摘要
铁是正常生命活动中的必需微量元素,因为这种金属元素不论缺乏或过量都很危险,它的吸收、转运和累积必须严格的调节。铁离子的平衡态的扰乱或含量水平的增加可能导致过载和神经退行性病变。针刺放血在很长一段时间内是降低过高铁含量的唯一途径。铁螯合法尽管可能有许多缺点,但确实是一种符合逻辑的、去除铁毒性水平的方法。在临床使用中有三种药物:去铁胺、去铁酮、地拉罗司。FBS0701是一种全新的口服铁螯合剂,正在进行临床研究,展示了良好的效果。发展新的铁结合作用的螯合剂是非常紧急的事情,这不仅为全身铁超载,也是为神经退行性病变,如帕金森病的治疗;去铁酮也被用于帕金森病的临床治疗。在神经退行性病变中,主要的目标不只是移除脑部组织的铁离子水平,同时也需调整其在全身的分配。有少量的螯合剂进行了潜在神经退行性病变活性的研究,例如氯碘羟喹的非卤代衍生物,这些化合物在神经退行性病变的动物模型上展示了很好的效果。能被用作神经退行性病变的药物必须满足一些标准,它们必须能够增加血脑屏障的通透性、低毒性和防止脂质过氧化。VK28是满足这些标准的化合物之一,在大鼠模型中它能够在低剂量水平保护神经元,而不明显改变肝脏和血浆中的铁离子水平。铁离子螯合剂调节单胺氧化酶的活性也进行了测试,多酚和黄酮能够阻止脂质过氧化并能表现出神经保护活性。然而癌症不与真实的铁离子超载相关,癌症细胞有更高的铁离子需求且倾向于消耗铁离子。研究表明去铁胺和地拉罗司在几种癌症类型中有抗增殖活性,缩氧硫脲类药是可能被用作抗癌药物,且非常有效的化合物,它们能够抑制与DNA合成相关核糖核苷酸还原酶。铁超载的发生、神经退行性病变、癌症与铁离子的关系非常复杂,铁离子动态平衡调节机制的研究在开发基于铁离子螯合的新药理策略中是一个关键因素,考察与这些疾病的发病机理密切相关的各种因素后,设计多功能的铁离子螯合剂可能是最有前景的治疗方式,但这仍需要很多的努力。从这个角度看,这个综述总结了系统的铁离子动态平衡;在脑和癌细胞中,铁失调和神经退行性病变的关系;以及在治疗铁离子系统过载、神经退行性病变和癌症中可能的螯合策略。
关键词: 癌症,螯合剂,铁离子,铁超载,神经退行性疾病
Current Medicinal Chemistry
Title:Iron Chelating Strategies in Systemic Metal Overload, Neurodegeneration and Cancer
Volume: 21 Issue: 33
Author(s): Elzbieta Gumienna-Kontecka, Monika Pyrkosz-Bulska, Agnieszka Szebesczyk and Malgorzata Ostrowska
Affiliation:
关键词: 癌症,螯合剂,铁离子,铁超载,神经退行性疾病
摘要: Iron is a trace element required for normal performance of cellular processes. Because both the deficiency and excess of this metal are dangerous, its absorption, distribution and accumulation must be tightly regulated. Disturbances of iron homeostasis and an increase in its level may lead to overload and neurodegenerative diseases. Phlebotomy was for a long time the only way of removing excess iron. But since there are many possible disadvantages of this method, chelation therapy seems to be a logical approach to remove toxic levels of iron. In clinical use, there are three drugs: desferrioxamine, deferiprone and deferasirox. FBS0701, a novel oral iron chelator, is under clinical trials with very promising results. Developing novel iron-binding chelators is an urgent matter, not only for systemic iron overload, but also for neurodegenerative disorders, such as Parkinson’s disease. Deferiprone is also used in clinical trials in Parkinson’s disease. In neurodegenerative disorders the main goal is not only to remove iron from brain tissues, but also its redistribution in system. Few chelators are tested for their potential use in neurodegeneration, such as nonhalogeneted derivatives of clioquinol. Such compounds gave promising results in animal models of neurodegenerative diseases. Drugs of possible use in neurodegeneration must meet certain criteria. Their development includes the improvement in blood brain barrier permeability, low toxicity and the ability to prevent lipid peroxidation. One of the compounds satisfying these requirements is VK28. In rat models it was able to protect neurons in very low doses without significantly changing the iron level in liver or serum. Also iron chelators able to regulate activity of monoamine oxidase were tested. Polyphenols and flavonoids are able to prevent lipid peroxidation and demonstrate neuroprotective activity. While cancer does not involve true iron overload, neoplastic cells have a higher iron requirement and are especially prone to its depletion. It was shown, that desferrioxamine and deferasirox are antiproliferative agents active in several types of cancer. Very potent compounds with possible use as anticancer drugs are thiosemicarbazones. They are able to inhibit ribonucleotide reductase, an enzyme involved in DNA synthesis. Because the relationship between the development of overload / neurodegenerative disorders, or cancer, and iron are very complex, comprehension of the mechanisms involved in the regulation of iron homeostasis is a crucial factor in the development of new pharmacological strategies based on iron chelation. In view of various factors closely involved in pathogenesis of such diseases, designing multifunctional metal-chelators seems to be the most promising approach, but it requires a lot of effort. In this perspective, the review summarizes systemic iron homeostasis, and in brain and cancer cells, iron dysregulation in neurodegenerative disease and possible chelation strategies in the treatment of metal systemic overload, neurodegeneration and cancer.
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Gumienna-Kontecka Elzbieta, Pyrkosz-Bulska Monika, Szebesczyk Agnieszka and Ostrowska Malgorzata, Iron Chelating Strategies in Systemic Metal Overload, Neurodegeneration and Cancer, Current Medicinal Chemistry 2014; 21 (33) . https://dx.doi.org/10.2174/0929867321666140706143402
DOI https://dx.doi.org/10.2174/0929867321666140706143402 |
Print ISSN 0929-8673 |
Publisher Name Bentham Science Publisher |
Online ISSN 1875-533X |
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