Effects of Alanyl-Glutamine Treatment on the Peritoneal Dialysis Effluent Proteome Reveal Pathomechanism-Associated Molecular Signatures

Peritoneal dialysis (PD) is a modality of renal replacement therapy in which the high volumes of available PD effluent (PDE) represents a rich source of biomarkers for monitoring disease and therapy. Although this information could help guide the management of PD patients, little is known about the...

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Autores principales: Herzog, Rebecca, Boehm, Michael, Unterwurzacher, Markus, Wagner, Anja, Parapatics, Katja, Májek, Peter, Mueller, André C., Lichtenauer, Anton, Bennett, Keiryn L., Alper, Seth L., Vychytil, Andreas, Aufricht, Christoph, Kratochwill, Klaus
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The American Society for Biochemistry and Molecular Biology 2018
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5836375/
https://www.ncbi.nlm.nih.gov/pubmed/29208752
http://dx.doi.org/10.1074/mcp.RA117.000186
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author Herzog, Rebecca
Boehm, Michael
Unterwurzacher, Markus
Wagner, Anja
Parapatics, Katja
Májek, Peter
Mueller, André C.
Lichtenauer, Anton
Bennett, Keiryn L.
Alper, Seth L.
Vychytil, Andreas
Aufricht, Christoph
Kratochwill, Klaus
author_facet Herzog, Rebecca
Boehm, Michael
Unterwurzacher, Markus
Wagner, Anja
Parapatics, Katja
Májek, Peter
Mueller, André C.
Lichtenauer, Anton
Bennett, Keiryn L.
Alper, Seth L.
Vychytil, Andreas
Aufricht, Christoph
Kratochwill, Klaus
author_sort Herzog, Rebecca
collection PubMed
description Peritoneal dialysis (PD) is a modality of renal replacement therapy in which the high volumes of available PD effluent (PDE) represents a rich source of biomarkers for monitoring disease and therapy. Although this information could help guide the management of PD patients, little is known about the potential of PDE to define pathomechanism-associated molecular signatures in PD. We therefore subjected PDE to a high-performance multiplex proteomic analysis after depletion of highly-abundant plasma proteins and enrichment of low-abundance proteins. A combination of label-free and isobaric labeling strategies was applied to PDE samples from PD patients (n = 20) treated in an open-label, randomized, two-period, cross-over clinical trial with standard PD fluid or with a novel PD fluid supplemented with alanyl-glutamine (AlaGln). With this workflow we identified 2506 unique proteins in the PDE proteome, greatly increasing coverage beyond the 171 previously-reported proteins. The proteins identified range from high abundance plasma proteins to low abundance cellular proteins, and are linked to larger numbers of biological processes and pathways, some of which are novel for PDE. Interestingly, proteins linked to membrane remodeling and fibrosis are overrepresented in PDE compared with plasma, whereas the proteins underrepresented in PDE suggest decreases in host defense, immune-competence and response to stress. Treatment with AlaGln-supplemented PD fluid is associated with reduced activity of membrane injury-associated mechanisms and with restoration of biological processes involved in stress responses and host defense. Our study represents the first application of the PDE proteome in a randomized controlled prospective clinical trial of PD. This novel proteomic workflow allowed detection of low abundance biomarkers to define pathomechanism-associated molecular signatures in PD and their alterations by a novel therapeutic intervention.
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spelling pubmed-58363752018-03-06 Effects of Alanyl-Glutamine Treatment on the Peritoneal Dialysis Effluent Proteome Reveal Pathomechanism-Associated Molecular Signatures Herzog, Rebecca Boehm, Michael Unterwurzacher, Markus Wagner, Anja Parapatics, Katja Májek, Peter Mueller, André C. Lichtenauer, Anton Bennett, Keiryn L. Alper, Seth L. Vychytil, Andreas Aufricht, Christoph Kratochwill, Klaus Mol Cell Proteomics Research Peritoneal dialysis (PD) is a modality of renal replacement therapy in which the high volumes of available PD effluent (PDE) represents a rich source of biomarkers for monitoring disease and therapy. Although this information could help guide the management of PD patients, little is known about the potential of PDE to define pathomechanism-associated molecular signatures in PD. We therefore subjected PDE to a high-performance multiplex proteomic analysis after depletion of highly-abundant plasma proteins and enrichment of low-abundance proteins. A combination of label-free and isobaric labeling strategies was applied to PDE samples from PD patients (n = 20) treated in an open-label, randomized, two-period, cross-over clinical trial with standard PD fluid or with a novel PD fluid supplemented with alanyl-glutamine (AlaGln). With this workflow we identified 2506 unique proteins in the PDE proteome, greatly increasing coverage beyond the 171 previously-reported proteins. The proteins identified range from high abundance plasma proteins to low abundance cellular proteins, and are linked to larger numbers of biological processes and pathways, some of which are novel for PDE. Interestingly, proteins linked to membrane remodeling and fibrosis are overrepresented in PDE compared with plasma, whereas the proteins underrepresented in PDE suggest decreases in host defense, immune-competence and response to stress. Treatment with AlaGln-supplemented PD fluid is associated with reduced activity of membrane injury-associated mechanisms and with restoration of biological processes involved in stress responses and host defense. Our study represents the first application of the PDE proteome in a randomized controlled prospective clinical trial of PD. This novel proteomic workflow allowed detection of low abundance biomarkers to define pathomechanism-associated molecular signatures in PD and their alterations by a novel therapeutic intervention. The American Society for Biochemistry and Molecular Biology 2018-03 2017-12-04 /pmc/articles/PMC5836375/ /pubmed/29208752 http://dx.doi.org/10.1074/mcp.RA117.000186 Text en © 2018 by The American Society for Biochemistry and Molecular Biology, Inc. Author's Choice—Final version free via Creative Commons CC-BY license (http://creativecommons.org/licenses/by/4.0) .
spellingShingle Research
Herzog, Rebecca
Boehm, Michael
Unterwurzacher, Markus
Wagner, Anja
Parapatics, Katja
Májek, Peter
Mueller, André C.
Lichtenauer, Anton
Bennett, Keiryn L.
Alper, Seth L.
Vychytil, Andreas
Aufricht, Christoph
Kratochwill, Klaus
Effects of Alanyl-Glutamine Treatment on the Peritoneal Dialysis Effluent Proteome Reveal Pathomechanism-Associated Molecular Signatures
title Effects of Alanyl-Glutamine Treatment on the Peritoneal Dialysis Effluent Proteome Reveal Pathomechanism-Associated Molecular Signatures
title_full Effects of Alanyl-Glutamine Treatment on the Peritoneal Dialysis Effluent Proteome Reveal Pathomechanism-Associated Molecular Signatures
title_fullStr Effects of Alanyl-Glutamine Treatment on the Peritoneal Dialysis Effluent Proteome Reveal Pathomechanism-Associated Molecular Signatures
title_full_unstemmed Effects of Alanyl-Glutamine Treatment on the Peritoneal Dialysis Effluent Proteome Reveal Pathomechanism-Associated Molecular Signatures
title_short Effects of Alanyl-Glutamine Treatment on the Peritoneal Dialysis Effluent Proteome Reveal Pathomechanism-Associated Molecular Signatures
title_sort effects of alanyl-glutamine treatment on the peritoneal dialysis effluent proteome reveal pathomechanism-associated molecular signatures
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5836375/
https://www.ncbi.nlm.nih.gov/pubmed/29208752
http://dx.doi.org/10.1074/mcp.RA117.000186
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