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首页> 外文期刊>Journal of health science. >Metal Response Element-binding Transcription Factor-1 Is Activated by Degradation of Metallothionein
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Metal Response Element-binding Transcription Factor-1 Is Activated by Degradation of Metallothionein

机译:金属硫蛋白的降解激活金属反应元素结合转录因子-1。

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摘要

Cytosolic zinc-binding protein, metallothionein (MT), is normally saturated with Zn. It is thought that Zn-saturated MT (Zn-MT) acts as a major intracellular Zn pool. Metal-response element-binding transcription factor-1 (MTF-1) plays an important role in Zn-mediated MT transcription. Here, we showed that degradation of Zn-MT activates MTF-1. We measured activated MTF-1 using an electrophoretic mobility shift assay. Interleukin-6 induced MT expression and increased MTF-1 activity. MTF-1 activation was not observed in MT-overexpressing cells. MT-dependent MTF-1 activation was observed only after treating MT-overexpressing cells with cyclohex-imide (CHX), a protein synthesis inhibitor. CHX-treatment increased the degradation/synthesis ratio of protein. An increase in the degradation/synthesis ratio for the MT protein is expected to increase the level of labile Zn and activate MTF-1. Recombinant MTF-1 was activated by H_2O_2 only in the presence of Zn-MT. Oxidative stress activated MTF-1 DNA-binding activity in primary cultured hepatocytes but not in MT-deficient hepatocytes. These findings suggest that degradation of Zn-MT activates MTF-1, and that MT plays an important role in zinc-mediated signal transduction.
机译:胞质锌结合蛋白,金属硫蛋白(MT)通常被锌饱和。认为锌饱和MT(Zn-MT)充当主要的细胞内锌库。金属反应元件结合转录因子-1(MTF-1)在锌介导的MT转录中起重要作用。在这里,我们表明Zn-MT的降解激活了MTF-1。我们使用电泳迁移率变动测定法测量了活化的MTF-1。白介素6诱导MT表达并增加MTF-1活性。在MT过表达的细胞中未观察到MTF-1激活。仅在用蛋白合成抑制剂环己酰亚胺(CHX)处理过表达MT的细胞后,才观察到MT依赖性的MTF-1活化。 CHX处理增加了蛋白质的降解/合成比率。预计MT蛋白降解/合成比的增加会增加不稳定Zn的水平并激活MTF-1。仅在Zn-MT存在下,重组MTF-1被H_2O_2激活。氧化应激激活了原代培养的肝细胞中的MTF-1 DNA结合活性,但没有激活MT缺失的肝细胞。这些发现表明,Zn-MT的降解会激活MTF-1,并且MT在锌介导的信号转导中起重要作用。

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