Copy number gain at Xp22.31 includes complex duplication rearrangements and recurrent triplications

Liu, Pengfei; Erez, Ayelet; Nagamani, Sandesh C. Sreenath; Bi, Weimin; Carvalho, Claudia M.B.; Simmons, Alexandra D.; Wiszniewska, Joanna; Fang, Ping; Eng, Patricia A.; Cooper, M. Lance; Sutton, V. Reid; Roeder, Elizabeth; Bodensteiner, John B.; Delgado, Mauricio R.; Prakash, Siddharth K.; Belmont, John W.; Stankiewicz, Paweł; Berg, Jonathan S.; Shinawi, Marwan; Patel, Ankita; Cheung, Sau Wai; Lupski, James R.

doi:10.1093/hmg/ddr078

Cited by 71 publications

(105 citation statements)

References 58 publications

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“…Nevertheless, precedence exist for penetrance of neuropsychiatric traits being related to further in increments of gene dosage; triplications at the STS locus appear to be more penetrant than duplications for a DD/ID-associated phenotype. 14 Triplications are very rare chromosomal rearrangements. 15 In general, the resulting clinical phenotype is consistent with, but more severe than, the duplication of the same locus.…”

Section: Discussionmentioning

confidence: 99%

“…15 In general, the resulting clinical phenotype is consistent with, but more severe than, the duplication of the same locus. 12,14,[16][17][18] Triplications of genomic loci associated with neurocognitive and neuropsychiatric abnormalities have been described, among others, at 22q11.2, 18 7p11.2, 19 Xq28 encompassing the MECP2 gene, 20 and 7q11.23 at the Williams syndrome critical region. 17 Triplications can, in general, be classified as types I and II, as well as being recurrent or non-recurrent, which relates to the molecular mechanism underlying their formation.…”

Section: Discussionmentioning

confidence: 99%

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CHRNA7 triplication associated with cognitive impairment and neuropsychiatric phenotypes in a three-generation pedigree

Soler‐Alfonso

Carvalho

et al. 2014

Eur J Hum Genet

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Although deletions of CHRNA7 have been associated with intellectual disability (ID), seizures and neuropsychiatric phenotypes, the pathogenicity of CHRNA7 duplications has been uncertain. We present the first report of CHRNA7 triplication. Three generations of a family affected with various neuropsychiatric phenotypes, including anxiety, bipolar disorder, developmental delay and ID, were studied with array comparative genomic hybridization (aCGH). High-resolution aCGH revealed a 650-kb triplication at chromosome 15q13.3 encompassing the CHRNA7 gene, which encodes the alpha7 subunit of the neuronal nicotinic acetylcholine receptor. A small duplication precedes the triplication at the proximal breakpoint junction, and analysis of the breakpoint indicates that the triplicated segment is in an inverted orientation with respect to the duplication. CHRNA7 triplication appears to occur by a replication-based mechanism that produces inverted triplications embedded within duplications. Co-segregation of the CHRNA7 triplication with neuropsychiatric and cognitive phenotypes provides further evidence for dosage sensitivity of CHRNA7.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

CHRNA7 triplication associated with cognitive impairment and neuropsychiatric phenotypes in a three-generation pedigree

Soler‐Alfonso

Carvalho

et al. 2014

Eur J Hum Genet

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“…We have only found 3 triplication cases in the literature, all with developmental delay, and in the 2 male individuals, aggressive behavior with features of ADHD was also described [Liu et al, 2011]. The triplication, as far as we know, has not been identified in the general population reinforcing the potential pathogenicity.…”

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confidence: 83%

“…laboratories but are challenging to interpret [Shaffer et al, 2007;Li et al, 2010;Furrow et al, 2011;Liu et al, 2011;Faletra et al, 2012;Esplin et al, 2014]. This recurrent duplication contains 4 known genes, PUDP , STS , VCX , and PNPLA4 as well as 2 microRNAs, MIR651 and MIR4767.…”

mentioning

confidence: 99%

“…There is a high incidence of this duplication in clinical cases referred for array comparative genomic hybridization (aCGH) and ascertained due to neurobehavioral abnormalities, but the duplication is also observed in the general population. In the majority of clinical cases, it is inherited from a parent, most of them clinically unaffected [Li et al, 2010;Furrow et al, 2011;Liu et al, 2011;Faletra et al, 2012;Esplin et al, 2014]. The duplication may predispose to disease, but the manifestation may require additional genetic and/or environmental factors.…”

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confidence: 99%

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Severe Neurological Phenotype in a Girl with Xp22.31 Triplication

Polo-Antúnez¹,

Arroyo-Carrera

2017

Mol Syndromol

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The Xp22.31 duplication is a copy number variant which is challenging to categorize as pathogenic or benign. There is an increasing number of patients with the duplication and a neurobehavioral phenotype, but the duplication is almost always inherited from a parent, who in some cases is phenotypically normal. Also, the duplication is detected in the general population, though in a smaller percentage than in clinically ascertained populations. The Xp22.31 triplication has only been identified in 3 individuals of a large cohort of developmental delay cases but never in the control cohorts or general population. We report a severely affected female with an Xp22.31 tetrasomy, inherited from duplications identified in both phenotypically normal parents. Although our study has limitations, it suggests that the Xp22.31 triplication seems to be more penetrant than the duplication and is associated with a neurological phenotype.

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Common structural features characterize interstitial intrachromosomal Xp and 18q triplications

Giorda

Beri

Bonaglia

et al. 2011

American J of Med Genetics Pt A

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Rare intrachromosomal triplications producing partial tetrasomies have been reported for a number of chromosomes. A detailed molecular characterization, necessary to define the mechanism of their formation, has so far been lacking. We report on the detailed clinical, cytogenetic, and molecular characterization of two triplications, one de novo involving chromosome 18q, the other familial on chromosome Xp. The clinical phenotype of the patient with 18q triplication, very likely due to overexpression of one or more of the genes in the region, consists mainly of facial dysmorphisms and developmental delay. The familial Xp triplication does not cause an increase in the number of copies of any gene and is almost certainly a polymorphism. The rearrangements are actually complex duplications/triplications. In both patients, their proximal breakpoints are located within complex segmental duplications, one containing the VCX gene cluster on chromosome Xp, the other the TCEB3 genes on chromosome 18q. A proximal duplicated region is also present in both patients. All junctions we analyzed were formed by non-homologous end joining (NHEJ). The structural features shared between our patients suggest the involvement of a common mechanism in the genesis of interstitial intrachromosomal triplications.

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Copy number gain at Xp22.31 includes complex duplication rearrangements and recurrent triplications

Cited by 71 publications

References 58 publications

CHRNA7 triplication associated with cognitive impairment and neuropsychiatric phenotypes in a three-generation pedigree

CHRNA7 triplication associated with cognitive impairment and neuropsychiatric phenotypes in a three-generation pedigree

Severe Neurological Phenotype in a Girl with Xp22.31 Triplication

Common structural features characterize interstitial intrachromosomal Xp and 18q triplications

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