Literature DB >> 34041745

The diversity of the plasmablast signature across species and experimental conditions: A meta-analysis.

Alexis Grasseau1, Marina Boudigou1, Magalie Michée-Cospolite1, Céline Delaloy2, Olivier Mignen1, Christophe Jamin1,3, Divi Cornec1,3, Jacques-Olivier Pers1,3, Laëtitia Le Pottier1, Sophie Hillion1,3.   

Abstract

Antibody-secreting cells (ASC) are divided into two principal subsets, including the long-lived plasma cell (PC) subset residing in the bone marrow and the short-lived subset, also called plasmablast (PB). PB are described as a proliferating subset circulating through the blood and ending its differentiation in tissues. Due to their inherent heterogeneity, the molecular signature of PB is not fully established. The purpose of this study was to decipher a specific PB signature in humans and mice through a comprehensive meta-analysis of different data sets exploring the PB differentiation in both species and across different experimental conditions. The present study used recent analyses using whole RNA sequencing in prdm1-GFP transgenic mice to define a reliable and accurate PB signature. Next, we performed similar analysis using current data sets obtained from human PB and PC. The PB-specific signature is composed of 155 and 113 genes in mouse and human being, respectively. Although only nine genes are shared between the human and mice PB signature, the loss of B-cell identity such as the down-regulation of PAX5, MS4A1, (CD20) CD22 and IL-4R is a conserved feature across species and across the different experimental conditions. Additionally, we observed that the IRF8 and IRF4 transcription factors have a specific dynamic range of expression in human PB. We thus demonstrated that IRF4/IRF8 intranuclear staining was useful to define PB in vivo and in vitro and able to discriminate between atypical PB populations and transient states.
© 2021 John Wiley & Sons Ltd.

Entities:  

Keywords:  B-cell differentiation; meta-analysis; plasmablast; transcriptome

Mesh:

Substances:

Year:  2021        PMID: 34041745      PMCID: PMC8358713          DOI: 10.1111/imm.13344

Source DB:  PubMed          Journal:  Immunology        ISSN: 0019-2805            Impact factor:   7.215


  61 in total

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7.  Analysis of interleukin-21-induced Prdm1 gene regulation reveals functional cooperation of STAT3 and IRF4 transcription factors.

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  1 in total

1.  Molecular Mechanisms Driving IL-10- Producing B Cells Functions: STAT3 and c-MAF as Underestimated Central Key Regulators?

Authors:  Magalie Michée-Cospolite; Marina Boudigou; Alexis Grasseau; Quentin Simon; Olivier Mignen; Jacques-Olivier Pers; Divi Cornec; Laëtitia Le Pottier; Sophie Hillion
Journal:  Front Immunol       Date:  2022-03-10       Impact factor: 7.561

  1 in total

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