Up-regulation of glutathione-related genes and enzyme activities in cultured human cells by sub-lethal concentrations of inorganic arsenic
Version 2 2024-09-17, 02:06Version 2 2024-09-17, 02:06
Version 1 2023-05-16, 18:34Version 1 2023-05-16, 18:34
journal contribution
posted on 2024-09-17, 02:06authored byM Schuliga, S Chouchane, ET Snow
Inorganic arsenic (iAs), a known human carcinogen, acts as a tumor promoter in part by inducing a rapid burst of reactive oxygen species (ROS) in mammalian cells. This causes oxidative stress and a subsequent increase in the level of cellular glutathione (GSH). Glutathione, a ubiquitous reducing sulfhydryl tripeptide, is involved in ROS detoxification and its increase may be part of an adaptive response to the oxidative stress. Glutathione related enzymes including glutathione reductase (GR) and glutathione S-transferase (GST) also play key roles in these processes. In this study the regulatory effects of inorganic arsenite (AsIII) on the activities of GSH-related enzymes were investigated in cultured human keratinocytes. Substantial increases in GR enzyme activity and mRNA levels were shown in keratinocytes and other human cell lines after exposure to low, subtoxic, micromolar concentrations of AsIII for 24 h. Upregulation of GSH synthesis paralleled the upregulation of GR as shown by increases in glutamate-cysteine lyase (GCL) enzyme activity and mRNA levels, cystine uptake, and intracellular GSH levels. Glutathione S-transferase activity was also shown to increase slightly in keratinocytes, but not in fibroblasts or breast tumor cells. Overall the results show that sublethal arsenic induces a multicomponent response in human keratinocytes that involves upregulation of parts, but not all of the GSH system and counteracts the acute toxic effects of iAs. The upregulation of GR has not previously been shown to be an integral part of this response, although GR is critical for maintaining levels of reduced GSH.
History
Publication title
Toxicological Sciences
Volume
70
Issue
2
Pagination
183-192
ISSN
1096-6080
Department/School
Health Sciences
Publisher
Oxford University Press
Publication status
Published
Place of publication
Oxford
Socio-economic Objectives
200499 Public health (excl. specific population health) not elsewhere classified