Early appearance of germinal center–derived memory B cells and plasma cells in blood after primary immunization

EJ Blink, A Light, A Kallies, SL Nutt… - The Journal of …, 2005 - rupress.org
The Journal of experimental medicine, 2005rupress.org
Immunization with a T cell–dependent antigen elicits production of specific memory B cells
and antibody-secreting cells (ASCs). The kinetic and developmental relationships between
these populations and the phenotypic forms they and their precursors may take remain
unclear. Therefore, we examined the early stages of a primary immune response, focusing
on the appearance of antigen-specific B cells in blood. Within 1 wk, antigen-specific B cells
appear in the blood with either a memory phenotype or as immunoglobulin (Ig) G1 ASCs …
Immunization with a T cell–dependent antigen elicits production of specific memory B cells and antibody-secreting cells (ASCs). The kinetic and developmental relationships between these populations and the phenotypic forms they and their precursors may take remain unclear. Therefore, we examined the early stages of a primary immune response, focusing on the appearance of antigen-specific B cells in blood. Within 1 wk, antigen-specific B cells appear in the blood with either a memory phenotype or as immunoglobulin (Ig)G1 ASCs expressing blimp-1. The memory cells have mutated VH genes; respond to the chemokine CXCL13 but not CXCL12, suggesting recirculation to secondary lymphoid organs; uniformly express B220; show limited differentiation potential unless stimulated by antigen; and develop independently of blimp-1 expression. The antigen-specific IgG1 ASCs in blood show affinity maturation paralleling that of bone marrow ASCs, raising the possibility that this compartment is established directly by blood-borne ASCs. We find no evidence for a blimp-1–expressing preplasma memory compartment, suggesting germinal center output is restricted to ASCs and B220+ memory B cells, and this is sufficient to account for the process of affinity maturation.
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