AI Article Synopsis

  • The study investigates how oral contraceptive (OC) use influences blood metabolite levels and whether these changes are linked to increased cortisol levels.
  • In a sample of 391 premenopausal women, researchers found 27 metabolites significantly related to OC intake, with 25 of these results confirmed in a second cohort.
  • Notably, while certain metabolites were influenced by cortisol, others were unaffected, suggesting that understanding these metabolic changes could help identify women at higher risk for adverse effects related to OC use.

Article Abstract

The use of oral contraceptives (OCs) has been associated with elevated blood cortisol concentrations. However, metabolic downstream effects of OC intake are not well described. Here, we aimed to determine if the blood metabolome is associated with the use of OCs and to estimate if these associations might be statistically mediated by serum cortisol concentrations. Plasma metabolites measured with the Biocrates Absolute p180 Kit and serum cortisol concentrations measured by an immunoassay were determined in 391 premenopausal women (116 OC users) participating in two independent cohorts of the Study of Health in Pomerania (SHIP). After correction for multiple testing, 27 metabolites were significantly associated with OC intake in SHIP-TREND (discovery cohort), of which 25 replicated in SHIP-2. Inter alia, associated metabolites included 12 out of 38 phosphatidylcholines with diacyl residue, 7 out of 14 lysophosphatidylcholines and 5 out of 21 amino acids. The associations with phosphatidylcholines were statistically mediated by cortisol, whereas lysophosphatidylcholines showed no mediation effect. The results represent a step toward a better understanding of the metabolic consequences of OC intake. Connecting cortisol with metabolic consequences of OC intake could help to understand the mechanisms underlying adverse effects. The blood metabolome may serve as a biomarker for identifying users at high risk for developing such adverse effects.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8064380PMC
http://dx.doi.org/10.3390/metabo11040193DOI Listing

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