Long-term clinical follow-up and molecular genetic findings in eight patients with triple A syndrome.

[triple a syndrome]

The triple A syndrome (Allgrove syndrome , OMIM #231550 ) is caused by autosomal recessively inherited mutations in the AAAS gene on chromosome 12 q 13 encoding the nuclear pore protein ALADIN . This multisystemic disease is characterised by achalasia , alacrima , adrenal insufficiency and neurological impairment . We analyse long -term clinical follow-up and results of sequencing of the AAAS gene in eight patients with triple A syndrome aged from 2 to 35 years . At the time of diagnosis , all patients presented with alacrima , neurological dysfunction , dermatological abnormalities , seven of them with adrenal insufficiency and five of them with achalasia . Sequencing of the AAAS gene identified the p .S 263 P mutation in five of eight patients , supporting the hypothesis that this mutation is a founder mutation in Slavic population . One of the patients is homozygous for the p .S 263 P mutation , two are compound heterozygous for the p .S 263 P and the p .G 14 fs mutation , two are compound heterozygous for the p .S 263 Pro mutation and p .S 296 Y mutation , two are compound heterozygous for the p .G 14 fs and the p .Q 387 X mutations and one is homozygous for the p .Q 387 X mutation . In the course of the follow-up time of 4 -29 years , progression of existing and appearance of new symptoms developed . Although severe , many of these symptoms presented in all six young adult patients are often overlooked or neglected : postural hypotension with blurred vision and syncope , hyposalivation resulting with complete edentulosis , talocrular contractures with permanent walking difficulties and erectile dysfunction in male patients . Triple A syndrome is a progressive debilitating disorder which may seriously affect quality of life and even be life-threatening in patients with severe neurological impairment .Long -term follow-up of patients with triple A syndrome revealed a variety of the clinical features involving many systems . Progressive natural course of the disease may seriously affect quality of life and even be life-threatening in patients with severe neurological impairment .