Differentially Tolerized Mouse Antigen Presenting Cells Share a Common miRNA Signature Including Enhanced mmu-miR-223-3p Expression Which Is Sufficient to Imprint a Protolerogenic State

Dendritic cells (DCs) are pivotal for the induction and maintenance of antigen-specific tolerance and immunity. miRNAs mediate post-transcriptional gene regulation and control in part the differentiation and stimulation-induced immunogenic function of DCs. However, the relevance of miRNAs for the in...

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Autores principales: Bros, Matthias, Youns, Mahmoud, Kollek, Verena, Buchmüller, Diana, Bollmann, Franziska, Seo, Ean-Jeong, Schupp, Jonathan, Montermann, Evelyn, Usanova, Svetlana, Kleinert, Hartmut, Efferth, Thomas, Reske-Kunz, Angelika B.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2018
Materias:
Pharmacology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6108336/
https://www.ncbi.nlm.nih.gov/pubmed/30174602
http://dx.doi.org/10.3389/fphar.2018.00915
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author Bros, Matthias
Youns, Mahmoud
Kollek, Verena
Buchmüller, Diana
Bollmann, Franziska
Seo, Ean-Jeong
Schupp, Jonathan
Montermann, Evelyn
Usanova, Svetlana
Kleinert, Hartmut
Efferth, Thomas
Reske-Kunz, Angelika B.
author_facet Bros, Matthias
Youns, Mahmoud
Kollek, Verena
Buchmüller, Diana
Bollmann, Franziska
Seo, Ean-Jeong
Schupp, Jonathan
Montermann, Evelyn
Usanova, Svetlana
Kleinert, Hartmut
Efferth, Thomas
Reske-Kunz, Angelika B.
author_sort Bros, Matthias
collection PubMed
description Dendritic cells (DCs) are pivotal for the induction and maintenance of antigen-specific tolerance and immunity. miRNAs mediate post-transcriptional gene regulation and control in part the differentiation and stimulation-induced immunogenic function of DCs. However, the relevance of miRNAs for the induction and maintenance of a tolerogenic state of DCs has scarcely been highlighted yet. We differentiated mouse bone marrow cells to conventional/myeloid DCs or to tolerogenic antigen presenting cells (APCs) by using a glucocorticoid (dexamethasone) or interleukin-10, and assessed the miRNA expression patterns of unstimulated and LPS-stimulated cell populations by array analysis and QPCR. Differentially tolerized mouse APCs convergingly down-regulated a set of miRNA species at either state of activation as compared with the corresponding control DC population (mmu-miR-9-5p, mmu-miR-9-3p, mmu-miR-155-5p). These miRNAs were also upregulated in control DCs in response to stimulation. In contrast, miRNAs that were convergingly upregulated in both tolerized APC groups at stimulated state (mmu-miR-223-3p, mmu-miR-1224-5p) were downregulated in control DCs in response to stimulation. Overexpression of mmu-miR-223-3p in DCs was sufficient to prevent stimulation-associated acquisition of potent T cell stimulatory capacity. Overexpression of mmu-miR-223-3p in a DC line resulted in attenuated expression of known (Cflar, Rasa1, Ras) mRNA targets of this miRNA species shown to affect pathways that control DC activation. Taken together, we identified sets of miRNAs convergingly regulated in differentially tolerized APCs, which may contribute to imprint stimulation-resistant tolerogenic function as demonstrated for mmu-miR-223-3p. Knowledge of miRNAs with protolerogenic function enables immunotherapeutic approaches aimed to modulate immune responses by regulating miRNA expression.
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spelling pubmed-61083362018-08-31 Differentially Tolerized Mouse Antigen Presenting Cells Share a Common miRNA Signature Including Enhanced mmu-miR-223-3p Expression Which Is Sufficient to Imprint a Protolerogenic State Bros, Matthias Youns, Mahmoud Kollek, Verena Buchmüller, Diana Bollmann, Franziska Seo, Ean-Jeong Schupp, Jonathan Montermann, Evelyn Usanova, Svetlana Kleinert, Hartmut Efferth, Thomas Reske-Kunz, Angelika B. Front Pharmacol Pharmacology Dendritic cells (DCs) are pivotal for the induction and maintenance of antigen-specific tolerance and immunity. miRNAs mediate post-transcriptional gene regulation and control in part the differentiation and stimulation-induced immunogenic function of DCs. However, the relevance of miRNAs for the induction and maintenance of a tolerogenic state of DCs has scarcely been highlighted yet. We differentiated mouse bone marrow cells to conventional/myeloid DCs or to tolerogenic antigen presenting cells (APCs) by using a glucocorticoid (dexamethasone) or interleukin-10, and assessed the miRNA expression patterns of unstimulated and LPS-stimulated cell populations by array analysis and QPCR. Differentially tolerized mouse APCs convergingly down-regulated a set of miRNA species at either state of activation as compared with the corresponding control DC population (mmu-miR-9-5p, mmu-miR-9-3p, mmu-miR-155-5p). These miRNAs were also upregulated in control DCs in response to stimulation. In contrast, miRNAs that were convergingly upregulated in both tolerized APC groups at stimulated state (mmu-miR-223-3p, mmu-miR-1224-5p) were downregulated in control DCs in response to stimulation. Overexpression of mmu-miR-223-3p in DCs was sufficient to prevent stimulation-associated acquisition of potent T cell stimulatory capacity. Overexpression of mmu-miR-223-3p in a DC line resulted in attenuated expression of known (Cflar, Rasa1, Ras) mRNA targets of this miRNA species shown to affect pathways that control DC activation. Taken together, we identified sets of miRNAs convergingly regulated in differentially tolerized APCs, which may contribute to imprint stimulation-resistant tolerogenic function as demonstrated for mmu-miR-223-3p. Knowledge of miRNAs with protolerogenic function enables immunotherapeutic approaches aimed to modulate immune responses by regulating miRNA expression. Frontiers Media S.A. 2018-08-17 /pmc/articles/PMC6108336/ /pubmed/30174602 http://dx.doi.org/10.3389/fphar.2018.00915 Text en Copyright © 2018 Bros, Youns, Kollek, Buchmüller, Bollmann, Seo, Schupp, Montermann, Usanova, Kleinert, Efferth and Reske-Kunz. 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) and the copyright owner(s) 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
Bros, Matthias
Youns, Mahmoud
Kollek, Verena
Buchmüller, Diana
Bollmann, Franziska
Seo, Ean-Jeong
Schupp, Jonathan
Montermann, Evelyn
Usanova, Svetlana
Kleinert, Hartmut
Efferth, Thomas
Reske-Kunz, Angelika B.
Differentially Tolerized Mouse Antigen Presenting Cells Share a Common miRNA Signature Including Enhanced mmu-miR-223-3p Expression Which Is Sufficient to Imprint a Protolerogenic State
title Differentially Tolerized Mouse Antigen Presenting Cells Share a Common miRNA Signature Including Enhanced mmu-miR-223-3p Expression Which Is Sufficient to Imprint a Protolerogenic State
title_full Differentially Tolerized Mouse Antigen Presenting Cells Share a Common miRNA Signature Including Enhanced mmu-miR-223-3p Expression Which Is Sufficient to Imprint a Protolerogenic State
title_fullStr Differentially Tolerized Mouse Antigen Presenting Cells Share a Common miRNA Signature Including Enhanced mmu-miR-223-3p Expression Which Is Sufficient to Imprint a Protolerogenic State
title_full_unstemmed Differentially Tolerized Mouse Antigen Presenting Cells Share a Common miRNA Signature Including Enhanced mmu-miR-223-3p Expression Which Is Sufficient to Imprint a Protolerogenic State
title_short Differentially Tolerized Mouse Antigen Presenting Cells Share a Common miRNA Signature Including Enhanced mmu-miR-223-3p Expression Which Is Sufficient to Imprint a Protolerogenic State
title_sort differentially tolerized mouse antigen presenting cells share a common mirna signature including enhanced mmu-mir-223-3p expression which is sufficient to imprint a protolerogenic state
topic Pharmacology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6108336/
https://www.ncbi.nlm.nih.gov/pubmed/30174602
http://dx.doi.org/10.3389/fphar.2018.00915
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