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首页> 外文期刊>ACS medicinal chemistry letters >Iron Chelators in Photodynamic Therapy Revisited: Synergistic Effect by Novel Highly Active Thiosemicarbazones
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Iron Chelators in Photodynamic Therapy Revisited: Synergistic Effect by Novel Highly Active Thiosemicarbazones

机译:铁螯合剂在光动力疗法中的再探讨:新型的高活性硫代咪唑啉酮的协同效应。

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摘要

In photodynamic therapy (PDT), a noninvasive anticancer treatment, visible light, is used as a magic bullet selectively destroying cancer cells by a photosensitizer that is nontoxic in the dark. Protoporphyrin IX (PpIX) is a natural photosensitizer synthesized in the cell, which is also a chelating agent that if bonded to Fe~(2+) forms heme, a central component of hemoglobin. Therefore, xenobiotic iron chelators can disturb iron homeostasis, increasing the accumulation of PpIX, obstructing the last step of heme biosynthesis, and enhancing PDT efficiency. However, the attempts to use this promising idea have not proved to be hugely successful. Herein, we revisited this issue by analyzing the application of iron chelators highly toxic in the dark, which should have higher Fe~(2+) affinity than the nontoxic chelators used so far. We have designed and prepared thiosemicarbazones (TSC) with the highest dark cellular cytotoxicity among TSCs ever reported. We demonstrate that compound 2 exerts powerful PDT enhancement when used in combination with 5-aminolevulinic acid (ALA), a precursor of PpIX.
机译:在光动力疗法(PDT)中,无创抗癌疗法,可见光,被用作通过在黑暗中无毒的光敏剂选择性破坏癌细胞的魔术子弹。原卟啉IX(PpIX)是在细胞中合成的天然光敏剂,它也是一种螯合剂,如果与Fe〜(2+)结合形成血红素(血红蛋白的主要成分)。因此,异源铁螯合剂可以干扰铁的稳态,增加PpIX的积累,阻碍血红素生物合成的最后一步,并提高PDT效率。但是,使用这一有前途的想法的尝试并未被证明是巨大的成功。在此,我们通过分析在黑暗中具有高毒性的铁螯合剂的应用来重新审视此问题,铁螯合剂应比迄今为止使用的无毒螯合剂具有更高的Fe〜(2+)亲和力。我们设计并制备了有史以来报道的TSC中具有最高暗细胞毒性的硫代半脲酮(TSC)。我们证明化合物2与5-氨基乙酰丙酸(ALA)(PpIX的前体)结合使用时,可以发挥强大的PDT增强作用。

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