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A unique population of IgG-expressing plasma cells lacking CD19 is enriched in human bone marrow

Authors :
Robby Engelmann
Daniela Frölich
Thomas Dörner
Ina Wirries
Henrik E. Mei
Joachim R. Grün
Anja A. Kühl
Stefanie Schmidt
Andreas Radbruch
Katarzyna Luda
Michael Dürr
Maria Bokarewa
Claudia Giesecke
Tobias Scheel
Tobias Alexander
Mikael Brisslert
Carsten Perka
Source :
Blood. 125:1739-1748
Publication Year :
2015
Publisher :
American Society of Hematology, 2015.

Abstract

Specific serum antibodies mediating humoral immunity and autoimmunity are provided by mature plasma cells (PC) residing in the bone marrow (BM), yet their dynamics and composition are largely unclear. We here characterize distinct subsets of human PC differing by CD19 expression. Unlike CD19 + PC, CD19 − PC were restricted to BM, expressed predominantly IgG, and they carried a prosurvival, distinctly mature phenotype, that is, HLA-DR low Ki-67 − CD95 low CD28 + CD56 +/− , with increased BCL2 and they resisted their mobilization from the BM after systemic vaccination. Fewer mutations within immunoglobulin V H rearrangements of CD19 − BMPC may indicate their differentiation in early life. Their resistance to in vivo B-cell depletion, that is, their independency from supply with new plasmablasts, is consistent with long-term stability of this PC subset in the BM. Moreover, CD19 − PC were detectable in chronically inflamed tissues and secreted autoantibodies. We propose a multilayer model of PC memory in which CD19 + and CD19 − PC represent dynamic and static components, respectively, permitting both adaptation and stability of humoral immune protection.

Details

ISSN :
15280020 and 00064971
Volume :
125
Database :
OpenAIRE
Journal :
Blood
Accession number :
edsair.doi.dedup.....15d2de3e5a9d149e7515ad8e8c6c5bef