Gene expression profiling of somatic and pluripotent cells reveals novel pathways involved in reprogramming

Yn, Cai; Xh, Dai; Qh, Zhang; Hu, Ruicheng; Zm, Dai

doi:10.4238/2015.october.5.21

Cited by 4 publications

(3 citation statements)

References 34 publications

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“…LRRN1 is associated with neuroepithelial boundary formations and its temporal expression changes during mammalian neural progenitor cell development [79, 80]. In embryonic SCs, LRRN1 , alias NLRR1, was one of four genes markedly higher expressed than in fibroblasts [81] and in a xenograft mouse model, LRRN1 expression in neuroblastoma cells resulted in enhanced tumor growth [82]. OLFML3 has been identified as a proangiogenic factor [83].…”

Section: Discussionmentioning

confidence: 99%

Array expression meta-analysis of cancer stem cell genes identifies upregulation of PODXL especially in DCC low expression meningiomas

Schulten

Hussein

2019

PLoS ONE

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Background Meningiomas are the most common intracranial tumors, with a subset of cases bearing a progressive phenotype. The DCC netrin 1 receptor ( DCC ) is a candidate gene for early meningioma progression. Cancer stem cell (CSC) genes are emerging as cancer therapeutic targets, as their expression is frequently associated with aggressive tumor phenotypes. The main objective of the study was to identify deregulated CSC genes in meningiomas. Materials and methods Interrogating two expression data repositories, significantly differentially expressed genes (DEGs) were determined using DCC low vs . DCC high expression groups and WHO grade I (GI) vs . grade II + grade III (GII + GIII) comparison groups. Human stem cell (SC) genes were compiled from two published data sets and were extracted from the DEG lists. Biofunctional analysis was performed to assess associations between genes or molecules. Results In the DCC low vs . DCC high expression groups, we assessed seven studies representing each between seven and 58 samples. The type I transmembrane protein podocalyxin like ( PODXL ) was markedly upregulated in DCC low expression meningiomas in six studies. Other CSC genes repeatedly deregulated included, e . g ., BMP/retinoic acid inducible neural specific 1 ( BRINP1 ), prominin 1 ( PROM1 ), solute carrier family 24 member 3 ( SLC24A3 ), rRho GTPase activating protein 28 ( ARHGAP28 ), Kruppel like factor 5 ( KLF5 ), and leucine rich repeat containing G protein-coupled receptor 4 ( LGR4 ). In the GI vs . GII + GIII comparison groups, we assessed six studies representing each between nine and 68 samples. DNA topoisomerase 2-alpha ( TOP2A ) was markedly upregulated in GII + GIII meningiomas in four studies. Other CSC genes repeatedly deregulated included, e . g ., ARHGAP28 and PODXL . Network analysis revealed associations of molecules with, e . g ., cellular development and movement; nervous system development and function; and cancer. Conclusions This meta-analysis on meningiomas identified a comprehensive list of deregulated CSC genes across different array expression studies. Especially, PODXL is of interest for functional assessment in progressive meningiomas.

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Section: Discussionmentioning

confidence: 99%

Array expression meta-analysis of cancer stem cell genes identifies upregulation of PODXL especially in DCC low expression meningiomas

Schulten

Hussein

2019

PLoS ONE

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“…Для гена Nts участие в формировании плюрипотентного фенотипа показано лишь в случае т.н. индуцированных плюрипотентных клеток [216]. И, наконец, для гена Crabp2 нет доказательств участия в формировании стволовости, а лишь показана специфическая экспрессия в нормальных и опухолевых стволовых клетках [217,218], что в сочетании с его непосредственным участием в метаболизме ретиноевых кислот и их производных делает его привлекательным в качестве потенциального маркера стволовости как опухолевых, так и нормальных стволовых клеток.…”

Section: индукция и поддержание стволовостиunclassified

Yin and Yang of Pluripotency: Results of Analysis of Genes Overexpressed In Tumor-Initiating Cells of Krebs-2 Ascites Carcinoma

Efremov¹,

Proskurina²,

Potter³

et al. 2019

Math.Biol.Bioinf.

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Functional analysis of 167 genes overexpressed in Krebs-2 tumor initiating cells was performed. Genes were assigned to the three functional groups that determine the malignant phenotype of cancer cells. These groups represent the following features of tumor cells: proliferative self-sufficiency, invasive growth and metastasis, and multiple drug resistance. Malignancy of cancer stem cells was found to be provided by the same genes that provide the stemness of normal pluri-/multipotent stem cells. These results suggest that the malignancy is just the ability to maintain the stem cell specific genes expression profile, and, as a consequence, the stemness itself regardless of the controlling effect of stem niches.

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“…Thus, for Cd55 and Il10 , no direct contribution to the formation or maintenance of stemness of normal pluri-/multipotent cells was proved, but the essential role in the realization of the reparative functions of mesenchymal and autologous-induced pluripotent stem cells by dint of the immunosuppressive action of the protein products of these genes was demonstrated (Ardianto et al, 2010 ; Liu et al, 2012 ; de Almeida et al, 2014 ; Lee et al, 2015b ). The role of Nts in the formation of the pluripotent phenotype has been proved only in the case of the so-called induced pluripotent cells (Cai et al, 2015 ). And, finally, for Crabp2 there was no direct evidence of its participation in the formation of stemness, but only demonstration of specific expression in normal human amniotic fluid-derived stem cells and in polycythemia vera-derived tumor stem cells (Steidl et al, 2005 ; Kim et al, 2010 ).…”

Section: The Yin and Yang Of Pluripotencymentioning

confidence: 99%

Cancer Stem Cells: Emergent Nature of Tumor Emergency

et al. 2018

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A functional analysis of 167 genes overexpressed in Krebs-2 tumor initiating cells was performed. In the first part of the study, the genes were analyzed for their belonging to one or more of the three groups, which represent the three major phenotypic manifestation of malignancy of cancer cells, namely (1) proliferative self-sufficiency, (2) invasive growth and metastasis, and (3) multiple drug resistance. 96 genes out of 167 were identified as possible contributors to at least one of these fundamental properties. It was also found that substantial part of these genes are also known as genes responsible for formation and/or maintenance of the stemness of normal pluri-/multipotent stem cells. These results suggest that the malignancy is simply the ability to maintain the stem cell specific genes expression profile, and, as a consequence, the stemness itself regardless of the controlling effect of stem niches. In the second part of the study, three stress factors combined into the single concept of “generalized cellular stress,” which are assumed to activate the expression of these genes, were defined. In addition, possible mechanisms for such activation were identified. The data obtained suggest the existence of a mechanism for the de novo formation of a pluripotent/stem phenotype in the subpopulation of “committed” tumor cells.

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Gene expression profiling of somatic and pluripotent cells reveals novel pathways involved in reprogramming

Cited by 4 publications

References 34 publications

Array expression meta-analysis of cancer stem cell genes identifies upregulation of PODXL especially in DCC low expression meningiomas

Array expression meta-analysis of cancer stem cell genes identifies upregulation of PODXL especially in DCC low expression meningiomas

Yin and Yang of Pluripotency: Results of Analysis of Genes Overexpressed In Tumor-Initiating Cells of Krebs-2 Ascites Carcinoma

Cancer Stem Cells: Emergent Nature of Tumor Emergency

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