Oxidative cross-linking of calprotectin occurs in vivo, altering its structure and susceptibility to proteolysis

Calprotectin, the major neutrophil protein, is a critical alarmin that modulates inflammation and plays a role in host immunity by strongly binding trace metals essential for bacterial growth. It has two cysteine residues favourably positioned to act as a redox switch. Whether their oxidation occurs...

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Autores principales: Hoskin, Teagan S., Crowther, Jennifer M., Cheung, Jeanette, Epton, Michael J., Sly, Peter D., Elder, Peter A., Dobson, Renwick C.J., Kettle, Anthony J., Dickerhof, Nina
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2019
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6477633/
https://www.ncbi.nlm.nih.gov/pubmed/31015146
http://dx.doi.org/10.1016/j.redox.2019.101202
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author Hoskin, Teagan S.
Crowther, Jennifer M.
Cheung, Jeanette
Epton, Michael J.
Sly, Peter D.
Elder, Peter A.
Dobson, Renwick C.J.
Kettle, Anthony J.
Dickerhof, Nina
author_facet Hoskin, Teagan S.
Crowther, Jennifer M.
Cheung, Jeanette
Epton, Michael J.
Sly, Peter D.
Elder, Peter A.
Dobson, Renwick C.J.
Kettle, Anthony J.
Dickerhof, Nina
author_sort Hoskin, Teagan S.
collection PubMed
description Calprotectin, the major neutrophil protein, is a critical alarmin that modulates inflammation and plays a role in host immunity by strongly binding trace metals essential for bacterial growth. It has two cysteine residues favourably positioned to act as a redox switch. Whether their oxidation occurs in vivo and affects the function of calprotectin has received little attention. Here we show that in saliva from healthy adults, and in lavage fluid from the lungs of patients with respiratory diseases, a substantial proportion of calprotectin was cross-linked via disulfide bonds between the cysteine residues on its S100A8 and S100A9 subunits. Stimulated human neutrophils released calprotectin and subsequently cross-linked it by myeloperoxidase-dependent production of hypochlorous acid. The myeloperoxidase-derived oxidants hypochlorous acid, taurine chloramine, hypobromous acid, and hypothiocyanous acid, all at 10 μM, cross-linked calprotectin (5 μM) via reversible disulfide bonds. Hypochlorous acid generated A9-A9 and A8-A9 cross links. Hydrogen peroxide (10 μM) did not cross-link the protein. Purified neutrophil calprotectin existed as a non-covalent heterodimer of A8/A9 which was converted to a heterotetramer - (A8/A9)(2) - with excess calcium ions. Low level oxidation of calprotectin with hypochlorous acid produced substantial proportions of high order oligomers, whether oxidation occurred before or after addition of calcium ions. At high levels of oxidation the heterodimer could not form tetramers with calcium ions, but prior addition of calcium ions afforded some protection for the heterotetramer. Oxidation and formation of the A8-A9 disulfide cross link enhanced calprotectin's susceptibility to proteolysis by neutrophil proteases. We propose that reversible disulfide cross-linking of calprotectin occurs during inflammation and affects its structure and function. Its increased susceptibility to proteolysis will ultimately result in a loss of function.
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spelling pubmed-64776332019-04-26 Oxidative cross-linking of calprotectin occurs in vivo, altering its structure and susceptibility to proteolysis Hoskin, Teagan S. Crowther, Jennifer M. Cheung, Jeanette Epton, Michael J. Sly, Peter D. Elder, Peter A. Dobson, Renwick C.J. Kettle, Anthony J. Dickerhof, Nina Redox Biol Research Paper Calprotectin, the major neutrophil protein, is a critical alarmin that modulates inflammation and plays a role in host immunity by strongly binding trace metals essential for bacterial growth. It has two cysteine residues favourably positioned to act as a redox switch. Whether their oxidation occurs in vivo and affects the function of calprotectin has received little attention. Here we show that in saliva from healthy adults, and in lavage fluid from the lungs of patients with respiratory diseases, a substantial proportion of calprotectin was cross-linked via disulfide bonds between the cysteine residues on its S100A8 and S100A9 subunits. Stimulated human neutrophils released calprotectin and subsequently cross-linked it by myeloperoxidase-dependent production of hypochlorous acid. The myeloperoxidase-derived oxidants hypochlorous acid, taurine chloramine, hypobromous acid, and hypothiocyanous acid, all at 10 μM, cross-linked calprotectin (5 μM) via reversible disulfide bonds. Hypochlorous acid generated A9-A9 and A8-A9 cross links. Hydrogen peroxide (10 μM) did not cross-link the protein. Purified neutrophil calprotectin existed as a non-covalent heterodimer of A8/A9 which was converted to a heterotetramer - (A8/A9)(2) - with excess calcium ions. Low level oxidation of calprotectin with hypochlorous acid produced substantial proportions of high order oligomers, whether oxidation occurred before or after addition of calcium ions. At high levels of oxidation the heterodimer could not form tetramers with calcium ions, but prior addition of calcium ions afforded some protection for the heterotetramer. Oxidation and formation of the A8-A9 disulfide cross link enhanced calprotectin's susceptibility to proteolysis by neutrophil proteases. We propose that reversible disulfide cross-linking of calprotectin occurs during inflammation and affects its structure and function. Its increased susceptibility to proteolysis will ultimately result in a loss of function. Elsevier 2019-04-13 /pmc/articles/PMC6477633/ /pubmed/31015146 http://dx.doi.org/10.1016/j.redox.2019.101202 Text en © 2019 The Authors http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Research Paper
Hoskin, Teagan S.
Crowther, Jennifer M.
Cheung, Jeanette
Epton, Michael J.
Sly, Peter D.
Elder, Peter A.
Dobson, Renwick C.J.
Kettle, Anthony J.
Dickerhof, Nina
Oxidative cross-linking of calprotectin occurs in vivo, altering its structure and susceptibility to proteolysis
title Oxidative cross-linking of calprotectin occurs in vivo, altering its structure and susceptibility to proteolysis
title_full Oxidative cross-linking of calprotectin occurs in vivo, altering its structure and susceptibility to proteolysis
title_fullStr Oxidative cross-linking of calprotectin occurs in vivo, altering its structure and susceptibility to proteolysis
title_full_unstemmed Oxidative cross-linking of calprotectin occurs in vivo, altering its structure and susceptibility to proteolysis
title_short Oxidative cross-linking of calprotectin occurs in vivo, altering its structure and susceptibility to proteolysis
title_sort oxidative cross-linking of calprotectin occurs in vivo, altering its structure and susceptibility to proteolysis
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6477633/
https://www.ncbi.nlm.nih.gov/pubmed/31015146
http://dx.doi.org/10.1016/j.redox.2019.101202
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