Real‐time quantitative PCR analysis of pediatric ependymomas identifies novel candidate genes including <i>TPR</i> at 1q25 and <i>CHIBBY</i> at 22q12‐q13

Karakoula, Katherine; Suárez-Merino, Blanca; Ward, Samantha; Phipps, Kim; Harkness, William; Hayward, Richard; Thompson, Dominic; Jacques, Thomas S.; Harding, Brian; Beck, John C.; Thomas, D. G. T.; Warr, Tracy

doi:10.1002/gcc.20607

Cited by 37 publications

(54 citation statements)

References 68 publications

(99 reference statements)

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“…Intracranial ependymomas have also demonstrated hypermethylation of the tumor suppressor gene HIC-1 (17p13.3) in 83% of cases, while such findings were not present in spinal cord ependymomas [4,59,60].…”

Section: Intracranial Tumorsmentioning

confidence: 93%

Genetic expression profiles of adult and pediatric ependymomas: Molecular pathways, prognostic indicators, and therapeutic targets

Nagasawa

Trang

Choy

et al. 2013

Clinical Neurology and Neurosurgery

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Section: Intracranial Tumorsmentioning

confidence: 93%

Genetic expression profiles of adult and pediatric ependymomas: Molecular pathways, prognostic indicators, and therapeutic targets

Nagasawa

Trang

Choy

et al. 2013

Clinical Neurology and Neurosurgery

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“…Reduced expression of other genes within 22q13.1-13.33 has been observed, including CBX7, G22P1, and MCM5, which may be involved in gene silencing, DNA repair, and cell proliferation, respectively (77,148). Real-time quantitative PCR of 47 pediatric intracranial ependymomas revealed frequent loss of C22orf2 and RAC2, the latter being associated with reduced overall survival in the cohort (112).…”

Section: Immunohistochemical and Genomic Markersmentioning

confidence: 99%

“…These genes and the locus 1q25 merit further investigation with high resolution genomic techniques and gene expression studies that analyze larger numbers of pediatric ependymomas as an independent cohort. These methods could also establish the prognostic role of genes such as NRXN2, TPR, SEMA5, NRCAM, CDK4, and ADRM1 that have already been associated with outcome in small studies of pediatric patients with intracranial ependymoma (83,112), or examine other regions of genomic imbalance potentially harboring markers of disease progression and prognosis in children including the loss of chromosomes 22q and 6q.…”

Section: Immunohistochemical and Genomic Markersmentioning

confidence: 99%

Pediatric Ependymoma: Biological Perspectives

Kilday

Rahman

Dyer

et al. 2009

Molecular Cancer Research

167

204

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Pediatric ependymomas are enigmatic tumors that continue to present a clinical management challenge despite advances in neurosurgery, neuroimaging techniques, and radiation therapy. Difficulty in predicting tumor behavior from clinical and histological factors has shifted the focus to the molecular and cellular biology of ependymoma in order to identify new correlates of disease outcome and novel therapeutic targets. This article reviews our current understanding of pediatric ependymoma biology and includes a meta-analysis of all comparative genomic hybridization (CGH) studies done on primary ependymomas to date, examining more than 300 tumors. From this meta-analysis and a review of the literature, we show that ependymomas in children exhibit a different genomic profile to those in adults and reinforce the evidence that ependymomas from different locations within the central nervous system (CNS) are distinguishable at a genomic level. Potential biological markers of prognosis in pediatric ependymoma are assessed and the ependymoma cancer stem cell hypothesis is highlighted with respect to tumor resistance and recurrence. We also discuss the shifting paradigm for treatment modalities in ependymoma that target molecular alterations in tumor-initiating cell populations. (Mol Cancer Res 2009;7(6):765-86)

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“…24,25 It has been reported that Cby1 expression is significantly downregulated in chronic myeloid leukemia 26 and pediatric ependymomas. 27 To gain insights into the function of Cby1 in colorectal tumorigenesis, we created Cby1-knockdown (K D ) SW480 clones stably expressing Cby1 small-hairpin (sh) RNAs.…”

Section: Introductionmentioning

confidence: 99%

Chibby1 knockdown promotes mesenchymal-to-epithelial transition-like changes

Fischer

Wong

et al. 2017

Cell Cycle

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Chibby1 (Cby1) was originally isolated as a binding partner for b-catenin, a dual function protein in cell-cell adhesion and in canonical Wnt signaling. The canonical Wnt/b-catenin pathway is dysregulated in various diseases including cancer, most notably of the gastrointestinal origin. To investigate the role of Cby1 in colorectal tumorigenesis, we generated stable Cby1-knockdown (K D ) SW480 colon cancer cells. Unexpectedly, we found that Cby1 K D induces mesenchymal-to-epithelial transition (MET)-like changes in SW480 as well as in HEK293 cells. Cby1-K D cells displayed a cuboidal epithelial morphology with tight cellcell contacts. In Cby1-K D cells, the plasma membrane localization of E-cadherin and b-catenin was dramatically increased with formation of cortical actin rings, while the levels of the mesenchymal marker vimentin were decreased. Consistent with these changes, in wound healing assays, Cby1-K D cells exhibited epithelial cell-like properties as they migrated collectively as epithelial sheets. Furthermore, the anchorage-independent growth of Cby1-K D cells was reduced as determined by soft agar assays. These findings suggest that chronic Cby1 K D in colon cancer cells may counteract tumor progression by promoting the MET process.

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Real‐time quantitative PCR analysis of pediatric ependymomas identifies novel candidate genes including TPR at 1q25 and CHIBBY at 22q12‐q13

Cited by 37 publications

References 68 publications

Genetic expression profiles of adult and pediatric ependymomas: Molecular pathways, prognostic indicators, and therapeutic targets

Genetic expression profiles of adult and pediatric ependymomas: Molecular pathways, prognostic indicators, and therapeutic targets

Pediatric Ependymoma: Biological Perspectives

Chibby1 knockdown promotes mesenchymal-to-epithelial transition-like changes

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