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血色素沉着症的当前治疗方法。

Current approach to hemochromatosis.

作者信息

Brissot Pierre, Troadec Marie-Bérengère, Bardou-Jacquet Edouard, Le Lan Caroline, Jouanolle Anne-Marie, Deugnier Yves, Loréal Olivier

机构信息

Liver Disease Unit, Liver Research Unit Inserm U-522, IFR 140, University of Rennes1, Hemochromatosis Reference Center, Laboratory of Molecular Genetics, University Hospital Pontchaillou, Rennes, France.

出版信息

Blood Rev. 2008 Jul;22(4):195-210. doi: 10.1016/j.blre.2008.03.001. Epub 2008 Apr 21.

Abstract

Iron overload diseases of genetic origin are an ever changing world, due to major advances in genetics and molecular biology. Five major categories are now established: HFE-related or type1 hemochromatosis, frequently found in Caucasians, and four rarer diseases which are type 2 (A and B) hemochromatosis (juvenile hemochromatosis), type 3 hemochromatosis (transferrin receptor 2 hemochromatosis), type 4 (A and B) hemochromatosis (ferroportin disease), and a(hypo)ceruloplasminemia. Increased duodenal iron absorption and enhanced macrophagic iron recycling, both due to an impairment of hepcidin synthesis, account for the development of cellular excess in types 1, 2, 3, and 4B hemochromatosis whereas decreased cellular iron egress is involved in the main form of type 4A) hemochromatosis and in aceruloplasminemia. Non-transferrin bound iron plays an important role in cellular iron excess and damage. The combination of magnetic resonance imaging (for diagnosing visceral iron overload) and of genetic testing has drastically reduced the need for liver biopsy. Phlebotomies remain an essential therapeutic tool but the improved understanding of the intimate mechanisms underlying these diseases paves the road for innovative therapeutic approaches.

摘要

由于遗传学和分子生物学的重大进展,遗传性铁过载疾病是一个不断变化的领域。目前已确定了五大类:与HFE相关的或1型血色素沉着症,常见于白种人;以及四种罕见疾病,即2型(A和B)血色素沉着症(青少年血色素沉着症)、3型血色素沉着症(转铁蛋白受体2血色素沉着症)、4型(A和B)血色素沉着症(铁转运蛋白病)和a(低)铜蓝蛋白血症。1型、2型、3型和4B型血色素沉着症中细胞内铁过量的发生是由于十二指肠铁吸收增加和巨噬细胞铁循环增强,这两者均由铁调素合成受损所致,而细胞内铁流出减少则与4A型血色素沉着症的主要形式和无铜蓝蛋白血症有关。非转铁蛋白结合铁在细胞内铁过量和损伤中起重要作用。磁共振成像(用于诊断内脏铁过载)和基因检测的结合大大减少了肝活检的必要性。放血疗法仍然是一种重要的治疗手段,但对这些疾病潜在内在机制的深入了解为创新治疗方法铺平了道路。

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