Novel 7-Chloro-4-aminoquinoline-benzimidazole Hybrids as Inhibitors of Cancer Cells Growth: Synthesis, Antiproliferative Activity, in Silico ADME Predictions, and Docking.
Luka KrstulovićMarijana LeventićVesna RastijaKristina StarčevićMaja JiroušIvana JanićMaja KarnašKornelija LasićMiroslav BajićLjubica Glavaš-ObrovacPublished in: Molecules (Basel, Switzerland) (2023)
In this study, new 7-chloro-4-aminoquinoline-benzimidazole compounds were synthesized and characterized by NMR, MS, and elemental analysis. These novel hybrids differ in the type of linker and in the substituent on the benzimidazole moiety. Their antiproliferative activities were evaluated on one non-tumor (MDCK1) and seven selected tumor (CaCo-2, MCF-7, CCRF-CEM, Hut78, THP-1, and Raji) cell lines by MTT test and flow cytometry analysis. The compounds with different types of linkers and an unsubstituted benzimidazole ring, 5d , 8d , and 12d, showed strong cytotoxic activity (the GI 50 ranged from 0.4 to 8 µM) and effectively suppressed the cell cycle progression in the leukemia and lymphoma cells. After 24 h of treatment, compounds 5d and 12d induced the disruption of the mitochondrial membrane potential as well as apoptosis in HuT78 cells. The drug-like properties and bioavailability of the compounds were calculated using the Swiss ADME web tool, and a molecular docking study was performed on tyrosine-protein kinase c-Src (PDB: 3G6H). Compound 12d showed good solubility and permeability and bound to c-Src with an energy of -119.99 kcal/mol, forming hydrogen bonds with Glu310 and Asp404 in the active site and other residues with van der Waals interactions. The results suggest that compound 12d could be a leading compound in the further design of effective antitumor drugs.
Keyphrases
- molecular docking
- molecular dynamics simulations
- cell cycle arrest
- cell cycle
- induced apoptosis
- flow cytometry
- oxidative stress
- cell death
- endoplasmic reticulum stress
- magnetic resonance
- cell proliferation
- protein kinase
- acute myeloid leukemia
- tyrosine kinase
- multiple sclerosis
- pi k akt
- mass spectrometry
- bone marrow
- drug induced
- ms ms
- signaling pathway
- diabetic rats
- electronic health record