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Poster Display & Cocktail

33P - LncRNAs as regulators of the PI3K/AKT/mTOR pathway in resistant gastric cancer: A novel strategy to enhance the response to chemotherapy

Date

03 Mar 2025

Session

Poster Display & Cocktail

Presenters

Ismael Riquelme

Citation

Annals of Oncology (2025) 10 (suppl_2): 1-5. 10.1016/esmoop/esmoop104185

Authors

I. Riquelme1, B. Mora1, V. Fritz1, S.R. Piccolo2, P.E. Yanez Weber3, J.C. Roa4, C. Ili5, P. Brebi6

Author affiliations

  • 1 Institute Of Biomedical Sciences, Universidad Autónoma de Chile, 4780000 - Temuco/CL
  • 2 Department Of Biology, Brigham Young University, 84602 - Provo/US
  • 3 Oncology Unit, Department Of Internal Medicine, School Of Medicine, Universidad De La Frontera, James Lind Cancer Center, 4810297 - Temuco/CL
  • 4 Department Of Pathology, Millennium Institute On Immunology And Immunotherapy, School Of Medicine, Pontificia Universidad Católica de Chile, Santiago/CL
  • 5 Laboratory Of Integrative Biology (libi), Centro De Excelencia En Medicina Traslacional (cemt), Scientific And Technological Bioresource Nucleus (bioren), Universidad De La Frontera, Millennium Institute on Immunology and Immunotherapy, 4810296 - Temuco/CL
  • 6 Laboratory Of Integrative Biology (libi), Centro De Excelencia En Medicina Traslacional (cemt), Scientific And Technological Bioresource Nucleus (bioren), Universidad De La Frontera, Millennium Institute on Immunology and Immunotherapy, Temuco/CL

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Abstract 33P

Background

Gastric cancer (GC) is a public health problem worldwide. Many signaling pathways chemical inhibitors have been developed to complement routine chemotherapy, usually based on cisplatin (CDDP) and/or 5-fluorouracil (5-FU). However, both chemical inhibitors and chemotherapeutics have shown resistance features in cancer patients. Therefore, it is pivotal to characterize new molecules that could improve treatment outcomes and offer broader options for patients. Long non-coding RNAs (lncRNAs)- epigenetic regulators that could lead to drug resistance- have recently emerged for this purpose.

Methods

19 treatment-naïve GC tissues (11 responders to CDDP/5-FU, and 8 non-responders to CDDP/5-FU), and 6 GC cell lines: wild-type (WT) AGS and MKN28; CDDP-resistant AGS and MKN28; and 5-FU-resistant AGS and MKN28 cells were sequenced by RNA-seq to determine the differentially expressed protein-coding genes (DEGs) and lncRNAs. Gene ontology, functional enrichment and prediction analyses were performed by several in silico tools.

Results

About 570 DEGs were differentially expressed (280 upregulated, 290 repressed), evidencing enrichment of “translation functions” and “anabolic functions”, implicating the PI3K/AKT/mTOR pathway. Glimma-plots showed that GC cases non-responders to CDDP/5-FU and/or resistant cell lines had a higher expression of AKT1, MTOR, RPS6KB1 genes, and especially PIK3CA gene compared to controls (p<0.005). Conversely, PTEN was repressed in these cases. Moreover, 57 lncRNAs were differentially expressed in non-responder GC tissues and resistant cell lines (34 upregulated, 23 repressed). 3 of the upregulated lncRNAs (AP000350.5, AC0022007.1, and FAM2254) showed a strong interaction with PIK3CA, AKT1, MTOR and RPS6KB1 genes, potentially acting as gene enhancers or competing-endogenous RNAs.

Conclusions

This study suggests that the upregulation of these 3 lncRNAs causes activation of the PI3K/AKT/mTOR pathway, which leads to chemoresistance to CDDP and/or 5-FU. Therefore, the biological or chemical repression of these lncRNAs could reduce this pathway activation, inducing re-sensitization of CDDP/5-FU-resistant GC tumors.

Clinical trial identification

Editorial acknowledgement

Legal entity responsible for the study

Ismael Riquelme.

Funding

DIUAV 03-2022; FONDECYT 11240398.

Disclosure

All authors have declared no conflicts of interest.

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