Clinical aspects of transfusional iron overload

B. Wonke, V. Sanctis
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引用次数: 9

Abstract

Most of our knowledge of transfusional iron overload has been obtained from patients with β-thalassemia major (TM). Iron overload causes multiple endocrinopathies presenting in the first decade of life with growth disturbance, followed by thyroid dysfunction. By the second decade of life, carbohydrate metabolism is disturbed in up to 25% of patients and failure of sexual development, even in well-chelated patients, appears as the commonest endocrine complication. In the third and fourth decades of life, osteopenia and osteoporosis are the causes of morbidity in over 50% of well-chelated and transfused TM patients. Cardiac disease, secondary to iron damage, causes death in developed countries as a result of noncompliance to desferrioxamine mesylate (DFX) from the third decade of life. In underdeveloped countries, cardiac death starts from 12 years of age, due to the nonavailability of the iron chelating agent DFX. With the emergence of the advanced cardiac magnetic resonance imaging technique, early diagnosis of heart iron will allow the use of parenteral and oral chelators in an innovative way to improve survival and the quality of life for TM patients.
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输注铁超载的临床特点
我们对输血铁超载的了解大多来自于β-地中海贫血(TM)患者。铁超载导致多种内分泌疾病,表现在生命的第一个十年,生长障碍,其次是甲状腺功能障碍。到生命的第二个十年,高达25%的患者的碳水化合物代谢紊乱,性发育失败,即使在螯合良好的患者中,也是最常见的内分泌并发症。在生命的第三和第四个十年,骨质减少和骨质疏松症是超过50%的良好螯合和输血的TM患者发病的原因。在发达国家,由于从生命的第三个十年开始不遵守甲磺酸地铁胺(DFX)治疗,继发于铁损伤的心脏病导致死亡。在不发达国家,由于无法获得铁螯合剂DFX,心脏性死亡从12岁开始。随着先进的心脏磁共振成像技术的出现,心脏铁的早期诊断将允许以创新的方式使用肠外和口服螯合剂,以提高TM患者的生存率和生活质量。
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