The following is a summary of “Distinct dynamics of antigen-specific induction and differentiation of different CD11c+Tbet+ B-cell subsets,” published in the SEPTEMBER 2023 issue of Allergy & Immunology by Steuten, et al.
In the realm of immunology, CD11c+Tbet+ B cells have garnered attention due to their presence in autoimmune conditions and chronic infections and their expansion during immune responses in healthy individuals. However, these B cells remain somewhat mysterious due to their intrinsic diversity.
For a study, researchers set out to investigate how three distinct subsets of CD11c+ B cells, namely age-associated B cells (ABCs), double-negative 2 (DN2) B cells and activated naive B cells, respond to the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) antigen. They aimed to shed light on the development and differentiation characteristics of these CD11c+ B-cell subsets compared to their conventional CD11c− counterparts.
The study used advanced spectral flow cytometry to track the dynamics of these three CD11c+ B-cell subsets in response to SARS-CoV-2 vaccination in healthy donors. Interestingly, while CD11c− memory B cells exhibited a lasting expansion following vaccination, both ABCs and DN2 cells experienced a robust expansion shortly after the second vaccination, only to contract later.
Moreover, the research delved into the functional aspects of these B-cell subsets, particularly their ability to differentiate into antibody-secreting cells. It was discovered that CD11c+Tbet+ B cells displayed a predisposition for antibody-secreting cell differentiation when compared to their conventional CD11c− counterparts.
In conclusion, the study highlighted the heterogeneity within CD11c+Tbet+ B cell populations and underscored the early and distinctive response of ABCs and DN2 B cells to immune challenges. The findings provided valuable insights into the intricate world of immune cell behavior during immune responses, particularly in the context of viral vaccinations.
Source: jacionline.org/article/S0091-6749(23)00234-8/fulltext
