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Real-time monitoring of redox changes in the mammalian endoplasmic reticulum

机译:实时监测哺乳动物内质网氧化还原变化

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摘要

Redox-sensitive GFPs with engineered disulphide bonds have been used previously to monitor redox status in the cytosol and mitochondria of living cells. The usefulness of these redox probes depends on the reduction potential of the disulphide, with low values suiting the cytosol and mitochondrion, and higher values suiting the more oxidising environment of the endoplasmic reticulum (ER). Here, we targeted a modified redox-sensitive GFP (roGFP1-iL), with a relatively high reduction potential, to the ER of mammalian cells. We showed that the disulphide is partially oxidised, allowing roGFP1-iL to monitor changes in ER redox status. When cells were treated with puromycin, the redox balance became more reducing, suggesting that the release of nascent chains from ribosomes alters the ER redox balance. In addition, downregulating Ero1α prevented normal rapid recovery from dithiothreitol (DTT), whereas downregulating peroxiredoxin IV had no such effect. This result illustrates the contribution of the Ero1α oxidative pathway to ER redox balance. This first report of the use of roGFP to study the ER of mammalian cells demonstrates that roGFP1-iL can be used to monitor real-time changes to the redox status in individual living cells.
机译:具有工程二硫键的氧化还原敏感的GFP以前已用于监视活细胞的细胞质和线粒体中的氧化还原状态。这些氧化还原探针的有用性取决于二硫化物的还原电位,低值适合于细胞质和线粒体,高值适合于内质网(ER)的更氧化的环境。在这里,我们针对哺乳动物细胞的ER靶向具有较高还原潜力的修饰的氧化还原敏感GFP(roGFP1-iL)。我们表明二硫化物被部分氧化,从而使roGFP1-iL可以监测ER氧化还原状态的变化。当用嘌呤霉素处理细胞时,氧化还原平衡变得更加减少,这表明从核糖体释放新生链会改变ER氧化还原平衡。此外,下调Ero1α不能正常地从二硫苏糖醇(DTT)中恢复,而下调过氧化物酶IV则没有这种作用。该结果说明了Ero1α氧化途径对ER氧化还原平衡的贡献。关于使用roGFP研究哺乳动物细胞ER的第一份报告表明,roGFP1-iL可用于监测单个活细胞中氧化还原状态的实时变化。

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