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镰状细胞病中的心脏铁过载。

Cardiac iron overload in sickle-cell disease.

机构信息

CMR Unit, Fondazione G. Monasterio CNR-Regione Toscana, Pisa, Italy; Division of Cardiology, Children's Hospital Los Angeles, Los Angeles, California.

出版信息

Am J Hematol. 2014 Jul;89(7):678-83. doi: 10.1002/ajh.23721. Epub 2014 Apr 15.

DOI:10.1002/ajh.23721
PMID:24664847
Abstract

Chronically transfused sickle cell disease (SCD) patients have lower risk of myocardial iron overload (MIO) than comparably transfused thalassemia major (TM) patients. However, cardioprotection is incomplete. We present the clinical characteristics of six patients who have prospectively developed MIO, to identify potential risk factors for cardiac iron accumulation. From 2002 to 2011, cardiac, hepatic, and pancreatic iron overload were assessed by R2 and R2 * magnetic resonance imaging techniques in 201 chronic transfused SCD patients as part of their clinical care. At the time, they developed MIO, five of six patients had been on chronic transfusion for more than 11 years; only one was on exchange transfusion. The time to MIO was correlated with reticulocyte and hemoglobin S percentages. All patients had qualitatively poor chelation compliance (<50%). All patients had serum ferritin levels >4600 ng/ml and liver iron concentration >22 mg/g. Pancreatic R2 * was >100 Hz in every patient studied (5/6). Cardiac iron rose proportionally to pancreas R2 *, with all patients having pancreas R2 *>100 Hz when cardiac iron was present. MIO had a threshold relationship with liver iron that was higher than observed in TM patients. In conclusion, MIO occurs in a small percentage of chronically transfused SCD patients and is only associated with exceptionally poor control of total body iron stores. Duration of chronic transfusion is clearly important but other factors, such as levels of effective erythropoiesis, appear to contribute to cardiac risk. Pancreas R2 * can serve as a valuable screening tool for cardiac iron in SCD patients.

摘要

慢性输血镰状细胞病(SCD)患者的心肌铁过载(MIO)风险低于同等输血的地中海贫血症(TM)患者。然而,心脏保护并不完全。我们介绍了 6 名前瞻性发生 MIO 的患者的临床特征,以确定心脏铁积累的潜在危险因素。

2002 年至 2011 年,作为其临床护理的一部分,通过 R2 和 R2磁共振成像技术评估了 201 名慢性输血的 SCD 患者的心脏、肝脏和胰腺铁过载。当时,他们发生了 MIO,其中 5 名患者的慢性输血时间超过 11 年,只有 1 名患者接受了换血治疗。MIO 的发生时间与网织红细胞和血红蛋白 S 的百分比相关。所有患者的螯合治疗依从性均较差(<50%)。所有患者的血清铁蛋白水平均>4600ng/ml,肝脏铁浓度>22mg/g。在研究的所有患者中,胰腺 R2均>100Hz(5/6)。心脏铁与胰腺 R2成正比增加,当心脏铁存在时,所有患者的胰腺 R2>100Hz。MIO 与肝脏铁呈阈值关系,高于 TM 患者观察到的关系。

总之,MIO 在一小部分慢性输血 SCD 患者中发生,并且仅与异常差的总铁储存控制有关。慢性输血的持续时间显然很重要,但其他因素,如有效红细胞生成的水平,似乎也会导致心脏风险。胰腺 R2*可以作为 SCD 患者心脏铁的有价值的筛查工具。

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