Cell Cycle Regulator Gene<i>CDC5L</i>, a Potential Target for 6p12-p21 Amplicon in Osteosarcoma

Lu, Xinyan; Lu, Yaojuan; Zhao, Yi-Jue; Kim, Jaeweon; Kang, Jason; Li, Xiaonan; Ge, Gouqing; Meyer, René; Perlaky, László; Hicks, John; Chintagumpala, Murali; Cai, Wei-Wen; Ladanyi, Marc; Görlick, Richard; Lau, Ching C.; Pati, Debananda; Sheldon, Michael; Rao, Pulivarthi H.

doi:10.1158/1541-7786.mcr-07-2115

Cited by 78 publications

(73 citation statements)

References 26 publications

(43 reference statements)

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“…The most commonly amplified genomic interval of 6p21-p23 harbors, among others, several candidate genes: angiogenesis-associated VEGFA, cell cycle-associated E2F3, CCND3, and RUNX2, and carcinomaassociated PTK7. These genes are directly or indirectly involved in the pathogenesis and pathways of malignant tumors, and amplifications have also been described in a high percentage of osteosarcomas (4,11,12,17,(37)(38)(39). In the present study, we found high amplification spots in 24% of the investigated tumors (Fig.…”

Section: Amplification Hotspotssupporting

confidence: 75%

“…There is not a single amplicon covering the whole central region of 6p; instead we found a few smaller hot spot regions harboring CCND3, RUNX2, and VEGFA. These genes have already been found to be overexpressed in osteosarcomas (38), and high expression of VEGFA has been correlated with a poor prognosis (40,41). Interestingly, the cell-cycle-associated E2F3, a downstream target of RB1, which has been found amplified and overexpressed in other tumors, e.g., in urothelial cancer (42), was the only gene located within a small amplified spot suggesting an alternative way to interfere with the RB1 pathway.…”

Section: Amplification Hotspotsmentioning

confidence: 93%

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Genomic Alterations and Allelic Imbalances Are Strong Prognostic Predictors in Osteosarcoma

Smida

Baumhoer

Rosemann

et al. 2010

Clinical Cancer Research

106

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Purpose: Osteosarcoma, the most common primary malignant tumor of the bone, is characterized by complex karyotypes with numerous structural and numerical alterations. Despite attempts to establish molecular prognostic markers at the time of diagnosis, the most accepted predictive factor remains the histologic evaluation of necrosis after neoadjuvant chemotherapy. The present approach was carried out to search for genome-wide recurrent loss of heterozygosity and copy number variations that could have prognostic and therapeutic impact for osteosarcoma patients.Experimental Design: Pretherapeutic biopsy samples of 45 osteosarcoma patients were analyzed using Affymetrix 10K2 high-density single nucleotide polymorphism arrays. Numerical aberrations and allelic imbalances were correlated with the histologically assessed response to therapy and clinical follow-up.

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Section: Amplification Hotspotssupporting

confidence: 75%

Section: Amplification Hotspotsmentioning

confidence: 93%

Genomic Alterations and Allelic Imbalances Are Strong Prognostic Predictors in Osteosarcoma

Smida

Baumhoer

Rosemann

et al. 2010

Clinical Cancer Research

106

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“…MDGA1 has been proposed as a new schizophrenia susceptibility gene involved in neuronal migration [35], meanwhile MDGA2 has been postulated as a novel autism susceptibility gene that shows a high similarity to contactin 4 (CNTN4), which has also been linked to this disease [36]. Moreover, MDGA1 expression has been found to be altered in tumor tissues [3,37]. Future studies to investigate the implication of the MDGAs in these human diseases should be promising.…”

Section: Discussionmentioning

confidence: 99%

Expression of Human MDGA1 Increases Cell Motility and Cell-Cell Adhesion and Reduces Adhesion to Extracellular Matrix Proteins in MDCK Cells

Díaz‐López

Iniesta

Morán

et al. 2010

Cancer Microenvironment

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Characterization of the novel human protein MDGA1 (MAM Domain containing Glycosylphosphatidylinositol Anchor-1) has been reported in our laboratory in the past few years. hMDGA1 is a glycoprotein containing 955 aminoacids (137 kDa) attached to the eukaryotic cell membrane by a GPI (Glycosylphosphatidylinositol) anchor and localized specifically into membrane microdomains known as lipid rafts. Moreover, MDGA1 protein contains structural features found in different types of cell adhesion molecules (CAMs) such as the presence of immunoglobulin domains and a MAM domain (Meprin, A5 protein, receptor protein-tyrosine phosphatase μ), suggesting a role of MDGA1 in cell migration and/or adhesion. In order to investigate this aim, stable MDCK cell lines expressing MDGA1 or the truncated proteins IgGPI (lacking the MAM domain) and MAMGPI (lacking Ig domains) were generated. Our results reveal that MDGA1 increases the ability of MDCK cells to migrate, as it contains both Ig and MAM domains which have been implicated in cell motility. In addition, cell adhesion to extracellular matrix proteins, mainly to collagen IV, is reduced by MDGA1 and the IgGPI and MAMGPI truncated proteins. Accordingly, silencing MDGA1 by siRNA revealed a significant increase in adhesion to collagen IV. Furthermore, MDGA1 expression, through the intrinsic properties of the MAM domain, increases cell-cell adhesion independently of the cell monolayer used, suggesting that MDGA1 mediates cell-cell adhesiveness in a heterophilic manner.

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“…Most importantly, gain of 6p is associated with advanced stages of cancer [Seute et al, 2001;Chochi et al, 2009], metastasis [Tanami et al, 2005], tumor cell proliferation [Tomovska et al, 2001], and poor event-free survival [Lu et al, 2008]. When one considers rearrangements across the entire genome, gain and/or amplification of the region 6p21-p12 is one of the most frequent aberrations in solid tumors and hematologic cancers [Baudis and Cleary, 2001].…”

Section: P Is a Hot Spot For Rearrangement In Human Cancersmentioning

confidence: 99%

“…In human osteosarcomas, recurrent amplification at chromosome 6p21-p12 has been documented [Lau et al, 2004;Lu et al, 2008;Selvarajah et al, 2008;Sadikovic et al, 2009] and has recently been shown to be associated with clinical response [Sadikovic et al, in press]. Gain and amplification of murine chromosomal regions homologous to human chromosome 6p are also reported in conditional mouse models of osteosarcoma [Walkley et al, 2008].…”

mentioning

confidence: 99%

Analysis of Segmental Duplications, Mouse Genome Synteny and Recurrent Cancer-Associated Amplicons in Human Chromosome 6p21–p12

Martin

Yoshimoto²,

Ludkovski³

et al. 2010

Cytogenet Genome Res

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It has been proposed that regions of microhomology in the human genome could facilitate genomic rearrangements, copy number transitions, and rapid genomic change during tumor progression. To investigate this idea, this study examines the role of repetitive sequence elements, and corresponding syntenic mouse genomic features, in targeting cancer-associated genomic instability of specific regions of the human genome. Automated database-mining algorithms designed to search for frequent copy number transitions and genomic breakpoints were applied to 2 publicly-available online databases and revealed that 6p21–p12 is one of the regions of the human genome most frequently involved in tumor-specific alterations. In these analyses, 6p21–p12 exhibited the highest frequency of genomic amplification in osteosarcomas. Analysis of repetitive elements in regions of homology between human chromosome 6p and the syntenic regions of the mouse genome revealed a strong association between the location of segmental duplications greater than 5 kilobase-pairs and the position of discontinuities at the end of the syntenic region. The presence of clusters of segmental duplications flanking these syntenic regions also correlated with a high frequency of amplification and genomic alteration. Collectively, the experimental findings, in silico analyses, and comparative genomic studies presented here suggest that segmental duplications may facilitate cancer-associated copy number transitions and rearrangements at chromosome 6p21–p12. This process may involve homology-dependent DNA recombination and/or repair, which may also contribute towards the overall plasticity of the human genome.

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Cell Cycle Regulator GeneCDC5L, a Potential Target for 6p12-p21 Amplicon in Osteosarcoma

Cited by 78 publications

References 26 publications

Genomic Alterations and Allelic Imbalances Are Strong Prognostic Predictors in Osteosarcoma

Genomic Alterations and Allelic Imbalances Are Strong Prognostic Predictors in Osteosarcoma

Expression of Human MDGA1 Increases Cell Motility and Cell-Cell Adhesion and Reduces Adhesion to Extracellular Matrix Proteins in MDCK Cells

Analysis of Segmental Duplications, Mouse Genome Synteny and Recurrent Cancer-Associated Amplicons in Human Chromosome 6p21–p12

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