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螯合疗法在治疗低至中度铅暴露中的潜在作用评估。

Evaluation of the potential role of chelation therapy in treatment of low to moderate lead exposures.

作者信息

Chisolm J J

机构信息

Department of Pediatrics, Johns Hopkins School of Medicine, Baltimore, MD.

出版信息

Environ Health Perspect. 1990 Nov;89:67-74. doi: 10.1289/ehp.908967.

Abstract

In the overall long-term management of lead poisoning, chelation therapy can have short-term benefits; however, these benefits must be accompanied by drastic reduction in environmental exposure to lead if therapy is to have any long-term benefit. This discussion is limited to calcium disodium ethylenediaminetetraacetate (CaNa2EDTA), the chelating agent that has been the mainstay of treatment of lead poisoning for the past 38 years, and to meso-2,3-dimercaptosuccinic acid (DMSA), a new and promising oral chelating agent, which is an orphan drug and is currently classified as an investigational new drug by the U.S. Food and Drug Administration. With both drugs, multiple courses of treatment will be needed if any substantial reduction in body lead burden is to be achieved. A major limitation of CaNa2EDTA is the enormous diuresis of zinc that it produces. DMSA produces a comparable diuresis of lead, a greater decrease in blood lead, and has negligible influence on the urinary losses of zinc, copper, iron, and calcium. Limited experience to date in man has revealed no significant adverse side effects of DMSA. In animals, DMSA will promptly reduce the concentration of lead in brain and kidney, in particular. By contrast, similar 5-day courses of CaNa2EDTA do not produce any net reduction in brain lead. This is important, as the brain is the critical organ of the adverse effects of lead in children. If the efficacy of DMSA is to be comprehensively evaluated ethically in children, new and more sensitive neurochemical, electrophysiologic, or other markers must be developed.

摘要

在铅中毒的整体长期管理中,螯合疗法可带来短期益处;然而,若要获得任何长期益处,这些益处必须伴随着大幅减少环境铅暴露。本讨论仅限于过去38年来一直是铅中毒治疗主要手段的螯合剂乙二胺四乙酸二钠钙(CaNa2EDTA),以及一种新的、有前景的口服螯合剂——内消旋-2,3-二巯基丁二酸(DMSA),它是一种孤儿药,目前被美国食品药品监督管理局列为研究性新药。对于这两种药物,若要大幅降低体内铅负荷,都需要多个疗程的治疗。CaNa2EDTA的一个主要局限性是它会导致大量锌随尿液排出。DMSA能使铅随尿液排出量相当,能更大程度地降低血铅水平,且对锌、铜、铁和钙的尿流失影响可忽略不计。迄今为止在人体的有限经验表明,DMSA没有明显的不良副作用。在动物实验中,DMSA尤其能迅速降低大脑和肾脏中的铅浓度。相比之下,类似的5天疗程的CaNa2EDTA并不会使大脑中的铅有任何净减少。这一点很重要,因为大脑是铅对儿童产生不良影响的关键器官。若要在儿童中对DMSA的疗效进行全面的伦理评估,必须开发新的、更敏感的神经化学、电生理或其他标志物。

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