首页> 外文期刊>Toxicology in vitro: an international journal published in association with BIBRA >Regulation of metallothioneins and ZnT-1 transporter expression in human hepatoma cells HepG2 exposed to zinc and cadmium.
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Regulation of metallothioneins and ZnT-1 transporter expression in human hepatoma cells HepG2 exposed to zinc and cadmium.

机译:暴露于锌和镉的人肝癌细胞HepG2中金属硫蛋白的调节和ZnT-1转运蛋白的表达。

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摘要

Essential and non-essential metals can affect vital cellular processes, when over-accumulated within the cells. For this reason, cells have evolved multiple protein sensors, transporters, and other type of proteins to regulate and control free metal homeostasis. Among these, metallothioneins (MT) and ZnT-1 transporter play a key role in the regulation of free Zn concentrations. Herewith, MT expression in Zn (170microM) and Cd (0.1 and 10microM) exposed HepG2 cells is analyzed and compared. In addition, the modulation and localization of the membrane transporter ZnT-1 has been investigated. MT-I and MT-II were up-regulated in response to both Zn and Cd exposure and, as expected, Cd represented the most potent inducer. Namely, 0.1microM Cd was able to up-regulate MT-I, and -II in a way comparable to 170microM Zn. This is in agreement with MT general function of metal-chelating protein, acting with higher tolerance to essential metals than to non-essential ones. ZnT-1 protein, a plasma membrane specific Zn transporter, was up-regulated as well by both Zn and Cd, although in the same way. Immunofluorescence technique provided evidence that high levels of ZnT-1 measured by biochemical techniques, are related to an increased localization of the transporter at the plasma membrane.
机译:必需金属和非必需金属在细胞内过度积累时会影响重要的细胞过程。由于这个原因,细胞已经进化出多种蛋白质传感器,转运蛋白和其他类型的蛋白质来调节和控制自由金属稳态。其中,金属硫蛋白(MT)和ZnT-1转运蛋白在调节游离Zn浓度中起关键作用。因此,分析并比较了Zn(170microM)和Cd(0.1和10microM)暴露的HepG2细胞中MT的表达。另外,已经研究了膜转运蛋白ZnT-1的调节和定位。响应于锌和镉的暴露,MT-I和MT-II上调,并且正如所预期的,Cd代表最有效的诱导剂。即,0.1microM Cd能够以与170microM Zn相当的方式上调MT-I和-II。这与金属螯合蛋白的MT一般功能一致,对必需金属的耐受性高于对非必需金属的耐受性。 ZnT-1蛋白(一种质膜特异性Zn转运蛋白)也被Zn和Cd上调,尽管以相同的方式。免疫荧光技术提供了证据,表明通过生化技术检测到的高水平的ZnT-1与转运蛋白在质膜上的定位增加有关。

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