Literature DB >> 26565917

Cell-Cycle-Dependent Reconfiguration of the DNA Methylome during Terminal Differentiation of Human B Cells into Plasma Cells.

Gersende Caron1, Mourad Hussein2, Marta Kulis3, Céline Delaloy2, Fabrice Chatonnet1, Amandine Pignarre2, Stéphane Avner4, Maud Lemarié2, Elise A Mahé4, Núria Verdaguer-Dot3, Ana C Queirós3, Karin Tarte1, José I Martín-Subero3, Gilles Salbert5, Thierry Fest6.   

Abstract

Molecular mechanisms underlying terminal differentiation of B cells into plasma cells are major determinants of adaptive immunity but remain only partially understood. Here we present the transcriptional and epigenomic landscapes of cell subsets arising from activation of human naive B cells and differentiation into plasmablasts. Cell proliferation of activated B cells was linked to a slight decrease in DNA methylation levels, but followed by a committal step in which an S phase-synchronized differentiation switch was associated with an extensive DNA demethylation and local acquisition of 5-hydroxymethylcytosine at enhancers and genes related to plasma cell identity. Downregulation of both TGF-?1/SMAD3 signaling and p53 pathway supported this final step, allowing the emergence of a CD23-negative subpopulation in transition from B cells to plasma cells. Remarkably, hydroxymethylation of PRDM1, a gene essential for plasma cell fate, was coupled to progression in S phase, revealing an intricate connection among cell cycle, DNA (hydroxy)methylation, and cell fate determination.
Copyright © 2015 The Authors. Published by Elsevier Inc. All rights reserved.

Entities:  

Keywords:  5hmC; B cell differentiation; DNA methylation; plasma cell differentiation; plasmablast

Mesh:

Substances:

Year:  2015        PMID: 26565917     DOI: 10.1016/j.celrep.2015.09.051

Source DB:  PubMed          Journal:  Cell Rep            Impact factor:   9.423


  27 in total

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