ARID1B-related disorder in 87 adults: Natural history and self-sustainability

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dc.contributor.authorvan der Sluijs, P. J.
dc.contributor.authorGösgens, M.
dc.contributor.authorDingemans, A. J. M.
dc.contributor.authorStriano, P.
dc.contributor.authorRiva, A.
dc.contributor.authorMignot, C.
dc.contributor.authorFaudet, A.
dc.contributor.authorVasileiou, G.
dc.contributor.authorWalther, M.
dc.contributor.authorSchrier Vergano, S. A.
dc.contributor.authorAlders, M.
dc.contributor.authorAlkuraya, F. S.
dc.contributor.authorAlorainy, I.
dc.contributor.authorAlsaif, H. S.
dc.contributor.authorAnderlid, B.
dc.contributor.authorBache, I.
dc.contributor.authorvan Beek, I.
dc.contributor.authorBlanluet, M.
dc.contributor.authorvan Bon, B. W.
dc.contributor.authorBrunet, T.
dc.contributor.authorBrunner, H.
dc.contributor.authorCarriero, M. L.
dc.contributor.authorCharles, P.
dc.contributor.authorChatron, N.
dc.contributor.authorCoccia, E.
dc.contributor.authorDubourg, C.
dc.contributor.authorEarl, R. K.
dc.contributor.authorEichler, E. E.
dc.contributor.authorFaivre, L.
dc.contributor.authorFoulds, N.
dc.contributor.authorGraziano, C.
dc.contributor.authorGuerrot, A. M.
dc.contributor.authorHashem, M. O.
dc.contributor.authorHeide, S.
dc.contributor.authorHeron, D.
dc.contributor.authorHickey, S. E.
dc.contributor.authorHopman, S. M. J.
dc.contributor.authorKattentidt-Mouravieva, A.
dc.contributor.authorKerkhof, J.
dc.contributor.authorKlein Wassink-Ruiter, J. S.
dc.contributor.authorKurtz-Nelson, E. C.
dc.contributor.authorKušíková, K.
dc.contributor.authorKvarnung, M.
dc.contributor.authorLecoquierre, F.
dc.contributor.authorLeszinski, G. S.
dc.contributor.authorLoberti, L.
dc.contributor.authorMagoulas, P. L.
dc.contributor.authorMari, F.
dc.contributor.authorMaystadt, I.
dc.contributor.authorMerla, G.
dc.contributor.authorMilunsky, J. M.
dc.contributor.authorMoortgat, S.
dc.contributor.authorNicolas, G.
dc.contributor.authorO'Leary, M.
dc.contributor.authorOdent, S.
dc.contributor.authorOzmore, J. R.
dc.contributor.authorParbhoo, K.
dc.contributor.authorPfundt, R.
dc.contributor.authorPiccione, M.
dc.contributor.authorPinto, A. M.
dc.contributor.authorPopp, B.
dc.contributor.authorPutoux, A.
dc.contributor.authorRehm, H. L.
dc.contributor.authorReis, A.
dc.contributor.authorRenieri, A.
dc.contributor.authorRosenfeld, J. A.
dc.contributor.authorRossi, M.
dc.contributor.authorSalzano, E.
dc.contributor.authorSaugier-Veber, P.
dc.contributor.authorSeri, M.
dc.contributor.authorSeveri, G.
dc.contributor.authorSonmez, F. M.
dc.contributor.authorStrobl-Wildemann, G.
dc.contributor.authorStuurman, K. E.
dc.contributor.authorUctepe, E.
dc.contributor.authorVan Esch, H.
dc.contributor.authorVitetta, G.
dc.contributor.authorde Vries, B. B. A.
dc.contributor.authorWahl, D.
dc.contributor.authorWang, T.
dc.contributor.authorZacher, P.
dc.contributor.authorHeitink, K. R.
dc.contributor.authorRopers, F. G.
dc.contributor.authorSteenbeek, D.
dc.contributor.authorRybak, T.
dc.contributor.authorSanten, G. W. E.
dc.contributor.departmentPediatrics, School of Medicine
dc.date.accessioned2025-01-27T12:20:33Z
dc.date.available2025-01-27T12:20:33Z
dc.date.issued2024-07-23
dc.description.abstractPurpose: ARID1B is one of the most frequently mutated genes in intellectual disability cohorts. Thus, far few adult-aged patients with ARID1B-related disorder have been described, which limits our understanding of the disease's natural history and our ability to counsel patients and their families. Methods: Data on patients aged 18+ years with ARID1B-related disorder were collected through an online questionnaire completed by clinicians and parents. Results: Eighty-seven adult patients with ARID1B were included. Cognitive functioning ranged from borderline to severe intellectual disability. Patients identified through the genetic workup of their child were either mosaic or had a variant in exon 1. New clinical features identified in this population are loss of skill (16/64, 25%) and recurrent patella luxation (12/45, 32%). Self-sustainability data showed that 88% (45/51) could eat independently, and 16% (7/45) could travel alone by public transport. Facial photo analysis showed that patients' photographs taken at different ages clustered consistently, separate from matched controls. Conclusion: The ARID1B spectrum is broad, and as patients age, there is a significant shift in the medical aspects requiring attention. To address the changing medical needs with increasing age, we have formulated recommendations to promote timely intervention in an attempt to mitigate disease progression.
dc.eprint.versionFinal published version
dc.identifier.citationvan der Sluijs PJ, Gösgens M, Dingemans AJM, et al. ARID1B-related disorder in 87 adults: Natural history and self-sustainability. Genet Med Open. 2024;2:101873. Published 2024 Jul 23. doi:10.1016/j.gimo.2024.101873
dc.identifier.urihttps://hdl.handle.net/1805/45483
dc.language.isoen_US
dc.publisherElsevier
dc.relation.isversionof10.1016/j.gimo.2024.101873
dc.relation.journalGenetics in Medicine Open
dc.rightsAttribution 4.0 Internationalen
dc.rights.urihttps://creativecommons.org/licenses/by/4.0
dc.sourcePMC
dc.subjectARID1B
dc.subjectAdult
dc.subjectCoffin–Siris syndrome
dc.subjectDevelopmental delay
dc.subjectIntellectual disability
dc.titleARID1B-related disorder in 87 adults: Natural history and self-sustainability
dc.typeArticle
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