In this work, we present studies on relatively new and still not well-explored potential anticancer targets which are shelterin proteins, in particular the TRF1 protein can be blocked by in silico designed "peptidomimetic" molecules. TRF1 interacts directly with the TIN2 protein, and this protein-protein interaction is crucial for the proper functioning of telomere, which could be blocked by our novel modified peptide molecules. Our chemotherapeutic approach is based on assumption that modulation of TRF1-TIN2 interaction may be more harmful for cancer cells as cancer telomeres are more fragile than in normal cells. We have shown in vitro within SPR experiments that our modified peptide PEP1 molecule interacts with TRF1, presumably at the site originally occupied by the TIN2 protein. Disturbance of the shelterin complex by studied molecule may not in short term lead to cytotoxic effects, however blocking TRF1-TIN2 resulted in cellular senescence in cellular breast cancer lines used as a cancer model. Thus, our compounds appeared useful as starting model compounds for precise blockage of TRF proteins.
Autorzy
- dr Wioletta Brankiewicz link otwiera się w nowej karcie ,
- Umesh Kalathiya link otwiera się w nowej karcie ,
- Monikaben Padariya,
- Katarzyna Wegrzyn,
- Maciej Prusinowski,
- Joanna Żebrowska,
- Agnieszka Zylicz-Stachula,
- prof. dr hab. Piotr Skowron,
- Marek Drab,
- Mariusz Szajewski,
- Maciej Ciesielski,
- Małgorzata Gawrońska,
- Anoop Kallingal link otwiera się w nowej karcie ,
- dr Mariusz Makowski,
- prof. dr hab. inż. Maciej Bagiński link otwiera się w nowej karcie
Informacje dodatkowe
- DOI
- Cyfrowy identyfikator dokumentu elektronicznego link otwiera się w nowej karcie 10.1002/chem.202300970
- Kategoria
- Publikacja w czasopiśmie
- Typ
- artykuły w czasopismach
- Język
- angielski
- Rok wydania
- 2023
