Terminal differentiation and loss of tumorigenicity of human cancers via pluripotency-based reprogramming

Zhang, Xi; Cruz, Filemon S. Dela; Terry, Melissa; Remotti, Fabrizio; Matushansky, Igor

doi:10.1038/onc.2012.237

Cited by 121 publications

(138 citation statements)

References 58 publications

(90 reference statements)

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“…Recent progress has demonstrated that P53 mutations can enhance the efficiency of reprogramming, and upregulation of KLF4 in mutant somatic cells, or P53-knockout cells, produces aggressive cancers in mice (Sarig et al, 2010). Reprogramming of cancer cells by pluripotency factors has been proposed as potential cancer therapies due to their capability to restore terminal differentiation of cancer cells in vitro, increase the responsiveness of cancer cells to chemotherapy in vitro, and reduce the tumorigenicity in vivo (Zhang et al, 2013).…”

Section: Role Of Klf4 In Cscsmentioning

confidence: 99%

Emerging Roles of Krüppel-Like Factor 4 in Cancer and Cancer Stem Cells

Ding¹,

Liu²,

Li³

et al. 2015

Asian Pacific Journal of Cancer Prevention

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Cancer stem cells (CSCs) are rare subpopulations within tumors which are recognized as culprits in cancer recurrence, drug resistance and metastasis. However, the molecular mechanisms of how CSCs are regulated remain elusive. Krüppel-like factors (KLFs) are evolutionarily conserved zinc finger-containing transcription factors with diverse functions in cell differentiation, proliferation, embryogenesis and pluripotency. Recent progress has highlighted the significance of KLFs, especially KLF4, in cancer and CSCs. Therefore, for better therapeutics of cancer disease, it is crucial to develop a deeper understanding of the mechanisms of how KLF4 regulate CSC functions. Herein we summarized the current understanding of the transcriptional regulation of KLF4 in CSCs, and discussed the functional implications of targeting CSCs for potential cancer therapeutics.

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Section: Role Of Klf4 In Cscsmentioning

confidence: 99%

Emerging Roles of Krüppel-Like Factor 4 in Cancer and Cancer Stem Cells

Ding¹,

Liu²,

Li³

et al. 2015

Asian Pacific Journal of Cancer Prevention

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“…These findings support the notion that the epigenetic modification of a cancer cell via nuclear reprogramming could correct some malignant effects of oncogene activation and oncosuppressor gene inactivation, which may constitute the basis for a novel strategy to control tumor progression. 81,82 Zhang et al 81 reported the terminal differentiation and loss of tumorigenicity of human sarcomas via pluripotency-based reprogramming, but these authors failed to observe benign mature tissue elements in their teratomas assays. Kim et al, 83 the only group that has reported the successful generation of a patient-derived iPS cell line from human pancreatic ductal adenocarcinoma (PDAC), only obtained one iPS-like line from a pancreatic cancer harboring a KRAS mutation, the predominant driver of PDAC, and a deletion in exon 2 of the pivotal tumor suppressor CDKN2A.…”

Section: Precrime-ips Mouse Avatars Generation and Utilitiesmentioning

confidence: 99%

“…However, these authors reported only xenograft formation with no histology or immunohistochemistry. Zhang et al 81 recently demonstrated that the reprogramming of sarcoma cells using the 4 canonical Yamanaka genes plus Nanog and Lin28 created cancer cells that lost their tumorigenicity, exhibited reduced drug resistance, and dedifferentiated as iPS cells into various lineages, such as fibroblasts and hematopoietic lineages. Interestingly, the expression of endogenous c-Myc appeared to be reduced in their cellular model, and it was hypermethylated during the reprogramming process.…”

Section: Precrime-ips Mouse Avatars Generation and Utilitiesmentioning

confidence: 99%

Xenopatients 2.0: Reprogramming the epigenetic landscapes of patient-derived cancer genomes

et al. 2014

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“…This paper presents an alternative approach to cancer cell reprogramming towards a differentiated state, by skipping the iPSCs production passage usually found in the literature [9]. We supposed that cancer cells already showed sufficient stem-cell-like behavior to be ready for direct differentiation towards other germ layer lineages.…”

Section: Commentarymentioning

confidence: 99%

“…This metabolic switch is evidenced by a modulation in the expression of glycolysis enzymes, with a lowered expression of the glycolytic enzyme isoforms involved in the Warburg effect such as HK2, IDH2 and PKM2 [7] Concomitantly, we observe an increase in oxidative phosphorylation, as deduced by the decreased ATP content in differentiated cells compared to SH-SY5Y cells, following the in vitro inhibition of the mitochondrial electron transport chain. Restoration of mitochondrial activity is accompanied by a marked increase in Sirt3 activity [8].This paper presents an alternative approach to cancer cell reprogramming towards a differentiated state, by skipping the iPSCs production passage usually found in the literature [9]. We supposed that cancer cells already showed sufficient stem-cell-like behavior to be ready for direct differentiation towards other germ layer lineages.…”

mentioning

confidence: 99%

Back on Track: New Perspectives on Cancer Cell Reprogramming

Arianna¹,

Diedenhofen²,

Gambacurta³

2016

Single Cell Biol

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The possibility to obtain induced pluripotent stem cells (iPSCs) starting from cancer cells has revealed itself to be a major step forward in the understanding of the mechanisms able to regulate stemness, differentiation and neoplastic transformation. Our work proposes a new differentiation method using rapamycin and an amorphous bone matrix to promote the commitment of neuroblastoma cells towards the osteogenic lineage, switching to a different germ layer, without an intermediate iPSCs step. We followed the process from a morphological point of view with immunofluorescence analysis, cytochemistry and electron microscopy and from a metabolic point of view with enzyme activity tests and protein expression analysis. We believe that the morphological and metabolic changes observed are the foundations for a new type of cancer cell reprogramming.Keywords: Neuroblastoma; Cancer cell differentiation; Rapamycin; Scaffolds; Metabolic reprogramming CommentaryOne of the greatest challenges cancer researchers face is unraveling the complex network of cellular signals and events that leads to cancer onset and progression. By approaching the study of cancer from different angles and viewpoints, we can expect to deepen our understanding and paint a richer picture of this network. Progress has been made by reprogramming cancer cells into iPSCs to then differentiate them into various cell types, however we were intrigued by the possibility to reach this end result more directly. The paper "differentiation of human neuroblastoma cells toward the osteogenic lineage by mTOR inhibitor" [1] demonstrates the possibility to directly differentiate a human neuroblastoma cell line (SH-SY5Y) into osteoblast-like cells, without the intermediate step of forming iPSCs by inserting transcription factors [2]. Given this evidence, can we hope that another type of "reprogramming" is possible?It is well known that a reprogramming of the healthy cell is observed during tumorigenesis, led by genetic mutations and/or physiological disturbances that deregulate basic processes in cellular homeostasis and, often also thanks to the tumor microenvironment, allow the acquisition of "stemness" features. This greater "stemness" leads to a particularly aggressive cancer phenotype with a greater tendency to form metastases. What is shared by the entire cancer population is a phenomenon known as "metabolic reprogramming", during which the cells favour energy production through the glycolytic pathway even in normoxic conditions, at the expense of the oxidative phosphorylation pathway. This phenomenon together with lactate production is recognized as the Warburg effect [3,4].We chose a human neuroblastoma cell line, SH-SY5Y, which is a highly aggressive and undifferentiated neuroendocrine cancer type derived from the neural crest. It provided us with a good and appropriate model to test the possibility of forcing a cancer cell to differentiate into a distinct germ layer sheet with respect to its origins. The aspects considered in this paper are both morph...

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Terminal differentiation and loss of tumorigenicity of human cancers via pluripotency-based reprogramming

Cited by 121 publications

References 58 publications

Emerging Roles of Krüppel-Like Factor 4 in Cancer and Cancer Stem Cells

Emerging Roles of Krüppel-Like Factor 4 in Cancer and Cancer Stem Cells

Xenopatients 2.0: Reprogramming the epigenetic landscapes of patient-derived cancer genomes

Back on Track: New Perspectives on Cancer Cell Reprogramming

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