Interrelationships Among Cortisol, 17-Hydroxyprogesterone, and Androstenendione Exposures in the Management of Children With Congenital Adrenal Hyperplasia.

[congenital adrenal hyperplasia]

: Hydrocortisone is the standard replacement therapy for children with congenital adrenal hyperplasia (CAH ). Relationships between cortisol exposures and pharmacodynamic responses of 17 -hydroxyprogesterone and androstenedione exposures have not been systematically evaluated .(1 ) Assess individual oral hydrocortisone pharmacokinetics ; (2 ) relate the observed cortisol exposure in each subject to the observed exposures of 17 -hydroxyprogesterone and androstenedione ; (3 ) determine potential individualized treatment regimens based on each subject 's pharmacokinetic and pharmacodynamic parameters .Thirty -four patients (18 boys , 16 girls , aged 1 .4 to 18 .1 years ) with CAH underwent 6 -hour pharmacokinetic studies . Results were analyzed by noncompartmental methods to obtain the area under the curve (AUC ) for cortisol , 17 -hydroxyprogesterone , and androstenedione ; maximum concentration and time-to -maximum concentration for cortisol ; and minimum and time-to -minimum concentration for 17 -hydroxyprogesterone and androstenedione .Mean (SD ) cortisol half -life and Cmax were 1 .01 (0 .20 ) hours and 24 .4 (5 .4 ) μg /dL , respectively . The AUCs for cortisol , 17 -hydroxyprogesterone and androstenedione were 40 .8 (14 .5 ) μg hour /dL , 29 ,490 (23 ,539 ) ng hour /dL , and 680 (795 ) ng hour /dL , respectively . No significant relationships existed between cortisol AUCs and the AUCs of either 17 -hydroxyprogesterone (P = 0 .32 ) or androstenedione (P = 0 .99 ); nor were there differences between the change -from-baseline concentrations for cortisol with either 17 -hydroxyprogesterone (P = 0 .80 ) or androstenedione (P = 0 .40 ). Cortisol simulations indicated that although four daily doses decreased 24 -hour hypercortisolemia and hypocortisolemia , substantial periods of each remained .Concentration profiles of cortisol , 17 -hydroxyprogesterone , and androstenedione are highly variable in children with CAH , and knowledge of them can assist in personalizing the therapy of CAH patients . Hydrocortisone 's rapid half -life and the lack of a sustained-released product make it difficult to closely approximate normal circadian profiles .