铁及其在癌症防御中的作用:一把双刃剑。

Frank Thévenod
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引用次数: 27

摘要

铁(Fe)是一种必需的金属,对生物功能至关重要,包括电子传递、DNA合成、解毒和红细胞生成,这些都有助于新陈代谢、细胞生长和增殖。Fe和O2之间的相互作用可以产生活性氧(ROS),这是基于Fe氧化还原循环的能力。过量的铁可能引起氧化损伤,导致细胞死亡,但DNA损伤也可能导致永久性突变。因此,铁具有致癌性,可能引发肿瘤的形成和生长,也可能滋养肿瘤微环境和转移。然而,铁也有助于预防癌症。铁可诱导毒性活性氧和/或启动特定形式的细胞死亡,包括有利于癌症治疗的铁下垂。此外,铁结合蛋白和铁调节蛋白,如hepcidin、lipocalin-2/NGAL、血红素加氧酶-1、铁蛋白和铁硫簇在特定条件下和特定癌症类型中可以显示抗肿瘤特性。此外,乳铁蛋白可能与其他已建立的抗癌药物协同作用,以预防和治疗癌症。因此,靶向肿瘤中铁代谢的药物是预防和治疗癌症的有希望的候选者,但考虑到环境特异性(例如,肿瘤类型;系统与肿瘤微环境Fe稳态)是必需的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Iron and Its Role in Cancer Defense: A Double-Edged Sword.

Iron (Fe) is an essential metal, vital for biological functions, including electron transport, DNA synthesis, detoxification, and erythropoiesis that all contribute to metabolism, cell growth, and proliferation. Interactions between Fe and O2 can result in the generation of reactive oxygen species (ROS), which is based on the ability of Fe to redox cycle. Excess Fe may cause oxidative damage with ensuing cell death, but DNA damage may also lead to permanent mutations. Hence Fe is carcinogenic and may initiate tumor formation and growth, and also nurture the tumor microenvironment and metastasis. However, Fe can also contribute to cancer defense. Fe may induce toxic ROS and/or initiate specific forms of cell death, including ferroptosis that will benefit cancer treatment. Furthermore, Fe-binding and Fe-regulatory proteins, such as hepcidin, lipocalin-2/NGAL, heme oxygenase-1, ferritin, and iron-sulfur clusters can display antitumor properties under specific conditions and in particular cancer types. In addition, the milk protein lactoferrin may synergize with other established anticancer agents in the prevention and therapy of cancer. Consequently, drugs that target Fe metabolism in tumors are promising candidates for the prevention and therapy of cancer, but consideration of context specificity (e.g., tumor type; systemic versus tumor microenvironment Fe homeostasis) is mandatory.

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