reverse transport of cholesterol after 3 weeks of food supplement consumption compared to placebo group3 months

Reverse transport of cholesterol

Time of complete elimination of phenolic compounds in a 24h-blood collection3 months

Phenolic compounds were measured after food supplement consumption at 7 points (T0, T1h, T2h, T4h, T6h, T10h, T24h).

Change from baseline of plasma paraoxonase activity after 3 weeks of food supplement consumption compared to placebo group3 months

Paraoxonase activity

Change from baseline of cholesterol load capacity after 3 weeks of food supplement consumption compared to placebo group3 months

Cholesterol load capacity

Maximum plasma concentration of oxidized LDL in a 24h-blood collection3 months

Oxidized LDL were measured after food supplement consumption at 7 points (T0, T1h, T2h, T4h, T6h, T10h, T24h).

Maximum concentration of urinary isoprostanes in a 48h-urine collection3 months

Urinary isoprostanes were measured after food supplement consumption at 7 points (from 22h the day before to 8h (T0), T0-6h, T6-10h, T10-14h, T14-24h, T24-32h, T32-48h).

Change from baseline of lipoproteins size distribution after 3 weeks of food supplement consumption compared to placebo group3 months

Lipoprotein size

Maximum plasma concentration of phenolic compounds in a 24h-blood collection3 months

Phenolic compounds were measured after food supplement consumption at 7 points (T0, T1h, T2h, T4h, T6h, T10h, T24h).

Change from baseline of carbohydrate metabolism after 3 weeks of food supplement consumption compared to placebo group3 months

glycemia, insulin

Trial Locations

Locations (1)

NutrINvest

🇫🇷

Lille, France

Related Trials

Dietary Polyphenols and Lipid Oxidation

CompletedNot Applicable
Maastricht University Medical Center
Posted 2/24/2011
Updated 9/9/2014

Effect of Olivomed (Olive Extract) on Endothelial, Cardiac and Vascular Function

RecruitingNot Applicable
University of Athens
Posted 8/20/2020
Updated 5/29/2024

Efficacy Study on the Lipid-lowering Effect of Plant Sterols and Fish Oil

CompletedNot Applicable
Unilever R&D
Posted 3/14/2011
Updated 2/7/2012

Effects of Lipoic Acid on Oxidative, Inflammatory and Functional Markers in Asthmatic Patients

CompletedNot Applicable
Centro Universitario de Ciencias de la Salud, Mexico
Posted 10/15/2010
Updated 11/8/2013

EPA Lipid Intervention and Atherosclerosis Prevention Study-ELIA Study

Phase 4
Center for Clinical Research, Yamaguchi University Hospital
Updated 10/17/2023
© Copyright 2025. All Rights Reserved by MedPath
HomeTerms & ConditionsPrivacy Policy