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Zastosuj identyfikator do podlinkowania lub zacytowania tej pozycji: http://hdl.handle.net/20.500.12128/19902
Tytuł: Novel benzenesulfonate scaffolds with a high anticancer activity and G2/M cell cycle arrest
Autor: Malarz, Katarzyna
Mularski, Jacek
Kuczak, Michał
Mrozek-Wilczkiewicz, Anna
Musioł, Robert
Słowa kluczowe: styrylquinazoline; sulfonic derivatives; anticancer activity; cell cycle inhibition; G2/M phase; apoptosis; autophagy
Data wydania: 2021
Źródło: Cancers, 2021, iss. 8, art. no. 1790
Abstrakt: Sulfonates, unlike their derivatives, sulphonamides, have rarely been investigated for their anticancer activity. Unlike the well-known sulphonamides, esters are mainly used as conve-nient intermediates in a synthesis. Here, we present the first in-depth investigation of quinazoline sulfonates. A small series of derivatives were synthesized and tested for their anticancer activity. Based on their structural similarity, these compounds resemble tyrosine kinase inhibitors and the p53 reactivator CP-31398. Their biological activity profile, however, was more related to sulphonamides because there was a strong cell cycle arrest in the G2/M phase. Further investigation revealed a multitargeted mechanism of the action that corresponded to the p53 protein status in the cell. Al-though the compounds expressed a high submicromolar activity against leukemia and colon cancers, pancreatic cancer and glioblastoma were also susceptible. Apoptosis and autophagy were confirmed as the cell death modes that corresponded with the inhibition of metabolic activity and the activation of the p53-dependent and p53-independent pathways. Namely, there was a strong activation of the p62 protein and GADD44. Other proteins such as cdc2 were also expressed at a higher level. More-over, the classical caspase-dependent pathway in leukemia was observed at a lower concentration, which again confirmed a multitargeted mechanism. It can therefore be concluded that the sulfonates of quinazolines can be regarded as promising scaffolds for developing anticancer agents.
URI: http://hdl.handle.net/20.500.12128/19902
DOI: 10.3390/cancers13081790
ISSN: 2072-6694
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