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Consequences and management of iron overload in sickle cell disease

机译:镰状细胞病中铁超负荷的后果和处理

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摘要

The aims of this review are to highlight the mechanisms and consequences of iron distribution that are most relevant to transfused sickle cell disease (SCD) patients and to address the particular challenges in the monitoring and treatment of iron overload. In contrast to many inherited anemias, in SCD, iron overload does not occur without blood transfusion. The rate of iron loading in SCD depends on the blood transfusion regime: with simple hypertransfusion regimes, rates approximate to thalassemia major, but iron loading can be minimal with automated erythrocyte apheresis. The consequences of transfusional iron overload largely reflect the distribution of storage iron. In SCD, a lower proportion of transfused iron distributes extrahepatically and occurs later than in thalassemia major, so complications of iron overload to the heart and endocrine system are less common. We discuss the mechanisms by which these differences may be mediated. Treatment with iron chelation and monitoring of transfusional iron overload in SCD aim principally at controlling liver iron, thereby reducing the risk of cirrhosis and hepatocellular carcinoma. Monitoring of liver iron concentration pretreatment and in response to chelation can be estimated using serum ferritin, but noninvasive measurement of liver iron concentration using validated and widely available MRI techniques reduces the risk of under- or overtreatment. The optimal use of chelation regimes to achieve these goals is described.
机译:这篇综述的目的是强调与输血的镰状细胞病(SCD)患者最相关的铁分布的机制和后果,并解决在监测和治疗铁超负荷方面的特殊挑战。与许多遗传性贫血相反,在SCD中,不输血不会发生铁超负荷。 SCD中铁的负荷率取决于输血方式:在简单的高输血方案中,铁的负荷率近似于地中海贫血的严重程度,但自动红细胞单采术可使铁负荷最小。输血铁超负荷的后果在很大程度上反映了储存铁的分布。在SCD中,较轻的地中海贫血患者,肝外分布的铁比例较低,发生的时间较晚,因此铁超负荷引起的心脏和内分泌系统并发症并不常见。我们讨论了可以介导这些差异的机制。 SCD中铁螯合的治疗和输血铁超负荷的监测主要旨在控制肝铁,从而降低肝硬化和肝细胞癌的风险。可以使用血清铁蛋白来评估对肝铁浓度的预处理以及对螯合反应的监测,但是使用经过验证且广泛使用的MRI技术对肝铁浓度的无创测量可以降低治疗不足或过度治疗的风险。描述了实现这些目标的螯合方案的最佳使用。

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