Publication | Open Access
ROS-activated Anticancer Prodrugs: a New Strategy for tumor-specific Damage
141
Citations
60
References
2012
Year
Chemoprevention StrategyRedox BiologyTumor BiologyOxidative StressMedicinal ChemistryOncologyAnti-cancer AgentRadiation OncologyCancer ResearchRos-activated Anticancer ProdrugsTumor TargetingCancer CellsReactive Oxygen SpeciePharmacologyCancer TherapiesTumor MicroenvironmentDrug TargetingMedicineDrug Discovery
Targeting tumor cells is an important strategy to improve the selectivity of cancer therapies. With the advanced studies in cancer biology, we know that cancer cells are usually under increased oxidative stress. The high level of reactive oxygen species in cancer cells has been exploited for developing novel therapeutic strategies to preferentially kill cancer cells. Our group, amongst others, have used boronic acids/esters as triggers for developing ROS-activated anticancer prodrugs that target cancer cells. The selectivity was achieved by combining a specific reaction between boronates and H2O2, with the efficient masking of drug toxicity in the prodrug via boronates. Prodrugs activated via ferrocene-mediated oxidation have also been developed to improve the selectivity of anticancer drugs. We describe how the strategies of ROS-activation can be used for further development of new ROS-targeting prodrugs, eventually leading to novel approaches and/or combined technology for more efficient and selective treatment of cancers.
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