Author: Masih, Anup; Agnihotri, Amol K.; Srivastava, Jitendra K.; Pandey, Nidhi; Bhat, Hans R.; Singh, Udaya P.
Title: Discovery of novel pyrazole derivatives as a potent antiâ€inflammatory agent in RAW264.7 cells via inhibition of NFâ€Ä¸B for possible benefit against SARSâ€CoVâ€2 Cord-id: 7npzx1jd Document date: 2020_10_23
ID: 7npzx1jd
Snippet: Due to unavailability of a specific drug/vaccine to attenuate severe acute respiratory syndrome coronavirus 2, the current strategy to combat the infection has been largely dependent upon the use of antiâ€inflammatory drugs to control cytokines storm responsible for respiratory depression. Thus, in this study, we discovered novel pyrazole analogs as a potent nuclear factor kappa B (NFâ€Ä¸B) inhibitor. The compounds were assessed for NFâ€Ä¸B transcriptional inhibitory activity in RAW264.7 cell
Document: Due to unavailability of a specific drug/vaccine to attenuate severe acute respiratory syndrome coronavirus 2, the current strategy to combat the infection has been largely dependent upon the use of antiâ€inflammatory drugs to control cytokines storm responsible for respiratory depression. Thus, in this study, we discovered novel pyrazole analogs as a potent nuclear factor kappa B (NFâ€Ä¸B) inhibitor. The compounds were assessed for NFâ€Ä¸B transcriptional inhibitory activity in RAW264.7 cells after stimulation with lipopolysaccharides (LPS), revealing Compound 6c as the most potent analog among the tested series. The effect of Compound 6c was further investigated on the levels of interleukinâ€1β, tumor necrosis factorâ€Î±, and interleukinâ€6 in LPSâ€stimulated RAW267.4 cells by enzyme immunoassay, where it causes a significant reduction in the level of these cytokines. In Western blot analysis, Compound 6c also causes the inhibition of inhibitor kappa Bâ€Î± and NFâ€ÎºB. It was found to be snugly fitted into the inner grove of the active site of NFâ€Ä¸B by forming Hâ€bonds and a nonbonded interaction with Asn28 in a docking analysis.
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