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铅、汞、镉和砷的一般亚细胞效应。

General subcellular effects of lead, mercury, cadmium, and arsenic.

作者信息

Fowler B A

出版信息

Environ Health Perspect. 1978 Feb;22:37-41. doi: 10.1289/ehp.782237.

Abstract

This working paper summarizes the known ultrastructural and biochemical effects of lead, mercury, cadmium, and arsenic on subcellular organelle systems following in vivo administration. Documented metal-induced alterations in nuclear, mitochondrial, microsomal, and lysosomal functions are discussed in relation to their potential impact on cellular responses to other environmental agents. Each of the above elements has been found to interfere with normal cellular replication and genetic processes. Mitochondrial swelling and depression of respiratory function are discussed in relation to known metal-specific perturbations of mitochondrial heme biosynthetic pathway enzymes. Inhibition of microsomal enzyme activities and protein synthesis by lead and mercury is compared to the apparent absence of such effects following arsenic or cadmium exposure. Lysosomal uptake of all the metals is documented, but biochemical alterations in these structures have been reported for only mercury and cadmium. It is concluded that these toxic metals are capable of interacting with, and biochemically altering major cellular systems at dose levels below those required to produce signs of overt metal toxicity. The impact of these effects on cellular response to other metals and xenobiotics in complex exposure situations is presently unknown, and further research is urgently needed in this area.

摘要

本工作论文总结了体内给药后铅、汞、镉和砷对亚细胞器系统已知的超微结构和生化影响。文中讨论了已记录的金属诱导的核、线粒体、微粒体和溶酶体功能改变,并阐述了这些改变对细胞对其他环境因子反应的潜在影响。已发现上述每种元素都会干扰正常的细胞复制和遗传过程。结合线粒体血红素生物合成途径酶已知的金属特异性扰动,讨论了线粒体肿胀和呼吸功能抑制。比较了铅和汞对微粒体酶活性和蛋白质合成的抑制作用与砷或镉暴露后明显不存在此类影响的情况。记录了所有金属被溶酶体摄取的情况,但仅报道了汞和镉会引起这些结构的生化改变。得出的结论是,这些有毒金属能够在低于产生明显金属毒性迹象所需剂量的水平下与主要细胞系统相互作用并对其进行生化改变。目前尚不清楚在复杂暴露情况下这些影响对细胞对其他金属和外源性物质反应的影响,该领域迫切需要进一步研究。

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