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镰状细胞病中铁过载的进展。

Progression of iron overload in sickle cell disease.

作者信息

Olivieri N F

机构信息

Hemoglobinopathy Program, University of Toronto, Ontario, Canada.

出版信息

Semin Hematol. 2001 Jan;38(1 Suppl 1):57-62. doi: 10.1016/s0037-1963(01)90060-5.

DOI:10.1016/s0037-1963(01)90060-5
PMID:11206962
Abstract

The expanding indications for transfusions in patients with sickle cell disease raise the issues of appropriate measurement of body iron burden and optimal timing of iron chelation therapy. In this study, we obtained 42 biopsy specimens from 20 patients with sickle cell disease (mean age, 15.7 years) who received transfusions. In 12 patients whose mean age was 11.3 years at the time of liver biopsy, hepatic iron concentration was measured to provide information about the rate of iron accumulation in sickle cell disease, as well as to guide the initiation of chelating therapy. Mean hepatic iron concentration after an average of 15.4 transfusions administered over 21 months was 9.4 +/- 1.2 mg/g liver, dry weight, which did not correlate significantly with determinations of serum transferrin or ferritin levels. On Initial liver biopsy, hepatic portal fibrosis was noted in 4 of 12 patients. Twenty-nine biopsies in 16 patients were performed after variable periods of treatment with deferoxamine. These 16 patients had received a mean of 38.5 transfusions over 4 years. Hepatic iron was 14.1 +/- 1.9 mg/g of liver, dry weight, Indicating poor control of body iron in many patients. Cirrhosis was reported in one of 29 and portal fibrosis in 10 biopsy specimens. Hepatic iron concentration in patients in whom fibrosis was observed varied from 8.9 to 37.7 mg/g of liver, dry weight. These data show that after 1 to 2 years of conventional transfusions, variable tissue iron concentrations and tissue damage are observed in patients with sickle cell disease. In some patients, iron chelation therapy may not be appropriate after 1 year of transfusions; in others, therapy is clearly indicated by this time to prevent tissue injury. The data also suggest that patients with sickle cell disease develop increased portal fibrosis at the thresholds previously described in young patients with thalassemia (approximately 7 mg/g of liver, dry weight).

摘要

镰状细胞病患者输血适应证的不断扩大,引发了体内铁负荷的恰当测量及铁螯合治疗最佳时机的问题。在本研究中,我们从20例接受输血的镰状细胞病患者(平均年龄15.7岁)身上获取了42份活检标本。在12例肝活检时平均年龄为11.3岁的患者中,测量了肝脏铁浓度,以提供有关镰状细胞病中铁蓄积速率的信息,并指导螯合治疗的开始。在21个月内平均输注15.4次后,肝脏干重平均铁浓度为9.4±1.2mg/g肝脏,与血清转铁蛋白或铁蛋白水平的测定无显著相关性。在最初的肝活检中,12例患者中有4例出现肝门纤维化。16例患者在接受去铁胺不同疗程治疗后进行了29次活检。这16例患者在4年内平均接受了38.5次输血。肝脏铁含量为14.1±1.9mg/g肝脏干重,表明许多患者体内铁控制不佳。29例中有1例报告有肝硬化,10份活检标本中有门脉纤维化。观察到有纤维化的患者肝脏铁浓度在8.9至37.

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