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Metabolism of meso-2,3-dimercaptosuccinic acid in lead-poisoned children and normal adults.

机译:铅中毒儿童和正常成年人的meso-2,3-二巯基琥珀酸代谢。

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摘要

Meso-2,3-dimercaptosuccinic acid (DMSA, or succimer) is an oral chelating agent for heavy-metal poisoning. While studying the urinary elimination of unaltered DMSA, altered DMSA (i.e., its mixed disulfides), and lead in children with lead poisoning, we observed a pattern of urinary drug elimination after meals suggestive of enterohepatic circulation. The excretion of lead in urine patterned the elimination of altered DMSA rather than the parent molecule. In addition, the half-life of elimination of DMSA via the kidney was positively associated with blood lead concentration. Two additional crossover studies of DMSA kinetics were conducted in normal adults to confirm the presence of enterohepatic circulation of DMSA after meals. In one, increases in plasma total DMSA concentration were observed after meals in all six subjects; these increases were prevented by cholestyramine administration 4, 8, and 12 hr after DMSA. In the second, the administration of neomycin also prevented increases in DMSA after meals. These studies indicate that 1) a metabolite(s) of DMSA undergoes enterohepatic circulation and that microflora are required for DMSA reentry; 2) in children, moderate lead exposure impairs renal tubular drug elimination; and 3) a metabolite of DMSA appears to be an active chelator.
机译:Meso-2,3-二巯基琥珀酸(DMSA或琥珀酸酯)是一种用于重金属中毒的口服螯合剂。在研究尿清除未改变的DMSA,改变DMSA(即其混合的二硫化物)以及铅中毒儿童中的铅时,我们观察到饭后尿液清除的模式提示肠肝循环。尿液中铅的排泄形成了消除改变的DMSA而不是母体分子的模式。另外,通过肾脏消除DMSA的半衰期与血铅浓度正相关。在正常成年人中进行了另外两项关于DMSA动力学的交叉研究,以确认饭后DMSA的肝肠循环的存在。在一项研究中,所有六名受试者餐后血浆总DMSA浓度均增加;通过在DMSA后4、8和12小时服用消胆胺可以防止这些增加。第二,新霉素的给药还可以防止饭后DMSA升高。这些研究表明:1)DMSA的代谢产物经历了肝肠循环,并且微生物菌群是DMSA再入所必需的; 2)对于儿童,中度铅暴露会损害肾小管药物的清除; 3)DMSA的代谢产物似乎是一种活性螯合剂。

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