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. 2018 Apr 25:150:817-828.
doi: 10.1016/j.ejmech.2018.03.039. Epub 2018 Mar 16.

Arylureas derived from colchicine: Enhancement of colchicine oncogene downregulation activity

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Arylureas derived from colchicine: Enhancement of colchicine oncogene downregulation activity

Víctor Blasco et al. Eur J Med Chem. .

Abstract

Our efforts to get therapeutically useful colchicine derivatives for the treatment of cancer have led us to synthetize and biologically evaluate twenty-seven N,N'-disubstituted ureas containing a colchicine moiety and an aryl fragment. The cytotoxicity of the compounds, their ability to inhibit the expression of oncogenes related to telomerase activation and to the VEGF/VEGFR-2 autocrine process, such as c-MYC, hTERT and VEGF and their capability to downregulate c-MYC and VEGFR-2 proteins and the secretion of VEGF have been measured. In these biological evaluations, we have found that the change of the acetyl group in colchicines for an N-arylurea unit causes a great improvement in anticancer properties. The most promising derivatives were compounds 6 (o-Cl) and 14 (o,o-di-F) as they were able to downregulate all the tested targets at a concentration below their IC50 values. Thus, the arylurea unit enhances the potential of colchicine as an anticancer agent.

Keywords: Colchicine; Cytotoxicity; Oncogenes downregulation; Urea derivatives.

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