细胞毒性
微管蛋白
化学
达皮
膜联蛋白
体外
细胞凋亡
苯并咪唑
微管
生物化学
细胞生物学
生物
有机化学
作者
Kritika Laxmikeshav,Ziaur Rahman,Ashutosh Mahale,Durgesh Gurukkala Valapil,Pravesh Sharma,Joel George,Regur Phanindranath,Manoj P. Dandekar,Onkar P. Kulkarni,Narayana Nagesh,Nagula Shankaraiah
标识
DOI:10.1016/j.bmcl.2023.129494
摘要
A new class of benzimidazole derivatives as tubulin polymerization inhibitors has been designed and synthesized in this study. The in vitro anticancer profile of the developed molecules was reconnoitred on selected human cancer cells. The highest cytotoxicity was illustrated by compounds 7n and 7u with IC50 values ranging from 2.55 to 17.89 µM with specificity toward SK-Mel-28 cells. They displayed 5-fold less cytotoxicity towards normal rat kidney epithelial NRK52E cells, which implies that they are not harmful to normal, healthy cells. The cellular staining procedures like AO/EB, DCFDA, and DAPI were applied to comprehend the inherent mechanism of apoptosis which displayed nuclear and morphological alterations. The Annexin V binding and JC-1 studies were executed to evaluate the extent of apoptosis and the decline in mitochondrial transmembrane potential in SK-Mel-28 cell lines. Compound 7n dose-dependently arrested the G2/M phase of the cell cycle and the target-based outcomes proposed tubulin polymerization inhibition by 7n (IC50 of 5.05±0.13 μM). Computational studies were also conducted on the tubulin protein (PDB ID: 3E22) to investigate the stabilized binding interactions of compounds 7n and 7u with tubulin, respectively.
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