Distinct Transcriptomic Features are Associated with Transitional and Mature B-Cell Populations in the Mouse Spleen

Splenic transitional B-cells (T1 and T2) are selected to avoid self-reactivity and to safeguard against autoimmunity, then differentiate into mature follicular (FO-I and FO-II) and marginal zone (MZ) subsets. Transcriptomic analysis by RNA-seq of the five B-cell subsets revealed T1 cell signature ge...

Descripción completa

Detalles Bibliográficos
Autores principales: Kleiman, Eden, Salyakina, Daria, De Heusch, Magali, Hoek, Kristen L., Llanes, Joan M., Castro, Iris, Wright, Jacqueline A., Clark, Emily S., Dykxhoorn, Derek M., Capobianco, Enrico, Takeda, Akiko, McCormack, Ryan M., Podack, Eckhard R., Renauld, Jean-Christophe, Khan, Wasif N.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2015
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4324157/
https://www.ncbi.nlm.nih.gov/pubmed/25717326
http://dx.doi.org/10.3389/fimmu.2015.00030
_version_ 1782356644772970496
author Kleiman, Eden
Salyakina, Daria
De Heusch, Magali
Hoek, Kristen L.
Llanes, Joan M.
Castro, Iris
Wright, Jacqueline A.
Clark, Emily S.
Dykxhoorn, Derek M.
Capobianco, Enrico
Takeda, Akiko
McCormack, Ryan M.
Podack, Eckhard R.
Renauld, Jean-Christophe
Khan, Wasif N.
author_facet Kleiman, Eden
Salyakina, Daria
De Heusch, Magali
Hoek, Kristen L.
Llanes, Joan M.
Castro, Iris
Wright, Jacqueline A.
Clark, Emily S.
Dykxhoorn, Derek M.
Capobianco, Enrico
Takeda, Akiko
McCormack, Ryan M.
Podack, Eckhard R.
Renauld, Jean-Christophe
Khan, Wasif N.
author_sort Kleiman, Eden
collection PubMed
description Splenic transitional B-cells (T1 and T2) are selected to avoid self-reactivity and to safeguard against autoimmunity, then differentiate into mature follicular (FO-I and FO-II) and marginal zone (MZ) subsets. Transcriptomic analysis by RNA-seq of the five B-cell subsets revealed T1 cell signature genes included RAG suggesting a potential for receptor revision. T1 to T2 B-cell differentiation was marked by a switch from Myb to Myc, increased expression of the PI3K adapter DAP10 and MHC class II. FO-II may be an intermediate in FO-I differentiation and may also become MZ B-cells as suggested by principle component analysis. MZ B-cells possessed the most distinct transcriptome including down-regulation of CD45 phosphatase-associated protein (CD45-AP/PTPRC-AP), as well as upregulation of IL-9R and innate molecules TLR3, TLR7, and bactericidal Perforin-2 (MPEG1). Among the endosomal TLRs, stimulation via TLR3 further enhanced Perforin-2 expression exclusively in MZ B-cells. Using gene-deleted and overexpressing transgenic mice we show that IL-9/IL-9R interaction resulted in rapid activation of STAT1, 3, and 5, primarily in MZ B-cells. Importantly, CD45-AP mutant mice had reduced transitional and increased mature MZ and FO B-cells, suggesting that it prevents premature entry of transitional B-cells to the mature B-cell pool or their survival and proliferation. Together, these findings suggest, developmental plasticity among splenic B-cell subsets, potential for receptor revision in peripheral tolerance whereas enhanced metabolism coincides with T2 to mature B-cell differentiation. Further, unique core transcriptional signatures in MZ B-cells may control their innate features.
format Online
Article
Text
id pubmed-4324157
institution National Center for Biotechnology Information
language English
publishDate 2015
publisher Frontiers Media S.A.
record_format MEDLINE/PubMed
spelling pubmed-43241572015-02-25 Distinct Transcriptomic Features are Associated with Transitional and Mature B-Cell Populations in the Mouse Spleen Kleiman, Eden Salyakina, Daria De Heusch, Magali Hoek, Kristen L. Llanes, Joan M. Castro, Iris Wright, Jacqueline A. Clark, Emily S. Dykxhoorn, Derek M. Capobianco, Enrico Takeda, Akiko McCormack, Ryan M. Podack, Eckhard R. Renauld, Jean-Christophe Khan, Wasif N. Front Immunol Immunology Splenic transitional B-cells (T1 and T2) are selected to avoid self-reactivity and to safeguard against autoimmunity, then differentiate into mature follicular (FO-I and FO-II) and marginal zone (MZ) subsets. Transcriptomic analysis by RNA-seq of the five B-cell subsets revealed T1 cell signature genes included RAG suggesting a potential for receptor revision. T1 to T2 B-cell differentiation was marked by a switch from Myb to Myc, increased expression of the PI3K adapter DAP10 and MHC class II. FO-II may be an intermediate in FO-I differentiation and may also become MZ B-cells as suggested by principle component analysis. MZ B-cells possessed the most distinct transcriptome including down-regulation of CD45 phosphatase-associated protein (CD45-AP/PTPRC-AP), as well as upregulation of IL-9R and innate molecules TLR3, TLR7, and bactericidal Perforin-2 (MPEG1). Among the endosomal TLRs, stimulation via TLR3 further enhanced Perforin-2 expression exclusively in MZ B-cells. Using gene-deleted and overexpressing transgenic mice we show that IL-9/IL-9R interaction resulted in rapid activation of STAT1, 3, and 5, primarily in MZ B-cells. Importantly, CD45-AP mutant mice had reduced transitional and increased mature MZ and FO B-cells, suggesting that it prevents premature entry of transitional B-cells to the mature B-cell pool or their survival and proliferation. Together, these findings suggest, developmental plasticity among splenic B-cell subsets, potential for receptor revision in peripheral tolerance whereas enhanced metabolism coincides with T2 to mature B-cell differentiation. Further, unique core transcriptional signatures in MZ B-cells may control their innate features. Frontiers Media S.A. 2015-02-11 /pmc/articles/PMC4324157/ /pubmed/25717326 http://dx.doi.org/10.3389/fimmu.2015.00030 Text en Copyright © 2015 Kleiman, Salyakina, De Heusch, Hoek, Llanes, Castro, Wright, Clark, Dykxhoorn, Capobianco, Takeda, McCormack, Podack, Renauld and Khan. 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) or licensor 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 Immunology
Kleiman, Eden
Salyakina, Daria
De Heusch, Magali
Hoek, Kristen L.
Llanes, Joan M.
Castro, Iris
Wright, Jacqueline A.
Clark, Emily S.
Dykxhoorn, Derek M.
Capobianco, Enrico
Takeda, Akiko
McCormack, Ryan M.
Podack, Eckhard R.
Renauld, Jean-Christophe
Khan, Wasif N.
Distinct Transcriptomic Features are Associated with Transitional and Mature B-Cell Populations in the Mouse Spleen
title Distinct Transcriptomic Features are Associated with Transitional and Mature B-Cell Populations in the Mouse Spleen
title_full Distinct Transcriptomic Features are Associated with Transitional and Mature B-Cell Populations in the Mouse Spleen
title_fullStr Distinct Transcriptomic Features are Associated with Transitional and Mature B-Cell Populations in the Mouse Spleen
title_full_unstemmed Distinct Transcriptomic Features are Associated with Transitional and Mature B-Cell Populations in the Mouse Spleen
title_short Distinct Transcriptomic Features are Associated with Transitional and Mature B-Cell Populations in the Mouse Spleen
title_sort distinct transcriptomic features are associated with transitional and mature b-cell populations in the mouse spleen
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4324157/
https://www.ncbi.nlm.nih.gov/pubmed/25717326
http://dx.doi.org/10.3389/fimmu.2015.00030
work_keys_str_mv AT kleimaneden distincttranscriptomicfeaturesareassociatedwithtransitionalandmaturebcellpopulationsinthemousespleen
AT salyakinadaria distincttranscriptomicfeaturesareassociatedwithtransitionalandmaturebcellpopulationsinthemousespleen
AT deheuschmagali distincttranscriptomicfeaturesareassociatedwithtransitionalandmaturebcellpopulationsinthemousespleen
AT hoekkristenl distincttranscriptomicfeaturesareassociatedwithtransitionalandmaturebcellpopulationsinthemousespleen
AT llanesjoanm distincttranscriptomicfeaturesareassociatedwithtransitionalandmaturebcellpopulationsinthemousespleen
AT castroiris distincttranscriptomicfeaturesareassociatedwithtransitionalandmaturebcellpopulationsinthemousespleen
AT wrightjacquelinea distincttranscriptomicfeaturesareassociatedwithtransitionalandmaturebcellpopulationsinthemousespleen
AT clarkemilys distincttranscriptomicfeaturesareassociatedwithtransitionalandmaturebcellpopulationsinthemousespleen
AT dykxhoornderekm distincttranscriptomicfeaturesareassociatedwithtransitionalandmaturebcellpopulationsinthemousespleen
AT capobiancoenrico distincttranscriptomicfeaturesareassociatedwithtransitionalandmaturebcellpopulationsinthemousespleen
AT takedaakiko distincttranscriptomicfeaturesareassociatedwithtransitionalandmaturebcellpopulationsinthemousespleen
AT mccormackryanm distincttranscriptomicfeaturesareassociatedwithtransitionalandmaturebcellpopulationsinthemousespleen
AT podackeckhardr distincttranscriptomicfeaturesareassociatedwithtransitionalandmaturebcellpopulationsinthemousespleen
AT renauldjeanchristophe distincttranscriptomicfeaturesareassociatedwithtransitionalandmaturebcellpopulationsinthemousespleen
AT khanwasifn distincttranscriptomicfeaturesareassociatedwithtransitionalandmaturebcellpopulationsinthemousespleen

Ejemplares similares