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Nitration of the Egg-Allergen Ovalbumin Enhances Protein Allergenicity but Reduces the Risk for Oral Sensitization in a Murine Model of Food Allergy

BACKGROUND: Nitration of proteins on tyrosine residues, which can occur due to polluted air under “summer smog” conditions, has been shown to increase the allergic potential of allergens. Since nitration of tyrosine residues is also observed during inflammatory responses, this modification could dir...

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Autores principales: Untersmayr, Eva, Diesner, Susanne C., Oostingh, Gertie Janneke, Selzle, Kathrin, Pfaller, Tobias, Schultz, Cornelia, Zhang, Yingyi, Krishnamurthy, Durga, Starkl, Philipp, Knittelfelder, Regina, Förster-Waldl, Elisabeth, Pollak, Arnold, Scheiner, Otto, Pöschl, Ulrich, Jensen-Jarolim, Erika, Duschl, Albert
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2010
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2996297/
https://www.ncbi.nlm.nih.gov/pubmed/21151984
http://dx.doi.org/10.1371/journal.pone.0014210
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author Untersmayr, Eva
Diesner, Susanne C.
Oostingh, Gertie Janneke
Selzle, Kathrin
Pfaller, Tobias
Schultz, Cornelia
Zhang, Yingyi
Krishnamurthy, Durga
Starkl, Philipp
Knittelfelder, Regina
Förster-Waldl, Elisabeth
Pollak, Arnold
Scheiner, Otto
Pöschl, Ulrich
Jensen-Jarolim, Erika
Duschl, Albert
author_facet Untersmayr, Eva
Diesner, Susanne C.
Oostingh, Gertie Janneke
Selzle, Kathrin
Pfaller, Tobias
Schultz, Cornelia
Zhang, Yingyi
Krishnamurthy, Durga
Starkl, Philipp
Knittelfelder, Regina
Förster-Waldl, Elisabeth
Pollak, Arnold
Scheiner, Otto
Pöschl, Ulrich
Jensen-Jarolim, Erika
Duschl, Albert
author_sort Untersmayr, Eva
collection PubMed
description BACKGROUND: Nitration of proteins on tyrosine residues, which can occur due to polluted air under “summer smog” conditions, has been shown to increase the allergic potential of allergens. Since nitration of tyrosine residues is also observed during inflammatory responses, this modification could directly influence protein immunogenicity and might therefore contribute to food allergy induction. In the current study we have analyzed the impact of protein nitration on sensitization via the oral route. METHODOLOGY/PRINCIPAL FINDINGS: BALB/c mice were immunized intragastrically by feeding untreated ovalbumin (OVA), sham-nitrated ovalbumin (snOVA) or nitrated ovalbumin (nOVA) with or without concomitant acid-suppression. To analyze the impact of the sensitization route, the allergens were also injected intraperitoneally. Animals being fed OVA or snOVA under acid-suppressive medication developed significantly elevated levels of IgE, and increased titers of specific IgG1 and IgG2a antibodies. Interestingly, oral immunizations of nOVA under anti-acid treatment did not result in IgG and IgE formation. In contrast, intraperitoneal immunization induced high levels of OVA specific IgE, which were significantly increased in the group that received nOVA by injection. Furthermore, nOVA triggered significantly enhanced mediator release from RBL cells passively sensitized with sera from allergic mice. Gastric digestion experiments demonstrated protein nitration to interfere with protein stability as nOVA was easily degraded, whereas OVA and snOVA remained stable up to 120 min. Additionally, HPLC-chip-MS/MS analysis showed that one tyrosine residue (Y(107)) being very efficiently nitrated is part of an ovalbumin epitope recognized exclusively after oral sensitization. CONCLUSIONS/SIGNIFICANCE: These data indicated that despite the enhanced triggering capacity in existing allergy, nitration of OVA may be associated with a reduced de novo sensitizing capability via the oral route due to enhanced protein digestibility and/or changes in antibody epitopes.
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spelling pubmed-29962972010-12-10 Nitration of the Egg-Allergen Ovalbumin Enhances Protein Allergenicity but Reduces the Risk for Oral Sensitization in a Murine Model of Food Allergy Untersmayr, Eva Diesner, Susanne C. Oostingh, Gertie Janneke Selzle, Kathrin Pfaller, Tobias Schultz, Cornelia Zhang, Yingyi Krishnamurthy, Durga Starkl, Philipp Knittelfelder, Regina Förster-Waldl, Elisabeth Pollak, Arnold Scheiner, Otto Pöschl, Ulrich Jensen-Jarolim, Erika Duschl, Albert PLoS One Research Article BACKGROUND: Nitration of proteins on tyrosine residues, which can occur due to polluted air under “summer smog” conditions, has been shown to increase the allergic potential of allergens. Since nitration of tyrosine residues is also observed during inflammatory responses, this modification could directly influence protein immunogenicity and might therefore contribute to food allergy induction. In the current study we have analyzed the impact of protein nitration on sensitization via the oral route. METHODOLOGY/PRINCIPAL FINDINGS: BALB/c mice were immunized intragastrically by feeding untreated ovalbumin (OVA), sham-nitrated ovalbumin (snOVA) or nitrated ovalbumin (nOVA) with or without concomitant acid-suppression. To analyze the impact of the sensitization route, the allergens were also injected intraperitoneally. Animals being fed OVA or snOVA under acid-suppressive medication developed significantly elevated levels of IgE, and increased titers of specific IgG1 and IgG2a antibodies. Interestingly, oral immunizations of nOVA under anti-acid treatment did not result in IgG and IgE formation. In contrast, intraperitoneal immunization induced high levels of OVA specific IgE, which were significantly increased in the group that received nOVA by injection. Furthermore, nOVA triggered significantly enhanced mediator release from RBL cells passively sensitized with sera from allergic mice. Gastric digestion experiments demonstrated protein nitration to interfere with protein stability as nOVA was easily degraded, whereas OVA and snOVA remained stable up to 120 min. Additionally, HPLC-chip-MS/MS analysis showed that one tyrosine residue (Y(107)) being very efficiently nitrated is part of an ovalbumin epitope recognized exclusively after oral sensitization. CONCLUSIONS/SIGNIFICANCE: These data indicated that despite the enhanced triggering capacity in existing allergy, nitration of OVA may be associated with a reduced de novo sensitizing capability via the oral route due to enhanced protein digestibility and/or changes in antibody epitopes. Public Library of Science 2010-12-02 /pmc/articles/PMC2996297/ /pubmed/21151984 http://dx.doi.org/10.1371/journal.pone.0014210 Text en Untersmayr et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Untersmayr, Eva
Diesner, Susanne C.
Oostingh, Gertie Janneke
Selzle, Kathrin
Pfaller, Tobias
Schultz, Cornelia
Zhang, Yingyi
Krishnamurthy, Durga
Starkl, Philipp
Knittelfelder, Regina
Förster-Waldl, Elisabeth
Pollak, Arnold
Scheiner, Otto
Pöschl, Ulrich
Jensen-Jarolim, Erika
Duschl, Albert
Nitration of the Egg-Allergen Ovalbumin Enhances Protein Allergenicity but Reduces the Risk for Oral Sensitization in a Murine Model of Food Allergy
title Nitration of the Egg-Allergen Ovalbumin Enhances Protein Allergenicity but Reduces the Risk for Oral Sensitization in a Murine Model of Food Allergy
title_full Nitration of the Egg-Allergen Ovalbumin Enhances Protein Allergenicity but Reduces the Risk for Oral Sensitization in a Murine Model of Food Allergy
title_fullStr Nitration of the Egg-Allergen Ovalbumin Enhances Protein Allergenicity but Reduces the Risk for Oral Sensitization in a Murine Model of Food Allergy
title_full_unstemmed Nitration of the Egg-Allergen Ovalbumin Enhances Protein Allergenicity but Reduces the Risk for Oral Sensitization in a Murine Model of Food Allergy
title_short Nitration of the Egg-Allergen Ovalbumin Enhances Protein Allergenicity but Reduces the Risk for Oral Sensitization in a Murine Model of Food Allergy
title_sort nitration of the egg-allergen ovalbumin enhances protein allergenicity but reduces the risk for oral sensitization in a murine model of food allergy
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2996297/
https://www.ncbi.nlm.nih.gov/pubmed/21151984
http://dx.doi.org/10.1371/journal.pone.0014210
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