nach oben

Erschienen in:

04.10.2022 | Original Article

The clinical and laboratory features of patients with triple A syndrome: a single-center experience in Turkey

verfasst von: Ruken Yıldırım, Edip Unal, Aysel Tekmenuray-Unal, Funda Feryal Taş, Şervan Özalkak, Atilla Çayır, Mehmet Nuri Özbek

Erschienen in: Endocrine | Ausgabe 2/2023

Einloggen, um Zugang zu erhalten

Abstract

Aim

Triple-A Syndrome (TAS) is a rare autosomal recessive disorder characterized by adrenal insufficiency, achalasia, and alacrimia. This disorder is caused by mutations in the AAAS gene. The aim of this study is to discuss the clinical, laboratory and molecular genetic analysis results of 12 patients with TAS.

Method

We evaluated 12 patients from 8 families. Clinical and laboratory data were retrospectively collected from the medical records of the patients in the database for the period 2015–2020. All exons and exon-intron junctions of the AAAS gene were evaluated by next-generation sequencing method. Detected variants were classified according to American Collage of Medical Genetics criteria.

Results

Alacrimia was found in all patients (100%); achalasia was found in 10 patients (83.3%) and adrenal insufficiency was found in 10 patients (83.3%). In addition, hyperreflexia(6/12), learning disability(5/12), hypernasal speech(5/12), muscle weakness(8/12), delayed walking(7/12), delayed speech(6/12), excessive sweating(7/12), optic atrophy(1/12), epilepsy(1/12), palmoplantar hyperkeratosis(5/12), multiple dental caries(9/12), atrophy of the thenar/hypothenar muscles(4/12) and short stature(4/12) were detected. The DHEA-S levels were measured in 10 patients and were found to be low in 8 of them. In all patients, the sodium and potassium levels were found to be normal. AAAS gene sequencing revealed four previously reported c.1066_1067del (p.Leu356fs*8), c.1432 C > T (p.Arg478*), c.688 C > T (p.Arg230*), and c.1368_1372del (p.Gln456fs*38) variants and two novel homozygous c.1250-1 G > A and c.398_399 + 2del variants in the AAAS gene.

Conclusion

We detected two novel variants in the AAAS gene. While the classic triad is present in 66.7% of the cases, neurological dysfunction, skin and dental pathologies also occur quite frequently. The earliest and most common finding of TAS is alacrimia. Therefore, adrenal insufficiency should be investigated in all patients with alacrimia and if necessary, genetic analysis should be performed for TAS. In addition, TAS should be followed up with a multidisciplinary approach since it involves many systems.

D.C. Sadowski, F. Ackah, B. Jiang, L.W. Svenson, Achalasia: incidence, prevalence and survival. A population-based study. Neurogastroenterol. Motil. 22, 256–261 (2010). https://doi.org/10.1111/j.1365-2982.2010.01511.x. Epub 2010 May 11CrossRef

J. Allgrove, G.S. Clayden, J.C. Macaulay, Familial glucocorticoid deficiency with achalasia of the cardia and deficient tear production. Lancet 311, 1284–1286 (1978). https://doi.org/10.1016/S0140-6736(78)91268-0CrossRef

K. Handschug, S. Sperling, S.J. Yoon, S. Hennig, A.J. Clark, A. Huebner, Triple A syndrome is caused by mutations in AAAS, a new WD-repeat protein gene. Hum. Mol. Genet 10, 283–290 (2001). https://doi.org/10.1093/hmg/10.3.283CrossRef

J.M. Cronshaw, A.N. Krutchinsky, W. Zhang, B.T. Chait, M.J. Matunis, Proteomic analysis of the mammalian nuclear pore complex. J. Cell Biol. 158, 915–927 (2002). https://doi.org/10.1083/jcb.200206106CrossRef

R. Prasad, L.A. Metherell, A.J. Clark, H.L. Storr, Deficiency of ALADIN impairs redox homeostasis in human adrenal cells and inhibits steroidogenesis. Endocrinology 154, 3209–3218 (2013). https://doi.org/10.1210/en.2013-1241CrossRef

R. Jühlen, J. Idkowiak, A.E. Taylor, et al. Role of ALADIN in human adrenocortical cells for oxidative stress response and steroidogenesis. PLoS ONE 10, e0124582 (2015). https://doi.org/10.1371/journal.pone.0124582CrossRef

F. Roucher-Boulez, A. Brac de la Perriere, A. Jacquez et al. Triple-A syndrome: a wide spectrum of adrenal dysfunction. Eur. J. Endocrinol. 178, 199–207 (2018)CrossRef

F. Kilicli, F. Acibucu, S. Senel et al. Allgrove syndrome. Singap. Med. J. 53, e92–4 (2012)

M. Ventura, J. Serra-Caetano, R. Cardoso, I. Dinis, M. Melo, F. Carrilho, A. Mirante, The spectrum of pediatric adrenal insufficiency: insights from 34 years of experience. J. Pediatr. Endocrinol. Metab. 32, 721–726 (2019)CrossRef

10.

C.E. Flück, Mechanısms In Endocrınology: Update on pathogenesis of primary adrenal insufficiency: beyond steroid enzyme deficiency and autoimmune adrenal destruction. Eur. J. Endocrinol. 177, 99–111 (2017). Epub 2017 Apr 27CrossRef

11.

R. Perry, O. Kecha, J. Paquette, C. Huot, G. Van Vliet, C. Deal, Primary adrenal insufficiency in children: twenty years experience at the Sainte-ustine Hospital, Montreal. J. Clin. Endocrinol. Metab. 90, 3243–3250 (2005). Epub 2005 Apr 5CrossRef

12.

M. Wijaya, M. Huamei, Z. Jun, M. Du, Y. Li, Q. Chen, H. Chen, G. Song, Etiology of primary adrenal insufficiency in children: a 29-year singlecenter experience. J. Pediatr. Endocrinol. Metab. 32, 615–622 (2019)CrossRef

13.

T. Kirkgoz, T. Guran, Primary adrenal insufficiency in children: diagnosis and management. Best. Pr. Res Clin. Endocrinol. Metab. 32, 397–424 (2018). https://doi.org/10.1016/j.beem.2018.05.010CrossRef

14.

E. Kurnaz, P. Duminuco, Z. Aycan, Ş. Savaş-Erdeve, N. Muratoğlu Şahin, M. Keskin, E. Bayramoğlu, M. Bonomi, S. Çetinkaya, Clinical and genetic characterisation of a series of patients with triple A syndrome. Eur. J. Pediatr. 177(3 Mar), 363–369 (2018). https://doi.org/10.1007/s00431-017-3068-8. Epub 2017 Dec 19CrossRef

15.

R. Polat, A. Ustyol, E. Tuncez, T. Guran, A broad range of symptoms in allgrove syndrome: single center experience in Southeast Anatolia. J. Endocrinol. Investig. 43(2 Feb), 185–196 (2020). https://doi.org/10.1007/s40618-019-01099-2. Epub 2019 Aug 21CrossRef

16.

T. Milenkovic, D. Zdravkovic, N. Savic, S. Todorovic, K. Mitrovic, K. Koehler, A. Huebner, Triple A syndrome: 32 years experience of a single centre (1977-2008). Eur. J. Pediatr. 169(11), 1323–8 (2010). https://doi.org/10.1007/s00431-010-1222-7. Epub 2010 May 25CrossRef

17.

F. Gaiani, P. Gismondi, R. Minelli, G. Casadio, N. de’Angelis, F. Fornaroli, G.L. de’Angelis, M. Manfredi, Case report of a familial triple: a syndrome and review of the literature. Med. (Baltim.) 29(22), e20474 (2020). https://doi.org/10.1097/MD.0000000000020474. 99CrossRef

18.

F. Kallabi, N. Belghuith, H. Aloulou et al. Clinical and genetic characterization of 26 Tunisian patients with Allgrove syndrome. Arch. Med. Res. 47, 105–110 (2016). https://doi.org/10.1016/j.arcmed.2016.04.004CrossRef

19.

L.M. Walter, E.F. Christa. Adrenal cortex and its disorders. Pediatric Endocrinology. In: ed A. Sperling Mark (Elsevier Saunders: Philadelphia, 2014), p. 471–532.

20.

H. Patt, K. Koehler, S. Lodha et al. Phenotype–genotype spectrum of AAA syndrome from Western India and systematic review of literature. Endocr. Connect. 6, 901–913 (2017). https://doi.org/10.1530/EC-17-0255CrossRef

21.

H.L. Storr, B. Kind, D.A. Parfitt et al. Deficiency of ferritin heavy-chain nuclear import in triple a syndrome implies nuclear oxidative damage as the primary disease mechanism. Mol. Endocrinol. 23, 2086–2094 (2009). https://doi.org/10.1210/me.2009-0056CrossRef

22.

M. Hirano, Y. Furiya, H. Asai, A. Yasui, S. Ueno, ALADINI482S causes selective failure of nuclear protein import and hypersensitivity to oxidative stress in triple A syndrome. Proc. Natl Acad. Sci. 103, 2298–2303 (2006). https://doi.org/10.1073/pnas.0505598103CrossRef

23.

E. Çamtosun, İ. Dündar, A. Akıncı, L. Kayaş, N. Çiftci, Pediatric Primary Adrenal Insufficiency: A 21-year Single Center Experience. J. Clin. Res Pediatr. Endocrinol. 13(1 Feb), 88–99 (2021). https://doi.org/10.4274/jcrpe.galenos.2020.2020.0132. Epub 2020 Sep 17CrossRef

24.

R. Lanes, L.P. Plotnick, T.E. Bynum et al. Glucocorticoid and partial mineralocorticoid deficiency associated with achalasia. J. Clin. Endocrinol. Metab. 50, 268–270 (1980). https://doi.org/10.1210/jcem-50-2-268CrossRef

25.

C.V. Collares, J. Antunes-Rodrigues, A.C. Moreira, S.N. Franca, L.A. Pereira, M.M. Soares, J. Elias Junior, A.J. Clark, M. de Castro, L.L. Elias, Heterogeneity in the molecular basis of ACTH resistance syndrome. Eur. J. Endocrinol. 159, 61–68 (2008). https://doi.org/10.1530/EJE-08-0079CrossRef

26.

M. Dumic, N. Barišic, V. Kusec, K. Stingl, M. Skegro, A. Stanimirovic, K. Koehler, A. Huebner, Long-term clinical follow-up and molecular genetic findings in eight patients with triple A syndrome. Eur. J. Pediatr. 171(10), 1453–9 (2012). https://doi.org/10.1007/s00431-012-1745-1. Epub 2012 Apr 28CrossRef

27.

A. Tebaibia, M.A. Boudjella, D. Boutarene, F. Benmediouni, H. Brahimi, N. Oumnia, Incidence, clinical features and para-clinical findings of achalasia in Algeria: experience of 25 years. World J. Gastroenterol. 22, 8615–8623 (2016). https://doi.org/10.3748/wjg.v22.i38.8615CrossRef

28.

C. Hallal, C.O. Kieling, D.L. Nunes, C.T. Ferreira, G. Peterson, S.G. Barros, C.A. Arruda, J.C. Fraga, H.A. Goldani, Diagnosis, misdiagnosis, and associated diseases of achalasia in children and adolescents: a twelve-year single center experience. Pediatr. Surg. Int. 28(12), 1211–1217 (2012). https://doi.org/10.1007/s00383-012-3214-3CrossRef

29.

A.E. Vallet, A. Verschueren, P. Petiot et al. Neurological features in adult Triple-A (Allgrove) syndrome. J. Neurol. 259, 39–46 (2012). https://doi.org/10.1007/s00415-011-6115-9CrossRef

30.

C. Goizet, B. Catargi, F. Tison, A. Tullio-Pelet, S. Hadj-Rabia, F. Pujol, A. Lagueny, S. Lyonnet, D. Lacombe, Progressive bulbospinal amyotrophy in triple A syndrome with AAAS gene mutation. Neurology 58(6), 962–965 (2002)CrossRef

31.

H. Houlden, S. Smith, M. De Carvalho, J. Blake, C. Mathias, N.W. Wood, M.M. Reilly, Clinical and genetic characterization of families with triple A (Allgrove) syndrome. Brain 125(Pt 12 Dec), 2681–90 (2002). https://doi.org/10.1093/brain/awf270CrossRef

32.

M. Gazarian, C.T. Cowell, M. Bonney, W.G. Grigor, The 4A syndrome: adrenocortical insufficiency associated with achalasia, alacrima, autonomic and other neurological abnormalities. Eur. J. Pediatr. 154, 18–23 (1995)CrossRef

33.

B. Kind, K. Koehler, M. Krumbholz, D. Landgraf, A. Huebner, Intracellular ROS level is increased in fibroblasts of triple A syndrome patients. J. Mol. Med (Berl.) 88, 1233–1242 (2010). https://doi.org/10.1007/s00109-010-0661-yCrossRef

Titel: The clinical and laboratory features of patients with triple A syndrome: a single-center experience in Turkey
verfasst von: Ruken Yıldırım
Edip Unal
Aysel Tekmenuray-Unal
Funda Feryal Taş
Şervan Özalkak
Atilla Çayır
Mehmet Nuri Özbek
Publikationsdatum: 04.10.2022
Verlag: Springer US
Erschienen in: Endocrine / Ausgabe 2/2023
Print ISSN: 1355-008X
Elektronische ISSN: 1559-0100
DOI: https://doi.org/10.1007/s12020-022-03206-5

Leitlinien kompakt für die Innere Medizin

Mit medbee Pocketcards sicher entscheiden.

^{Seit 2022 gehört die medbee GmbH zum Springer Medizin Verlag}

Kostenlos registrieren

Neu im Fachgebiet Innere Medizin

Notfall-TEP der Hüfte ist auch bei 90-Jährigen machbar

26.04.2024 Hüft-TEP Nachrichten

Ob bei einer Notfalloperation nach Schenkelhalsfraktur eine Hemiarthroplastik oder eine totale Endoprothese (TEP) eingebaut wird, sollte nicht allein vom Alter der Patientinnen und Patienten abhängen. Auch über 90-Jährige können von der TEP profitieren.

Niedriger diastolischer Blutdruck erhöht Risiko für schwere kardiovaskuläre Komplikationen

25.04.2024 Hypotonie Nachrichten

Wenn unter einer medikamentösen Hochdrucktherapie der diastolische Blutdruck in den Keller geht, steigt das Risiko für schwere kardiovaskuläre Ereignisse: Darauf deutet eine Sekundäranalyse der SPRINT-Studie hin.

Bei schweren Reaktionen auf Insektenstiche empfiehlt sich eine spezifische Immuntherapie

25.04.2024 Allergien und Intoleranzreaktionen Nachrichten

Insektenstiche sind bei Erwachsenen die häufigsten Auslöser einer Anaphylaxie. Einen wirksamen Schutz vor schweren anaphylaktischen Reaktionen bietet die allergenspezifische Immuntherapie. Jedoch kommt sie noch viel zu selten zum Einsatz.

Therapiestart mit Blutdrucksenkern erhöht Frakturrisiko

25.04.2024 Hypertonie Nachrichten

Beginnen ältere Männer im Pflegeheim eine Antihypertensiva-Therapie, dann ist die Frakturrate in den folgenden 30 Tagen mehr als verdoppelt. Besonders häufig stürzen Demenzkranke und Männer, die erstmals Blutdrucksenker nehmen. Dafür spricht eine Analyse unter US-Veteranen.

Update Innere Medizin

Bestellen Sie unseren Fach-Newsletter und bleiben Sie gut informiert.

Newsletter bestellen

Springer Medizin

Abstract

Aim

Method

Results

Conclusion

Bitte loggen Sie sich ein, um Zugang zu diesem Inhalt zu erhalten

Weitere Artikel der Ausgabe 2/2023

Clinical characteristics and prognostic nomogram for patients with insular thyroid carcinoma: a population-based analysis

Impact of the COVID-19 pandemic on the incidence, seasonal distribution, and characteristics of subacute thyroiditis

COVID-19 and its treatments: lights and shadows on testicular function

Longitudinal trends in lipid profile in indian children and youth with type-1 diabetes: a 5-year follow up from a single centre

Optimal method for detecting cervical lymph node metastasis from papillary thyroid cancer