AI Article Synopsis

  • DNA intercalating agents are effective in treating tumors, with a focus on improving indeno[1,2-c]cinnoline-11-one derivatives for better efficacy.
  • New compounds were created to enhance intercalating properties, especially with G-quadruplex sequences, showing promising results in fluorescence melting and displacement tests.
  • Notable compounds demonstrated strong anti-tumor activity, with one showing significant proliferation inhibition in cancer cell lines, suggesting their potential for further development in cancer therapy.

Article Abstract

DNA intercalating agents are a consolidated therapeutic option in the treatment of tumor diseases. Starting from previous findings in the antiproliferative efficacy of a series of indeno[1,2-c]cinnoline-11-one derivatives, we performed a suitable decoration of this scaffold by means of a simple and straightforward chemistry, aiming to a) enlarge the planar core to a pentacyclic benzo[h]indeno[1,2-c]cinnoline-13-one and b) introduce a basic head tethered through a simple polymethylene chain. In fluorescence melting and fluorescence intercalator displacement assays, these new compounds displayed fair to very good intercalating properties on different nucleic acid strands, with preference for G-quadruplex sequences. Inhibition of human topoisomerase IIα and antiproliferative assays on HeLa and MCF7 tumor cell lines outlined a multitarget antiproliferative profile for tetracyclic 6 and pentacyclic derivative 20, both bearing a N,N-dimethylamine as the protonatable moiety. Particularly, compound 6 displayed a very potent inhibition of tumor cell proliferation, while 20 returned the highest thermal stabilization in melting experiments. In summary, these results outlined a potential of such highly planar scaffolds for nucleic acid binding and antiproliferative effects.

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Source
http://dx.doi.org/10.1016/j.bmc.2017.03.019DOI Listing

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