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A novel calix[4]pyrrole derivative as a potential anticancer agent that forms genotoxic adducts with DNA

Academic Article
Publication Date:
2018
abstract:
meso-(p-acetamidophenyl)-calix[4]pyrrole 3 was found to exhibit remarkable cytotoxicity towards A549 cancer cells. A comparative study including the isomer of 3 meso-(m-acetamidophenyl)-calix[4]pyrrole 5, as well as molecules containing ‘fragments’ of these structures, demonstrated that both the calix[4]pyrrole and the acetamidophenyl units are essential for high cytotoxicity. Although calix[4]pyrroles and other anion-complexing ionophores have recently been reported to induce apoptosis by perturbing cellular chloride concentrations, in our study an alternative mechanism has emerged, as proven by the isolation of covalent DNA adducts revealed by the 32P postlabelling technique. Preliminary pharmacokinetic studies indicate that 3 is able to cross the Blood-Brain-Barrier, therefore being a potential drug that could kill primary and brain metastatic cancer cells simultaneously.
Iris type:
14.a.1 Articolo su rivista
Keywords:
Multidisciplinary, HOST-GUEST CHEMISTRY, BIS-CARBOXYLATES, ANION, BINDING, APOPTOSIS, RECEPTOR, CELLS, INHIBITION, POLYAMIDE, TOXICIT
List of contributors:
Geretto, Marta; Ponassi, Marco; Casale, Martina; Pulliero, Alessandra; Cafeo, Grazia; Malagreca, Ferdinando; Profumo, Aldo; Balza, Enrica; Bersimbaev, Rakhmetkazhi; Kohnke, Franz Heinrich; Rosano, Camillo; Izzotti, Alberto
Authors of the University:
CAFEO Grazia
Handle:
https://iris.unime.it/handle/11570/3128994
Full Text:
https://iris.unime.it//retrieve/handle/11570/3128994/209116/s41598-018-29314-9.pdf
Published in:
SCIENTIFIC REPORTS
Journal
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URL

https://www.nature.com/articles/s41598-018-29314-9
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