Mutations in the Small GTPase Gene RAB39B Are Responsible for X-linked Mental Retardation Associated with Autism, Epilepsy, and Macrocephaly

Giannandrea, Maila; Bianchi, Veronica; Mignogna, Maria Lidia; Sirri, A.; Carrabino, Salvatore; Delia, E.; Vecellio, Matteo; Russo, Silvia; Cogliati, Francesca; Larizza, Lidia; Ropers, Hans Hilger; Tzschach, Andreas; Kalscheuer, Vera M.; Oehl-Jaschkowitz, Barbara; Skinner, Cindy; Schwartz, Charles E.; Gécz, Jozef; Esch, Hilde Van; Raynaud, Martine; Chelly, Jamel; Brouwer, Arjan P.M. de; Toniolo, Daniela; D’Adamo, Patrizia

doi:10.1016/j.ajhg.2010.01.011

Cited by 207 publications

(271 citation statements)

References 26 publications

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“…Alterations in signaling pathways involving the Rho family of small GTPases contribute to syndromic and nonsyndromic mental retardation, 17 and mutations in the small GTPase gene RAB39B (OMIM300774) were also identified in two patients with mental retardation. 18 In this study, magnetic resonance imaging analysis did not reveal structural abnormalities in the brain of these two brothers. Furthermore, the brothers' normal electroencephalograms and lack of history of seizures indicate that this microdeletion does not affect the development of gross brain structure and does not cause epilepsy.…”

Section: Discussionmentioning

confidence: 78%

Identification of a microdeletion at Xp22.13 in a Taiwanese family presenting with Nance-Horan syndrome

et al. 2010

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,9,10 Nance-Horan syndrome (NHS) is a rare X-linked disorder characterized by congenital cataracts, dental anomalies and mental retardation. The disease has been linked to a novel gene termed NHS located at Xp22.13. The majority of pathogenic mutations of the disease include nonsense mutations and small deletions and insertions that lead to truncation of the NHS protein. In this study, we identified a microdeletion of B0.92 Mb at Xp22.13 detected by array-based comparative genomic hybridization in two brothers presenting congenital cataract, dental anomalies, facial dysmorphisms and mental retardation. The deleted region encompasses the REPS2, NHS, SCML1 and RAI2 genes, and was transmitted from their carrier mother who presented only mild cataract. Our findings are in line with several recent case reports to indicate that genomic rearrangement involving the NHS gene is an important genetic etiology underlying NHS.

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Section: Discussionmentioning

confidence: 78%

Identification of a microdeletion at Xp22.13 in a Taiwanese family presenting with Nance-Horan syndrome

et al. 2010

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“…Indeed, while the manuscript was in preparation, we realized that RAB39B had just been discovered as an actual XLMR gene. 31 Moreover, during the revision process, the GSPT2 gene had been proposed independently as a strong XLMR candidate by a copy-number variation study. 32 We think that the case of USP9X illustrates particularly well the potential usefulness of our approach for selecting the most promising candidates and making hypothesis about their functional interactions with the validated genes.…”

Section: Discussionmentioning

confidence: 99%

An atlas of tissue-specific conserved coexpression for functional annotation and disease gene prediction

et al. 2011

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Gene coexpression relationships that are phylogenetically conserved between human and mouse have been shown to provide important clues about gene function that can be efficiently used to identify promising candidate genes for human hereditary disorders. In the past, such approaches have considered mostly generic gene expression profiles that cover multiple tissues and organs. The individual genes of multicellular organisms, however, can participate in different transcriptional programs, operating at scales as different as single-cell types, tissues, organs, body regions or the entire organism. Therefore, systematic analysis of tissue-specific coexpression could be, in principle, a very powerful strategy to dissect those functional relationships among genes that emerge only in particular tissues or organs. In this report, we show that, in fact, conserved coexpression as determined from tissue-specific and condition-specific data sets can predict many functional relationships that are not detected by analyzing heterogeneous microarray data sets. More importantly, we find that, when combined with disease networks, the simultaneous use of both generic (multi-tissue) and tissue-specific conserved coexpression allows a more efficient prediction of human disease genes than the use of generic conserved coexpression alone. Using this strategy, we were able to identify high-probability candidates for 238 orphan disease loci. We provide proof of concept that this combined use of generic and tissue-specific conserved coexpression can be very useful to prioritize the mutational candidates obtained from deep-sequencing projects, even in the case of genetic disorders as heterogeneous as XLMR.

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“…REPS2 is associated with a small G protein and shows strong expression in brain tissue (LSBM, http://www.lsbm.org/index.html). As alterations in signaling pathways involving the Rho family of small GTPases contribute to both syndromic and nonsyndromic MR disorders 36 and mutation in the small GTPase gene RAB39B (OMIM300774) were identified in two MR patients, 37 it is possible that deregulated expression of REPS2 contributes to MR. Protein-truncation mutations in NHS have been identified in patients with Nance-Horan syndrome (OMIM 302350), an X-linked developmental disorder characterized by congenital cataracts, dental anomalies, facial dysmorphism and MR in some cases. As our patients in both families did not have cataracts or dental anomalies, the genomic rearrangement involved in NHS may not affect the function of this gene.…”

Section: Cnvs In Xlmr S Honda Et Almentioning

confidence: 99%

Copy-number variations on the X chromosome in Japanese patients with mental retardation detected by array-based comparative genomic hybridization analysis

et al. 2010

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Mental Retardation Consortium 8X-linked mental retardation (XLMR) is a common, clinically complex and genetically heterogeneous disease arising from many mutations along the X chromosome. Although research during the past decade has identified 490 XLMR genes, many more remain uncharacterized. In this study, copy-number variations (CNVs) were screened in individuals with MR from 144 families by array-based comparative genomic hybridization (aCGH) using a bacterial artificial chromosome-based X-tiling array. Candidate pathogenic CNVs (pCNVs) were detected in 10 families (6.9%). Five of the families had pCNVs involving known XLMR genes, duplication of Xq28 containing MECP2 in three families, duplication of Xp11.22-p11.23 containing FTSJ1 and PQBP1 in one family, and deletion of Xp11.22 bearing SHROOM4 in one family. New candidate pCNVs were detected in five families as follows: identical complex pCNVs involved in dup(X)(p22.2) and dup(X)(p21.3) containing part of REPS2, NHS and IL1RAPL1 in two unrelated families, duplication of Xp22.2 including part of FRMPD4, duplication of Xq21.1 including HDX and deletion of Xq24 noncoding region in one family, respectively. Both parents and only mother samples were available in six and three families, respectively, and pCNVs were inherited from each of their mothers in those families other than a family of the proband with deletion of SHROOM4. This study should help to identify the novel XLMR genes and mechanisms leading to MR and reveal the clinical conditions and genomic background of XLMR.

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Mutations in the Small GTPase Gene RAB39B Are Responsible for X-linked Mental Retardation Associated with Autism, Epilepsy, and Macrocephaly

Cited by 207 publications

References 26 publications

Identification of a microdeletion at Xp22.13 in a Taiwanese family presenting with Nance-Horan syndrome

Identification of a microdeletion at Xp22.13 in a Taiwanese family presenting with Nance-Horan syndrome

An atlas of tissue-specific conserved coexpression for functional annotation and disease gene prediction

Copy-number variations on the X chromosome in Japanese patients with mental retardation detected by array-based comparative genomic hybridization analysis

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