Clinical Presentation of a Complex Neurodevelopmental Disorder Caused by Mutations in ADNP

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Title:	Clinical Presentation of a Complex Neurodevelopmental Disorder Caused by Mutations in ADNP
Author(s):	Dijck, A. Van; Vulto-van Silfhout, A.T. ; Cappuyns, E.; Werf, I.M. van der; Mancini, G.M.S.; Tzschach, A.; Bernier, R.; Gozes, I.; Eichler, E.E.; Romano, C; Lindstrand, A.; Nordgren, A.; Kvarnung, M.; Kleefstra, T. ; Vries, B.B. de ; Kury, S.; Rosenfeld, J.A.; Meuwissen, M.E.; Vandeweyer, G.; Kooy, R.F.; Schouten, M.I. ; Willemsen, M.H. ; Marcelis, C.L. ; Ockeloen, C.W. ; Burgt, I. van der ; Feenstra, I. ; Manning, M.A.; Slattery, L.
Publication year:	2019
Source:	Biological Psychiatry, vol. 85, iss. 4, (2019), pp. 287-297
ISSN:	0006-3223
DOI:	https://doi.org/10.1016/j.biopsych.2018.02.1173
Publication type:	Article / Letter to editor
Please use this identifier to cite or link to this item : https://hdl.handle.net/2066/202777
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Subject:	Radboudumc 7: Neurodevelopmental disorders DCMN: Donders Center for Medical Neuroscience Radboudumc 9: Rare cancers RIHS: Radboud Institute for Health Sciences
Organization:	Human Genetics
Journal title:	Biological Psychiatry
Volume:	vol. 85
Issue:	iss. 4
Page start:	p. 287
Page end:	p. 297
Abstract:	BACKGROUND: In genome-wide screening studies for de novo mutations underlying autism and intellectual disability, mutations in the ADNP gene are consistently reported among the most frequent. ADNP mutations have been identified in children with autism spectrum disorder comorbid with intellectual disability, distinctive facial features, and deficits in multiple organ systems. However, a comprehensive clinical description of the Helsmoortel-Van der Aa syndrome is lacking. METHODS: We identified a worldwide cohort of 78 individuals with likely disruptive mutations in ADNP from January 2014 to October 2016 through systematic literature search, by contacting collaborators, and through direct interaction with parents. Clinicians filled in a structured questionnaire on genetic and clinical findings to enable correlations between genotype and phenotype. Clinical photographs and specialist reports were gathered. Parents were interviewed to complement the written questionnaires. RESULTS: We report on the detailed clinical characterization of a large cohort of individuals with an ADNP mutation and demonstrate a distinctive combination of clinical features, including mild to severe intellectual disability, autism, severe speech and motor delay, and common facial characteristics. Brain abnormalities, behavioral problems, sleep disturbance, epilepsy, hypotonia, visual problems, congenital heart defects, gastrointestinal problems, short stature, and hormonal deficiencies are common comorbidities. Strikingly, individuals with the recurrent p.Tyr719* mutation were more severely affected. CONCLUSIONS: This overview defines the full clinical spectrum of individuals with ADNP mutations, a specific autism subtype. We show that individuals with mutations in ADNP have many overlapping clinical features that are distinctive from those of other autism and/or intellectual disability syndromes. In addition, our data show preliminary evidence of a correlation between genotype and phenotype.