Assessment of the gonadotrophin-gonadal axis in androgen insensitivity syndrome
a Department of
Paediatrics, University of Cambridge Clinical School, Box 116, Addenbrookes Hospital, Hills Road, Cambridge CB2 2QQ, UK, b Department of
Paediatrics, Princess Margaret Hospital, Lai Chi Kok, Kowloon, Hong
Kong
Correspondence to: Dr Ahmed. email: sfa21{at}cam.ac.uk
Accepted 19 October
1998
OBJECTIVE
To study the
value of measuring serum luteinising hormone (LH), follicle stimulating
hormone (FSH), testosterone, and dihydrotestosterone (DHT) in androgen
insensitivity syndrome (AIS).
DESIGN
Retrospective
study of patients on a nationwide register of AIS.
PATIENTS
Sixty one
cases of AIS with androgen receptor (AR) dysfunction (abnormalities of
the AR gene and/or abnormal AR binding) were divided into three age
groups: infants, < 1 year old; children, 1-13 years old; and
postpubertal, > 13 years old.
MEASUREMENTS
Age, dose
of human chorionic gonadotrophin (hCG) stimulation, pre-hCG and
post-hCG serum testosterone values, serum DHT values, and serum LH and
FSH values before and after LH releasing hormone (LHRH) stimulation.
RESULTS
In 23 of 30 infants testosterone was within age related reference ranges; six were
above this range. The median testosterone rise following variable
dosage of hCG was 9.5 times the basal value. The increment was not
related to the hCG dose, age, or basal concentration of testosterone.
The median basal and stimulated testosterone:DHT ratios were 2.5 and
6.1, respectively. The median increment in DHT was 2.2-fold. Seventeen
of 18 FSH and 11 of 19 LH measurements were within age related ranges
in infants; in seven patients LH values were above the range. LHRH
stimulation performed in 39 patients showed an exaggerated LH in all
age groups. The FSH response was not exaggerated in children.
CONCLUSION
Although a
positive hCG test excludes biosynthetic defects of testosterone, an
inadequate response does not exclude AIS. Basal LH and testosterone may
not be raised during early infancy. An LHRH stimulation test might be
useful for evaluating cases of suspected AIS presenting in
mid-childhood.
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Key messages
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© 1999 by Archives of Disease in Childhood
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