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- W2344492324 abstract "Many viruses induce oxidative stress and cause S-glutathionylation of Cys residues of the host and viral proteins. Changes in cell functioning during viral infection may be associated with glutathionylation of a number of key proteins including Na,K-ATPase which creates a gradient of sodium and potassium ions. It was found that Na,K-ATPase α -subunit has a basal glutathionylation which is not abrogated by reducing agent. We have shown that acute hypoxia leads to increase of total glutathionylation level of Na,K-ATPase α -subunit; however, basal glutathionylation of α -subunit increases under prolonged hypoxia only. The role of basal glutathionylation in Na,K-ATPase function remains unclear. Understanding significance of basal glutathionylation is complicated by the fact that there are no X-ray structures of Na,K-ATPase with the identified glutathione molecules. We have analyzed all X-ray structures of the Na,K-ATPase α -subunit from pig kidney and found that there are a number of isolated cavities with unresolved electron density close to the relevant cysteine residues. Analysis of the structures showed that this unresolved density in the structure can be occupied by glutathione associated with cysteine residues. Here, we discuss the role of basal glutathionylation of Na,K-ATPase α -subunit and provide evidence supporting the view that this modification is cotranslational." @default.
- W2344492324 created "2016-06-24" @default.
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- W2344492324 date "2016-01-01" @default.
- W2344492324 modified "2023-10-16" @default.
- W2344492324 title "Basal Glutathionylation of Na,K-ATPase<i>α</i>-Subunit Depends on Redox Status of Cells during the Enzyme Biosynthesis" @default.
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- W2344492324 doi "https://doi.org/10.1155/2016/9092328" @default.
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