Your search keyword '"Hampton, Mark B."' showing total 18 results

1. Oxidation of caspase-8 by hypothiocyanous acid enables TNF-mediated necroptosis

Author

Bozonet, Stephanie M., Magon, Nicholas J., Schwartfeger, Abigail J., Konigstorfer, Andreas, Heath, Sarah G., Vissers, Margreet C.M., Morris, Vanessa K., Göbl, Christoph, Murphy, James M., Salvesen, Guy S., and Hampton, Mark B.

Published

2023

2. A newly identified flavoprotein disulfide reductase Har protects Streptococcus pneumoniae against hypothiocyanous acid

Author

Shearer, Heather L., primary, Pace, Paul E., additional, Paton, James C., additional, Hampton, Mark B., additional, and Dickerhof, Nina, additional

Published

2022

3. Inhibition of DNA methylation in proliferating human lymphoma cells by immune cell oxidants

Author

O'Connor, Karina M., primary, Das, Andrew B., additional, Winterbourn, Christine C., additional, and Hampton, Mark B., additional

Published

2020

4. Structure-function analyses of alkylhydroperoxidase D from Streptococcus pneumoniae reveal an unusual three-cysteine active site architecture

Author

Meng, Yanxiang, primary, Sheen, Campbell R., additional, Magon, Nicholas J., additional, Hampton, Mark B., additional, and Dobson, Renwick C.J., additional

Published

2020

5. Exposure of Pseudomonas aeruginosa to bactericidal hypochlorous acid during neutrophil phagocytosis is compromised in cystic fibrosis

Author

Dickerhof, Nina, primary, Isles, Vivienne, additional, Pattemore, Philip, additional, Hampton, Mark B., additional, and Kettle, Anthony J., additional

Published

2019

6. Thioredoxin reductase 1 and NADPH directly protect protein tyrosine phosphatase 1B from inactivation during H2O2 exposure

Author

Dagnell, Markus, primary, Pace, Paul E., additional, Cheng, Qing, additional, Frijhoff, Jeroen, additional, Östman, Arne, additional, Arnér, Elias S.J., additional, Hampton, Mark B., additional, and Winterbourn, Christine C., additional

Published

2017

7. Myeloperoxidase-dependent Lipid Peroxidation Promotes the Oxidative Modification of Cytosolic Proteins in Phagocytic Neutrophils

Author

Wilkie-Grantham, Rachel P., primary, Magon, Nicholas J., additional, Harwood, D. Tim, additional, Kettle, Anthony J., additional, Vissers, Margreet C., additional, Winterbourn, Christine C., additional, and Hampton, Mark B., additional

Published

2015

8. Hyperoxidation of Peroxiredoxins 2 and 3

Author

Peskin, Alexander V., primary, Dickerhof, Nina, additional, Poynton, Rebecca A., additional, Paton, Louise N., additional, Pace, Paul E., additional, Hampton, Mark B., additional, and Winterbourn, Christine C., additional

Published

2013

9. Model for the Exceptional Reactivity of Peroxiredoxins 2 and 3 with Hydrogen Peroxide

Author

Nagy, Péter, primary, Karton, Amir, additional, Betz, Andrea, additional, Peskin, Alexander V., additional, Pace, Paul, additional, O'Reilly, Robert J., additional, Hampton, Mark B., additional, Radom, Leo, additional, and Winterbourn, Christine C., additional

Published

2011

10. Direct Modification of the Proinflammatory Cytokine Macrophage Migration Inhibitory Factor by Dietary Isothiocyanates

Author

Brown, Kristin K., primary, Blaikie, Frances H., additional, Smith, Robin A.J., additional, Tyndall, Joel D.A., additional, Lue, Hongqi, additional, Bernhagen, Jürgen, additional, Winterbourn, Christine C., additional, and Hampton, Mark B., additional

Published

2009

11. The High Reactivity of Peroxiredoxin 2 with H2O2 Is Not Reflected in Its Reaction with Other Oxidants and Thiol Reagents

Author

Peskin, Alexander V., primary, Low, Felicia M., additional, Paton, Louise N., additional, Maghzal, Ghassan J., additional, Hampton, Mark B., additional, and Winterbourn, Christine C., additional

Published

2007

12. Modeling the Reactions of Superoxide and Myeloperoxidase in the Neutrophil Phagosome

Author

Winterbourn, Christine C., primary, Hampton, Mark B., additional, Livesey, John H, additional, and Kettle, Anthony J., additional

Published

2006

13. Diphenyleneiodonium Triggers the Efflux of Glutathione from Cultured Cells

Author

Pullar, Juliet M., primary and Hampton, Mark B., additional

Published

2002

14. Chlorination of Bacterial and Neutrophil Proteins during Phagocytosis and Killing of Staphylococcus aureus

Author

Chapman, Anna L.P., primary, Hampton, Mark B., additional, Senthilmohan, Revathy, additional, Winterbourn, Christine C., additional, and Kettle, Anthony J., additional

Published

2002

15. Regulation of Apoptosis by Vitamin C

Author

Vissers, Margret C.M., primary, Lee, Wai-Gin, additional, and Hampton, Mark B., additional

Published

2001

16. Structure-function analyses of alkylhydroperoxidase D from Streptococcus pneumoniae reveal an unusual three-cysteine active site architecture.

Author

Yanxiang Meng, Sheen, Campbell R., Magon, Nicholas J., Hampton, Mark B., and Dobson, Renwick C. J.

Subjects

*STREPTOCOCCUS pneumoniae, *QUATERNARY structure, *HYDROGEN peroxide, *MYCOBACTERIUM tuberculosis, *ARCHITECTURE, *CRYSTAL structure, *CHARGE exchange

Abstract

During aerobic growth, the Gram-positive facultative anaerobe and opportunistic human pathogen Streptococcus pneumoniae generates large amounts of hydrogen peroxide that can accumulate to millimolar concentrations. The mechanism by which this catalase-negative bacterium can withstand endogenous hydrogen peroxide is incompletely understood. The enzyme alkylhydroperoxidase D (AhpD) has been shown to contribute to pneumococcal virulence and oxidative stress responses in vivo. We demonstrate here that SpAhpD exhibits weak thiol-dependent peroxidase activity and, unlike the previously reported Mycobacterium tuberculosis AhpC/D system, SpAhpD does not mediate electron transfer to SpAhpC. A 2.3-Å resolution crystal structure revealed several unusual structural features, including a three-cysteine active site architecture that is buried in a deep pocket, in contrast to the two-cysteine active site found in other AhpD enzymes. All single-cysteine SpAhpD variants remained partially active, and LC-MS/MS analyses revealed that the third cysteine, Cys-163, formed disulfide bonds with either of two cysteines in the canonical Cys-78-X-X-Cys-81 motif. We observed that SpAhpD formed a dimeric quaternary structure both in the crystal and in solution, and that the highly conserved Asn-76 of the AhpD core motif is important for SpAhpD folding. In summary, SpAhpD is a weak peroxidase and does not transfer electrons to AhpC, and therefore does not fit existing models of bacterial AhpD antioxidant defense mechanisms. We propose that it is unlikely that SpAhpD removes peroxides either directly or via AhpC, and that SpAhpD cysteine oxidation may act as a redox switch or mediate electron transfer with other thiol proteins. [ABSTRACT FROM AUTHOR]

Published

2020

17. Thioredoxin reductase 1 and NADPH directly protect protein tyrosine phosphatase 1B from inactivation during H2O2 exposure.

Author

Dagnell, Markus, Pace, Paul E., Qing Cheng, Frijhoff, Jeroen, Östman, Arne, Arnér, Elias S. J., Hampton, Mark B., and Winterbourn, Christine C.

Subjects

*THIOREDOXIN reductase (NADPH), *PROTEIN-tyrosine phosphatase, *ANTIOXIDANTS, *FIBROBLASTS, *SELENOCYSTEINE

Abstract

Regulation of growth factor signaling involves reversible inactivation of protein tyrosine phosphatases (PTPs) through the oxidation and reduction of their active site cysteine. However, there is limited mechanistic understanding of these redox events and their co-ordination in the presence of cellular antioxidant networks. Here we investigated interactions between PTP1B and the peroxiredoxin 2 (Prx2)/thioredoxin 1 (Trx1)/thioredoxin reductase 1 (TrxR1) network. We found that Prx2 becomes oxidized in PDGF-treated fibroblasts, but only when TrxR1 has first been inhibited. Using purified proteins, we also found that PTP1B is relatively insensitive to inactivation by H2O2 but found no evidence for a relay mechanism in which Prx2 or Trx1 facilitates PTP1B oxidation. Instead, these proteins prevented PTP1B inactivation by H2O2. Intriguingly, we discovered that TrxR1/NADPH directly protects PTP1B from inactivation when present during the H2O2 exposure. This protection was dependent on the concentration of TrxR1 and independent of Trx1 and Prx2. The protection was blocked by auranofin and required an intact selenocysteine residue in TrxR1. This activity likely involves reduction of the sulfenic acid intermediate form of PTP1B by TrxR1 and is therefore distinct from the previously described reactivation of end-point oxidized PTP1B, which requires both Trx1 and TrxR1. The ability of TrxR1 to directly reduce an oxidized phosphatase is a novel activity that can help explain previously observed increases in PTP1 Boxidation and PDGF receptor phosphorylation in TrxR1 knockout cells. The activity of TrxR1 is therefore of potential relevance for understanding the mechanisms of redox regulation of growth factor signaling pathways. [ABSTRACT FROM AUTHOR]

Published

2017

18. Thioredoxin reductase 1 and NADPH directly protect protein tyrosine phosphatase 1B from inactivation during H 2 O 2 exposure.

Author

Dagnell M, Pace PE, Cheng Q, Frijhoff J, Östman A, Arnér ESJ, Hampton MB, and Winterbourn CC

Subjects

Animals, Auranofin pharmacology, Catalytic Domain, Cells, Cultured, Dimerization, Embryo, Mammalian cytology, Homeodomain Proteins chemistry, Homeodomain Proteins genetics, Homeodomain Proteins metabolism, Humans, Hydrogen Peroxide pharmacology, Mice, Oxidants pharmacology, Oxidation-Reduction, Peptide Fragments chemistry, Peptide Fragments genetics, Peptide Fragments metabolism, Protein Interaction Domains and Motifs, Protein Tyrosine Phosphatase, Non-Receptor Type 1 antagonists & inhibitors, Protein Tyrosine Phosphatase, Non-Receptor Type 1 genetics, Rats, Receptor-Like Protein Tyrosine Phosphatases, Class 3 chemistry, Receptor-Like Protein Tyrosine Phosphatases, Class 3 genetics, Recombinant Fusion Proteins chemistry, Recombinant Fusion Proteins metabolism, Selenocysteine chemistry, Selenocysteine metabolism, Thioredoxin Reductase 1 antagonists & inhibitors, Thioredoxin Reductase 1 chemistry, Thioredoxin Reductase 1 genetics, Thioredoxins chemistry, Thioredoxins genetics, Thioredoxins metabolism, NADP metabolism, Protein Tyrosine Phosphatase, Non-Receptor Type 1 metabolism, Receptor-Like Protein Tyrosine Phosphatases, Class 3 metabolism, Thioredoxin Reductase 1 metabolism

Abstract

Regulation of growth factor signaling involves reversible inactivation of protein tyrosine phosphatases (PTPs) through the oxidation and reduction of their active site cysteine. However, there is limited mechanistic understanding of these redox events and their co-ordination in the presence of cellular antioxidant networks. Here we investigated interactions between PTP1B and the peroxiredoxin 2 (Prx2)/thioredoxin 1 (Trx1)/thioredoxin reductase 1 (TrxR1) network. We found that Prx2 becomes oxidized in PDGF-treated fibroblasts, but only when TrxR1 has first been inhibited. Using purified proteins, we also found that PTP1B is relatively insensitive to inactivation by H 2 O 2 but found no evidence for a relay mechanism in which Prx2 or Trx1 facilitates PTP1B oxidation. Instead, these proteins prevented PTP1B inactivation by H 2 O 2 Intriguingly, we discovered that TrxR1/NADPH directly protects PTP1B from inactivation when present during the H 2 O 2 exposure. This protection was dependent on the concentration of TrxR1 and independent of Trx1 and Prx2. The protection was blocked by auranofin and required an intact selenocysteine residue in TrxR1. This activity likely involves reduction of the sulfenic acid intermediate form of PTP1B by TrxR1 and is therefore distinct from the previously described reactivation of end-point oxidized PTP1B, which requires both Trx1 and TrxR1. The ability of TrxR1 to directly reduce an oxidized phosphatase is a novel activity that can help explain previously observed increases in PTP1B oxidation and PDGF receptor phosphorylation in TrxR1 knockout cells. The activity of TrxR1 is therefore of potential relevance for understanding the mechanisms of redox regulation of growth factor signaling pathways., (© 2017 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2017