Bariatric surgery is currently the most efficient treatment for obesity. The sustained weight loss and metabolic improvement seen following Roux-en-Y gastric bypass (RYGB), is explained partly by modifications in hormones including bile acids (BA). After RYGB, an increased total BA pool and a reduction in hepatic cortisol exposure is observed. Hydroxysteroid 11-β dehydrogenase 1 (HSD11B1), steroid 5α-reductases (SRD5A), and steroid 5β-reductases, AKR1D1 (also a BA metabolizing enzyme), are three enzymes involved in the metabolism of cortisol in the liver and are known to participate in metabolic syndrome. Their activity has been shown to be decreased after RYGB. Interestingly, the mechanisms explaining the modification of hepatic cortisol exposure and the activity of theses enzymes after RYGB are unknown. In view of the few data suggesting a link between cortisol metabolism and bile acids, this work aim to study and characterize this link in a context of RYBP
Study Type
OBSERVATIONAL
Enrollment
30
Blood sampling urine collections before RYGP and 1 month and 1 year after.
Hôpital Huriez - Service d'endocrinologie, diabétologie, nutrition et métabolisme
Lille, France
RECRUITINGCorrelation between the variations of urinary cortisol metabolites and plasmatic total BA level before and after RYGB
Time frame: At 1 year
Urinary cortisol metabolite profile modification
Time frame: At 1 month after RYGP, at 1 year after RYGP
Urinary and plasmatic BA profile modification
Time frame: At 1 month after RYGP, at 1 year after RYGP
Correlation between the variations of cortisol metabolites and the variations of metabolic parameters 1 year after gastric bypass
Time frame: at 1 year
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