Frontiers in Immunology (Aug 2021)

Coupled Antigen and BLIMP1 Asymmetric Division With a Large Segregation Between Daughter Cells Recapitulates the Temporal Transition From Memory B Cells to Plasma Cells and a DZ-to-LZ Ratio in the Germinal Center

  • Elena Merino Tejero,
  • Danial Lashgari,
  • Rodrigo García-Valiente,
  • Jiaojiao He,
  • Jiaojiao He,
  • Philippe A. Robert,
  • Michael Meyer-Hermann,
  • Michael Meyer-Hermann,
  • Jeroen E. J. Guikema,
  • Huub Hoefsloot,
  • Antoine H. C. van Kampen,
  • Antoine H. C. van Kampen

DOI
https://doi.org/10.3389/fimmu.2021.716240
Journal volume & issue
Vol. 12

Abstract

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Memory B cells and antibody-secreting plasma cells are generated within germinal centers during affinity maturation in which B-cell proliferation, selection, differentiation, and self-renewal play important roles. The mechanisms behind memory B cell and plasma cell differentiation in germinal centers are not well understood. However, it has been suggested that cell fate is (partially) determined by asymmetric cell division, which involves the unequal distribution of cellular components to both daughter cells. To investigate what level and/or probability of asymmetric segregation of several fate determinant molecules, such as the antigen and transcription factors (BCL6, IRF4, and BLIMP1) recapitulates the temporal switch and DZ-to-LZ ratio in the germinal center, we implemented a multiscale model that combines a core gene regulatory network for plasma cell differentiation with a model describing the cellular interactions and dynamics in the germinal center. Our simulations show that BLIMP1 driven plasma cell differentiation together with coupled asymmetric division of antigen and BLIMP1 with a large segregation between the daughter cells results in a germinal center DZ-to-LZ ratio and a temporal switch from memory B cells to plasma cells that have been observed in experiments.

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