Recent Advances in Anticancer Copper Compounds

Andrew Kellett, Zara Molphy, Vickie McKee, Creina Slator

Research output: Chapter in Book/Report/Conference proceedingBook chapterResearchpeer-review

Abstract

There have been significant advances in the discovery of developmental copper complexes for the treatment of human cancer. The enzyme-active sites of several copper-containing enzymes suggest a starting point for metallodrug development and successful strategies have, so far, employed phenanthroline or bipyridine ligands to supply two pyridyl donors (modelling histidine residues) along with other oxygen or nitrogen donor ligands that tune specific properties. Suitably designed copper(ii) metallodrugs can generate reactive oxygen species (ROS) and reactive nitrogen species (RNS) that overwhelm innate cellular antioxidant defences to trigger oxidative damage and cell death. Recently, several complexes of this class were screened by the National Cancer Institute's (NCI) Developmental Therapeutics Program (DTP). The 60-cancer cell line screening results indicate copper(ii) metallodrug leads have unique activity and alternative mechanisms to clinically established anticancer agents such as cisplatin and bleomycin. Although DNA is a valid cellular target, mechanistic evidence suggests cell death is triggered by metal-catalysed pro-apoptotic ROS and RNS that damage cytoplasmic, mitochondrial, and genome function. In addition to copper complexes screened within the DTP, a number of other structurally relevant compounds are described, along with mechanistic aspects of their chemotherapeutic activity.

Original languageEnglish
Title of host publicationMetal-based Anticancer Agents
EditorsAnne Vessieres, Samuel M. Meier-Menches, Angela Casini
PublisherRoyal Society of Chemistry
Publication date1. Jan 2019
Pages91-119
Chapter4
ISBN (Print)978-1-78801-406-9
DOIs
Publication statusPublished - 1. Jan 2019
SeriesRSC Metallobiology
Number14
Volume2019-January
ISSN2045-547X

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