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不稳定复合物促进 Caco-2 细胞摄取镉。

Labile complexes facilitate cadmium uptake by Caco-2 cells.

机构信息

Division of Soil and Water Management, K.U.Leuven, Kasteelpark Arenberg 20, Box 2459, 3001 Heverlee, Belgium.

出版信息

Sci Total Environ. 2012 Jun 1;426:90-9. doi: 10.1016/j.scitotenv.2012.03.044. Epub 2012 Apr 12.

DOI:10.1016/j.scitotenv.2012.03.044
PMID:22503671
Abstract

The Free Ion Activity Model (FIAM) predicts that metal uptake in biota is related to the free ion activity in the external solution and that metal complexes do not contribute. However, studies with plants have shown that labile metal complexes enhance metal bioavailability when the uptake is rate-limited by transport of the free ion in solution to the uptake site. Here, the role of labile complexes of Cd on metal bioavailability was assessed using Caco-2 cells, the cell model for intestinal absorption. At low Cd(2+) concentration (1 nM), the CdCl(n)(2-n) complexes contributed to the uptake almost to the same extent as the free ion. At large Cd(2+) concentration (10 μM), the contribution of the complexes was much smaller. At constant Cd(2+) concentration, Cd intake in the cells from solutions containing synthetic ligands such as EDTA increased as the dissociation rate of the cadmium complexes increased, and correlated well with the Cd diffusion flux in solution measured with the Diffusive Gradient in Thin Films technique (DGT). The Cd intake fluxes in the cells were well predicted assuming that the specific uptake is limited by diffusion of the free Cd(2+) ion to the cell surface. Our results underline that speciation of Cd has a major effect on its uptake by intestinal cells, but the availability is not simply related to the free ion concentration. Labile complexes of Cd enhance metal bioavailability in these cells, likely by alleviating diffusive limitations.

摘要

自由离子活度模型(FIAM)预测生物体内金属的摄取与外部溶液中的自由离子活度有关,而金属配合物没有贡献。然而,植物研究表明,当摄取受到溶液中自由离子向摄取部位运输的限制时,不稳定的金属配合物可增强金属的生物利用度。在这里,使用 Caco-2 细胞(肠吸收的细胞模型)评估了 Cd 的不稳定配合物对金属生物利用度的作用。在低 Cd(2+)浓度(1 nM)下,CdCl(n)(2-n)配合物对摄取的贡献几乎与自由离子相同。在大 Cd(2+)浓度(10 μM)下,配合物的贡献要小得多。在恒定的 Cd(2+)浓度下,来自含有 EDTA 等合成配体的溶液中的细胞 Cd 摄入量随着镉配合物的离解速率增加而增加,并且与用薄膜扩散梯度技术(DGT)测量的溶液中 Cd 扩散通量很好地相关。假设特定的摄取受到向细胞表面扩散的自由 Cd(2+)离子的限制,那么细胞中的 Cd 摄取通量可以很好地预测。我们的结果强调了 Cd 的形态对肠细胞摄取的影响很大,但可用性与自由离子浓度无关。Cd 的不稳定配合物通过减轻扩散限制,增强了这些细胞中金属的生物利用度。

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