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Novel hydrazone‐isatin derivatives as potential EGFR inhibitors: Synthesis and in vitro pharmacological profiling

Marwa F. Ahmed, Radwan El‐Haggar, Atiah H. Almalki, Omeima Abdullah, Mahmoud A. El Hassab, Nicolas Masurier, Sherif Hammad

2023Archiv der Pharmazie30 citationsDOIOpen Access PDF

Abstract

Merging isatin and arylhydrazone moieties constitutes an efficient strategy to access new potential anticancer derivatives. Consequently, 14 hydrazone-isatin derivatives were synthesized and evaluated for their antiproliferative activity against the NCI-60 cancer cell line panel. A kinase assay demonstrated that compound VIIIb inhibited the epidermal growth factor receptor (EGFR), which was confirmed by docking studies, molecular dynamics, and binding free energy calculations. Further characterizations showed that this compound possesses drug-likeness properties, showed a significant decrease of the cell population in the G2/M phase and led to a significant increase in early and late apoptosis, comparable to erlotinib. Also, VIIIb increased the expression of caspase-3 and Bax and decreased the expression of Bcl-2, confirming its potential as a new proapoptotic compound.

Topics & Concepts

IsatinHydrazoneErlotinibChemistryApoptosisDocking (animal)In vitroCell cultureEGFR inhibitorsStereochemistryEpidermal growth factor receptorCombinatorial chemistryPharmacologyBiochemistryReceptorBiologyOrganic chemistryMedicineGeneticsNursingCancer therapeutics and mechanismsComputational Drug Discovery MethodsSynthesis and biological activity
Novel hydrazone‐isatin derivatives as potential EGFR inhibitors: Synthesis and in vitro pharmacological profiling | Litcius