Animal Cells and Systems (Dec 2024)

MiR-29 and MiR-140 regulate TRAIL-induced drug tolerance in lung cancer

  • Suyeon Kim,
  • Ki Wook Lee,
  • Yongjin Yoo,
  • Sang Hee Park,
  • Ji Won Lee,
  • Suhyun Jeon,
  • Shaginyan Illia,
  • Pooja Joshi,
  • Hyun Woo Park,
  • Han-En Lo,
  • Jimin Seo,
  • Yeonwoo Kim,
  • Min Chang,
  • Tae Jin Lee,
  • Jong Bae Seo,
  • Sung-Hak Kim,
  • Carlo M. Croce,
  • Inki Kim,
  • Sung-Suk Suh,
  • Young-Jun Jeon

DOI
https://doi.org/10.1080/19768354.2024.2345644
Journal volume & issue
Vol. 28, no. 1
pp. 184 – 197

Abstract

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ABSTRACTTumor necrosis factor-related apoptosis-inducing ligand (TRAIL) has chemotherapeutic potential as a regulator of an extrinsic apoptotic ligand, but its effect as a drug is limited by innate and acquired resistance. Recent findings suggest that an intermediate drug tolerance could mediate acquired resistance, which has made the main obstacle for limited utility of TRAIL as an anti-cancer therapeutics. We propose miRNA-dependent epigenetic modification drives the drug tolerant state in TRAIL-induced drug tolerant (TDT). Transcriptomic analysis revealed miR-29 target gene activation in TDT cells, showing oncogenic signature in lung cancer. Also, the restored TRAIL-sensitivity was associated with miR-29ac and 140-5p expressions, which is known as tumor suppressor by suppressing oncogenic protein RSK2 (p90 ribosomal S6 kinase), further confirmed in patient samples. Moreover, we extended this finding into 119 lung cancer cell lines from public data set, suggesting a significant correlation between TRAIL-sensitivity and RSK2 mRNA expression. Finally, we found that increased RSK2 mRNA is responsible for NF-κB activation, which we previously showed as a key determinant in both innate and acquired TRAIL-resistance. Our findings support further investigation of miR-29ac and -140-5p inhibition to maintain TRAIL-sensitivity and improve the durability of response to TRAIL in lung cancer.

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