Cancers (Jan 2021)

The lncRNA H19-Derived MicroRNA-675 Promotes Liver Necroptosis by Targeting FADD

  • Rona Harari-Steinfeld,
  • Maytal Gefen,
  • Alina Simerzin,
  • Elina Zorde-Khvalevsky,
  • Mila Rivkin,
  • Ezra Ella,
  • Tomer Friehmann,
  • Mordechay Gerlic,
  • Jessica Zucman-Rossi,
  • Stefano Caruso,
  • Mélissa Leveille,
  • Jennifer L. Estall,
  • Daniel S. Goldenberg,
  • Hilla Giladi,
  • Eithan Galun,
  • Zohar Bromberg

DOI
https://doi.org/10.3390/cancers13030411
Journal volume & issue
Vol. 13, no. 3
p. 411

Abstract

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The H19-derived microRNA-675 (miR-675) has been implicated as both tumor promoter and tumor suppressor and also plays a role in liver inflammation. We found that miR-675 promotes cell death in human hepatocellular carcinoma (HCC) cell lines. We show that Fas-associated protein with death domain (FADD), a mediator of apoptotic cell death signaling, is downregulated by miR-675 and a negative correlation exists between miR-675 and FADD expression in mouse models of HCC (p = 0.014) as well as in human samples (p = 0.017). We demonstrate in a mouse model of liver inflammation that overexpression of miR-675 promotes necroptosis, which can be inhibited by the necroptosis-specific inhibitor Nec-1/Nec-1s. miR-675 induces the level of both p-MLKL (Mixed Lineage Kinase Domain-Like Pseudokinase) and RIP3 (receptor-interacting protein 3), which are key signaling molecules in necroptosis, and enhances MLKL binding to RIP3. miR-675 also inhibits the levels of cleaved caspases 8 and 3, suggesting that miR-675 induces a shift from apoptosis to a necroptotic cellular pathway. In conclusion, downregulation of FADD by miR-675 promotes liver necroptosis in response to inflammatory signals. We propose that this regulation cascade can stimulate and enhance the inflammatory response in the liver, making miR-675 an important regulator in liver inflammation and potentially also in HCC.

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