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Metal‐induced developmental toxicity in mammals: A review

 

作者: J. L. Domingo,  

 

期刊: Journal of Toxicology and Environmental Health  (Taylor Available online 1994)
卷期: Volume 42, issue 2  

页码: 123-141

 

ISSN:0098-4108

 

年代: 1994

 

DOI:10.1080/15287399409531868

 

出版商: Taylor & Francis Group

 

数据来源: Taylor

 

摘要:

It is well established that certain metals are toxic to embryonic and fetal tissues and can induce teratogenicity in mammals. The main objective of this paper has been to summarize the toxic effects that excesses of certain metals may cause on mammalian development. The reviewed elements have been divided into four groups: (a) metals of greatest toxicological significance (arsenic, cadmium, lead, mercury, and uranium) that are widespread in the human environment, (b) essential trace metals (chromium, cobalt, manganese, selenium, and zinc), (c) other metals with evident biological interest (nickel and vanadium), and (d) metals of pharmacological interest (aluminum, gallium, and lithium). A summary of the therapeutic use of chelaling agents in the prevention of metal‐induced developmental toxicity has also been included. meso‐2,3‐Dimercaptosuccinic acid (DMSA) and sodium 2,3‐dimercaptopropane‐1‐sulfonate (DMPS) have been reported to be effective in alleviating arsenic‐ and mercury‐induced teratogenesis, whereas sodium 4,5‐dihydroxybenzene‐1,3‐disulfonate (Tiron) would protect against vanadium‐ and uranium‐induced developmental toxicity.

 

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