关键词: 11β-hydroxysteroid dehydrogenase Addison disease cortisol metabolism dual-release hydrocortisone hydrocortisone primary adrenal insufficiency

Mesh : Addison Disease / drug therapy metabolism urine Adult Aged Cortisone / metabolism urine Cross-Over Studies Delayed-Action Preparations / pharmacokinetics therapeutic use Europe Female Humans Hydrocortisone / pharmacokinetics therapeutic use urine Male Metabolome / drug effects Middle Aged Pregnanes / metabolism urine Steroids / metabolism urine Tetrahydrocortisol / metabolism urine Tetrahydrocortisone / metabolism urine Urinalysis

来  源:   DOI:10.1210/clinem/dgaa862   PDF(Sci-hub)   PDF(Pubmed)

Abstract:
Oral once-daily dual-release hydrocortisone (DR-HC) replacement therapy has demonstrated an improved metabolic profile compared to conventional 3-times-daily (TID-HC) therapy among patients with primary adrenal insufficiency. This effect might be related to a more physiological cortisol profile, but also to a modified pattern of cortisol metabolism.
This work aimed to study cortisol metabolism during DR-HC and TID-HC.
A randomized, 12-week, crossover study was conducted.
DC-HC and same daily dose of TID-HC were administered to patients with primary adrenal insufficiency (n = 50) vs healthy individuals (n = 124) as controls.
Urinary corticosteroid metabolites were measured by gas chromatography/mass spectrometry at 24-hour urinary collections.
Total cortisol metabolites decreased during DR-HC compared to TID-HC (P < .001) and reached control values (P = .089). During DR-HC, 11β-hydroxysteroid dehydrogenase type 1 (11β-HSD1) activity measured by tetrahydrocortisol + 5α-tetrahydrocortisol/tetrahydrocortisone ratio was reduced compared to TID-HC (P < .05), but remained increased vs controls (P < .001). 11β-HSD2 activity measured by urinary free cortisone/free cortisol ratio was decreased with TID-HC vs controls (P < .01) but normalized with DR-HC (P = .358). 5α- and 5β-reduced metabolites were decreased with DR-HC compared to TID-HC. Tetrahydrocortisol/5α-tetrahydrocortisol ratio was increased during both treatments, suggesting increased 5β-reductase activity.
The urinary cortisol metabolome shows striking abnormalities in patients receiving conventional TID-HC replacement therapy, with increased 11β-HSD1 activity that may account for the unfavorable metabolic phenotype in primary adrenal insufficiency. Its change toward normalization with DR-HC may mediate beneficial metabolic effects. The urinary cortisol metabolome may serve as a tool to assess optimal cortisol replacement therapy.
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