Project title: Reversing Epitranscriptomic Alterations for CHemosensitization of Pancreatic Cancer (REACH)

Project No.: 

Period: 1 April 2025 – 31 March 2028

Project costs: 300 000,00 EUR

Principal Investigator BMC: Dr.biol. Vita Rovīte

Cooperation partner: coordinator – The Ramón y Cajal Institute for Health Research (IRYCIS), Biomedical Research Center, Slovak Academy of Sciences, Cancer Research Institute (BMC SAS), Fraunhofer Institute for Biomedical Engineering IBMT (IBMT), Maimonides Biomedical Research Institute of Córdoba (IMIBIC)

Project summary:

Rationale. While pancreatic ductal adenocarcinoma (PDAC) is not a common cancer, it is one of the most lethal and hard-to-treat tumors with a 5-year survival rate of 10-11%. Apart from the addition of FOLFIRINOX and nab-Paclitaxel, the standard of care for PDAC has not substantially changed over the past 30 years, and overall survival (OS) continues to hover around 6-12 months. The latter is primarily due to the inherent chemo/radio-resistance of this tumor and the presence of highly tumorigenic and chemoresistant stem-like cells, known as cancer stem cells (CSCs), with unique transcriptional features under epigenetic and epitranscriptomic regulation. However, PDAC epitranscriptomics and their translational potential remain vastly unexplored.

Hypothesis. Based on emerging evidence, we hypothesize that the epitranscriptomic landscape [regulated by N⁶-Methyladenosine (m⁶A) marks on mRNAs] of PDAC tumor cells and CSCs modulates key transcripts that drive PDAC chemoresistance, and targeting m⁶A with inhibitors of the “writer”, “eraser” and “reader” enzymes of these m⁶A marks will render PDAC cells and CSCs highly sensitive to standard chemotherapeutics.

Aims. The Main Aim of REACH is to make epitranscriptomic-based therapies in PDAC a clinical reality, by altering the epitranscriptomic nature of PDAC tumor cells and CSCs with targeted therapies to modulate m⁶A marks, the main epitranscriptomic modification that shapes the PDAC transcriptional landscape. Specifically, REACH will use functionalized tumor-tropic nanoparticles (NPs) to both penetrate the impermeable PDAC stroma and home to PDAC cells to deliver epitranscriptomic modulators of m⁶A “writers”, “erasers” and/or “readers. The ability of our approach to sensitize PDAC tumors to chemotherapy will be tested in advanced preclinical animal models.

Expected results and potential impact. As the social, economic and healthcare impact of PDAC are significant, novel ideas are required to make this tumor more sensitive to currently available therapies. If successful, REACH will make PDAC chemo-sensitive, providing an effective therapeutic solution to a currently unsolvable health care problem, with a true possibility of extending the overall survival of PDAC patients, even of those with advanced disease, who currently rely only on palliative treatment options.

Information published 01.04.2025.