| Literature DB >> 27435006 |
Sinara Mônica Vitalino de Almeida1, Elizabeth Almeida Lafayette2, Willams Leal Silva2, Vanessa de Lima Serafim3, Thais Meira Menezes4, Jorge Luiz Neves4, Ana Lucia Tasca Gois Ruiz5, João Ernesto de Carvalho5, Ricardo Olímpio de Moura6, Eduardo Isidoro Carneiro Beltrão7, Luiz Bezerra de Carvalho Júnior7, Maria do Carmo Alves de Lima2.
Abstract
Two new spiro-acridines were synthesized by introducing cyano-N-acylhydrazone between the acridine and phenyl rings followed by spontaneous cyclization. The final compounds (E)-1'-(benzylideneamino)-5'-oxo-1',5'-dihydro-10H-spiro[acridine-9,2'-pyrrole]-4'-carbonitrile (AMTAC-01) and (E)-1'-((4-methoxybenzylidene)amino)-5'-oxo-1',5'-dihydro-10H-spiro[acridine-9,2'-pyrrole]-4'-carbonitrile (AMTAC-02) were evaluated for their interactions with calf thymus DNA, antiproliferative and human topoisomerase I and IIα inhibitory activities. Both compounds presented ability to bind DNA. The binding constant determined by UV-vis spectroscopy was found to be 104M-1. Antiproliferative assay demonstrated that AMTAC-01 and AMTAC-02 were most active against prostate and melanoma tumor cell lines, respectively. The compound did not present Topo I inhibitory activity. However, both derivatives displayed topoisomerase IIα inhibitory activity comparable to amsacrine, and AMTAC-02 was more potent than AMTAC-01 with methoxy substituent group on phenyl ring. This study demonstrates that the new derivatives are promising molecules with topoisomerase IIα inhibitory and antiproliferative activities.Entities:
Keywords: DNA-binding; Spiro-acridine; Topoisomerase
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Year: 2016 PMID: 27435006 DOI: 10.1016/j.ijbiomac.2016.07.057
Source DB: PubMed Journal: Int J Biol Macromol ISSN: 0141-8130 Impact factor: 6.953