首页> 美国卫生研究院文献>International Journal of Molecular Sciences >Mobilization of Intracellular Copper by Gossypol and Apogossypolone Leads to Reactive Oxygen Species-Mediated Cell Death: Putative Anticancer Mechanism
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Mobilization of Intracellular Copper by Gossypol and Apogossypolone Leads to Reactive Oxygen Species-Mediated Cell Death: Putative Anticancer Mechanism

机译:棉酚和阿朴棉酚动员细胞内铜导致活性氧介导的细胞死亡:推测的抗癌机制。

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摘要

There is compelling evidence that serum, tissue and intracellular levels of copper are elevated in all types of cancer. Copper has been suggested as an important co-factor for angiogenesis. It is also a major metal ion present inside the nucleus, bound to DNA bases, particularly guanine. We have earlier proposed that the interaction of phenolic-antioxidants with intracellular copper leads to the generation of reactive oxygen species (ROS) that ultimately serve as DNA cleaving agents. To further validate our hypothesis we show here that the antioxidant gossypol and its semi-synthetic derivative apogossypolone induce copper-mediated apoptosis in breast MDA-MB-231, prostate PC3 and pancreatic BxPC-3 cancer cells, through the generation of ROS. MCF10A breast epithelial cells refractory to the cytotoxic property of these compounds become sensitized to treatment against gossypol, as well as apogossypolone, when pre-incubated with copper. Our present results confirm our earlier findings and strengthen our hypothesis that plant-derived antioxidants mobilize intracellular copper instigating ROS-mediated cellular DNA breakage. As cancer cells exist under significant oxidative stress, this increase in ROS-stress to cytotoxic levels could be a successful anticancer approach.
机译:有令人信服的证据表明,血清,组织和细胞内铜的水平在所有类型的癌症中均升高。铜被认为是血管生成的重要辅助因子。它也是存在于细胞核内的主要金属离子,与DNA碱基(特别是鸟嘌呤)结合。我们较早提出,酚类抗氧化剂与细胞内铜的相互作用会导致活性氧(ROS)的产生,而活性氧最终可作为DNA裂解剂。为了进一步验证我们的假设,我们在这里显示抗氧化剂棉酚及其半合成衍生物载脂孢酮通过ROS的产生诱导铜介导的乳腺癌MDA-MB-231,前列腺PC3和胰腺BxPC-3癌细胞的凋亡。在与铜预孵育后,对这些化合物具有细胞毒性的特性无法抵抗的MCF10A乳腺上皮细胞对棉酚和载脂孢子酮的治疗变得敏感。我们目前的结果证实了我们较早的发现,并加强了植物来源的抗氧化剂动员细胞内铜刺激ROS介导的细胞DNA断裂的假说。由于癌细胞在明显的氧化应激下存在,因此ROS应激增加至细胞毒性水平可能是成功的抗癌方法。

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