Copy-Number Gains of HUWE1 Due to Replication- and Recombination-Based Rearrangements

Froyen, Guy; Belet, Stefanie; Martı́nez, Francisco; Santos-Rebouças, Cíntia Barros; Declercq, M.; Verbeeck, Johan; Donckers, Lene; Berland, Siren; Mayo, Sonia; Roselló, Mónica; Pimentel, Márcia Mattos Gonçalves; Fintelman-Rodrigues, Natália; Hovland, Randi; Santos, Suely Rodrigues dos; Raymond, F. Lucy; Bose, T.; Corbett, Mark; Sheffield, Leslie J.; Ravenswaaij-Arts, Conny M. A. van; Dijkhuizen, Trijnie; Coutton, Charles; Satre, Véronique; Siu, Victoria Mok; Marynen, Peter

doi:10.1016/j.ajhg.2012.06.010

Cited by 76 publications

(97 citation statements)

References 48 publications

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“…Regarding clinical features in females, these are less severe due to the presence of a normal X-chromosome, which has been previously described. 9,11 I2 II2 II4 II5 II6 III1 Olson et al 30 Gandomi et al 31 Tran Mau-Them et al 5 Tran Mau-Them et al 5 Gilissen et al 32 33 Moey et al 34 Moey et al 34 Moey et al 34 Moey et al 34 Froyen et al 35 Froyen et al 35 Froyen et al 35 Gedeon et al 36 Froyen et al 37 Froyen et al 37 Froyen et al 37 Froyen et al 37 Patient 1 IQSEC2 splicing mutation and ID I Madrigal et al…”

Section: Discussionmentioning

confidence: 99%

“…2,5,[30][31][32][33][34][35][36][37][38][39][40][41] Tables 1 and 2 summarize the clinical manifestations of patients with deletions or duplications in the IQSEC2 gene and Table 3 summarizes the clinical manifestations of patients with point variants in this gene. It has been proposed that non-synonymous variants in this gene are responsible for non-syndromic ID, whereas truncating variants may generate a more severe neurodevelopmental phenotype related to the loss of function of IQSEC2.…”

Section: Mutationmentioning

confidence: 99%

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A novel splicing mutation in the IQSEC2 gene that modulates the phenotype severity in a family with intellectual disability

et al. 2016

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The IQSEC2 gene is located on chromosome Xp11.22 and encodes a guanine nucleotide exchange factor for the ADPribosylation factor family of small GTPases. This gene is known to have a significant role in cytoskeletal organization, dendritic spine morphology and synaptic organization. Variants in IQSEC2 cause moderate to severe intellectual disability in males and a variable phenotype in females because this gene escapes from X-chromosome inactivation. Here we report on the first splicing variant in IQSEC2 (g.88032_88033del; NG_021296.1) that co-segregates in a family diagnosed with an X-linked form of ID. In a percentage of the cells, the variant activates an intraexonic splice acceptor site that abolishes 26 amino acids from the highly conserved PH domain of IQSEC2 and creates a premature stop codon 36 amino acids later in exon 13. Interestingly, the percentage of aberrant splicing seems to correlate with the severity of the disease in each patient. The impact of this variant in the target tissue is unknown, but we can hypothesize that these differences may be related to the amount of abnormal IQSEC2 transcript. To our knowledge, we are reporting a novel mechanism of IQSEC2 involvement in ID. Variants that affect splicing are related to many genetic diseases and the understanding of their role in disease expands potential opportunities for gene therapy. Modulation of aberrant splicing transcripts can become a potent therapeutic approach for many of these diseases.

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Section: Discussionmentioning

confidence: 99%

Section: Mutationmentioning

confidence: 99%

A novel splicing mutation in the IQSEC2 gene that modulates the phenotype severity in a family with intellectual disability

et al. 2016

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“…Patients with a duplication involving HUWE1 are usually described to have a nonsyndromic mild to moderate ID [13,15]. Few affected individuals are reported to have minor dysmorphic features, but a consistent pattern among all duplication carriers is lacking.…”

Section: Discussionmentioning

confidence: 99%

“…HUWE1 is a dosage-sensitive gene and copy number variations of this gene have recurrently been linked to ID [13,15]. Here, we would like to emphasize the importance of pathological point mutations in the gene.…”

Section: Discussionmentioning

confidence: 99%

HUWE1 mutation explains phenotypic severity in a case of familial idiopathic intellectual disability

Isrie¹,

Kalscheuer²,

Holvoet³

et al. 2013

European Journal of Medical Genetics

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a b s t r a c tThe advent of next-generation sequencing has proven to be a key force in the identification of new genes associated with intellectual disability. In this study, high-throughput sequencing of the coding regions of the X-chromosome led to the identification of a missense variant in the HUWE1 gene. The same variant has been reported before by Froyen et al. (2008). We compare the phenotypes and demonstrate that, in the present family, the HUWE1 mutation segregates with the more severe ID phenotypes of two out of three brothers. The third brother has a milder form of ID and does not carry the mutation.

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“…13 The slides were scanned on an Agilent DNA Microarray Scanner (Agilent Technologies Inc.) and images were extracted using the Feature Extraction software v9.1.3.1 (Agilent Technologies Inc.). The QC report was carefully examined to ensure proper hybridization and grid placement.…”

Section: Array Cgh and Real-time Quantitative Pcr (Qpcr) Analysismentioning

confidence: 99%

A novel in-frame deletion affecting the BAR domain of OPHN1 in a family with intellectual disability and hippocampal alterations

et al. 2013

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Oligophrenin-1 (OPHN1) is one of at least seven genes located on chromosome X that take part in Rho GTPase-dependent signaling pathways involved in X-linked intellectual disability (XLID). Mutations in OPHN1 were primarily described as an exclusive cause of non-syndromic XLID, but the re-evaluation of the affected individuals using brain imaging displayed fronto-temporal atrophy and cerebellar hypoplasia as neuroanatomical marks. In this study, we describe clinical, genetic and neuroimaging data of a three generation Brazilian XLID family co-segregating a novel intragenic deletion in OPHN1. This deletion results in an in-frame loss of exon 7 at transcription level (c.781_891del; r.487_597del), which is predicted to abolish 37 amino acids from the highly conserved N-terminal BAR domain of OPHN1. cDNA expression analysis demonstrated that the mutant OPHN1 transcript is stable and no abnormal splicing was observed. Features shared by the affected males of this family include neonatal hypotonia, strabismus, prominent root of the nose, deep set eyes, hyperactivity and instability/ intolerance to frustration. Cranial MRI scans showed large lateral ventricles, vermis hypoplasia and cystic dilatation of the cisterna magna in all affected males. Interestingly, hippocampal alterations that have not been reported in patients with loss-of-function OPHN1 mutations were found in three affected individuals, suggesting an important function for the BAR domain in the hippocampus. This is the first description of an in-frame deletion within the BAR domain of OPHN1 and could provide new insights into the role of this domain in relation to brain and cognitive development or function.

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Copy-Number Gains of HUWE1 Due to Replication- and Recombination-Based Rearrangements

Cited by 76 publications

References 48 publications

A novel splicing mutation in the IQSEC2 gene that modulates the phenotype severity in a family with intellectual disability

A novel splicing mutation in the IQSEC2 gene that modulates the phenotype severity in a family with intellectual disability

HUWE1 mutation explains phenotypic severity in a case of familial idiopathic intellectual disability

A novel in-frame deletion affecting the BAR domain of OPHN1 in a family with intellectual disability and hippocampal alterations

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