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首页> 外文期刊>Free radical research >New method for the detection of reactive oxygen species in anti-tumoural activity of adriamycin: A comparison between hypoxic and normoxic cells
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New method for the detection of reactive oxygen species in anti-tumoural activity of adriamycin: A comparison between hypoxic and normoxic cells

机译:检测阿霉素抗肿瘤活性中活性氧的新方法:低氧和常氧细胞的比较

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Tumour hypoxia plays a role in chemoresistance in several human tumours. However, how hyperbaric oxygen leads to chemotherapeutic gain is unclear. This study investigates the relation of reactive oxygen species (ROS) generation with anti-tumoural effect of adriamycin (ADR) on CCRF-CEM cells under hypoxic (2% O2) and normoxic (21% O2) conditions. A new method was used to measure intracellular ROS variations through the fluorescence lifetime of 1-pyrenebutyric acid. At 24 h, ADR, probably via semiquinone radical, enhances ROS levels in normoxic cells compared to hypoxic cells. Long-term studies show that ROS are also generated by a second mechanism related to cell functions perturbation. ADR arrests the cell cycle progression both under hypoxia and normoxia, indicating that oxygen and ROS does not influence the DNA damaging activity of ADR. The findings reveal that moderate improvement of ADR cytotoxicity results from higher ROS formation in normoxic cells, leading to elevated induction of cell death.
机译:肿瘤缺氧在几种人类肿瘤的化学抗性中起作用。然而,高压氧如何导致化学疗法的增益尚不清楚。这项研究调查了活性氧(ROS)生成与阿霉素(ADR)在缺氧(2%O2)和常氧(21%O2)条件下对CCRF-CEM细胞的抗肿瘤作用之间的关系。一种新的方法被用来通过1-pyrenebutyricate酸的荧光寿命来测量细胞内ROS的变化。与缺氧细胞相比,在24小时时,ADR可能通过半醌自由基提高了常氧细胞中的ROS水平。长期研究表明,ROS也由与细胞功能扰动有关的第二种机制产生。在缺氧和常氧下,ADR都可阻止细胞周期进程,这表明氧气和ROS不会影响ADR的DNA破坏活性。这些发现表明,常氧细胞中较高的ROS形成可导致ADR细胞毒性的适度改善,从而导致细胞死亡的诱导增加。

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