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铅中毒

Lead intoxication.

作者信息

Ibels L S, Pollock C A

出版信息

Med Toxicol. 1986 Nov-Dec;1(6):387-410. doi: 10.1007/BF03259851.

Abstract

Lead intoxication was recognised as early as 2000 BC and the widespread use of lead has been a cause of endemic chronic plumbism in several societies throughout history. In the twentieth century, lead intoxication is still a common problem. In children it is largely due to ingestion of pica and environmental exposure, whereas adult groups at greatest risk are the industrially exposed: thus, screening of these workers should be undertaken at regular intervals. The clinical features of lead intoxication are nonspecific and often go unrecognised. The early manifestations are largely neuropsychiatric, followed by more significant disturbances of the central and peripheral nervous systems, symptomatic gastrointestinal, musculoskeletal, haematological and endocrine abnormalities. The association of lead poisoning with renal disease is well documented and must be considered, particularly if there is associated hypertension and/or gout. Blood lead concentrations are an unreliable predictor of body lead stores as they are indicative only of recent exposure. Haematological parameters have been used to assess those at risk of toxicity, but although more reliable than blood concentrations, they also fail to predict those patients at risk of toxicity. The recommended assessment for patients with suspected lead intoxication is a calcium disodium edetate chelation test, which is a sensitive marker for assessing body stores and subsequent intoxication. In children the dosage should be 50 mg/kg up to 1000 mg, and in adults 1000 mg administered intravenously or 2000 mg intramuscularly in divided doses 12 hours apart with subsequent 72 hour urinary lead estimations. Lead excretion levels greater than 350 micrograms/72 hours should be considered as suggestive of intoxication, particularly if supported by historical, clinical or biochemical evidence of lead exposure. Treatment of patients with positive chelation tests involves symptomatic treatment and a course of chelation therapy utilising calcium disodium edetate in doses similar to those used for testing, and in the more severely intoxicated patient, the addition of dimercaprol in doses of 75 mg/m2 every 4 hours to a total of 300 mg/m2/day. The safety of these treatment regimens is well documented.

摘要

早在公元前2000年就已认识到铅中毒,在历史上的几个社会中,铅的广泛使用一直是地方性慢性铅中毒的一个原因。在20世纪,铅中毒仍然是一个常见问题。在儿童中,主要是由于异食癖和环境暴露导致摄入铅,而风险最大的成年人群是工业接触者:因此,应定期对这些工人进行筛查。铅中毒的临床特征不具有特异性,常常未被识别。早期表现主要是神经精神方面的,随后是中枢和周围神经系统更明显的紊乱、有症状的胃肠道、肌肉骨骼、血液学和内分泌异常。铅中毒与肾脏疾病的关联已有充分记录,必须予以考虑,特别是如果伴有高血压和/或痛风。血铅浓度并不能可靠地预测体内铅储存情况,因为它们仅表明近期的接触情况。血液学参数已被用于评估有中毒风险的人,但尽管比血铅浓度更可靠,但它们也无法预测哪些患者有中毒风险。对于疑似铅中毒的患者,推荐的评估方法是依地酸钙钠螯合试验,这是评估体内铅储存和后续中毒情况的一个敏感指标。儿童的剂量应为50mg/kg,最大剂量为1000mg,成人静脉注射1000mg或分剂量肌肉注射2000mg,每隔12小时一次,随后进行72小时尿铅测定。尿铅排泄水平大于350微克/72小时应被视为提示中毒,特别是如果有铅接触的病史、临床或生化证据支持。螯合试验呈阳性的患者的治疗包括对症治疗和一个疗程的螯合疗法,使用与测试时相似剂量的依地酸钙钠,对于中毒更严重的患者,每4小时添加75mg/m²的二巯丙醇,每天总量为300mg/m²。这些治疗方案的安全性已有充分记录。

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