International Journal of Molecular Sciences (Dec 2020)

Pharmacological Inhibition of mTORC2 Reduces Migration and Metastasis in Melanoma

  • Jessica Guenzle,
  • Harue Akasaka,
  • Katharina Joechle,
  • Wilfried Reichardt,
  • Aina Venkatasamy,
  • Jens Hoeppner,
  • Claus Hellerbrand,
  • Stefan Fichtner-Feigl,
  • Sven A. Lang

DOI
https://doi.org/10.3390/ijms22010030
Journal volume & issue
Vol. 22, no. 1
p. 30

Abstract

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Despite recent advances in therapy, liver metastasis from melanoma is still associated with poor prognosis. Although targeting the mTOR signaling pathway exerts potent anti-tumor activity, little is known about specific mTORC2 inhibition regarding liver metastasis. Using the novel mTORC2 specific inhibitor JR-AB2-011, we show significantly reduced migration and invasion capacity by impaired activation of MMP2 in melanoma cells. In addition, blockade of mTORC2 induces cell death by non-apoptotic pathways and reduces tumor cell proliferation rate dose-dependently. Furthermore, a significant reduction of liver metastasis was detected in a syngeneic murine metastasis model upon therapy with JR-AB2-011 as determined by in vivo imaging and necropsy. Hence, our study for the first time highlights the impact of the pharmacological blockade of mTORC2 as a potent novel anti-cancer approach for liver metastasis from melanoma.

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