SOX2 regulates self-renewal and tumorigenicity of human melanoma-initiating cells

Santini, Roberta; Pietrobono, Silvia; Pandolfi, Silvia; Montagnani, Valentina; D’Amico, Massimo; Penachioni, Junia Y.; Vinci, Maria; Borgognoni, Lorenzo; Stecca, Barbara

doi:10.1038/onc.2014.71

Cited by 179 publications

(207 citation statements)

References 73 publications

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“…Nonetheless, our findings do not rule out that SOX2 can exert certain activities in melanoma cells, for instance in isolated cells exposed to varying culture conditions or in the non-physiological environment encountered by human cells upon xenotransplantation into immunocompromised mouse model systems 22 . Of note, studies performed solely in vitro or in combination with xenotransplantation assays provided controversial results, either implicating SOX2 in melanoma cell proliferation or invasion, or also failing to reveal a crucial role in melanoma as in our experiments performed with CRISPR-Cas-mediated knock out cells [20][21][22][23][24] .…”

Section: Sox2 Is Dispensable For Primary Tumor and Metastasis Formationcontrasting

confidence: 74%

“…Tissue microarray (TMA) expression analysis revealed that SOX2 protein is expressed in around 50% of all human melanoma 20,21 . In a recent study, RNAi-mediated silencing of SOX2 led to reduced melanoma sphere self-renewal and tumor growth of xenotransplanted cells, supporting an important role of Sox2 in tumor initiation and tumor maintenance 22 . In other reports, however, knockdown of SOX2 did not affect proliferation of human melanoma cells 20,21,23 .…”

Section: Introductionmentioning

confidence: 85%

“…Of note, studies performed solely in vitro or in combination with xenotransplantation assays provided controversial results, either implicating SOX2 in melanoma cell proliferation or invasion, or also failing to reveal a crucial role in melanoma as in our experiments performed with CRISPR-Cas-mediated knock out cells [20][21][22][23][24] . While the discrepancies between our work and previously published data could potentially be explained by different experimental settings 37 , they could also reflect the heterogeneity of melanoma and, thus, leave open whether SOX2 might fulfill a role in some cases of human melanoma.…”

Section: Sox2 Is Dispensable For Primary Tumor and Metastasis Formationmentioning

confidence: 99%

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Sox2 is dispensable for primary melanoma and metastasis formation

et al. 2017

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Tumor initiation and metastasis formation in many cancers have been associated with emergence of a gene expression program normally active in embryonic or organ-specific stem cells. In particular, the stem cell transcription factor Sox2 is not only expressed in a variety of tumors, but is also required for their formation. Melanoma, the most aggressive skin tumor, derives from melanocytes that during development originate from neural crest stem cells. While neural crest stem cells do not express Sox2, expression of this transcription factor has been reported in melanoma. However, the role of Sox2 in melanoma is controversial. To study the requirement of Sox2 for melanoma formation, we therefore performed CRISPR-Cas9-mediated gene inactivation in human melanoma cells. In addition, we conditionally inactivated Sox2 in a genetically engineered mouse model, in which melanoma spontaneously develops in the context of an intact stroma and immune system. Surprisingly, in both models, loss of Sox2 did neither affect melanoma initiation, nor growth, nor metastasis formation. The lack of a tumorigenic role of Sox2 in melanoma might reflect a distinct stem cell program active in neural crest stem cells and during melanoma formation.

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Section: Sox2 Is Dispensable For Primary Tumor and Metastasis Formationcontrasting

confidence: 74%

Section: Introductionmentioning

confidence: 85%

Section: Sox2 Is Dispensable For Primary Tumor and Metastasis Formationmentioning

confidence: 99%

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Sox2 is dispensable for primary melanoma and metastasis formation

et al. 2017

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“…The shRNA oligonucleotides for SOX2 gene knockdown were designed and synthesized as previously described [23] . Two different shRNA sequences and one scramble sequence as a control were subcloned into plasmid vector pGCsi-H1 following manufacturer's instructions.…”

Section: Silencing Sox2 In Crc Cellsmentioning

confidence: 99%

Physcion inhibits the metastatic potential of human colorectal cancer SW620 cells in vitro by suppressing the transcription factor SOX2

et al. 2015

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Aim: Physcion, an anthraquinone derivative, exhibits hepatoprotective, anti-inflammatory, anti-microbial and anti-cancer activities. In this study we examined whether and how physcion inhibited metastatic potential of human colorectal cancer cells in vitro. Methods: Human colorectal cancer cell line SW620 was tested. Cell migration and invasion were assessed using a wound healing and Transwell assay, respectively. The expression levels of transcription factor SOX2 in the cells were modulated with shRNA targeting SOX2 and SOX2 overexpressing plasmid. The expression of target molecules involved in epithelial-mesenchymal transition (EMT) process and the signaling pathways was determined with Western blots or qRT-PCR. ROS levels were measured using DCF-DA. Results: Physcion (2.5, 5 mol/L) did not affect the cell viability, but dose-dependently inhibited the cell adhesion, migration and invasion. Physcion also inhibited the EMT process in the cells, as evidenced by the increased epithelial marker E-cadherin expression, and by decreased expression of mesenchymal markers N-cadherin, vimentin, fibronectin and α-SMA, as well as transcriptional repressors Snail, Slug and Twist. Physcion suppressed the expression of SOX2, whereas overexpression of SOX2 abrogated the inhibition of physcion on metastatic behaviors. Physcion markedly increased ROS production and phosphorylation of AMPK and GSK3β in the cells, whereas the AMPK inhibitor compound C or the ROS inhibitor NAC abolished the inhibition of physcion on metastatic behaviors. Conclusion: Physcion inhibits the metastatic potential of human colorectal cancer cells in vitro via activating ROS/AMPK/GSK3β signaling pathways and suppressing SOX2.

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“…Consequently, the ALDEFLUOR assay has been widely used to isolate CSC subpopulations in various tumors including different types of sarcomas 23,[27][28][29][30][31] . These CSC subpopulations commonly overexpress pluripotency factors such as Sex-determining region Y-Box2 (SOX2), which plays important roles in the regulation of self-renewal and tumorigenicity in CSC subpopulations of several types of cancer [32][33][34][35][36][37] . The process of emergence/evolution of CSC subpopulations from the cell-of-origin in sarcomagenesis has barely been addressed.…”

mentioning

confidence: 99%

ALDH1 expression and activity increase during tumor evolution in sarcoma cancer stem cell populations

Martinez-Cruzado¹,

Tornín²,

Santos³

et al. 2016

European Journal of Cancer

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Tumors evolve from initial tumorigenic events into increasingly aggressive behaviors in a process usually driven by subpopulations of cancer stem cells (CSCs). Mesenchymal stromal/stem cells (MSCs)may act as the cell-of-origin for sarcomas, and CSCs that present MSC features have been identified in sarcomas due to their ability to grow as self-renewed floating spheres (tumorspheres). Accordingly, we previously developed sarcoma models using human MSCs transformed with relevant oncogenic events. To study the evolution/emergence of CSC subpopulations during tumor progression, we compared the tumorigenic properties of bulk adherent cultures and tumorsphere-forming subpopulations both in the sarcoma cell-of-origin models (transformed MSCs) and in their corresponding tumor xenograft-derived cells. Tumor formation assays showed that the tumorsphere cultures from xenograft-derived cells, but not from the cell-of-origin models, were enriched in CSCs, providing evidence of the emergence of bona fide CSCs subpopulations during tumor progression. Relevant CSC-related factors, such as ALDH1 and SOX2, were increasingly upregulated in CSCs during tumor progression, and importantly, the increased levels and activity of ALDH1 in these subpopulations were associated with enhanced tumorigenicity. In addition to being a CSC marker, our findings indicate that ALDH1 could also be useful for tracking the malignant potential of CSC subpopulations during sarcoma evolution.Tumors initiate from a permissible cell-of-origin that receives the first oncogenic events needed to trigger tumoral proliferation 1,2 . According to the hierarchical model of cancer, after this initial step, tumors gain complexity and cellular heterogeneity, among other factors, through the emergence of tumor-propagating subpopulations or CSCs, which exhibit stem cells properties and are responsible for sustaining tumorigenesis 3,4 . Therefore, the evolution of these subpopulations through gaining new genetic and/or epigenetic alterations drives the evolution of tumors toward enhanced aggressiveness 5 . Sarcomas comprise a heterogeneous group of aggressive mesenchymal malignancies that often show a limited clinical response to current therapies 6 . Experimental evidence supports the notion that many types of sarcomas are hierarchically organized and sustained by subpopulations of self-renewing CSCs that can generate the full repertoire of tumor cells and display tumor re-initiating properties 7,8 . In addition, it has been recently established that transformed MSCs and/or their immediate lineage progenitors are the most likely cell-of-origin for many types of sarcomas [8][9][10] . Accordingly, many of the CSC sub-populations identified in different types of sarcomas displayed MSC phenotype and functional properties 7,8,[11][12][13] . Therefore, many efforts have been made to produce models of sarcomas based on MSCs transformed with relevant oncogenic events 8,10 . These types of models represent unparalleled systems for unraveling the mechanisms underlying sarcomagen...

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SOX2 regulates self-renewal and tumorigenicity of human melanoma-initiating cells

Cited by 179 publications

References 73 publications

Sox2 is dispensable for primary melanoma and metastasis formation

Sox2 is dispensable for primary melanoma and metastasis formation

Physcion inhibits the metastatic potential of human colorectal cancer SW620 cells in vitro by suppressing the transcription factor SOX2

ALDH1 expression and activity increase during tumor evolution in sarcoma cancer stem cell populations

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