Molecular Cancer (Feb 2024)

The therapeutically actionable long non-coding RNA ‘T-RECS’ is essential to cancer cells’ survival in NRAS/MAPK-driven melanoma

  • Valentin Feichtenschlager,
  • Linan Chen,
  • Yixuan James Zheng,
  • Wilson Ho,
  • Martina Sanlorenzo,
  • Igor Vujic,
  • Eleanor Fewings,
  • Albert Lee,
  • Christopher Chen,
  • Ciara Callanan,
  • Kevin Lin,
  • Tiange Qu,
  • Dasha Hohlova,
  • Marin Vujic,
  • Yeonjoo Hwang,
  • Kevin Lai,
  • Stephanie Chen,
  • Thuan Nguyen,
  • Denise P Muñoz,
  • Yoshinori Kohwi,
  • Christian Posch,
  • Adil Daud,
  • Klemens Rappersberger,
  • Terumi Kohwi-Shigematsu,
  • Jean-Philippe Coppé,
  • Susana Ortiz-Urda

DOI
https://doi.org/10.1186/s12943-024-01955-7
Journal volume & issue
Vol. 23, no. 1
pp. 1 – 21

Abstract

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Abstract Finding effective therapeutic targets to treat NRAS-mutated melanoma remains a challenge. Long non-coding RNAs (lncRNAs) recently emerged as essential regulators of tumorigenesis. Using a discovery approach combining experimental models and unbiased computational analysis complemented by validation in patient biospecimens, we identified a nuclear-enriched lncRNA (AC004540.4) that is upregulated in NRAS/MAPK-dependent melanoma, and that we named T-RECS. Considering potential innovative treatment strategies, we designed antisense oligonucleotides (ASOs) to target T-RECS. T-RECS ASOs reduced the growth of melanoma cells and induced apoptotic cell death, while having minimal impact on normal primary melanocytes. Mechanistically, treatment with T-RECS ASOs downregulated the activity of pro-survival kinases and reduced the protein stability of hnRNPA2/B1, a pro-oncogenic regulator of MAPK signaling. Using patient- and cell line- derived tumor xenograft mouse models, we demonstrated that systemic treatment with T-RECS ASOs significantly suppressed the growth of melanoma tumors, with no noticeable toxicity. ASO-mediated T-RECS inhibition represents a promising RNA-targeting approach to improve the outcome of MAPK pathway-activated melanoma.

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