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Heterogeneity of germinal center B cells: New insights from single‐cell studies

Noudjoud Attaf, Sabrina Baaklini, Laurine Binet, Pierre Milpied

2021European Journal of Immunology31 citationsDOIOpen Access PDF

Abstract

Upon antigen exposure, activated B cells in antigen-draining lymphoid organs form microanatomical structures, called germinal centers (GCs), where affinity maturation occurs. Within the GC microenvironment, GC B cells undergo proliferation and B cell receptor (BCR) genes somatic hypermutation in the dark zone (DZ), and affinity-based selection in the light zone (LZ). In the current paradigm of GC dynamics, high-affinity LZ B cells may be selected by cognate T- follicular helper cells to either differentiate into plasma cells or memory B cells, or re-enter the DZ and initiate a new round of proliferation and BCR diversification, before migrating back to the LZ. Given the diversity of cell states and potential cell fates that GC B cells may adopt, the two-state DZ-LZ paradigm has been challenged by studies that explored GC B-cell heterogeneity with a variety of single-cell technologies. Here, we review studies and single-cell technologies which have allowed to refine the working model of GC B-cell cellular and molecular heterogeneity during affinity maturation. This review also covers the use of single-cell quantitative data for mathematical modeling of GC reactions, and the application of single-cell genomics to the study of GC-derived malignancies.

Topics & Concepts

BiologyGerminal centerCenter (category theory)Evolutionary biologyComputational biologyB cellGeneticsChemistryCrystallographyAntibodyT-cell and B-cell ImmunologyImmune Cell Function and InteractionSingle-cell and spatial transcriptomics
Heterogeneity of germinal center B cells: New insights from single‐cell studies | Litcius