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显性特发性血色素沉着症的新诊断与治疗可能性

New diagnostic and therapeutic possibilities in manifest idiopathic hemochromatosis.

作者信息

Volkholz H J, Sailer D, Rödl W

出版信息

Hepatogastroenterology. 1984 Dec;31(6):289-94.

PMID:6519641
Abstract

Up until recently in clinical practice suspected hemochromatosis with a pathological iron-screening test (plasma iron, percentage transferrin saturation, serum ferritin, desferrioxamine-induced urinary iron excretion) made a liver biopsy necessary. Today, as a first step, the density of the liver parenchyma can be measured by means of computed tomography. Normal findings obviate the need for laparoscopy. Since the late forties weekly or twice weekly phlebotomy has been the sole form of treatment for manifest idiopathic hemochromatosis. In the mid-sixties the hopes placed in chelating substances (desferrioxamine) were not fulfilled, because the plasma half-life (only 7-10 minutes) of this drug was too short. Even with several daily injections only a small amount of iron was removed from the body tissue (10-25 mg daily urinary iron excretion). The introduction of portable infusion pumps in the late seventies offered us a new possibility of administering desferrioxamine by subcutaneous injection (Propper et al., 1976). Until that time such treatment was successfully used only in the field of pediatrics to treat secondary transfusion hemochromatosis in thalassemia. In one case of idiopathic hemochromatosis with severe organic involvement (right heart failure, repeated esophageal hemorrhage and bronzed diabetes) we had to achieve rapid iron elimination, and for this purpose we used continuous long-term desferrioxamine administration by means of a portable infusion pump (Autosyringe) in addition to phlebotomy. Since, particularly in the critical initial phase of treatment when heart failure was always threatening, great care had to be exercised in the use of phlebotomy, iron removal was achieved largely by desferrioxamine administration (daily up to 240 mg iron elimination in urine and stools).(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

直到最近,在临床实践中,对于疑似血色素沉着症且铁筛查试验(血浆铁、转铁蛋白饱和度百分比、血清铁蛋白、去铁胺诱导的尿铁排泄)呈病理性的情况,进行肝脏活检是必要的。如今,作为第一步,可以通过计算机断层扫描测量肝实质密度。正常结果可避免进行腹腔镜检查。自四十年代后期以来,每周或每两周进行一次静脉放血一直是明显特发性血色素沉着症的唯一治疗方式。六十年代中期,对螯合剂(去铁胺)寄予的希望并未实现,因为这种药物的血浆半衰期(仅7 - 10分钟)太短。即使每天注射几次,从身体组织中去除的铁量也很少(每天尿铁排泄量为10 - 25毫克)。七十年代后期便携式输液泵的引入为我们提供了通过皮下注射给予去铁胺的新可能性(普罗珀等人,1976年)。在此之前,这种治疗仅在儿科领域成功用于治疗地中海贫血中的继发性输血性血色素沉着症。在一例伴有严重器官受累(右心衰竭、反复食管出血和青铜色糖尿病)的特发性血色素沉着症病例中,我们必须实现快速排铁,为此我们除了进行静脉放血外,还通过便携式输液泵(自动注射器)持续长期给予去铁胺。由于特别是在治疗的关键初始阶段,心力衰竭总是构成威胁,在进行静脉放血时必须格外小心,排铁主要通过给予去铁胺实现(每天尿和粪便中的铁排泄量高达240毫克)。(摘要截断于250字)

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Hepatic iron concentration in hereditary hemochromatosis does not saturate or accurately predict phlebotomy requirements.遗传性血色素沉着症中的肝脏铁浓度不会饱和,也不能准确预测放血治疗的需求量。
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