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首页> 外文期刊>Seminars in cancer biology >Motexafin gadolinium: a novel redox active drug for cancer therapy.
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Motexafin gadolinium: a novel redox active drug for cancer therapy.

机译:Motexafin lin:一种用于癌症治疗的新型氧化还原活性药物。

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摘要

Motexafin gadolinium (MGd, Xcytrin) is an aromatic macrocycle that has a strong affinity for electrons, i.e., it is easily reduced. In the presence of oxygen, MGd accepts electrons from various cellular reducing metabolites and forms superoxide and other reactive oxygen species (ROS) by redox cycling. The reaction with NADPH is dramatically accelerated by various oxido-reductases including thioredoxin reductase. In vitro studies with various cancer cell lines have shown an increase in ROS and intracellular free zinc in cells treated with MGd. MGd increases cytotoxicity of ionizing radiation and various chemotherapy agents and may be directly cytotoxic to tumor cells under certain conditions. MGd selectively localizes in tumors, perhaps due to their metabolic perturbations. MGd treatment in murine models enhances tumor response to radiation and chemotherapy agents. In controlled, randomized clinical trials, combining MGd treatment with ionizing radiation improves time to neurologic progression in lung cancer patients with brain metastases. The molecular target for MGd appears to be thioredoxin reductase which, when inhibited, results in cellular redox stress, cytotoxicity and an increase in tumor responsiveness to a variety of treatments.
机译:Motexafin((MGd,Xcytrin)是一种芳香族大环,对电子具有很强的亲和力,即易于还原。在氧气存在下,MGd接受来自各种细胞还原性代谢物的电子,并通过氧化还原循环形成超氧化物和其他活性氧(ROS)。各种氧化还原酶(包括硫氧还蛋白还原酶)可大大促进与NADPH的反应。各种癌细胞系的体外研究表明,用MGd处理的细胞中ROS和细胞内游离锌的增加。 MGd可增加电离辐射和各种化学治疗剂的细胞毒性,并且在某些条件下可能直接对肿瘤细胞产生细胞毒性。 MGd选择性地定位在肿瘤中,可能是由于它们的代谢扰动。鼠模型中的MGd治疗可增强肿瘤对放射线和化学疗法的反应。在受控的随机临床试验中,将MGd治疗与电离辐射相结合可改善患有脑转移的肺癌患者神经发育的时间。 MGd的分子靶标似乎是硫氧还蛋白还原酶,该酶被抑制后会导致细胞氧化还原应激,细胞毒性和肿瘤对多种治疗的反应性增加。

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