High affinity germinal center B cells are actively selected into the plasma cell compartment

Author:

Phan Tri Giang12,Paus Didrik12,Chan Tyani D.12,Turner Marian L.3,Nutt Stephen L.3,Basten Antony12,Brink Robert12

Affiliation:

1. Centenary Institute of Cancer Medicine and Cell Biology, Newtown NSW 2042, Australia

2. Garvan Institute of Medical Research, Darlinghurst NSW 2010, Australia

3. Walter and Eliza Hall Institute for Medical Research, Parkville VIC 3050, Australia

Abstract

A hallmark of T cell–dependent immune responses is the progressive increase in the ability of serum antibodies to bind antigen and provide immune protection. Affinity maturation of the antibody response is thought to be connected with the preferential survival of germinal centre (GC) B cells that have acquired increased affinity for antigen via somatic hypermutation of their immunoglobulin genes. However, the mechanisms that drive affinity maturation remain obscure because of the difficulty in tracking the affinity-based selection of GC B cells and their differentiation into plasma cells. We describe a powerful new model that allows these processes to be followed as they occur in vivo. In contrast to evidence from in vitro systems, responding GC B cells do not undergo plasma cell differentiation stochastically. Rather, only GC B cells that have acquired high affinity for the immunizing antigen form plasma cells. Affinity maturation is therefore driven by a tightly controlled mechanism that ensures only antibodies with the greatest possibility of neutralizing foreign antigen are produced. Because the body can sustain only limited numbers of plasma cells, this “quality control” over plasma cell differentiation is likely critical for establishing effective humoral immunity.

Publisher

Rockefeller University Press

Subject

Immunology,Immunology and Allergy

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