Effects of cadmium and uranium on some in vitro renal targets

被引:29
作者
L'Azou, B
Henge-Napoli, MH
Minaro, L
Mirto, H
Barrouillet, MP
Cambar, J
机构
[1] Univ Victor Segalen, UFR Pharm, Biol Cellulaire Lab, F-33076 Bordeaux, France
[2] Inst Protect & Surete Nucl, DPHP, SDOS, Fontenay Aux Roses, France
关键词
cadmium; cytotoxicity; environmental factors; in vitro models; uranium;
D O I
10.1023/A:1019536115152
中图分类号
Q2 [细胞生物学];
学科分类号
071009 ; 090102 ;
摘要
Metals are major pollutants not only in occupational settings but also in the general environment. Chronic exposure of workers has been related to severe damage, especially at the renal level. While toxic compounds such as metals are well known to severely impair tubular functions, it is clear that nephrotoxicants can act on various other renal targets, i.e., vascular and glomerular ones. In vitro models are available to assess these toxicities and can be used to better understand the different cell targets. This paper summarizes data obtained in our laboratory after exposure of isolated renal structures such as glomeruli, and cell cultures such as glomerular mesangial and tubular epithelial cells, to cadmium and uranium. Morphometric studies by image analysis of isolated glomeruli and mesangial cultured cells showed that cadmium and uranium induced a dose- and time-dependent glomerular contraction accompanied by disorganization of the cytoskeleton. Classical viability tests demonstrated various factors influencing the metal toxicity. The important roles of pH, extracellular protein concentrations and the nature of the anion accompanying the metal were demonstrated. These data obtained in in vitro models provide better understanding of the cytotoxicity after metal uptake and accumulation in glomerular and tubular cells. Moreover, the glomerular and tubular cytotoxicity they induce may be correlated with severe renal hemodynamic changes in vivo. Finally, we briefly present eventual improvements for in vitro renal models by the use of new cell models such as immortalized human cell lines or by the introduction of porous supports and perifusion devices.
引用
收藏
页码:329 / 340
页数:12
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