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Follicular dendritic cells restrict interleukin-4 availability in germinal centers and foster memory B cell generation.


ABSTRACT: B cells within germinal centers (GCs) enter cycles of antibody affinity maturation or exit the GC as memory cells or plasma cells. Here, we examined the contribution of interleukin (IL)-4 on B cell fate decisions in the GC. Single-cell RNA-sequencing identified a subset of light zone GC B cells expressing high IL-4 receptor-a (IL4Ra) and CD23 and lacking a Myc-associated signature. These cells could differentiate into pre-memory cells. B cell-specific deletion of IL4Ra or STAT6 favored the pre-memory cell trajectory, and provision of exogenous IL-4 in a wild-type context reduced pre-memory cell frequencies. IL-4 acted during antigen-specific interactions but also influenced bystander cells. Deletion of IL4Ra from follicular dendritic cells (FDCs) increased the availability of IL-4 in the GC, impaired the selection of affinity-matured B cells, and reduced memory cell generation. We propose that GC FDCs establish a niche that limits bystander IL-4 activity, focusing IL-4 action on B cells undergoing selection and enhancing memory cell differentiation.

SUBMITTER: Duan L 

PROVIDER: S-EPMC8516727 | biostudies-literature | 2021 Oct

REPOSITORIES: biostudies-literature

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Follicular dendritic cells restrict interleukin-4 availability in germinal centers and foster memory B cell generation.

Duan Lihui L   Liu Dan D   Chen Hsin H   Mintz Michelle A MA   Chou Marissa Y MY   Kotov Dmitri I DI   Xu Ying Y   An Jinping J   Laidlaw Brian J BJ   Cyster Jason G JG  

Immunity 20210922 10


B cells within germinal centers (GCs) enter cycles of antibody affinity maturation or exit the GC as memory cells or plasma cells. Here, we examined the contribution of interleukin (IL)-4 on B cell fate decisions in the GC. Single-cell RNA-sequencing identified a subset of light zone GC B cells expressing high IL-4 receptor-a (IL4Ra) and CD23 and lacking a Myc-associated signature. These cells could differentiate into pre-memory cells. B cell-specific deletion of IL4Ra or STAT6 favored the pre-m  ...[more]

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