4.6 Article

Antibody Mediated Intercommunication of Germinal Centers

Journal

CELLS
Volume 11, Issue 22, Pages -

Publisher

MDPI
DOI: 10.3390/cells11223680

Keywords

germinal centers; antibody feedback; germinal center intercommunication; germinal center shutdown; broadly neutralizing antibodies; mathematical modeling

Categories

Funding

  1. European Union [765158]
  2. Marie Curie Actions (MSCA) [765158] Funding Source: Marie Curie Actions (MSCA)

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In this study, computer simulations were used to investigate the role of soluble antibodies in the interaction between germinal centers (GCs). The findings suggest that intense interactions by soluble antibodies can limit the magnitude and lifetime of GC responses, and also lead to a bias in epitope recognition. The study also highlights the importance of GC-GC interactions in the affinity maturation towards antigenic variants during an ongoing GC reaction.
Antibody diversification and selection of B cells occur in dynamic structures called germinal centers (GCs). Passively administered soluble antibodies regulate the GC response by masking the antigen displayed on follicular dendritic cells (FDCs). This suggests that GCs might intercommunicate via naturally produced soluble antibodies, but the role of such GC-GC interactions is unknown. In this study, we performed in silico simulations of interacting GCs and predicted that intense interactions by soluble antibodies limit the magnitude and lifetime of GC responses. With asynchronous GC onset, we observed a higher inhibition of late formed GCs compared to early ones. We also predicted that GC-GC interactions can lead to a bias in the epitope recognition even in the presence of equally dominant epitopes due to differences in founder cell composition or initiation timing of GCs. We show that there exists an optimal range for GC-GC interaction strength that facilitates the affinity maturation towards an incoming antigenic variant during an ongoing GC reaction. These findings suggest that GC-GC interactions might be a contributing factor to the unexplained variability seen among individual GCs and a critical factor in the modulation of GC response to antigenic variants during viral infections.

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