| Literature DB >> 15020647 |
Sergio Arce1, Elke Luger, Gwendolin Muehlinghaus, Giuliana Cassese, Anja Hauser, Alexander Horst, Katja Lehnert, Marcus Odendahl, Dirk Hönemann, Karl-Dieter Heller, Harald Kleinschmidt, Claudia Berek, Thomas Dörner, Veit Krenn, Falk Hiepe, Ralf Bargou, Andreas Radbruch, Rudolf A Manz.
Abstract
Despite the important role immunoglobulin G (IgG)-secreting plasma cells play in memory immune responses, the differentiation and homeostasis of these cells are not completely understood. Here, we studied the differentiation of human IgG-secreting cells ex vivo and in vitro, identifying these cells by the cellular affinity matrix technology. Several subpopulations of IgG-secreting cells were identified among the cells isolated from tonsils and bone marrow, particularly differing in the expression levels of CD9, CD19, and CD38. CD38 low IgG-secreting cells were present exclusively in the tonsils. A major fraction of these cells appeared to be early plasma cell precursors, as upon activation of B cells in vitro, IgG secretion preceded up-regulation of CD38, and on tonsillar sections, IgG-containing, CD38 low cells with a plasmacytoid phenotype were found in follicles, where plasma cell differentiation starts. A unitary phenotype of migratory peripheral blood IgG-secreting cells suggests that all bone marrow plasma cell populations share a common precursor cell. These data are compatible with a multistep model for plasma cell differentiation and imply that a common CD38 low IgG-secreting precursor gives rise to a diverse plasma cell compartment.Entities:
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Year: 2004 PMID: 15020647 DOI: 10.1189/jlb.0603279
Source DB: PubMed Journal: J Leukoc Biol ISSN: 0741-5400 Impact factor: 4.962