Obesity Clinical Trial
Official title:
The Effects of Cortisol Blockade on Nutritional Sympathetic Nervous System Responsiveness in Overweight and Obese Subjects With Metabolic Syndrome
This project will examine whether short-term (over a 12-hour period) pharmacological
lowering of the stress hormone 'cortisol' improves the nervous system response to food
intake in overweight or obese individuals who have metabolic syndrome.
The investigators know from our previous research that overweight/obese persons who are
insulin resistant, have a blunted sympathetic nervous response to carbohydrate ingestion.
This means that they are less able to dissipate energy from caloric intake, which would
favour the maintenance of the obese state. Cortisol adversely impacts on insulin action and
transport into the brain and cortisol levels are often elevated in persons with central
(abdominal) obesity.
A randomized, double-blind, placebo controlled, cross-over design will be used to compare
the effects of overnight treatment with metyrapone (15 mg/kg at midnight and 15 mg/kg at 6
am) versus placebo on sympathetic nervous system activity in response to a standard 75-g
oral sugar (glucose) tolerance test. A 2 week washout will separate treatments.
Metyrapone is a drug that reversibly inhibits the enzyme 11beta-hydroxylase, and therefore
the production of cortisol. It is used clinically to test the activity of the adrenal gland
(the key site of cortisol production) and the pituitary gland. The investigators anticipate
that at the dosage used, it will lower blood cortisol concentration by 44 to 64% during the
experimental morning.
The study protocol comprises two screening visits and two experimental mornings. Key
procedures will include:
- Assessment of insulin action (sensitivity) using the gold standard 'clamp' method.
- Measurement of sympathetic nervous system activity by both biochemical methods (isotope
dilution which provides a measure of the apparent rate of release of
'noradrenaline'-the key neurotransmitter in the sympathetic nervous system) and direct
intra-neuronal nerve recordings from the peroneal nerve in the lower leg.
- Indirect calorimetry to assess resting metabolic rate and the response to sugar
ingestion.
- DEXA scan to quantify fat and lean mass.
- Assessment of arterial elasticity and calf blood flow by non-invasive methods.
- A standard 75g oral sugar tolerance test.
The results will provide important new information regarding the role of cortisol on nervous
system function in overweight/obese individuals.
Similarities between metabolic syndrome obesity and hypercortisolemic conditions such as
Cushing's syndrome have raised interest in the pathogenic role of glucocorticoid excess in
this clinical setting. Cortisol is a well known counter-regulator of insulin action and
increased levels of serum cortisol have been linked to insulin resistance in many studies.
Moreover, treatment with the synthetic glucocorticoid dexamethasone reduced central nervous
system insulin uptake by 49% in dogs. We have previously identified in metabolic syndrome
subjects, an inverse relationship between morning fasting cortisol levels and sympathetic
neural responsiveness to oral glucose ingestion. This concurs with other evidence that
cortisol and synthetic glucocorticoids have sympathoinhibitory effects.
This project will test the hypothesis that short-term lowering of plasma cortisol levels by
overnight metyrapone treatment, will improve nutritional sympathetic nervous system
responses to carbohydrate ingestion in obese insulin resistant subjects with metabolic
syndrome.
;
Allocation: Randomized, Intervention Model: Crossover Assignment, Masking: Double Blind (Subject, Investigator), Primary Purpose: Treatment
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