Novel synthetic acridine derivatives as potent DNA-binding and apoptosis-inducing antitumor agents

Acridine derivatives have been explored as DNA-binding Anticancer agents. Some derivatives show undesired pharmacokinetic properties and new derivatives need to be explored. In this work, a series of novel acridine analogues were synthesized by modifying previously unexplored linkers between the acridine and benzene groups and their antiproliferative activity and the DNA-binding ability were evaluated. Among these derivatives, compound 5c demonstrated DNA-binding capability and Topoisomerase I inhibitory activity. In K562 cell lines, 5c induced Apoptosis through mitochondria-dependent intrinsic pathways. These data suggested that compound 5c and Other acridine derivatives with modified linkers between the acridine and benzene groups might be potent DNA-binding agents.