A Rationale for Mineralocorticoid Supplementation in Classic Congenital Adrenal Hyperplasia.

most common example of this phenomenon is Cushing syndrome due to high endogenous or exogenous cortisol exposure. Iatrogenic Cushing syndrome, characterized by inhibition of statural growth in children, excess weight gain, metabolic syndrome, and hypertension, may be observed in CAH patients receiving excessive glucocorticoid treatment [6] . This is why it is important to balance the need for suppression of adrenal androgen precursors with the opposing practical dictum of minimizing glucocorticoid exposure, particularly in growing children. One way to achieve the desired balance is to treat classic CAH patients from infancy with a combination of moderate doses of both glucocorticoid and mineralocorticoid supplements. A systematic review and meta-analysis of treatment outcomes in CAH patients revealed that those children who received long-term treatment with mineralocorticoids achieved significantly better adult heights compared with those who were prescribed glucocorticoids alone [7] . On the other hand, investigators have observed elevated 24-hour ambulatory blood pressure in children [8] and adults [9] with CAH. However, it has not been demonstrated that young adults with CAH suffer clinically significant cardiac morbidities or mortality [10] . Taken together, the implication of the available data is that clinicians should prudently prescribe minerThe study by Mooij et al. [1] in this issue underscores the interrelatedness of adrenal cortical steroids in achieving balance in the treatment of patients with congenital adrenal hyperplasia (CAH). In this set of in vitro experiments, the investigators delineate the nature of 17-hydroxyprogesterone and progesterone interference with the ability of aldosterone to transactivate the mineralocorticoid receptor (MR). This occurs at the level of receptor transactivation, rather than nuclear translocation. It is reasonable to infer from these data that a similar in vivo phenomenon occurs at the high 17-hydroxyprogesterone levels and low physiologic aldosterone levels measured in inadequately controlled classic CAH patients. It has long been recognized that elevated plasma renin levels reflecting low aldosterone production and/or activity are found among CAH patients with elevated steroid 21-hydroxylase precursors [2, 3] . Previous in vitro studies have confirmed the hypothesis that progesterone and its analogs are the culprits inhibiting MR [4] . An obvious corollary of these findings is exacerbation of sodium wasting in CAH patients, potentially impeding normal growth and even triggering adrenal crisis. In contrast to the ability of progesterones to interfere with aldosterone-induced MR activity, cortisol may bind to and activate the MR causing hypertension [5] . The Received: January 19, 2015 Accepted: January 26, 2015 Published online: April 25, 2015 HORMONE RESEARCH IN PÆDIATRICS