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Pentathiepins: A Novel Class of Glutathione Peroxidase 1 Inhibitors that Induce Oxidative Stress,Loss of Mitochondrial Membrane Potential and Apoptosis in Human Cancer Cells
Authors:Dr. Steven Behnisch-Cornwell  Siva Sankar Murthy Bandaru  Martin Napierkowski  Lisa Wolff  Dr. Muhammad Zubair  Claudia Urbainsky  Dr. Christopher Lillig  Prof. Dr. Carola Schulzke  Prof. Dr. Patrick J. Bednarski
Affiliation:1. Pharmazeutische/Medizinische Chemie, Institut für Pharmazie, Universität Greifswald, 17489 Greifswald, Germany;2. Bioanorganische Chemie, Institut für Biochemie, Universität Greifswald, 17489 Greifswald, Germany;3. Institut für Medizinische Biochemie und Molekulare Biologie, Universitätsmedizin, Universität Greifswald, 17475 Greifswald, Germany
Abstract:A novel class of glutathione peroxidase 1 (GPx1) inhibitors, namely tri- and tetracyclic pentathiepins, has been identified that is approximately 15 times more potent than the most active known GPx1 inhibitor, mercaptosuccinic acid. Enzyme kinetic studies with bovine erythrocyte GPx1 indicate that pentathiepins reversibly inhibit oxidation of the substrate glutathione (GSH). Moreover, no inhibition of superoxide dismutase, catalase, thioredoxin reductase or glutathione reductase was observed at concentrations that effectively inhibit GPx1. As well as potent enzyme inhibitory activity, the pentathiepins show strong anticancer activity in various human cancer cell lines, with IC50 values in a low-micromolar range. A representative tetracyclic pentathiepin causes the formation of reactive oxygen species in these cells, the fragmentation of nuclear DNA and induces apoptosis via the intrinsic pathway. Moreover, this pentathiepin leads to a rapid and strong loss of mitochondrial membrane potential in treated cancer cells. On the other hand, evidence for the induction of ferroptosis as a form of cell death was negative. These new findings show that pentathiepins possess interesting biological activities beyond those originally ascribed to these compounds.
Keywords:apoptosis  cancer cells  cytotoxicity  DNA fragmentation  glutathione peroxidase  oxidative stress  pentathiepin
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