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. 2018 Jan:42:1-10.
doi: 10.1016/j.cellsig.2017.10.002. Epub 2017 Oct 6.

KiSS1 gene as a novel mediator of TGFβ-mediated cell invasion in triple negative breast cancer

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KiSS1 gene as a novel mediator of TGFβ-mediated cell invasion in triple negative breast cancer

Jun Tian et al. Cell Signal. 2018 Jan.

Abstract

The invasive and metastatic phenotypes of breast cancer correlate with high recurrence rates and poor survival outcomes. Transforming growth factor-β (TGFβ) promotes tumor progression and metastasis in aggressive breast cancer. Here, we identified the kisspeptin KiSS1 as a downstream target of canonical TGFβ/Smad2 pathway in triple negative breast cancer cells. We also found KiSS1 expression to be required for TGFβ-induced cancer cell invasion. Indeed, knockdown expression of KiSS1 blocked TGFβ-mediated cancer cell invasion as well as metalloproteinase (MMP9) expression and activity. Interestingly, Kisspeptin-10 (KP-10), the smallest active form of kisspeptin also stimulates cancer cell invasive behavior through activation of MAPK/Erk pathway. We described a positive feedback loop between KiSS1 and p21 downstream of TGFβ, further contributing to TGFβ-induced cancer cell invasion. Lastly, we explored both the clinical utility of KiSS1 as a lymph node involvement predictive tool and its potential as a therapeutic target. We found KiSS1 high expression to correlate with lymph node positive status. Furthermore, blocking KiSS1 using a specific small peptide antagonist (p234) impaired TGFβ-mediated cell invasion and MMP9 induction. Together, our results define an essential role of KiSS1 in regulating TGFβ pro-invasive effects and define KiSS1 as a therapeutic new target for triple negative breast cancer.

Keywords: Cancer cell invasion; KiSS1; Lymph node positive; MMP9; TGFβ; Triple negative breast cancer; p234 kisspeptin antagonist.

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