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口服铁螯合剂地拉罗司对铁过载血液透析患者的长期影响。

Long-term effects of an oral iron chelator, deferasirox, in hemodialysis patients with iron overload.

作者信息

Chen Cheng-Hsu, Shu Kuo-Hsiung, Yang Youngsen

出版信息

Hematology. 2015 Jun;20(5):304-10. doi: 10.1179/1607845414Y.0000000199. Epub 2014 Sep 9.

Abstract

Background/Purpose Retention of excess iron from transfused blood in organs in patients with renal anemia may lead to various systemic complications. Iron chelating agents such as deferasirox (DFX) decrease such iron overload. This study assessed the efficacy, safety, and tolerability of DFX in hemodialysis (HD) patients with iron overload. Methods We retrospectively (February 2008 to June 2012) reviewed data for eight HD patients with end-stage renal disease who were prescribed DFX (15 mg/kg/day) for transfusion-induced iron overload. Baseline and post-treatment levels of hematocrit, ferritin, erythropoietin (EPO), transferrin saturation (TSAT), total and unsaturated iron-binding capacity (TIBC and UIBC, respectively), and blood transfusion volumes were measured. Treatment efficacy was evaluated by observing changes in ferritin and TSAT during the study period; monthly EPO doses and blood transfusions were also recorded. Safety was evaluated in the form of adverse events. Results DFX administration caused statistically significant reductions in TSAT (68.2-49.2%; P = 0.036) and ferritin (3133.1-1215.6 ng/ml; P = 0.017). Significant post-treatment increases in UIBC (63.3-196.6 µg/dl; P = 0.018) and TIBC (210.0-422.4 µg/dl; P = 0.012) were also observed. While there were no significant differences in hematocrit values or EPO requirements after treatment, significant reductions in average monthly transfusion volumes (P = 0.026) were recorded. DFX was generally well tolerated; common adverse effects included nausea, vomiting, diarrhea, and abdominal pain. Conclusion DFX significantly improved iron metabolism in HD patients with iron overload and had an acceptable frequency of adverse effects.

摘要

背景/目的 肾性贫血患者体内输注血液中的过量铁在器官中的潴留可能导致各种全身并发症。地拉罗司(DFX)等铁螯合剂可减少此类铁过载。本研究评估了DFX在铁过载血液透析(HD)患者中的疗效、安全性和耐受性。方法 我们回顾性分析(2008年2月至2012年6月)了8例终末期肾病HD患者的数据,这些患者因输血所致铁过载而服用DFX(15mg/kg/天)。测量了血细胞比容、铁蛋白、促红细胞生成素(EPO)、转铁蛋白饱和度(TSAT)、总铁结合力和不饱和铁结合力(分别为TIBC和UIBC)的基线水平和治疗后水平,以及输血体积。通过观察研究期间铁蛋白和TSAT的变化来评估治疗效果;还记录了每月的EPO剂量和输血情况。以不良事件的形式评估安全性。结果 服用DFX导致TSAT(68.2 - 49.2%;P = 0.036)和铁蛋白(3133.1 - 1215.6 ng/ml;P = 0.017)在统计学上显著降低。治疗后还观察到UIBC(63.3 - 196.6 μg/dl;P = 0.018)和TIBC(210.0 - 422.4 μg/dl;P = 0.012)显著升高。虽然治疗后血细胞比容值或EPO需求没有显著差异,但记录到平均每月输血量显著减少(P = 0.026)。DFX总体耐受性良好;常见不良反应包括恶心、呕吐、腹泻和腹痛。结论 DFX显著改善了铁过载HD患者的铁代谢,且不良反应发生率可接受。

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