CD27 is acquired by primed B cells at the centroblast stage and promotes germinal center formation

Y Xiao, J Hendriks, P Langerak, H Jacobs… - The Journal of …, 2004 - journals.aai.org
Y Xiao, J Hendriks, P Langerak, H Jacobs, J Borst
The Journal of Immunology, 2004journals.aai.org
Studies on human B cells have featured CD27 as a marker and mediator of the B cell
response. We have studied CD27 expression and function on B cells in the mouse. We find
that B cells acquire CD27 at the centroblast stage and lose it progressively upon further
differentiation. It is not a marker for somatically mutated B cells and is present at very low
frequency on memory B cells. Enrichment of CD27 among centroblasts and the presence of
its ligand CD70 on occasional T and B cells in or near germinal centers (GCs) suggested a …
Abstract
Studies on human B cells have featured CD27 as a marker and mediator of the B cell response. We have studied CD27 expression and function on B cells in the mouse. We find that B cells acquire CD27 at the centroblast stage and lose it progressively upon further differentiation. It is not a marker for somatically mutated B cells and is present at very low frequency on memory B cells. Enrichment of CD27 among centroblasts and the presence of its ligand CD70 on occasional T and B cells in or near germinal centers (GCs) suggested a role for CD27/CD70 interactions in clonal B cell expansion. Accordingly, GC formation in response to influenza virus infection was delayed in CD27 knockout mice. CD27 deficiency did not affect somatic hypermutation or serum levels of virus-specific IgM, IgG, and IgA attained in primary and recall responses. Adoptive transfer of T and B cells into CD27/CD28−/− mice revealed that CD27 promotes GC formation and consequent IgG production by two distinct mechanisms. Stimulation of CD27 on B cells by CD28+ Th cells accelerates GC formation, most likely by promoting centroblast expansion. In addition, CD27 on T cells can partially substitute for CD28 in supporting GC formation.
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