EGF hijacks miR-198/FSTL1 wound-healing switch and steers a two-pronged pathway toward metastasis

Sundaram, Gopinath M; Ismail, Hisyam M; Bashir, Mohsin; Muhuri, Manish; Vaz, Candida; Nama, Srikanth; Ow, Ghim Siong; Vladimirovna, Ivshina Anna; Rajkumar, R.; Burke, Brian; Tanavde, Vivek; Kuznetsov, Vladimir A.; Lane, E. Birgitte; Sampath, Prabha

doi:10.1084/jem.20170354

Cited by 54 publications

(60 citation statements)

References 34 publications

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“…Second, high levels of p-ERK1/2, a measure of MAPK signaling, were reported in TA cells (21). Third, RSPO3, a Wnt sensitizer, was shown to inhibit MAPK signaling and block osteogenic differentiation of adipocyte stem cells in culture (22,23). Therefore, the intestinal samples of C59-or vehicle-treated mice were stained for p-ERK1/2 by immunohistochemistry (IHC).…”

Section: Resultsmentioning

confidence: 99%

Wnt signaling suppresses MAPK-driven proliferation of intestinal stem cells

Kabiri¹,

Greicius²,

Zaribafzadeh³

et al. 2018

Journal of Clinical Investigation

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Section: Resultsmentioning

confidence: 99%

Wnt signaling suppresses MAPK-driven proliferation of intestinal stem cells

Kabiri¹,

Greicius²,

Zaribafzadeh³

et al. 2018

Journal of Clinical Investigation

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“…This paper further elaborates on the downstream mechanisms involved, showing that FSTL1 promotes expression of the matrix metalloprotein MMP9, which can degrade extracellular matrix, through an effect on Wnt and mitogen-activated protein kinase (MAP kinase) signaling. Additionally, Sundaram et al (2017) find that the miR-198 target DIA PH, which is known to promote migration, is increased in this setting. The physiological relevance of these findings is supported by in vivo data the authors provide showing that knockdown of FSTL1 and DIA PH collaboratively block pulmonary metastases in a tail vein injection model and by clinical data showing that HNS CC patients whose tumors express high levels of both factors have a very poor prognosis (Sundaram et al, 2017).…”

mentioning

confidence: 72%

“…Although typically diagnosed as a local condition, most patients ultimately succumb as a result of metastasis, and therefore a detailed understanding of the mechanisms involved may yield important therapeutic opportunities. EGFR has long been considered an important oncogenic driver in HNS CC, and the work by Sundaram et al (2017) demonstrates yet another mechanism by which activation of this receptor contributes to pathogenesis in this disease. Unfortunately, therapeutic targeting of the EGFR pathway has been a relative disappointment to date, despite numerous clinical trials involving both antibodies and small molecules that inhibit EGFR itself (Sharafinski et al, 2010).…”

mentioning

confidence: 99%

A wound-healing program is hijacked to promote cancer metastasis

Ellisen

2017

Journal of Experimental Medicine

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“…Many of these events also operate during cancer progression . A number of promigratory proteins required for keratinocyte migration are also abundantly expressed in epithelial cancers . Here we provide a discourse into the commonalities between wound healing and epithelial cancers, with a focus on invasive and metastatic squamous cell carcinomas (SCCs).…”

Section: Molecular Similarities Between Wound Healing and Cancermentioning

confidence: 99%

“…This creates a feed‐forward loop which locks the switch in its defective position , creating a cellular state resembling a prolonged wound healing phase. In this state, uncontrolled cell migration is highly conducive to metastasis . The effects of this faulty switch may not be limited to epithelial cancers.…”

Section: Noncoding Rnas In Wound Healing and Cancermentioning

confidence: 99%

Cancer: the dark side of wound healing

2018

Self Cite

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Complex multicellular organisms have evolved sophisticated mechanisms to rapidly resolve epithelial injuries. Epithelial integrity is critical to maintaining internal homeostasis. An epithelial breach represents the potential for pathogen ingress and fluid loss, both of which may have severe consequences if not limited. The mammalian wound healing response involves a finely tuned, self‐limiting series of cellular and molecular events orchestrated by the transient activation of specific signalling pathways. Accurate regulation of these events is essential; failure to initiate key steps at the right time delays healing and leads to chronic wounds, while aberrant initiation of wound healing processes may produce cell behaviours that promote cancer progression. In this review, we discuss how wound healing pathways co‐opted in cancer lose their stringent regulation and become compromised in their reversibility. We hypothesize on how the commandeering of wound healing ‘master regulators’ is involved in this process, and also highlight the implications of these findings in the treatment of both chronic wounds and cancer.

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EGF hijacks miR-198/FSTL1 wound-healing switch and steers a two-pronged pathway toward metastasis

Abstract: Exploring the parallels between wound healing and epithelial cancers, Sundaram et al. elucidate the mechanism by which cancer cells hijack the wound healing switch to enhance invasion and metastasis in head and neck squamous cell carcinoma.

Cited by 54 publications

References 34 publications

Wnt signaling suppresses MAPK-driven proliferation of intestinal stem cells

Wnt signaling suppresses MAPK-driven proliferation of intestinal stem cells

A wound-healing program is hijacked to promote cancer metastasis

Cancer: the dark side of wound healing

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