Over-expression of a human chromosome 22q11.2 segment including TXNRD2, COMT and ARVCF developmentally affects incentive learning and working memory in mice

Suzuki, Go; Harper, Kathryn M.; Hiramoto, Takeshi; Funke, Birgit; Lee, Moonsook; Kang, Gina; Buell, Mahalah R.; Geyer, Mark A.; Kucherlapati, Raju; Morrow, Bernice E.; Männistö, Pekka T.; Agatsuma, Soh; Hiroi, Noboru

doi:10.1093/hmg/ddp334

Cited by 46 publications

(57 citation statements)

References 57 publications

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“…Duplication of chromosome 22q11.2 is associated with elevated rates of mental retardation, autism, and other behavioral phenotypes, and probably includes abnormalities in several key genes such as TXNRD2, COMT, ARVCF, and TBX1. TXNRD2 is a thioredoxin reductase that directly reduces proteins (Gasdaska et al, 1999); COMT is one of the most extensively studied 22q11.2 genes related to cognitive function (Rosa et al, 2004) and ARVCF may contribute to the phenotype of VCFS (Suzuki et al, 2009). Moreover, TBX1 has been shown to be the major genetic component responsible for the features of DGS/VCFS.…”

Section: Discussionmentioning

confidence: 99%

A rare case of trisomy 11q23.3-11q25 and trisomy 22q11.1-22q11.21

Ps¹,

Hf²,

Chen³

et al. 2016

Genet. Mol. Res.

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ABSTRACT. Partial duplication of the long arm of chromosome 11 and the partial trisomy of 22q are uncommon karyotypic abnormalities. Here, we report the case of a 6-year-old girl who showed partial trisomy of 11q and 22q, as a result of a maternal balanced reciprocal translocation (11;22), and exhibited dysmorphic features, severe intellectual disability, brain malformations, and speech delay related to this unique chromosomal abnormality. Array comparative genomic hybridization (array CGH) revealed a gain in copy number on the long arm of chromosome 11, spanning at least 18.22 Mb. Additionally, there was a gain in copy number on the long arm of chromosome 22, spanning at least 3.46 Mb. FISH analysis using a chromosome 11 short arm telomere probe (11p14.2), a chromosome 11 long arm telomere probe (11q24.3), and a chromosome 22 long arm telomere probe (22q13.33) confirmed the origin of the marker chromosome. It has been confirmed by the State Key Laboratory of Medical Genetics of China that this is the first reported instance of the karyotype 47,XX, +der (22

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Section: Discussionmentioning

confidence: 99%

A rare case of trisomy 11q23.3-11q25 and trisomy 22q11.1-22q11.21

Ps¹,

Hf²,

Chen³

et al. 2016

Genet. Mol. Res.

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“…with schizophrenia 36,37,41,42 ; overexpression of the region in mice leads to alterations in incentive learning and working memory 43 ; common variants in ARVCF are associated with an intermediate MRI phenotype that includes altered FA in patients who have schizophrenia 44 ; and SNPs in COMT are associated with white matter changes in preterm-born adults. 45 The association between a tag SNP in ARVCF and reduced FA in white matter after preterm birth could be explained by: common variation at ARVCF influencing white matter microstructure, which has been reported in adult-onset schizophrenia 44 ; the SNP being in strong linkage disequilibrium (LD) with nongenotyped SNPs that span COMT (Supplementary Fig 1A); or a regulatory role on gene expression.…”

Section: Figurementioning

confidence: 99%

Common Genetic Variants and Risk of Brain Injury After Preterm Birth

et al. 2014

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“…As a pair of mice is placed in a cage that is novel to both, there is no ‘resident’ mouse in this task; aggressive social interaction is minimized and affiliative social interaction is maximally evaluated [93,108]. Unlike a “sociability” task in which one of the mice is confined in a small wire cage, reciprocal interaction can be evaluated in this naturalistic social interaction task [111].…”

Section: Introductionmentioning

confidence: 99%

Mouse Models of 22q11.2-Associated Autism Spectrum Disorder

Hiroi¹,

Hiramoto

Harper

et al. 2012

Autism

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Copy number variation (CNV) of human chromosome 22q11.2 is associated with an elevated rate of autism spectrum disorder (ASD) and represents one of syndromic ASDs with rare genetic variants. However, the precise genetic basis of this association remains unclear due to its relatively large hemizygous and duplication region, including more than 30 genes. Previous studies using genetic mouse models suggested that although not all 22q11.2 genes contribute to ASD symptomatology, more than one 22q11.2 genes have distinct phenotypic targets for ASD symptoms. Our data show that deficiency of the two 22q11.2 genesTbx1 and Sept5 causes distinct phenotypic sets of ASD symptoms.

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Over-expression of a human chromosome 22q11.2 segment including TXNRD2, COMT and ARVCF developmentally affects incentive learning and working memory in mice

Cited by 46 publications

References 57 publications

A rare case of trisomy 11q23.3-11q25 and trisomy 22q11.1-22q11.21

A rare case of trisomy 11q23.3-11q25 and trisomy 22q11.1-22q11.21

Common Genetic Variants and Risk of Brain Injury After Preterm Birth

Mouse Models of 22q11.2-Associated Autism Spectrum Disorder

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