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  • Mitochondrially Targeted α-Tocopheryl SuccinateIs Antiangiogenic: Potential Benefit Against Tumor Angiogenesis but Caution Against Wound Healing

    Author(s)
    Rohlena, Jakub
    Dong, Lan-Feng
    Kluckova, Katarina
    Zobalova, Renata
    Goodwin, Jacob
    Tilly, David
    Stursa, Jan
    Pecinova, Alena
    Philimonenko, Anatoly
    Hozak, Pavel
    Banerjee, Jaideep
    Ledvina, Miroslav
    Sen, Chandan K
    Houstek, Josef
    Coster, Mark J
    Neuzil, Jiri
    Griffith University Author(s)
    Neuzil, Jiri
    Year published
    2011
    Metadata
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    Abstract
    Aims: A plausible strategy to reduce tumor progress is the inhibition of angiogenesis. Therefore, agents that efficiently suppress angiogenesis can be used for tumor suppression. We tested the antiangiogenic potential of a mitochondrially targeted analog of a-tocopheryl succinate (MitoVES), a compound with high propensity to induce apoptosis. Results: MitoVES was found to efficiently kill proliferating endothelial cells (ECs) but not contact-arrested ECs or ECs deficient in mitochondrial DNA, and suppressed angiogenesis in vitro by inducing accumulation of reactive oxygen species and induction of apoptosis in ...
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    Aims: A plausible strategy to reduce tumor progress is the inhibition of angiogenesis. Therefore, agents that efficiently suppress angiogenesis can be used for tumor suppression. We tested the antiangiogenic potential of a mitochondrially targeted analog of a-tocopheryl succinate (MitoVES), a compound with high propensity to induce apoptosis. Results: MitoVES was found to efficiently kill proliferating endothelial cells (ECs) but not contact-arrested ECs or ECs deficient in mitochondrial DNA, and suppressed angiogenesis in vitro by inducing accumulation of reactive oxygen species and induction of apoptosis in proliferating/angiogenic ECs. Resistance of arrested ECs was ascribed, at least in part, to the lower mitochondrial inner transmembrane potential compared with the proliferating ECs, thus resulting in the lower level of mitochondrial uptake of MitoVES. Shorterchain homologs of MitoVES were less efficient in angiogenesis inhibition, thus suggesting a molecular mechanism of its activity. Finally, MitoVES was found to suppress HER2-positive breast carcinomas in a transgenic mouse as well as inhibit tumor angiogenesis. The antiangiogenic efficacy of MitoVES was corroborated by its inhibitory activity on wound healing in vivo. Innovation and Conclusion: We conclude that MitoVES, a mitochondrially targeted analog of a-tocopheryl succinate, is an efficient antiangiogenic agent of potential clinical relevance, exerting considerably higher activity than its untargeted counterpart. MitoVES may be helpful against cancer but may compromise wound healing.
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    Journal Title
    Antioxidants & Redox Signaling
    Volume
    15
    Issue
    12
    DOI
    https://doi.org/10.1089/ars.2011.4192
    Subject
    Biochemistry and cell biology
    Medical biochemistry and metabolomics
    Medical biochemistry and metabolomics not elsewhere classified
    Pharmacology and pharmaceutical sciences
    Publication URI
    http://hdl.handle.net/10072/43436
    Collection
    • Journal articles

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