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首页> 外文期刊>Hemoglobin: International Journal for Hemoglobin Research >Iron chelation therapy in hereditary hemochromatosis and thalassemia intermedia: regulatory and non regulatory mechanisms of increased iron absorption.
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Iron chelation therapy in hereditary hemochromatosis and thalassemia intermedia: regulatory and non regulatory mechanisms of increased iron absorption.

机译:遗传性血色素沉着和地中海贫血的铁螯合疗法:增加铁吸收的调节和非调节机制。

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摘要

Millions of people are affected by hereditary hemochromatosis (HH) and thalassemia intermedia (TI), the iron overloading disorders caused by chronic increases in iron absorption. Genetic factors, regulatory pathways involving proteins of iron metabolism, non regulatory molecules, dietary constituents and iron binding drugs could affect iron absorption and could lead to iron overload or iron deficiency. Chelators and chelating drugs can affect both iron absorption and excretion. Deferoxamine (DFO), deferiprone (L1) and the DFO/L1 combination therapies have been used effectively for reversing the toxic side effects of iron overload including cardiac and liver damage in TI and HH patients where venesection is contraindicated. Selected protocols using DFO, L1 and their combination could be designed for optimizing chelation therapy in TI and HH. The use of deferasirox (DFRA) in HH and TI could cause an increase in iron and other toxic metal absorption. Future treatments of HH and TI could involve the use of iron chelating and other drugs not only for increasing iron excretion but also for preventing iron absorption.
机译:数以百万计的人受到遗传性血色素沉着病(HH)和中间地中海贫血(TI)的影响,这是铁吸收的慢性增加导致的铁超负荷疾病。遗传因素,涉及铁代谢蛋白的调控途径,非调控分子,饮食成分和铁结合药物可能会影响铁的吸收并可能导致铁超负荷或铁缺乏。螯合剂和螯合剂会影响铁的吸收和排泄。去铁胺(DFO),去铁酮(L1)和DFO / L1组合疗法已被有效用于逆转禁忌穿刺术的TI和HH患者铁过载的毒性副作用,包括心脏和肝脏损害。可以设计使用DFO,L1及其组合的选定方案,以优化TI和HH中的螯合疗法。在HH和TI中使用地拉罗司(DFRA)可能会导致铁和其他有毒金属的吸收增加。 HH和TI的未来治疗方法可能包括使用铁螯合剂和其他药物,不仅可以增加铁的排泄,还可以防止铁的吸收。

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