Characterization of iPSCs derived from low grade gliomas revealed early regional chromosomal amplifications during gliomagenesis

Liu, Zhong; Che, Pulin; Mercado, Juan J.; Hackney, James R.; Friedman, Gregory K.; Zhang, Cheng; You, Zhiying; Zhao, Xinyang; Ding, Qiang; Kim, Kitai; Li, Hu; Liu, Xiaoguang; Markert, James M.; Nabors, Burt; Gillespie, G. Yancey; Zhao, Rui; Han, Xiaosi

doi:10.1007/s11060-018-03047-1

Cited by 12 publications

(15 citation statements)

References 52 publications

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“…Interestingly, 4F-MCF10A showed relatively higher expression of endogenous mRNA and protein level rather than 4F-MCF7. When considering for reprogramming potential, MCF10A seems to be more likely to be reprogrammed than the MCF7, consistent with previous report (22).…”

Section: Discussionsupporting

confidence: 91%

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Reprogramming of Cancer Cells into Induced Pluripotent Stem Cells Questioned

Bang

Choi

Lee

et al. 2019

IJSC

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Background and ObjectivesSeveral recent studies have claimed that cancer cells can be reprogrammed into induced pluripotent stem cells (iPSCs). However, in most cases, cancer cells seem to be resistant to cellular reprogramming. Furthermore, the underlying mechanisms of limited reprogramming in cancer cells are largely unknown. Here, we identified the candidate barrier genes and their target genes at the early stage of reprogramming for investigating cancer reprogramming.MethodsWe tried induction of pluripotency in normal human fibroblasts (BJ) and both human benign (MCF10A) and malignant (MCF7) breast cancer cell lines using a classical retroviral reprogramming method. We conducted RNA-sequencing analysis to compare the transcriptome of the three cell lines at early stage of reprogramming.ResultsWe could generate iPSCs from BJ, whereas we were unable to obtain iPSCs from cancer cell lines. To address the underlying mechanism of limited reprogramming in cancer cells, we identified 29 the candidate barrier genes based on RNA-sequencing data. In addition, we found 40 their target genes using Cytoscape software.ConclusionsOur data suggest that these genes might one of the roadblock for cancer cell reprogramming. Furthermore, we provide new insights into application of iPSCs technology in cancer cell field for therapeutic purposes.

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Section: Discussionsupporting

confidence: 91%

“…Recent study implies that induction of pluripotency from malignant cancer cells was challenging compared to benign cancer cells (22). However, the exact reason for the differences regarding to reprogramming between malignant and benign cancer cells is unknown.…”

Section: Introductionmentioning

confidence: 99%

Reprogramming of Cancer Cells into Induced Pluripotent Stem Cells Questioned

Bang

Choi

Lee

et al. 2019

IJSC

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“…Their results demonstrate that cells containing the IDH1 mutation are resistant to reprogramming. Their explanation is the high sensitivity of the pluripotent stem cells to D2HG 59 because when human embryonic stem cells (hESCs) were treated with D2HG for 24 h, the hESCs could not tolerate D2HG and die. They found, however, that reprogrammed colonies showed genetic changes, such as amplification of chromosome Xq23 or chromosome 11 and deletion of chromosome 1p, 4, 19q, and Y, amplification of 1.4 Mb region on chromosome 7q31, with co-amplification of genes located in this region.…”

Section: Procedures Of In Vitro Modelingmentioning

confidence: 99%

“…Due to the toxicity of Table 2 Listing/summary of model generation strategies using overexpression of IDH MUT on wild-type background. D2HG on hiPSCs 59 , scientists should investigate ways to by-pass this issue. 2D disease modeling by human iPSC can show some disease phenotypes, but there are no tissue or organ level structures.…”

Section: Healthy Donor-derived Disease Modelsmentioning

confidence: 99%

Current biomarker-associated procedures of cancer modeling-a reference in the context of IDH1 mutant glioma

2020

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Isocitrate dehydrogenases (IDH1/2) are central molecular markers for glioblastoma. Providing in vitro or in vivo models with mutated IDH1/2 can help prepare facilities to understand the biology of these mutated genes as glioma markers, as well as help, improve therapeutic strategies. In this review, we first summarize the biology principles of IDH and its mutations and outline the core primary findings in the clinical context of neuro-oncology. Given the extensive research interest and exciting developments in current stem cell biology and genome editing, the central part of the manuscript is dedicated to introducing various routes of disease modeling strategies of IDH mutation (IDHMut) glioma and comparing the scientific-technological findings from the field using different engineering methods. Lastly, by giving our perspective on the benefits and limitations of patient-derived and donor-derived disease modeling respectively, we aim to propose leading research questions to be answered in the context of IDH1 and glioma.

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“…paratuberculosis infection (Jacobsen et al, 2010;McGovern et al, 2019). Furthermore, gene amplifications of LRCH2 and LRCH3 are associated with tumorigenesis of low grade gliomas and melanomas, respectively (Liu et al, 2019;Williams et al, 2020).…”

Section: Genomic Analysesmentioning

confidence: 99%

Structure and Emerging Functions of LRCH Proteins in Leukocyte Biology

Rivière

Bader

Pogoda

et al. 2020

Front. Cell Dev. Biol.

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Actin-dependent leukocyte trafficking and activation are critical for immune surveillance under steady state conditions and during disease states. Proper immune surveillance is of utmost importance in mammalian homeostasis and it ensures the defense against pathogen intruders, but it also guarantees tissue integrity through the continuous removal of dying cells or the elimination of tumor cells. On the cellular level, these processes depend on the precise reorganization of the actin cytoskeleton orchestrating, e.g., cell polarization, migration, and vesicular dynamics in leukocytes. The fine-tuning of the actin cytoskeleton is achieved by a multiplicity of actin-binding proteins inducing, e.g., the organization of the actin cytoskeleton or linking the cytoskeleton to membranes and their receptors. More than a decade ago, the family of leucine-rich repeat (LRR) and calponin homology (CH) domain-containing (LRCH) proteins has been identified as cytoskeletal regulators. The LRR domains are important for protein-protein interactions and the CH domains mediate actin binding. LRR and CH domains are frequently found in many proteins, but strikingly the simultaneous expression of both domains in one protein only occurs in the LRCH protein family. To date, one LRCH protein has been described in drosophila and four LRCH proteins have been identified in the murine and the human system. The function of LRCH proteins is still under investigation. Recently, LRCH proteins have emerged as novel players in leukocyte function. In this review, we summarize our current understanding of LRCH proteins with a special emphasis on their function in leukocyte biology.

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Characterization of iPSCs derived from low grade gliomas revealed early regional chromosomal amplifications during gliomagenesis

Cited by 12 publications

References 52 publications

Reprogramming of Cancer Cells into Induced Pluripotent Stem Cells Questioned

Reprogramming of Cancer Cells into Induced Pluripotent Stem Cells Questioned

Current biomarker-associated procedures of cancer modeling-a reference in the context of IDH1 mutant glioma

Structure and Emerging Functions of LRCH Proteins in Leukocyte Biology

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