Glucocorticoid Effect
Conditions
Keywords
cortisol, overfeeding, glucocorticoids, insulin sensitivity
Brief 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 overfeeding periods with each treatment. With the block and replace therapy, food-induced GC peak will be suppressed. Metabolic and autonomic parameters will be compared to reveal, whether GCs mediate the physiological adaptions to excessive food intake. Understanding acute effects of GCs upon food intake is critical, since repetitive disruptions of GC secretion may become harmful in chronic conditions.
Detailed description
Obesity is one of the most serious health problems of the 21st century. To understand how we regulate our body weight is crucial for developing new treatment targets. Even though body mass index of populations is increasing, the body weight of adults is usually kept stable over time. Indeed, acute excessive food intake triggers a set of adaptions in order to prevent weight gain. The signal that triggers these beneficial adaptions is still unknown. Glucocorticoid (GC) secretion increases with acute food intake and many physiological adaptions to overfeeding coincide with classical glucocorticoid actions. The investigators therefore hypothesize that GCs are the signal that prevents weight gain during acute overfeeding. The objective of this project is to test whether food-induced GCs represent the physiological signal that defends against weight gain. The primary objective is to investigate whether reduction in insulin sensitivity is abolished with the block and replace therapy. Secondary objectives are to investigate whether suppression of GC secretion during excessive food intake impairs the activation of sympathetic nervous system, satiety, satiation, energy expenditure, substrate utilization, blood pressure, secretion of neuroendocrine hormones, lipids and immune cells. This is a double-blind, randomized, placebo-controlled cross-over study. After screening, subjects will be randomized to two crossover 8-day study periods with a washout 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 per os (starting with a dose of 500 mg/d on day 1 to 2500mg/d on day 4, and then will be kept constant until day 8) B) Participants will receive placebo (0,9% NaCl solution) 19.9 mg/d subcutaneously via a pump in a pulsed fashion and placebo pills per os (starting with a dose of 500 mg/d on day 1 to 2500mg/d on day 4, and then will be kept constant until day 8)
Interventions
Placebo (0,9% NaCl solution) 19.9 mg/d subcutaneously via a pump in a pulsed fashion with a flow rate of 10μl/s from day 1 to day 8
During one phase of the study: Metyrapone (pills of 250mg) on full stomach: Day 1 0-1-1, day 2 1-2-2, day 3 2-2-3 day 4 3-3-4 day 5 3-3-4 day 6 3-3-4 day 7 3-3-4 day 8 3-0-0
During another phase of the study: identical looking placebo pills starting Day 1 0-1-1, day 2 1-2-2, day 3 2-2-3 day 4 3-3-4 day 5 3-3-4 day 6 3-3-4 day 7 3-3-4 day 8 3-0-0
DRUGHydrocortisone 19,9mg s.c., pulsatile with a flow rate of 10μl/s
Hydrocortisone will be delivered subcutaneously via a pump in a pulsed fashion with a flow rate of 10μl/s from day 1 to day 8 in a total daily dose of 19.9mg
Sponsors
Eleonora Seelig
Study design
Allocation
RANDOMIZED
Intervention model
CROSSOVER
Primary purpose
PREVENTION
Masking
DOUBLE (Subject, Investigator)
Masking description
Placebo-controlled
Intervention model description
Double-blind, randomized, placebo-controlled cross-over study
Eligibility
Sex/Gender
MALE
Age
18 Years to 40 Years
Healthy volunteers
Yes
Inclusion criteria
* BMI 18.5 - 25 kg/m2
Exclusion criteria
* Previous medical history for any chronic condition in the last three months, active disease or abnormal physical examination as verified by a qualified physician. * Casual smoking (\>6 cigarettes per day) * Frequent, heavy alcohol consumption (\>30g/day) * Frequent, heavy caffeine consumption (\>4 caffeinated drinks/day) * Regular physical exercise (\>4hrs per week) * Shift workers * Participation in an investigational drug trail within the past two months * Intake of any drugs (prescribed, over the counter or recreational) including topical steroids and inhalers, within 48 hours of the study initiation * Known allergy to metyrapone * Inability or unwillingness to provide informed consent
Design outcomes
Primary
| Measure | Time frame | Description |
|---|---|---|
| Insulin sensitivity | Two 8-day intervention periods | Change in insulin sensitivity assessed with a mixed meal tolerance test |
Secondary
| Measure | Time frame | Description |
|---|---|---|
| T3 (nmol/l) | Two 8-day intervention periods | Blood Sample |
| T4 (nmol/l) | Two 8-day intervention periods | Blood Sample |
| TSH (mIU/l) | Two 8-day intervention periods | Blood Sample |
| HGH (mIU/l) | Two 8-day intervention periods | Blood Sample |
| Corticosteron (Adrenal Steroid Hormones) | Two 8-day intervention periods | Blood Sample |
| Weight | Two 8-day intervention periods | Measurement of weight with a standard scale |
| Energy expenditure | Two 8-day intervention periods | Basal metabolic rate measured with indirect calorimetry |
| Substrate utilisation | Two 8-day intervention periods | Respiratory quotient assessed with indirect calorimetry |
| Satiety | Two 8-day intervention periods | Appetite rating with visual analogue scale (VAS) from 0mm-100mm (0mm=not at all and 100mm=extreme) |
| Satiation | Two 8-day intervention periods | Amount of food intake with ad libitum buffet |
| Cortisol (nmol/l) total and free | Two 8-day intervention periods | Blood sample |
| Renin | Two 8-day intervention periods | Blood Sample |
| Aldosterone (Adrenal Steroid Hormones) | Two 8-day intervention periods | Blood Sample |
| Pregnenolon (Adrenal Steroid Hormones) | Two 8-day intervention periods | Blood Sample |
| Progesteron (Adrenal Steroid Hormones) | Two 8-day intervention periods | Blood Sample |
| 11-Deoxycorticosteron (Adrenal Steroid Hormones) | Two 8-day intervention periods | Blood Sample |
| PYY (pg/ml) | Two 8-day intervention periods | Blood Sample |
| 18-Hydroxycorticosteron (Adrenal Steroid Hormones) | Two 8-day intervention periods | Blood Sample |
| 17-Hydroxypregnenolon (Adrenal Steroid Hormones) | Two 8-day intervention periods | Blood Sample |
| 17-Hydroxyprogesteron (Adrenal Steroid Hormones) | Two 8-day intervention periods | Blood Sample |
| 11-Deoxycortisol (Adrenal Steroid Hormones) | Two 8-day intervention periods | Blood Sample |
| GLP-1 (nmol/l) | Two 8-day intervention periods | Blood sample |
| GIP (nmol/l) | Two 8-day intervention periods | Blood Sample |
| Lipids (mmol/l) ((total cholesterol, LDL-cholesterol, HDL-cholesterol and triglycerides) | Two 8-day intervention periods | Blood Sample |
| GDF-15 (pg/mL) | Two 8-day intervention periods | Blood Sample |
| Sympathetic nervous system activity | Two 8-day intervention periods | Heart rate variability analysis |
| Systolic and diastolic blood pressure | Two 8-day intervention periods | Assessment of blood pressure with a standard blood pressure monitor. |
Other
| Measure | Time frame | Description |
|---|---|---|
| IL-1RA (Inflammatory markers) | Two 8-day intervention periods | Blood Sample |
| IL-8 (Inflammatory markers) | Two 8-day intervention periods | Blood Sample |
| CRP (Inflammatory markers) | Two 8-day intervention periods | Blood Sample |
| Metabolomics | Two 8-day intervention periods | Metabolomics will be performed in blood plasma |
| IL-6 (Inflammatory markers) | Two 8-day intervention periods | Blood Sample |
Countries
Switzerland
Outcome results
None listed