Triple A syndrome in a patient with genetic growth hormone insensitivity: phenotypic effects of two genetic disorders.

[triple a syndrome]

Primary growth hormone insensitivity (GHI ) and triple A syndrome are rare autosomal recessive disorders .The patient , a 12 -year -old boy from consanguineous parents , was referred for short stature at the age of 7 years (height : -5 .4 SD score ). He had low serum insulin -like growth factor I (IGF-I ) and IGF binding protein 3 and a blunted IGF-I response to recombinant human GH ; molecular analysis of the GH receptor disclosed a homozygous A (-1 )→G (-1 ) at the 5 ' pseudoexon 6 Ψ splice site . Recombinant IGF-I therapy (mecasermin , Increlex ®, twice daily ) initiated at the age of 9 years resulted in an increase of height velocity (HV ) from 4 .0 to 9 .5 cm /year . At the age of 10 .5 years , he presented with asthenia , anorexia , weight loss , a decrease in HV and very low cortisol levels ; adrenal insufficiency was confirmed and glucocorticoid therapy was initiated . Subsequent peripheral motor neuropathy , achalasia and alacrima raised the suspicion of triple A syndrome , which was confirmed by the presence of a homozygous R 194 X mutation in the AAAS gene .T his unusual combination of diseases , to our knowledge , has not been reported to date . Although the patient responded to recombinant IGF-I therapy for GHI , we hypothesize that the treatment could have had an inhibitory effect on 11 β-hydroxysteroid dehydrogenase type 1 activity , thereby reducing the availability of cortisol and precipitating adrenal insufficiency .