| Literature DB >> 27028784 |
Oleg Babii1, Sergii Afonin2, Liudmyla V Garmanchuk3, Viktoria V Nikulina3, Tetiana V Nikolaienko3, Olha V Storozhuk3, Dmytro V Shelest3, Olga I Dasyukevich4, Liudmyla I Ostapchenko3, Volodymyr Iurchenko5, Sergey Zozulya5, Anne S Ulrich6,7, Igor V Komarov8.
Abstract
Conventional photodynamic treatment strategies are based on the principle of activating molecular oxygen in situ by light, mediated by a photosensitizer, which leads to the generation of reactive oxygen species and thereby causes cell death. A diarylethene-derived peptidomimetic is presented that is suitable for photodynamic cancer therapy without any involvement of oxygen. This light-sensitive molecule is not a mediator but is itself the cytotoxic agent. As a derivative of the cyclic amphiphilic peptide gramicidin S, the peptidomimetic exists in two thermally stable photoforms that are interconvertible by light of different wavelengths. The isomer generated by visible light shows much stronger toxicity against tumor cells than the UV-generated isomer. First in vivo applications are demonstrated on a tumor animal model to illustrate how the peptidomimetic can be administered in the less toxic form and then activated locally in a solid tumor by visible light.Entities:
Keywords: cancer; drug design; peptidomimetics; photodynamic therapy; photoswitches
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Year: 2016 PMID: 27028784 DOI: 10.1002/anie.201600506
Source DB: PubMed Journal: Angew Chem Int Ed Engl ISSN: 1433-7851 Impact factor: 15.336