Experimental Hematology & Oncology (Aug 2024)

Epigenetic alterations of TP53INP1 by EHMT2 regulate the cell cycle in gastric cancer

  • Tae Young Ryu,
  • In Hwan Tae,
  • Tae-Su Han,
  • Jinkwon Lee,
  • Kwangho Kim,
  • Yunsang Kang,
  • Solbi Kim,
  • Hyo Jin Lee,
  • Cho-Rok Jung,
  • Jung Hwa Lim,
  • Dae-Soo Kim,
  • Mi-Young Son,
  • Hyun-Soo Cho

DOI
https://doi.org/10.1186/s40164-024-00554-y
Journal volume & issue
Vol. 13, no. 1
pp. 1 – 6

Abstract

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Abstract Background Gastric cancer (GC) is a type of cancer with high incidence and mortality rates. Although various chemical interventions are being developed to treat gastric cancer, there is a constant demand for research into new GC treatment targets and modes of action (MOAs) because of the low effectiveness and side effects of current treatments. Methods Using the TCGA data portal, we identified EHMT2 overexpression in GC samples. Using RNA-seq and EHMT2-specific siRNA, we investigated the role of EHMT2 in GC cell proliferation and validated its function with two EHMT2-specific inhibitors. Through the application of 3D spheroid culture, patient-derived gastric cancer organoids (PDOs), and an in vivo model, we confirmed the role of EHMT2 in GC cell proliferation. Results In this study, we found that EHMT2, a histone 3 lysine 9 (H3K9) methyltransferase, is significantly overexpressed in GC patients compared with healthy individuals. Knockdown of EHMT2 with siRNA induced G1 cell cycle arrest and attenuated GC cell proliferation. Furthermore, we confirmed that TP53INP1 induction by EHMT2 knockdown induced cell cycle arrest and inhibited GC cell proliferation. Moreover, specific EHMT2 inhibitors, BIX01294 and UNC0638, induced cell cycle arrest in GC cell lines through TP53INP1 upregulation. The efficacy of EHMT2 inhibition was further confirmed in a 3D spheroid culture system, PDOs, and a xenograft model. Conclusions Our findings suggest that EHMT2 is an attractive therapeutic target for GC treatment.

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