Author
Listed:
- Marion Espéli
(University of Cambridge School of Clinical Medicine, Cambridge Biomedical Campus
Univ Paris-Sud, Université Paris-Saclay)
- Rachael Bashford-Rogers
(University of Cambridge School of Clinical Medicine, Cambridge Biomedical Campus
Wellcome Centre for Human Genetics)
- John M. Sowerby
(University of Cambridge School of Clinical Medicine, Cambridge Biomedical Campus
University of Cambridge)
- Nagham Alouche
(Univ Paris-Sud, Université Paris-Saclay)
- Limy Wong
(University of Cambridge School of Clinical Medicine, Cambridge Biomedical Campus)
- Alice E. Denton
(University of Cambridge School of Clinical Medicine, Cambridge Biomedical Campus
Babraham Institute)
- Michelle A. Linterman
(University of Cambridge School of Clinical Medicine, Cambridge Biomedical Campus
Babraham Institute)
- Kenneth G. C. Smith
(University of Cambridge School of Clinical Medicine, Cambridge Biomedical Campus
University of Cambridge)
Abstract
Several tolerance checkpoints exist throughout B cell development to control autoreactive B cells and prevent the generation of pathogenic autoantibodies. FcγRIIb is an Fc receptor that inhibits B cell activation and, if defective, is associated with autoimmune disease, yet its impact on specific B cell tolerance checkpoints is unknown. Here we show that reduced expression of FcγRIIb enhances the deletion and anergy of autoreactive immature B cells, but in contrast promotes autoreactive B cell expansion in the germinal center and serum autoantibody production, even in response to exogenous, non-self antigens. Our data thus show that FcγRIIb has opposing effects on pre-immune and post-immune tolerance checkpoints, and suggest that B cell tolerance requires the control of bystander germinal center B cells with low or no affinity for the immunizing antigen.
Suggested Citation
Marion Espéli & Rachael Bashford-Rogers & John M. Sowerby & Nagham Alouche & Limy Wong & Alice E. Denton & Michelle A. Linterman & Kenneth G. C. Smith, 2019.
"FcγRIIb differentially regulates pre-immune and germinal center B cell tolerance in mouse and human,"
Nature Communications, Nature, vol. 10(1), pages 1-14, December.
Handle:
RePEc:nat:natcom:v:10:y:2019:i:1:d:10.1038_s41467-019-09434-0
DOI: 10.1038/s41467-019-09434-0
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