Population heterogeneity in the epithelial to mesenchymal transition is controlled by NFAT and phosphorylated Sp1

Gould, Russell A.; Chakrabarti, Anirikh; Varner, Jeffrey D.; Butcher, Jonathan T.

doi:10.1101/028993

Cited by 6 publications

(11 citation statements)

References 124 publications

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“…Moreover, cells isolated from in vivo tumors contain hybrid E/M cells [ 39 , 103 , 163 ]. Thus, hybrid E/M state can be a stable phenotype, especially in the presence of phenotypic stability factors (PSFs) such as OVOL, NRF2, GRHL2, NUMB, ∆NP63α, and NFATc that can promote and stabilize hybrid E/M state and increase the mean residence times of cells in hybrid E/M states [ 63 , 83 , 85 , 87 , 162 , [164] , [165] , [166] ]. Knockdown of these PSFs in H1975 lung cancer cell line impaired a stable hybrid E/M phenotype and collective migration and drove the cells towards a complete EMT [ 63 , 165 ].…”

Section: Stabilizers Of Partial Emt Phenotypementioning

confidence: 99%

Hypoxia, partial EMT and collective migration: Emerging culprits in metastasis

Saxena

Jolly

Balamurugan

2020

Translational Oncology

150

112

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Epithelial-mesenchymal transition (EMT) is a cellular biological process involved in migration of primary cancer cells to secondary sites facilitating metastasis. Besides, EMT also confers properties such as stemness, drug resistance and immune evasion which can aid a successful colonization at the distant site. EMT is not a binary process; recent evidence suggests that cells in partial EMT or hybrid E/M phenotype(s) can have enhanced stemness and drug resistance as compared to those undergoing a complete EMT. Moreover, partial EMT enables collective migration of cells as clusters of circulating tumor cells or emboli, further endorsing that cells in hybrid E/M phenotypes may be the ‘fittest’ for metastasis. Here, we review mechanisms and implications of hybrid E/M phenotypes, including their reported association with hypoxia. Hypoxia-driven activation of HIF-1α can drive EMT. In addition, cyclic hypoxia, as compared to acute or chronic hypoxia, shows the highest levels of active HIF-1α and can augment cancer aggressiveness to a greater extent, including enriching for a partial EMT phenotype. We also discuss how metastasis is influenced by hypoxia, partial EMT and collective cell migration, and call for a better understanding of interconnections among these mechanisms. We discuss the known regulators of hypoxia, hybrid EMT and collective cell migration and highlight the gaps which needs to be filled for connecting these three axes which will increase our understanding of dynamics of metastasis and help control it more effectively.

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Section: Stabilizers Of Partial Emt Phenotypementioning

confidence: 99%

Hypoxia, partial EMT and collective migration: Emerging culprits in metastasis

Saxena

Jolly

Balamurugan

2020

Translational Oncology

150

112

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“…In presence of NFATc, cells undergo a delayed or stalled EMT; thus maintaining cells in hybrid E/M phenotypes; knockdown of NFATc in H1975 NSCLC cells drove the progression towards a complete EMT phenotype, reminiscent of observations made for other PSFs -GRHL2, OVOL2, NUMB and NRF2 (17)(18)(19)(20)(21)(22). Similar effects of NFATc knockdown were also seen in MCF10A and DLD1 cells where treatment with VIVIT, a soluble inhibitor of NFATc transcriptional activity, significantly reduced E-cadherin expression and protein level, and increased Slug and Vimentin levels (28), thus driving EMT. NFATc transcriptional activity was shown to be capable of maintaining Ecadherin levels even in the presence of TGFβ induced EMT (28), suggesting that NFATc acted as a "molecular brake" or "guardian" of epithelial traits, preventing a complete EMT (39).…”

Section: Discussionmentioning

confidence: 54%

“…Similar effects of NFATc knockdown were also seen in MCF10A and DLD1 cells where treatment with VIVIT, a soluble inhibitor of NFATc transcriptional activity, significantly reduced E-cadherin expression and protein level, and increased Slug and Vimentin levels (28), thus driving EMT. NFATc transcriptional activity was shown to be capable of maintaining Ecadherin levels even in the presence of TGFβ induced EMT (28), suggesting that NFATc acted as a "molecular brake" or "guardian" of epithelial traits, preventing a complete EMT (39). Consistently, NFATc1 was identified to be a master regulator of chromatin remodeling to regulate hybrid E/M phenotypes in skin cancer in vivo; the proportion of hybrid E/M phenotypes was also shown to be increased by GRHL2, OVOL1/2, and ΔNP63α at the expense of complete EMT cells, thus lending further credence to our results indicating a functional equivalence between NFATc1 and previously identified PSFs such as GRHL2, OVOL1/2, ΔNP63α, and NRF2 (6).…”

Section: Discussionmentioning

confidence: 55%

“…On one hand, overexpression of NFATc increased the levels of TWIST, ZEB1, SNAI1; its downregulation decreased the levels of these EMT-TFs as well as mesenchymal markers such as N-cadherin and Vimentin ZEB (27). On the other hand, NFATc transcriptional activity was also shown to be crucial for maintaining E-cadherin levels (28), which can inhibit ZEB1 indirectly (29,30) and restrict EMT. Moreover, NFATc can activate SOX2 (27,31) which can upregulate levels of miR-200 (32); overexpression of miR-200 can drive MET (33).…”

Section: Introductionmentioning

confidence: 99%

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NFATc acts as a non-canonical phenotypic stability factor for a hybrid epithelial/mesenchymal phenotype

Subbalakshmi

Kundnani²,

Biswas

et al. 2020

Preprint

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Metastasis remains the cause of over 90% of cancer-related deaths. Cells undergoing metastasis use phenotypic plasticity to adapt to their changing environmental conditions and avoid therapy and immune response. Reversible transitions between epithelial and mesenchymal phenotypes -Epithelial-Mesenchymal Transition (EMT) and its reverse Mesenchymal-Epithelial Transition (MET) -form a key axis of phenotypic plasticity during metastasis and therapy resistance. Recent studies have shown that the cells undergoing EMT/MET can attain one or more hybrid epithelial/mesenchymal (E/M) phenotypes, the process of which is termed as partial EMT/MET. Cells in hybrid E/M phenotype(s) can be more aggressive than those in either epithelial or mesenchymal state. Thus, it is crucial to identify the factors and regulatory networks enabling such hybrid E/M phenotypes. Here, employing an integrated computational-experimental approach, we show that the transcription factor NFATc can inhibit the process of complete EMT, thus stabilizing the hybrid E/M phenotype. It increases the range of parameters enabling the existence of a hybrid E/M phenotype, thus behaving as a phenotypic stability factor (PSF). However, unlike previously identified PSFs, it does not increase the mean residence time of the cells in hybrid E/M phenotypes, as shown by stochastic simulations; rather it enables the coexistence of epithelial, mesenchymal and hybrid E/M phenotypes and transitions among them. Clinical data suggests the effect of NFATc on patient survival in a tissue-specific or contextdependent manner. Together, our results indicate that NFATc behaves as a non-canonical phenotypic stability factor for a hybrid E/M phenotype.

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“…Mathematical modeling approaches have been further used to characterize phenotypic stability factors (PSFs) that can promote and stabilize hybrid E/M states. These PSFs include the transcription factors OVOL, GRHL2, NRF2, NP63, NUMB and miR-145/OCT4 [50][51][52][53][54]. These PSFs can function in two related manners.…”

Section: Hybrid E/m Phenotypes Are Predicted By Mathematical Modelingmentioning

confidence: 99%

Quantifying Cancer Epithelial-Mesenchymal Plasticity and Its Association with Stemness and Immune Response

Jia

Bocci

et al. 2019

Preprint

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Cancer cells can acquire a spectrum of stable hybrid epithelial/mesenchymal (E/M) states during epithelial-mesenchymal transition (EMT). Cells in these hybrid E/M phenotypes often combine epithelial and mesenchymal features and tend to migrate collectively commonly as small clusters. Such collectively migrating cancer cells play a pivotal role in seeding metastases and their presence in cancer patients indicates an adverse prognostic factor. Moreover, cancer cells in hybrid E/M phenotypes tend to be more associated with stemness which endows them with tumor-initiation ability and therapy resistance. Most recently, cells undergoing EMT have been shown to promote immune suppression for better survival. A systematic understanding of the emergence of hybrid E/M phenotypes and the connection of EMT with stemness and immune suppression would contribute to more effective therapeutic strategies. In this review, we first discuss recent efforts combining theoretical and experimental approaches to elucidate mechanisms underlying EMT multi-stability (i.e. the existence of multiple stable phenotypes during EMT) and the properties of hybrid E/M phenotypes. Following we discuss non-cell-autonomous regulation of EMT by cell cooperation and extracellular matrix. Afterwards, we discuss various metrics that can be used to quantify EMT spectrum. We further describe possible mechanisms underlying the formation of clusters of circulating tumor cells. Last but not least, we summarize recent systems biology analysis of the role of EMT in the acquisition of stemness and immune suppression.

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Population heterogeneity in the epithelial to mesenchymal transition is controlled by NFAT and phosphorylated Sp1

Cited by 6 publications

References 124 publications

Hypoxia, partial EMT and collective migration: Emerging culprits in metastasis

Hypoxia, partial EMT and collective migration: Emerging culprits in metastasis

NFATc acts as a non-canonical phenotypic stability factor for a hybrid epithelial/mesenchymal phenotype

Quantifying Cancer Epithelial-Mesenchymal Plasticity and Its Association with Stemness and Immune Response

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