Litcius/Paper detail

The Shaping of a B Cell Pool Maximally Responsive to Infections

Nicole Baumgarth

2021Annual Review of Immunology61 citationsDOIOpen Access PDF

Abstract

B cell subsets differ in development, tissue distribution, and mechanisms of activation. In response to infections, however, all can differentiate into extrafollicular plasmablasts that rapidly provide highly protective antibodies, indicating that these plasmablasts are the main humoral immune response effectors. Yet, the effectiveness of this response type depends on the presence of antigen-specific precursors in the circulating mature B cell pool, a pool that is generated initially through the stochastic processes of B cell receptor assembly. Importantly, germinal centers then mold the repertoire of this B cell pool to be increasingly responsive to pathogens by generating a broad array of antimicrobial memory B cells that act as highly effective precursors of extrafollicular plasmablasts. Such B cell repertoire molding occurs in two ways: continuously via the chronic germinal centers of mucosal lymphoid tissues, driven by the presence of the microbiome, and via de novo generated germinal centers following acute infections. For effectively evaluating humoral immunity as a correlate of immune protection, it might be critical to measure memory B cell pools in addition to antibody titers.

Topics & Concepts

Germinal centerBiologyMemory B cellImmune systemImmunologyB cellAntibodyHumoral immunityImmunoglobulin class switchingB-1 cellAffinity maturationCell biologyT cellAntigen-presenting cellT-cell and B-cell ImmunologyImmunotherapy and Immune ResponsesImmune Cell Function and Interaction