Design, Synthesis, and Biological Evaluation of a Novel VEGFR-2 Inhibitor Based on a 1,2,5-Oxadiazole-2-Oxide Scaffold with MAPK Signaling Pathway Inhibition.
Mater H MahnashiFardous F El-SendunyMohammed Abdulrahman AlshahraniMahrous A Abou-SalimPublished in: Pharmaceuticals (Basel, Switzerland) (2022)
Over the past few decades, the development of broad-spectrum anticancer agents with anti-angiogenic activity has witnessed considerable progress. In this study, a new series of pyrazolo[3,4-d]pyrimidines based on a phenylfuroxan scaffold were designed, synthesized, and evaluated, in terms of their anticancer activities. NCI-60 cell one-dose screening revealed that compounds 12a - c and 14a had the best MGI%, among the tested compounds. The target fluorinated compound 12b , as the most active one, showed better anticancer activity compared to the reference drug sorafenib, with IC 50 values of 11.5, 11.6, and 13 µM against the HepG-2, A2780CP, and MDA-MB-231 cell lines, respectively. Furthermore, compound 12b (IC 50 = 0.092 µM) had VEGFR-2-inhibitory activity comparable to that of the standard inhibitor sorafenib (IC 50 = 0.049 µM). Furthermore, the ability of compound 12b in modulating MAPK signaling pathways was investigated. It was found to decrease the level of total ERK and its phosphorylated form, as well as leading to the down-regulation of metalloproteinase MMP-9 and the over-expression of p21 and p27, thus leading to subG1 cell-cycle arrest and, thus, the induction of apoptosis. Additionally, compound 12b decreased the rate of wound healing in the absence of serum, in comparison to DMSO-treated cells, providing a significant impact on metastasis inhibition. The quantitative RT-PCR results for E-cadherin and N-cadherin showed lower expression of the neuronal N-cadherin and increased expression of epithelial E-cadherin , indicating the ability of 12b to suppress metastasis. Furthermore, 12b -treated HepG2 cells expressed a low level of anti-apoptotic BCL-2 and over-expressed proapoptotic Bax genes, respectively. Using the DAF-FM DA fluorescence probe, compound 12b produced NO intracellularly as efficiently as the reference drug JS-K. In silico molecular docking studies showed a structural similarity through an overlay of 12b with sorafenib. Interestingly, the drug-likeness properties of compound 12b met the expectations of Pfizer's rule for the design of new drug candidates. Therefore, this study presents a novel anticancer lead compound that is worthy of further investigation and activity improvement.
Keyphrases
- cell migration
- cell cycle arrest
- pi k akt
- signaling pathway
- induced apoptosis
- cell death
- molecular docking
- poor prognosis
- cell proliferation
- epithelial mesenchymal transition
- oxidative stress
- single cell
- stem cells
- binding protein
- genome wide
- dna methylation
- long non coding rna
- molecular dynamics simulations
- bone marrow
- endothelial cells
- gene expression
- wound healing
- mesenchymal stem cells
- drug induced
- subarachnoid hemorrhage
- mass spectrometry
- living cells
- fluorescent probe