Clinical Trials Logo

Clinical Trial Summary

In a randomized, cross-over study, 20 healthy volunteers will receive a block and replace therapy that mimics physiological GC rhythm (metyrapone plus hydrocortisone) or placebo. Participants will undergo two identical fasting periods with each treatment. With the block and replace therapy, fasting-induced GC peak will be suppressed. Metabolic and autonomic parameters will be compared to reveal whether GCs mediate the physiological adaptions to caloric restriction. Understanding acute effects of GCs upon caloric restriction is critical, since repetitive disruptions of GC secretion may become harmful in chronic conditions.


Clinical Trial Description

Obesity is one of the major causes of morbidity and mortality worldwide. Achieving long-term weight loss is challenging, as the body counteracts weight loss to preserve energy by increasing appetite and lowering energy expenditure. These physiological defense mechanisms are the main obstacle to successful weight reduction in obese people. Therefore, identifying the signals that defend body weight during caloric restriction is essential for developing new antiobesity drugs. Corticosteroids mediate the physiological defense to starvation in rodents. Whether cortisol has the same impact on humans is unknown. Therefore, we investigate whether cortisol regulates the physiological adaptions to caloric restriction in humans. The general objective of this project is to investigate whether cortisol mediates physiological adaptions to caloric restriction. The primary objective is to test whether cortisol mediates the increased appetite during caloric restriction. Secondary objectives are to test whether the cortisol response to caloric restriction affects satiation, satiety, energy expenditure, substrate utilization, blood pressure, weight, body composition, secretion of neuroendocrine hormones, lipids, glucose, ketone bodies, sympathetic nervous system activity, immune cells, and inflammatory markers. This is a double-blind, randomized, placebo-controlled crossover study. After screening, subjects will be randomized to two crossover 7-day study periods with a wash-out period of 28 days: A) Participants will receive hydrocortisone 19.9 mg/d subcutaneously via a pump in a pulsed fashion (eight times/day) and metyrapone capsules per os (starting with a dose of 500 mg/d on day 1 to 3000mg/d on day 5, and then will be kept constant until day 7). B) Participants will receive a placebo (0,9% NaCl solution) subcutaneously via a pump in a pulsed fashion and identical-looking placebo capsules per os with the same regimen as for metyrapone. During both study periods, participants will undergo two days of caloric restriction. ;


Study Design


Related Conditions & MeSH terms


NCT number NCT05919992
Study type Interventional
Source University Hospital, Basel, Switzerland
Contact Eleonora Seelig, MD
Phone 0041 61 328 63 23
Email eleonora.seelig@usb.ch
Status Recruiting
Phase Early Phase 1
Start date May 15, 2023
Completion date August 31, 2024

See also
  Status Clinical Trial Phase
Completed NCT05167084 - Acute Consequences Of Food-induced Glucocorticoid Secretion In Healthy Individuals Early Phase 1
Completed NCT04659915 - Counteracting Deleterious Metabolic Glucocorticoid Effects With Metformin Phase 4