Genotypic heterogeneity and clinical phenotype in triple A syndrome: a review of the NIH experience 2000-2005

Genotypic heterogeneity and clinical phenotype in triple A syndrome: a review of the NIH experience 2000-2005

Triple A syndrome (AAAS, OMIM#231550) is an autosomal recessive condition characterized by adrenal insufficiency, achalasia, alacrima, neurodegeneration and autonomic dysfunction. Mutations in the AAAS gene on chromosome 12q13 have been reported in several subjects with AAAS. Over the last 5 years,...

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Veröffentlicht in:Clinical genetics 2005-09, Vol.68 (3), p.215-221
Hauptverfasser: Brooks, BP, Kleta, R, Stuart, C, Tuchman, M, Jeong, A, Stergiopoulos, SG, Bei, T, Bjornson, B, Russell, L, Chanoine, J-P, Tsagarakis, S, Kalsner, LR, Stratakis, CA
Format: Artikel
Sprache:eng
Schlagworte:
achalasia
Adolescent
adrenal insufficiency
Adrenal Insufficiency - genetics
Adrenals. Adrenal axis. Renin-angiotensin system (diseases)
Adult
alacrima
autonomic dysfunction
Base Sequence
Biological and medical sciences
Child
Child, Preschool
Chromosomes, Human, Pair 12
Chromosomes, Human, Pair 13
Endocrinopathies
Esophageal Achalasia - genetics
Esophagus
Female
Gastroenterology. Liver. Pancreas. Abdomen
General aspects. Genetic counseling
Genes, Recessive
Genetic Heterogeneity
Humans
Lacrimal Apparatus Diseases - genetics
Male
Malformations
Medical genetics
Medical sciences
Mutation
National Institutes of Health (U.S.)
Nerve Tissue Proteins
Non tumoral diseases. Target tissue resistance. Benign neoplasms
nuclear pore complex
Nuclear Pore Complex Proteins
Phenotype
Proteins
Syndrome
triple A syndrome
United States
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Zusammenfassung:Triple A syndrome (AAAS, OMIM#231550) is an autosomal recessive condition characterized by adrenal insufficiency, achalasia, alacrima, neurodegeneration and autonomic dysfunction. Mutations in the AAAS gene on chromosome 12q13 have been reported in several subjects with AAAS. Over the last 5 years, we have evaluated six subjects with the clinical diagnosis of AAAS. Three subjects had mutations in the AAAS gene – including one novel mutation (IVS8+1 G>A) – and a broad spectrum of clinical presentations. However, three subjects with classic AAAS did not have mutations in the AAAS gene on both alleles. This finding supports the notion of genetic heterogeneity for this disorder, although other genetic mechanisms cannot be excluded.
ISSN:0009-9163
1399-0004
DOI:10.1111/j.1399-0004.2005.00482.x