Potential role of glutathione in evolution of thiol-based redox signaling sites in proteins

Cysteine is susceptible to a variety of modifications by reactive oxygen and nitrogen oxide species, including glutathionylation; and when two cysteines are involved, disulfide formation. Glutathione-cysteine adducts may be removed from proteins by glutaredoxin, whereas disulfides may be reduced by...

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Autores principales: Mohanasundaram, Kaavya A., Haworth, Naomi L., Grover, Mani P., Crowley, Tamsyn M., Goscinski, Andrzej, Wouters, Merridee A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2015
Materias:
Pharmacology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4354306/
https://www.ncbi.nlm.nih.gov/pubmed/25805991
http://dx.doi.org/10.3389/fphar.2015.00001
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author Mohanasundaram, Kaavya A.
Haworth, Naomi L.
Grover, Mani P.
Crowley, Tamsyn M.
Goscinski, Andrzej
Wouters, Merridee A.
author_facet Mohanasundaram, Kaavya A.
Haworth, Naomi L.
Grover, Mani P.
Crowley, Tamsyn M.
Goscinski, Andrzej
Wouters, Merridee A.
author_sort Mohanasundaram, Kaavya A.
collection PubMed
description Cysteine is susceptible to a variety of modifications by reactive oxygen and nitrogen oxide species, including glutathionylation; and when two cysteines are involved, disulfide formation. Glutathione-cysteine adducts may be removed from proteins by glutaredoxin, whereas disulfides may be reduced by thioredoxin. Glutaredoxin is homologous to the disulfide-reducing thioredoxin and shares similar binding modes of the protein substrate. The evolution of these systems is not well characterized. When a single Cys is present in a protein, conjugation of the redox buffer glutathione may induce conformational changes, resulting in a simple redox switch that effects a signaling cascade. If a second cysteine is introduced into the sequence, the potential for disulfide formation exists. In favorable protein contexts, a bistable redox switch may be formed. Because of glutaredoxin's similarities to thioredoxin, the mutated protein may be immediately exapted into the thioredoxin-dependent redox cycle upon addition of the second cysteine. Here we searched for examples of protein substrates where the number of redox-active cysteine residues has changed throughout evolution. We focused on cross-strand disulfides (CSDs), the most common type of forbidden disulfide. We searched for proteins where the CSD is present, absent and also found as a single cysteine in protein orthologs. Three different proteins were selected for detailed study—CD4, ERO1, and AKT. We created phylogenetic trees, examining when the CSD residues were mutated during protein evolution. We posit that the primordial cysteine is likely to be the cysteine of the CSD which undergoes nucleophilic attack by thioredoxin. Thus, a redox-active disulfide may be introduced into a protein structure by stepwise mutation of two residues in the native sequence to Cys. By extension, evolutionary acquisition of structural disulfides in proteins can potentially occur via transition through a redox-active disulfide state.
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spelling pubmed-43543062015-03-24 Potential role of glutathione in evolution of thiol-based redox signaling sites in proteins Mohanasundaram, Kaavya A. Haworth, Naomi L. Grover, Mani P. Crowley, Tamsyn M. Goscinski, Andrzej Wouters, Merridee A. Front Pharmacol Pharmacology Cysteine is susceptible to a variety of modifications by reactive oxygen and nitrogen oxide species, including glutathionylation; and when two cysteines are involved, disulfide formation. Glutathione-cysteine adducts may be removed from proteins by glutaredoxin, whereas disulfides may be reduced by thioredoxin. Glutaredoxin is homologous to the disulfide-reducing thioredoxin and shares similar binding modes of the protein substrate. The evolution of these systems is not well characterized. When a single Cys is present in a protein, conjugation of the redox buffer glutathione may induce conformational changes, resulting in a simple redox switch that effects a signaling cascade. If a second cysteine is introduced into the sequence, the potential for disulfide formation exists. In favorable protein contexts, a bistable redox switch may be formed. Because of glutaredoxin's similarities to thioredoxin, the mutated protein may be immediately exapted into the thioredoxin-dependent redox cycle upon addition of the second cysteine. Here we searched for examples of protein substrates where the number of redox-active cysteine residues has changed throughout evolution. We focused on cross-strand disulfides (CSDs), the most common type of forbidden disulfide. We searched for proteins where the CSD is present, absent and also found as a single cysteine in protein orthologs. Three different proteins were selected for detailed study—CD4, ERO1, and AKT. We created phylogenetic trees, examining when the CSD residues were mutated during protein evolution. We posit that the primordial cysteine is likely to be the cysteine of the CSD which undergoes nucleophilic attack by thioredoxin. Thus, a redox-active disulfide may be introduced into a protein structure by stepwise mutation of two residues in the native sequence to Cys. By extension, evolutionary acquisition of structural disulfides in proteins can potentially occur via transition through a redox-active disulfide state. Frontiers Media S.A. 2015-03-10 /pmc/articles/PMC4354306/ /pubmed/25805991 http://dx.doi.org/10.3389/fphar.2015.00001 Text en Copyright © 2015 Mohanasundaram, Haworth, Grover, Crowley, Goscinski and Wouters. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) or licensor are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Pharmacology
Mohanasundaram, Kaavya A.
Haworth, Naomi L.
Grover, Mani P.
Crowley, Tamsyn M.
Goscinski, Andrzej
Wouters, Merridee A.
Potential role of glutathione in evolution of thiol-based redox signaling sites in proteins
title Potential role of glutathione in evolution of thiol-based redox signaling sites in proteins
title_full Potential role of glutathione in evolution of thiol-based redox signaling sites in proteins
title_fullStr Potential role of glutathione in evolution of thiol-based redox signaling sites in proteins
title_full_unstemmed Potential role of glutathione in evolution of thiol-based redox signaling sites in proteins
title_short Potential role of glutathione in evolution of thiol-based redox signaling sites in proteins
title_sort potential role of glutathione in evolution of thiol-based redox signaling sites in proteins
topic Pharmacology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4354306/
https://www.ncbi.nlm.nih.gov/pubmed/25805991
http://dx.doi.org/10.3389/fphar.2015.00001
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