CONICET | Buscador de Institutos y Recursos Humanos

AbstractBackgroundHeat shock protein 90 (Hsp90) is an encouraging anticancer target for the development of clinically significant molecules. Schiff bases play a crucial role in anticancer research because of their ease of synthesis and excellent antiproliferative effect against multiple cancer cell lines. Therefore, we started our research work with the discovery of resorcinol/4-chloro resorcinol derived Schiff bases as Hsp90 inhibitors, which resulted in the discovery of a viable anticancer lead molecule.ObjectiveThe objective of the study is to discover more promising lead molecules using our previously established drug discovery program, where in the rational drug design is achieved by molecular docking studies.MethodThe docking studies were carried out by using Surflex Geom X programme of Sybyl X-1.2 version software. The molecules with good docking score were synthesized and their structures were confirmed by IR, 1H NMR and mass spectral analysis. Subsequently, the molecules were evaluated for their potential to attenuate Hsp90 ATPase activity by Malachite green assay. The anticancer effect of the molecules was examined on PC3 prostate cancer cell lines by utilizing 3-(4,5-dimethythiazol-2-yl)-2,5-diphenyl tetrazolium bromide (MTT) assay methodology.ResultsSchiff base 11, 12, 20, 23 and 27 exhibiting IC50 value below 1 μM and 15 μM, in malachite green assay and MTT assay, respectively, emerged as viable lead molecules for future optimization.ConclusionThe research work will pave the way for the rational development of cost effective Schiff bases as Hsp90 inhibitors as the method employed for the synthesis of the molecules is simple, economic and facile.

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