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Thymidylate synthase dimer disrupters induce DNA damage, halt cell growth, overcome drug resistance in colorectal cancer

Project
Thymidylate synthase (TS) is an important target for cancer chemotherapy. Cells selected for high TS protein activity have low sensitivity to TS-targeting chemotherapeutic agents (5-FU and pemetrexed) and show cross- resistance to other chemotherapeutics (e.g., oxalilplatin). This causes failure of therapy in 30% of patients. To prevent/delay treatment-induced resistance, novel therapeutic strategies are required. In response to this need, we propose a new paradigm in TS inhibition consisting in small molecules, such as E7, that target the enzyme dimer interface and favor dissociation of the catalytically active dimer to the inactive monomers (Ddis). The Ddis are active in vivo against pancreatic cancer models.
  • Overview
  • Skills
  • Research Outputs

Overview

Contributor

COSTI Maria Paola   Scientific Manager  

Representatives

NOTARSANTO Maria Cristina   Administrative  

Leading department

Department of Life Sciences   Principale  

Term type

BANDI FONDAZIONE AIRC

Financier

Fondazione AIRC per la Ricerca sul Cancro ETS
Funding Organization

Partner

Università degli Studi di MODENA e REGGIO EMILIA

Total Contribution (assigned) University (EUR)

140,000€

Date/time interval

January 1, 2024 - December 31, 2024

Project duration

12 months

Skills

Concepts (3)


PE5_18 - Medicinal chemistry - (2022)

Goal 3: Good health and well-being

Settore CHIM/08 - Chimica Farmaceutica

Research Outputs

Research outputs (3)

Integrating MS proteomics in the Medicinal Chemistry pipeline as powerful tool to overcome drug resistance issues in colorectal cancer 
2024
Abstract
Optimization of chemical-biological tools for characterizing the activity of dissociative inhibitor of human thymidylate synthase 
2024
Abstract
Precision medicine through proteomics studies in drug resistant colorectal cancer 
2024
Abstract
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