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镰状细胞病中的铁代谢与铁螯合作用

Iron metabolism and iron chelation in sickle cell disease.

作者信息

Walter Patrick B, Harmatz Paul, Vichinsky Elliott

机构信息

Children's Hospital & Research Center Oakland, Oakland, Calif., USA.

出版信息

Acta Haematol. 2009;122(2-3):174-83. doi: 10.1159/000243802. Epub 2009 Nov 10.

Abstract

This review highlights recent advances in iron metabolism that are relevant to sickle cell disease (SCD). SCD is a common hemoglobinopathy that results in chronic inflammation. Improved understanding of how iron metabolism is controlled by proteins such as hepcidin, ferroportin, hypoxia-inducible factor 1, and growth differentiation factor 15 have revealed how they are involved in the organ toxicity of SCD. SCD patients have lower levels of non-transferrin-bound iron (NTBI) relative to other hemoglobinopathies, such as thalassemia. Care for SCD now commonly uses transfusion that results in iron overload and necessitates the need for chelation. New oral chelation therapy using deferasirox (Exjade/ICL670) appears to be safe and may even lower the amount of toxic free NTBI and enhance patient compliance. Finally, we suggest that iron metabolism and trafficking is different in SCD compared to other hemoglobinopathies. The high levels of inflammatory cytokines in SCD may enhance macrophage/reticuloendothelial cell iron and/or renal cell iron retention. This makes the tissues that retain iron different in SCD, and thus the organs that fail in SCD are different from those of other hemoglobinopathies, such as the cardiomyopathy or endocrinopathies of thalassemia.

摘要

本综述重点介绍了与镰状细胞病(SCD)相关的铁代谢方面的最新进展。SCD是一种常见的血红蛋白病,可导致慢性炎症。对铁代谢如何受铁调素、铁转运蛋白、缺氧诱导因子1和生长分化因子15等蛋白质控制的进一步了解,揭示了它们如何参与SCD的器官毒性。与其他血红蛋白病(如地中海贫血)相比,SCD患者的非转铁蛋白结合铁(NTBI)水平较低。目前对SCD的治疗通常采用输血,这会导致铁过载,因此需要进行螯合治疗。使用地拉罗司(Exjade/ICL670)的新型口服螯合疗法似乎是安全的,甚至可能降低有毒游离NTBI的量并提高患者的依从性。最后,我们认为与其他血红蛋白病相比,SCD中的铁代谢和运输有所不同。SCD中高水平的炎性细胞因子可能会增强巨噬细胞/网状内皮细胞铁和/或肾细胞铁潴留。这使得SCD中保留铁的组织不同,因此SCD中发生功能衰竭的器官与其他血红蛋白病(如地中海贫血的心肌病或内分泌病)不同。

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