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Abstract
Inspired by the well-documented tumor protecting ability of paullones, recently, we synthesized novel paullone-like scaffolds, indole-fused benzo-oxazepines (IFBOs), and screened them against hepatocellular carcinoma (HCC) specific Hep-G2 cells. Three of the synthesized compounds significantly attenuated the progression of HCC in vitro. By computational studies, we further discovered that IFBOs exhibited a stable binding complex with the IL-6 receptor. In this context, we investigated in vivo study using the nitrosodiethyl amine (NDEA)-induced HCC model, which strengthened our previous findings by showing the blockade of the IL-6 mediated JAK2/STAT3 oncogenic signaling pathway. Treatment with IFBOs showed remarkable attenuation of cellular proliferation, as evidenced through a decrease in the number of nodules, restoration of body weight, oxidative stress parameters, liver marker enzymes and histological architecture. Interestingly, using a metabolomic approach we further discovered that IFBOs can restore the perturbed metabolic profile associated with the HCC condition to normalcy. Particularly, the efficacy of compound 6a for an anti-HCC response was significantly better than the marketed chemotherapeutic drug, 5-fluorouracil. Altogether, these remarkable findings open up possibilities of developing IFBOs as novel future candidate molecules for plausible alternatives for HCC treatment.
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Details
1 Babasaheb Bhimrao Ambedkar University, Vidya Vihar, Raibareli Road, Department of Pharmaceutical Sciences, Lucknow, India (GRID:grid.440550.0)
2 Shri Ramswaroop Memorial University, Faculty of Mathematical and Statistical Sciences, Lucknow, India (GRID:grid.459970.6) (ISNI:0000 0004 1781 2531)
3 SGPGIMS Campus, Raebareli Road, Centre of Biomedical Research, Lucknow, India (GRID:grid.263138.d) (ISNI:0000 0000 9346 7267)
4 Babasaheb Bhimrao Ambedkar University, Vidya Vihar, Raibareli Road, Department of Biotechnology, Lucknow, India (GRID:grid.440550.0)