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The NFκB signaling system in the generation of B-cell subsets: from germinal center B cells to memory B cells and plasma cells

Koushik Roy, Mainak Chakraborty, Ashok Kumar, Asit Manna, Neeladri Sekhar Roy

2023Frontiers in Immunology16 citationsDOIOpen Access PDF

Abstract

Memory B cells and antibody-secreting cells are the two prime effector B cell populations that drive infection- and vaccine-induced long-term antibody-mediated immunity. The antibody-mediated immunity mostly relies on the formation of specialized structures within secondary lymphoid organs, called germinal centers (GCs), that facilitate the interactions between B cells, T cells, and antigen-presenting cells. Antigen-activated B cells may proliferate and differentiate into GC-independent plasmablasts and memory B cells or differentiate into GC B cells. The GC B cells undergo proliferation coupled to somatic hypermutation of their immunoglobulin genes for antibody affinity maturation. Subsequently, affinity mature GC B cells differentiate into GC-dependent plasma cells and memory B cells. Here, we review how the NFκB signaling system controls B cell proliferation and the generation of GC B cells, plasmablasts/plasma cells, and memory B cells. We also identify and discuss some important unanswered questions in this connection.

Topics & Concepts

Germinal centerB-1 cellCD40Naive B cellMemory B cellSomatic hypermutationB cellCell biologyPlasma cellBiologyB-cell receptorAntibodyAntigen-presenting cellImmunologyImmune systemT cellCytotoxic T cellIn vitroBiochemistryNF-κB Signaling PathwaysT-cell and B-cell ImmunologyImmune Cell Function and Interaction
The NFκB signaling system in the generation of B-cell subsets: from germinal center B cells to memory B cells and plasma cells | Litcius