Memory B cell subsets have divergent developmental origins that are coupled to distinct imprinted epigenetic states.
Derrick CallahanShuchi SmitaStephen JoachimKenneth B HoehnSteven H KleinsteinFlorian J WeiselMaria ChikinaMark J ShlomchikPublished in: Nature immunology (2024)
Memory B cells (MBCs) are phenotypically and functionally diverse, but their developmental origins remain undefined. Murine MBCs can be divided into subsets by expression of CD80 and PD-L2. Upon re-immunization, CD80/PD-L2 double-negative (DN) MBCs spawn germinal center B cells (GCBCs), whereas CD80/PD-L2 double-positive (DP) MBCs generate plasmablasts but not GCBCs. Using multiple approaches, including generation of an inducible GCBC-lineage reporter mouse, we demonstrate in a T cell-dependent response that DN cells formed independently of the germinal center (GC), whereas DP cells exhibited either extrafollicular (DP EX ) or GCBC (DP GC ) origins. Chromatin and transcriptional profiling revealed similarity of DN cells with an early memory precursor. Reciprocally, GCBC-derived DP cells shared distinct genomic features with GCBCs, while DP EX cells had hybrid features. Upon restimulation, DP EX cells were more prone to divide, while DP GC cells differentiated toward IgG1 + plasmablasts. Thus, MBC functional diversity is generated through distinct developmental histories, which imprint characteristic epigenetic patterns onto their progeny, thereby programming them for divergent functional responses.