antioxidant

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Oxidative Stress in Caenorhabditis Elegans: Protective Effects of the Omega Class Glutathione Transferase (GSTO-1)

Journal Title, Volume, Page: 
The FASEB Journal. 2008;22:343-354
Year of Publication: 
2008
Authors: 
Ayman Hussein
Faculty of Science, An-Najah National University, PO Box 7, Nablus, Palestine, West Bank
Current Affiliation: 
Faculty of Medicine & Health Sciences, Department of Biomedical Sciences, An-Najah National University, Nablus, Palestine
Cora Burmeister
Institute of Animal Physiology, University of Muenster, Germany
Kai Lu¨ersen
Institute of Animal Physiology, University of Muenster, Germany
Alexander Heinick
Institute of Animal Physiology, University of Muenster, Germany
Marzena Domagalski
Bernhard Nocht Institute, Hamburg, Germany
Rolf D. Walter
Bernhard Nocht Institute, Hamburg, Germany
Eva Liebau
Institute of Animal Physiology, University of Muenster, Germany
Preferred Abstract (Original): 

To elucidate the function of Omega class glutathione transferases (GSTs) (EC 2.5.1.18) in multicellular organisms, the GSTO-1 from Caenorhabditis elegans (GSTO-1; C29E4.7) was investigated. Disc diffusion assays using Escherichia coli overexpressing GSTO-1 provided a test of resistance to long-term exposure under oxidative stress. After affinity purification, the recombinant GSTO-1 had minimal catalytic activity toward classic GST substrates but displayed significant thiol oxidoreductase and dehydroascorbate reductase activity. Microinjection of the GSTO-1-promoter green fluorescent protein construct and immunolocalization by electron microscopy localized the protein exclusively in the intestine of all postembryonic stages of C. elegans. Deletion analysis identified an 300-nucleotide sequence upstream of the ATG start site necessary for GSTO-1 expression. Site-specific mutagenesis of a GATA transcription factor binding motif in the minimal promoter led to the loss of reporter expression. Similarly, RNA interference (RNAi) of Elt-2 indicated the involvement of this gut-specific transcription factor in GSTO-1 expression. Transcriptional up-regulation under stress conditions of GSTO-1 was confirmed by analyzing promoter-reporter constructs in transgenic C. elegans strains. To investigate the function of GSTO-1 in vivo, transgenic animals overexpressing GSTO-1 were generated exhibiting an increased resistance to juglone-, paraquat-, and cumene hydroperoxide-induced oxidative stress. Specific silencing of the GSTO-1 by RNAi created worms with an increased sensitivity to several prooxidants, arsenite, and heat shock. We conclude that the stress-responsive GSTO-1 plays a key role in counteracting environmental stress.—Burmeister, C., Lüersen, K., Heinick, A., Hussein, A., Domagalski, M., Walter, R. D., Liebau, E. Oxidative stress in Caenorhabditis elegans: protective effects of the Omega class glutathione transferase (GSTO-1).
 

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