Exploring Novel Coumarin-Tethered Bis-Triazoles: Apoptosis Induction in Human Pancreatic Cancer Cells, Antimicrobial Effects, and Molecular Modelling Investigations.

探索新型香豆素连接的双三唑:诱导人胰腺癌细胞凋亡、抗菌作用及分子建模研究

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作者:Dhawan Sanjeev, Singh Ashona, Manhas Neha, Seboletswe Pule, Khubone Lungisani, Kumar Gobind, Jonnalagadda Sreekantha B, Raza Asif, Sharma Arun K, Singh Parvesh
In the present study, we identified that two representative compounds (7 c and 9 f) of our newly synthesized coumarin-tagged bis-triazoles induced apoptosis in human pancreatic cells (PANC-1) by caspase 3/7mediated pathway. Both 7 c and 9 f (IC(50)=7.15±1.19 and 6.09±0.79†μM, respectively) were found to be ~100 times superior against PANC-1 as compared to the standard drug Gemcitabine (IC(50)=>500†μM), without showing any toxicity to the normal pancreatic epithelial cells (H6C7). Molecular docking studies further endorsed them as potential pancreatic cancer therapeutics due to their strong hydrogen bonding interactions with the epidermal growth factor receptor (EGFR) enzyme, which is overexpressed in cancerous cells including pancreatic cancer. Additionally, these compounds also showed moderate inhibitory activity against a panel of microbial strains. Overall, our findings reveal that the coumarin hybrids 7 c and 9 f are viable chemotypes to be adopted as templates for the development of new anticancer drugs, particularly against pancreatic cancer.

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