| Literature DB >> 33614708 |
Raphael Enoque Ferraz de Paiva1, Eduardo Guimarães Vieira1, Daniel Rodrigues da Silva1, Camila Anchau Wegermann1, Ana Maria Costa Ferreira1.
Abstract
In this review we compare and discuss results of compounds already reported as anticancer agents based on isatin-derivatives, metalated as well as non-metallated. Isatin compounds can be obtained from plants, marine animals, and is also found in human fluids as a metabolite of amino acids. Its derivatives include imines, hydrazones, thiosemicarbazones, among others, already focused on numerous anticancer studies. Some of them have entered in pre-clinical and clinical tests as antiangiogenic compounds or inhibitors of crucial proteins. As free ligands or coordinated to metal ions, such isatin derivatives showed promising antiproliferative properties against different cancer cells, targeting different biomolecules or organelles. Binding to metal ions usually improves its biological properties, indicating a modulation by the metal and by the ligand in a synergistic process. They also reveal diverse mechanisms of action, being able of binding DNA, generating reactive species that cause oxidative damage, and inhibiting selected proteins. Strategies used to improve the efficiency and selectivity of these compounds comprise structural modification of the ligands, metalation with different ions, syntheses of mononuclear and dinuclear species, and use of inserted or anchored compounds in selected drug delivery systems.Entities:
Keywords: anticancer activity; improvement strategies; isatin; mechanisms of action; metallodrugs; oxindoles
Year: 2021 PMID: 33614708 PMCID: PMC7889591 DOI: 10.3389/fmolb.2020.627272
Source DB: PubMed Journal: Front Mol Biosci ISSN: 2296-889X