A series of new phosphorylated derivatives of didanosine were designed, synthesized and evaluated their anticancer effects on human breast cancer cells. Their binding affinities were evaluated against aromatase enzyme and the molecular docking studies demonstrated that 9a , 9h and 9i exhibited high binding interactions than the parent molecule (ddI) and other derivatives; evaluated the aromatase enzyme inhibition. The cell viability, cell proliferation, lactate dehydrogenase showed potential anti-proliferative in dose dependent manner, these results were well correlated with hoesch stain and DNA fragmentation on MDA-MB-231 breast cancer cell lines. Cytotoxicity results disclosed that tryptophan amino acid ester substituted derivative 9i showed potential cell death against MDA-MB-231 cancer cell lines. Furthermore, compound 9i has great potential significance for further investigations ( in vivo ).
Keyphrases
- cell cycle
- molecular docking
- breast cancer cells
- cell proliferation
- cell death
- cell cycle arrest
- molecular dynamics simulations
- amino acid
- endothelial cells
- human health
- papillary thyroid
- case control
- binding protein
- single molecule
- cell free
- induced pluripotent stem cells
- circulating tumor
- young adults
- climate change
- childhood cancer
- pluripotent stem cells