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Exogenous Ketone Supplementation in Females with Polycystic Ovary Syndrome

Not Applicable
Recruiting
Conditions
PCOS
Interventions
Dietary Supplement: Water
Dietary Supplement: Ketone
Registration Number
NCT06155708
Lead Sponsor
McGill University
Brief Summary

Polycystic ovary syndrome (PCOS) affects 1 in 5 females of reproductive age. Commonly characterized as a disorder of infertility, PCOS is often accompanied by 3 potent cardiovascular disease (CVD) risk factors: insulin resistance, endothelial dysfunction, and elevated blood pressure. Accordingly, PCOS is associated with the development of CVD, the second leading cause of death in females in Canada. However, effective treatments to improve cardiovascular health in PCOS are lacking.

Exogenous ketone monoester (KME) ingestion has been shown to improves outcomes associated with insulin resistance, endothelial function, and blood pressure regulation in healthy individuals and individuals predisposed to CVD. Therefore, oral ketone supplements offer a practical and effective strategy for improving cardiovascular health; however, this treatment has yet to be evaluated in PCOS.

Therefore, the overall goal of this project is to employ KME ingestion to improve markers of cardiovascular health in females with PCOS.

On two different days, participants will consume either a beverage containing a ketone supplement or a beverage containing a placebo supplement. The objectives are to compare responses between KME and placebo ingestion, and examine all outcomes related to cardiovascular health in females with PCOS in comparison with female controls of similar age and body mass index. The effects of KME ingestion will be quantified on: 1) glycemic control during an oral glucose tolerance test; 2) endothelial function using the flow-mediated dilation test; 3) blood pressure and acute blood pressure regulation; and 4) hemodynamic responses to acute exercise.

Detailed Description

Not available

Recruitment & Eligibility

Status
RECRUITING
Sex
All
Target Recruitment
60
Inclusion Criteria
  • All female participants will report female sex assigned at birth
  • All participants will be aged 18 to 40
  • PCOS diagnosis
Exclusion Criteria
  • Current smokers or a prolonged history of smoking
  • Presence or history of overt cardiometabolic disease (e.g., stage 2 hypertension, diabetes, heart disease), neurologic disease, or endocrinopathy (with the exception of PCOS)
  • Current pregnancy or currently breastfeeding
  • Current use of medications which may affect our outcomes of interest (e.g., anti-hypertensives, anti-androgens, metformin)

Study & Design

Study Type
INTERVENTIONAL
Study Design
CROSSOVER
Arm && Interventions
GroupInterventionDescription
PlaceboWater100 ml water combined with 10ml bitter flavor and vanilla-flavored stevia
KetoneKetone- Ketone monoester supplement in the form of (R)-3-hydroxybutyl (R)-3-hydroxybutyrate based on participants' body weight (0.45ml/kg body weight) ingested with water and vanilla-flavored stevia in a total volume of 100 ml.
Primary Outcome Measures
NameTimeMethod
Systolic Blood Pressure (SBP)2 hours

- SBP, measured in mmHg

Diastolic Blood Pressure (DBP)2 hours

- DBP, measured in mmHg

Glycemic responses to a 2-hr oral glucose tolerance test0-2.5 hours in the post-prandial period

- Glucose is calculated by the area under the curve using the trapezoid method.

Flow mediated dilation (FMD)30 minutes

- Endothelial function is assessed using the standard FMD; quantified as the percent increase in diameter from rest to peak diameter observed during reactive hyperemia (%FMD). The % change in diameter reflects the ability of the vessel to dilate in response to sheer stress induced by the flow following the release of occlusion. This reflects the function of the endothelium, or release of nitric oxide.

Secondary Outcome Measures
NameTimeMethod
Serum sex hormone binding globulin5 minutes

- Measured in pg/ml.

Glucose-dependent insulinotropic polypeptide (GIP)0-2.5 hours in the post-prandial period

- GIP area under the curve during oral glucose tolerance test.

Triglycerides0-2.5 hours in the post-prandial period

- Triglycerides area under the curve during oral glucose tolerance test

Serum estradiol5 minutes

- Measured in pg/ml.

Arterial artery blood flow0-2.5 hours in the post-prandial period

- Calculated as the product of mean blood flow velocity (cm/sec) and cross-sectional area (2Πr2) x 60 sec/min.

Shear rate and low-flow mediated vasoconstriction to the FMD30 minutes

- Shear rate calculated as area under the curve from cuff deflation to the time of peak dilation using the trapezoidal rule, as well as low flow-mediated vasoconstriction during forearm occlusion, which provides an index of the endothelial contribution to resting vascular tone and which predicts cardiovascular disease risk.

Glucagon-like peptide-1 (GLP-1)0-2.5 hours in the post-prandial period

- GLP-1 area under the curve during oral glucose tolerance test.

Insulin area under the curve0-2.5 hours in the post-prandial period

- Insulin area under the curve during oral glucose tolerance test

Insulinogenic index0-2.5 hours in the post-prandial period

- (Insulin at 30 min - fasting insulin)/ (plasma glucose at 30 min- fasting plasma glucose).

Muscle sympathetic nerve activity (MSNA)2 hours

- Measured using microneurography, and expressed in burst/min or bursts/100 heart beats

Neurovascular transduction2 hours

- Assessed by the MSNA signal (recorded in both raw and filtered/rectified/integrated formats for subsequent analyses) and arterial blood flow extracted on a beat-by-beat basis and processed using custom transduction software.

Capillary blood Beta-OHB concentrations0-2.5 hours in the post-prandial period

- Measures in mmol/L

C-peptide0-2.5 hours in the post-prandial period

- C-peptide area under the curve during oral glucose tolerance test

Vascular resistance2 hours

- Calculated as mean arterial pressure divided by Finometer-derived cardiac output

Serum testosterone5 minutes

- Measured in pg/ml.

Serum Progesterone5 minutes

- Measured in pg/ml.

Related Research Topics

Explore scientific publications, clinical data analysis, treatment approaches, and expert-compiled information related to the mechanisms and outcomes of this trial. Click any topic for comprehensive research insights.

What molecular pathways mediate exogenous ketone monoester effects on insulin resistance and endothelial function in PCOS?
How does exogenous ketone supplementation compare to metformin in improving CVD risk factors in PCOS patients?
Which biomarkers predict response to ketone monoester intervention in PCOS-associated endothelial dysfunction?
What adverse events are associated with exogenous ketone monoester in PCOS patients and how are they managed?
Are there synergistic effects of combining exogenous ketones with lifestyle interventions for PCOS cardiovascular risk factors?

Trial Locations

Locations (1)

Cardiovascular Health and Autonomic Research Laboratory

🇨🇦

Montréal, Quebec, Canada

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