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Anticancer Aminoferrocene Derivatives Inducing Production of Mitochondrial Reactive Oxygen Species
Authors:Hülya Gizem Özkan  Vanrajsinh Thakor  Hong-Gui Xu  Galyna Bila  Prof. Dr. Rostyslav Bilyy  Daria Bida  Dr. Martin Böttcher  Prof. Dr. Dimitrios Mougiakakos  Dr. Rainer Tietze  Prof. Dr. Andriy Mokhir
Affiliation:1. Department of Chemistry and Pharmacy, Friedrich-Alexander-University of Erlangen Nuremberg (FAU), Organic Chemistry II, 91058 Erlangen, Germany;2. Danylo Halytsky Lviv National Medical University, Pekarska str. 69, 79010 Lviv, Ukraine;3. Department of Otorhinolaryngology, Otto-von-Guericke-University of Magdeburg, Medicinal Faculty, University Hospital for Hematology and Oncology, Leipzigerstraße 44, 39120 Magdeburg, Germany;4. Department of Otorhinolaryngology, Head and Neck Surgery, Section of Experimental Oncology and Nanomedicine (SEON), Friedrich-Alexander-University of Erlangen Nuremberg (FAU), University Hospital, Glückstraße 10a, 91054 Erlangen, Germany
Abstract:Elevated levels of reactive oxygen species (ROS) and deficient mitochondria are two weak points of cancer cells. Their simultaneous targeting is a valid therapeutic strategy to design highly potent anticancer drugs. The remaining challenge is to limit the drug effects to cancer cells without affecting normal ones. We have previously developed three aminoferrocene (AF)-based derivatives, which are activated in the presence of elevated levels of ROS present in cancer cells with formation of electron-rich compounds able to generate ROS and reduce mitochondrial membrane potential (MMP). All of them exhibit important drawbacks including either low efficacy or high unspecific toxicity that prevents their application in vivo up to date. Herein we describe unusual AF-derivatives lacking these drawbacks. These compounds act via an alternative mechanism: they are chemically stable in the presence of ROS, generate mitochondrial ROS in cancer cells, but not normal cells and exhibit anticancer effect in vivo.
Keywords:anticancer drugs  ferrocene  mitochondrion  reactive oxygen species
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