Auxological data is the gold standard index of the therapeutic condition in CYP21A2
deficiency over a long-range period, whereas urinary pregnanetriol for 24 h (PT) is
variable for a shorter-range period. Ideal PT levels in comparison with auxological data
have not been reported. The main purpose of this study was to analyze ideal PT values as
an index of optimal control for CYP21A2 deficiency. First, inter-daily fluctuation of PT
was analyzed in one participant. PT levels were distributed over a wide range of 0.44–14.7
mg/day (n=42) in this participant, suggesting that the therapeutic condition should be
judged by multiple PT samples. Second, the therapeutic periods of 15 participants with
CYP21A2 deficiency were classified using auxological data and Cushing-like symptoms, and
the PT levels were analyzed in each period retrospectively. The 95% confidence intervals
for the means of the PT levels in the excessive, good and poor control periods were
0.03–1.25 (n=26), 1.23–2.09 (n=116), and 5.35–8.37 (n=72) mg/m2/day,
respectively. In conclusion, 1.2–2.1 mg/m2/day of PT values can be used as an
index of optimal control in CYP21A2 deficiency.
Auxological data are the gold standard indexes of the therapeutic conditions in patients
with CYP21 deficiency over long-term periods, whereas urinary pregnanetriol (PT) for 24 h
has been used as an index for short-term periods. We previously reported that the range of
1.2–2.1 mg/m2/day of PT for 24 h (24-h PT) could be used as an index of optimal
control in patients with CYP21 deficiency. The purpose of this study was to analyze the
range of PT in the first morning urine samples (morning PT) as an index of optimal control
in patients with CYP21 deficiency. First, the therapeutic periods of 15 participants (aged
2 yr and 5 mo to 17 yr and 4 mo) were classified into excessive, good or poor control
periods using auxological data and Cushing-like symptoms, and 24-h PT levels were analyzed
in each period, retrospectively. The 95% confidence intervals for the means of 24-h PT
levels in the excessive, good and poor control periods were 0.24–2.24 (n=25), 2.88–4.92
(n=114) and 13.26–21.28 (n=72) mg/gCr, respectively. Subsequently, 24-h PT and morning PT
levels collected on the same day were analyzed for 14 participants (aged 9 mo to 29 yr and
8 mo). There was a significant correlation between the above two PT levels (n=25,
p<0.0001). When the 24-h PT range of the good control period, 2.88–4.92 mg/gCr, was
adjusted by the correlation, the ideal morning PT range became 2.15–3.34 mg/gCr. In
conclusion, a morning PT in the range of 2.2–3.3 mg/gCr can be used as an index of optimal
control in patients with CYP21 deficiency.
Adrenal crises (ACs) sometimes progress rapidly and can be fatal. The aims of
the present study were to reveal whether stress doses of glucocorticoids (SDGs) can
prevent progression of severe ACs and to suggest a method of prevention, through analysis
of its clinical features. We studied 24 severe ACs (nine patients) that occurred after
diagnosis of primary or secondary adrenal insufficiency, retrospectively. The following
information was analyzed: 1) whether SDGs were given orally and/or sc; 2) duration from
the time when some symptoms started to the time when the patient came to the hospital; and
3) presence of hypoglycemia and electrolyte disturbance (hyponatremia, hyperkalemia).
Eleven crises occurred after taking SDGs. Ten crises progressed within 3 h. Six of these
ten crises progressed to severe ACs despite the fact that the patients took SDGs. Six
crises were observed in association with hypoglycemia, and five of these six crises
occurred in patients under 5 yr of age. Three of the six crises in association with
hypoglycemia progressed to ACs within 3 h. Two of the three crises progressed to severe
status within 3 h despite the fact that the patients took SDGs. Electrolyte disturbance
was observed in only one crisis. In conclusion, SDGs cannot prevent progression of all
ACs. Progression can be associated with hypoglycemia, particularly in patients under 5 yr
of age. Patients should be given guidance on an ongoing basis on how to prevent ACs and
hypoglycemia.
A patient with congenital hypopituitarism associated with cholestasis is reported here.
Large doses of fat-soluble hormones (hydrocortisone (20 mg/m2/day) and
L-thyroxine (14 μg/kg/day)) were needed to resolve hypoglycemia and hypothyroidism during
cholestasis. The doses could be reduced to 10 mg/m2/day and 3.5 μg/kg/day,
respectively, after improvement of cholestasis. Sodium valproate, which is a water-soluble
drug, did not need any dose adjustments during cholestasis. Adjustment of fat-soluble
hormone doses during cholestasis should be considered in patients with cholestasis.
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