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Modulation of iron metabolism by iron chelation regulates intracellular calcium and increases sensitivity to doxorubicin

机译:铁螯合作用调节铁代谢,调节细胞内钙并增加对阿霉素的敏感性

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Increased intracellular iron levels can both promote cell proliferation and death, as such; iron has a “two-sided effect” in the delicate balance of human health. Though the role of iron in the development of cancer remains unclear, investigations of iron chelators as anti-tumor agents have revealed promising results. Here, we investigated the influence of iron and desferrioxamine (DFO), the iron chelating agent on intracellular calcium in a human leukemia cell line, K562. Iron uptake is associated with increased reactive oxygen species (ROS) generation. Therefore, we showed that iron also caused dose-dependent ROS generation in K562 cells. The measurement of intracellular calcium was determined using Furo-2 with a fluorescence spectrophotometer. The iron delivery process to the cytoplasmic iron pool was examined by monitoring the fluorescence of cells loaded with calcein-acetoxymethyl. Our data showed that iron increased intracellular calcium, and this response was 8 times higher when cells were incubated with DFO. K562 cells with DFO caused a 3.5 times increase of intracellular calcium in the presence of doxorubicin (DOX). In conclusion, DFO induces intracellular calcium and increases their sensitivity to DOX, a chemotherapeutic agent.
机译:如此,增加的细胞内铁水平可以促进细胞增殖和死亡。铁在人体健康的微妙平衡中具有“双面作用”。尽管铁在癌症发展中的作用尚不清楚,但对铁螯合剂作为抗肿瘤药物的研究显示出令人鼓舞的结果。在这里,我们研究了铁和去铁胺(DFO)(铁螯合剂)对人白血病细胞系K562中细胞内钙的影响。铁吸收与活性氧(ROS)生成增加有关。因此,我们表明铁还可以在K562细胞中引起剂量依赖性ROS的产生。使用Furo-2和荧光分光光度计测定细胞内钙的含量。通过监测装有钙黄绿素-乙酰氧甲基的细胞的荧光检查铁向细胞质铁池的转运过程。我们的数据表明,铁增加了细胞内钙的含量,当细胞与DFO一起孵育时,这种反应要高8倍。在存在阿霉素(DOX)的情况下,具有DFO的K562细胞引起的细胞内钙增加3.5倍。总之,DFO诱导细胞内钙并增加其对化学治疗药物DOX的敏感性。

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