Transient SNAIL1 Expression Is Necessary for Metastatic Competence in Breast Cancer

Tran, Hung D.; Luitel, Krishna; Kim, Michael; Zhang, Kaihua; Longmore, Gregory D.; Tran, David

doi:10.1158/0008-5472.can-14-0923

Cited by 198 publications

(205 citation statements)

References 42 publications

(65 reference statements)

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“…This finding supports the notion that EMT is required for early seeding of metastasis, while MET is essential for metastatic outgrowth (Tsai et al 2012). Indeed, other studies have shown that an extreme EMT can lock cancer cells into a terminally differentiated state, depriving them of stem cell-like properties and cell plasticity and reducing tumor growth (Tran et al 2011(Tran et al , 2014Celia-Terrassa et al 2012).…”

Section: Epithelial-mesenchymal Plasticity and The Acquisition Of Stesupporting

confidence: 81%

Distinctive properties of metastasis-initiating cells

2016

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Primary tumors are known to constantly shed a large number of cancer cells into systemic dissemination, yet only a tiny fraction of these cells is capable of forming overt metastases. The tremendous rate of attrition during the process of metastasis implicates the existence of a rare and unique population of metastasis-initiating cells (MICs). MICs possess advantageous traits that may originate in the primary tumor but continue to evolve during dissemination and colonization, including cellular plasticity, metabolic reprogramming, the ability to enter and exit dormancy, resistance to apoptosis, immune evasion, and co-option of other tumor and stromal cells. Better understanding of the molecular and cellular hallmarks of MICs will facilitate the development and deployment of novel therapeutic strategies.

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Section: Epithelial-mesenchymal Plasticity and The Acquisition Of Stesupporting

confidence: 81%

Distinctive properties of metastasis-initiating cells

2016

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“…tumor fibrosis) that affect tumor progression, invasion, metastasis and response to therapy, despite the continued presence of TWIST1. In sum, the TWIST1 data, our SNAIL1 data herein, and the SNAIL1 data from Stanisavljevic et al (2015) suggest that the primary role for TWIST1 in breast tumorigenesis could be in the tumor cell, whereas SNAIL1 function might be most important in CAFs, although genetic data also supports a role for SNAIL1 in tumor cells (Moody et al, 2005;Tran et al, 2014;Ye et al, 2015).…”

Section: Discussionmentioning

confidence: 55%

“…8E). SNAIL1 already has well described functions in tumor cells, where it can influence tumor-initiating cells and the invasion and metastasis of tumor cells (Ye et al, 2015;Moody et al, 2005;Tran et al, 2014). Less appreciated, perhaps, is the importance of SNAIL1 in mesenchymal cells (e.g.…”

Section: Discussionmentioning

confidence: 99%

Mechanical signals regulate and activate SNAIL1 protein to control the fibrogenic response of cancer-associated fibroblasts

Zhang

Grither

Hove

et al. 2016

Journal of Cell Science

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Increased deposition of collagen in extracellular matrix (ECM) leads to increased tissue stiffness and occurs in breast tumors. When present, this increases tumor invasion and metastasis. Precisely how this deposition is regulated and maintained in tumors is unclear. Much has been learnt about mechanical signal transduction in cells, but transcriptional responses and the pathophysiological consequences are just becoming appreciated. Here, we show that the SNAIL1 (also known as SNAI1) protein level increases and accumulates in nuclei of breast tumor cells and cancer-associated fibroblasts (CAFs) following exposure to stiff ECM in culture and in vivo. SNAIL1 is required for the fibrogenic response of CAFs when exposed to a stiff matrix. ECM stiffness induces ROCK activity, which stabilizes SNAIL1 protein indirectly by increasing intracellular tension, integrin clustering and integrin signaling to ERK2 (also known as MAPK1). Increased ERK2 activity leads to nuclear accumulation of SNAIL1, and, thus, avoidance of cytosolic proteasome degradation. SNAIL1 also influences the level and activity of YAP1 in CAFs exposed to a stiff matrix. This work describes a mechanism whereby increased tumor fibrosis can perpetuate activation of CAFs to sustain tumor fibrosis and promote tumor metastasis through regulation of SNAIL1 protein level and activity.

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“…PTK6 specifically regulates the expression of SNAIL, and not other transcriptional repressors. SNAIL has been linked to generation of cancer stem cell properties (41), drug resistance (37), cancer recurrence and metastasis, all contributors to poor prognosis for patients (16,42). Although SNAIL is often transcriptionally regulated by EMT-inducing stimuli, here we show that PTK6 regulates the proteasome-dependent degradation of SNAIL protein.…”

Section: Discussionmentioning

confidence: 59%

PTK6 Inhibition Suppresses Metastases of Triple-Negative Breast Cancer via SNAIL-Dependent E-Cadherin Regulation

et al. 2016

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Patients with triple-negative breast cancers (TNBC) are at high risk for recurrent or metastatic disease despite standard treatment, underscoring the need for novel therapeutic targets and strategies. Here we report that protein tyrosine kinase 6 (PTK6) is expressed in approximately 70% of TNBCs where it acts to promote survival and metastatic lung colonization. PTK6 downregulation in mesenchymal TNBC cells suppressed migration and three-dimensional culture growth, and enhanced anoikis, resistance to which is considered a prerequisite for metastasis. PTK6 downregulation restored E-cadherin levels via proteasome-dependent degradation of the E-cadherin repressor SNAIL. Beyond being functionally required in TNBC cells, kinase-active PTK6 also suppressed E-cadherin expression, promoted cell migration, and increased levels of mesenchymal markers in nontransformed MCF10A breast epithelial cells, consistent with a role in promoting an epithelial-mesenchymal transition (EMT). SNAIL downregulation and E-cadherin upregulation mediated by PTK6 inhibition induced anoikis, leading to impaired metastatic lung colonization in vivo. Finally, effects of PTK6 downregulation were phenocopied by treatment with a recently developed PTK6 kinase inhibitor, further implicating kinase activity in regulation of EMT and metastases. Our findings illustrate the clinical potential for PTK6 inhibition to improve treatment of patients with high-risk TNBC.Cancer Res; 76(15); 4406-17. Ó2016 AACR.

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Transient SNAIL1 Expression Is Necessary for Metastatic Competence in Breast Cancer

Cited by 198 publications

References 42 publications

Distinctive properties of metastasis-initiating cells

Distinctive properties of metastasis-initiating cells

Mechanical signals regulate and activate SNAIL1 protein to control the fibrogenic response of cancer-associated fibroblasts

PTK6 Inhibition Suppresses Metastases of Triple-Negative Breast Cancer via SNAIL-Dependent E-Cadherin Regulation

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