Spectrum of mutations of the AAAS gene in Allgrove syndrome: lack of mutations in six kindreds with isolated resistance to corticotropin.

[triple a syndrome]

Familial glucocorticoid deficiency due to corticotropin (ACTH ) resistance consists of two distinct genetic syndromes that are both inherited as autosomal recessive traits : isolated ACTH resistance (iACTHR ), which may be caused by inactivating mutations of the ACTH receptor (the MC 2 R gene ) or mutations in an as yet unknown gene (s ), and Allgrove syndrome (AS ). The latter is also known as triple-A syndrome (MIM 231550 ). In three large cohorts of AS kindreds , the disease has been mapped to chromosome 12 ; most recently , mutations in the AAAS gene on 12 q 13 were found in these AS families . AAAS codes for the WD-repeat containing ALADIN (for alacrima -achalasia -adrenal insufficiency -neurologic disorder ) protein . We investigated families with iACTHR (n = 4 ) and AS (n = 6 ) and a Bedouin family with ACTHR and a known defect of the TSH receptor . Four AS families were of mixed extraction from Puerto Rico (PR ); most of the remaining six families were Caucasian families from North America (NA ). Sequencing analysis found no MC 2 R genetic defects in any of the kindreds . No iACTHR kindreds , but all of AS families , had AAAS mutations . The previously reported IVS 14 +1 G-->A splice donor mutation was found in all PR families , apparently due to a founder effect ; one NA kindred was heterozygous for this mutation . In the latter family , long -range PCR failed to identify a deletion or other rearrangements of the AAAS gene . No other heterozygote or transmitting parent had any phenotype that could be considered part of AS . The IVS 14 +1 G-->A mutation results in a premature termination of the predicted protein ; although it was present in all PR families (in the homozygote state in three of them ), there was substantial clinical variation between them . One PR family also carried a novel splice donor mutation of the AAAS gene in exon 11 , IVS 11 +1 G-->A ; the proband was a compound heterozygote . A novel point mutation , 43 C-->A (Gln 15 L ys ), in exon 1 of the AAAS gene was identified in the homozygote state in a Canadian AS kindred with a milder AS phenotype . The predicted amino acid substitution in this family is located in a sequence that may participate in the preservation of stability of ALADIN beta -strands , whereas the splicing mutation in exon 11 may interfere with the formation of WD repeats in this molecule . We conclude that 1 ) AAAS does not appear to be frequently mutated in families with iACTHR ; 2 ) AAAS is mutated in AS families from PR (that had previously been mapped to 12 q 13 ) and NA ; and , 3 ) there is significant clinical variability between patients with the same AAAS defect .