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      ATRX mutation in two adult brothers with non-specific moderate intellectual disability identified by exome sequencing

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          Abstract

          In this report, we describe two adult brothers affected by moderate non-specific intellectual disability (ID). They showed minor facial anomalies, not clearly ascribable to any specific syndromic patterns, microcephaly, brachydactyly and broad toes. Both brothers presented seizures. Karyotype, subtelomeric and FMR1 analysis were normal in both cases.

          We performed array-CGH analysis that revealed no copy-number variations potentially associated with ID. Subsequent exome sequence analysis allowed the identification of the ATRX c.109C>T (p.R37X) mutation in both the affected brothers. Sanger sequencing confirmed the presence of the mutation in the brothers and showed that the mother is a healthy carrier.

          Mutations in the ATRX gene cause the X-linked alpha thalassemia/mental retardation (ATR-X) syndrome (MIM #301040), a severe clinical condition usually associated with profound ID, facial dysmorphism and alpha thalassemia. However, the syndrome is clinically heterogeneous and some mutations, including the c.109C>T, are associated with a broad phenotypic spectrum, with patients displaying a less severe phenotype with only mild-moderate ID. In the case presented here, exome sequencing provided an effective strategy to achieve the molecular diagnosis of ATR-X syndrome, which otherwise would have been difficult to consider due to the mild non-specific phenotype and the absence of a family history with typical severe cases.

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          Genetics of early onset cognitive impairment.

          H Hilger Ropers (2009)
          Intellectual disability (ID) is the leading socio-economic problem of health care, but compared to autism and schizophrenia, it has received very little public attention. Important risk factors for ID are malnutrition, cultural deprivation, poor health care, and parental consanguinity. In the Western world, fetal alcohol exposure is the most common preventable cause. Most severe forms of ID have genetic causes. Cytogenetically detectable and submicroscopic chromosomal rearrangements account for approximately 25% of all cases. X-linked gene defects are responsible in 10-12% of males with ID; to date, 91 of these defects have been identified. In contrast, autosomal gene defects have been largely disregarded, but due to coordinated efforts and the advent of next-generation DNA sequencing, this is about to change. As shown for Fra(X) syndrome, this renewed focus on autosomal gene defects will pave the way for molecular diagnosis and prevention, shed more light on the pathogenesis of ID, and reveal new opportunities for therapy.
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            A novel transcription regulatory complex containing death domain-associated protein and the ATR-X syndrome protein.

            Annie Wu, O. Barak, H. Liu (2004)
            Death domain-associated protein (Daxx) is a multi-functional protein that modulates both apoptosis and transcription. Within the nucleus, Daxx is a component of the promyelocytic leukemia protein (PML) nuclear bodies (NBs) and interacts with a number of transcription factors, yet its precise role in transcription remains elusive. To further define the function of Daxx, we have isolated its interacting proteins in the nucleus using epitope-tagged affinity purification and identified X-linked mental retardation and alpha-thalassaemia syndrome protein (ATRX), a putative member of the SNF2 family of ATP-dependent chromatin remodeling proteins that is mutated in several X-linked mental retardation disorders. We show that substantial amounts of endogenous Daxx and ATRX exist in a nuclear complex. Daxx binds to ATRX through its paired amphipathic alpha helices domains. ATRX has ATPase activity that is stimulated by mononucleosomes, and patient mutations in the ATPase domain attenuate this activity. ATRX strongly represses transcription when tethered to a promoter. Daxx does not affect the ATPase activity of ATRX, however, it alleviates its transcription repression activity. In addition, ATRX is found in the PML-NBs, and this localization is mediated by Daxx. These results show that the ATRX.Daxx complex is a novel ATP-dependent chromatin-remodeling complex, with ATRX being the core ATPase subunit and Daxx being the targeting subunit. Moreover, the localization of ATRX to the PML-NBs supports the notion that these structures may play an important role in transcription regulation.
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              Mutations in the chromatin-associated protein ATRX.

              Takahito Wada, Alan Fryer, Ian D. Krantz (2008)
              ATRX belongs to the SNF2 family of proteins, many of which have been demonstrated to have chromatin remodeling activity. Constitution mutations in the X-encoded gene give rise to alpha thalassemia mental retardation (ATR-X) syndrome and a variety of related conditions that are often associated with profound developmental delay, facial dysmorphism, genital abnormalities, and alpha thalassemia. Acquired mutations in ATRX are observed in the preleukemic condition alpha thalassemia myelodysplastic syndrome (ATMDS). Mutations in ATRX have been shown to perturb gene expression and DNA methylation. This is a comprehensive report of 127 mutations including 32 reported here for the first time. Missense mutations are shown to cluster in the two main functional domains. The truncating mutations appear to be "rescued" to some degree and so it appears likely that most if not all constitutional ATRX mutations are hypomorphs. (c) 2008 Wiley-Liss, Inc.
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                Author and article information

                Contributors
                M. Venturin
                Journal
                Journal ID (nlm-ta): Meta Gene
                Journal ID (iso-abbrev): Meta Gene
                Title: Meta Gene
                Publisher: Elsevier
                ISSN (Electronic): 2214-5400
                Publication date PMC-release: 29 October 2013
                Publication date Collection: December 2013
                Publication date (Electronic): 29 October 2013
                Volume: 1
                Pages: 102-108
                Affiliations
                [a ]Dipartimento di Biotecnologie Mediche e Medicina Traslazionale, Università degli Studi di Milano, Milan, Italy
                [b ]UOD Genetica Medica, Fondazione IRCCS Ca' Granda Ospedale Maggiore Policlinico, Milan, Italy
                [c ]Laboratorio di Citogenetica Medica e Genetica Molecolare, Istituto Auxologico Italiano, Cusano Milanino (MI), Italy
                [d ]IRCCS “E Medea”, Bosisio Parini, Lecco, Centro di Riabilitazione “La nostra Famiglia” Sesto San Giovanni, Italy
                Author notes
                [* ]Corresponding author at: Dipartimento di Biotecnologie Mediche e Medicina Traslazionale, Università degli Studi di Milano, Via Viotti 3/5, 20133 Milan, Italy. Tel.: + 39 02 50315841; fax: + 39 02 50315864. marco.venturin@ 123456unimi.it
                [1]

                These authors equally contributed to the work.

                Article
                Publisher ID: S2214-5400(13)00006-6
                DOI: 10.1016/j.mgene.2013.09.004
                PMC ID: 4205036
                SO-VID: be6c40ff-9f35-4e3e-b136-79d6122106ca
                Copyright © © 2013 The authors
                License:

                This is an open access article under the CC BY-NC-SA license (http://creativecommons.org/licenses/by-nc-sa/3.0/).

                History
                Date received : 20 September 2013
                Date accepted : 21 September 2013
                Categories
                Subject: Article

                Keywords: atrx mutation,atr-x syndrome,exome sequencing,intellectual disability,non-specific phenotype
                Data availability:
                Keywords: atrx mutation, atr-x syndrome, exome sequencing, intellectual disability, non-specific phenotype

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