Abstract
Durable serological protection is maintained through the persistence of antigen-specific plasma cells (PCs), but key factors regulating the survival of nascent PCs remain unclear. Previously, we reported that bone marrow (BM) PCs partially organize into clusters that are enriched for long-lived PCs, suggesting that clusters are survival niches. Here, we report that acute blockade of a proliferation-inducing ligand (APRIL) and B cell activating factor (BAFF) using transmembrane activator and CAML interactor (TACI)-Fc rapidly disrupts clusters and mobilizes BM PCs. CD138, a surface co-receptor that is abundant on PCs and binds APRIL but not BAFF, regulates PC retention in the BM and adhesion and motility on fibronectin. Cell-intrinsic CD138 levels control competition for survival between nascent CD138low PCs and mature CD138high PCs, and enhanced survival of CD138high PCs correlates with retention in clusters. Collectively, these results indicate that PC clusters are survival niches and that dynamic competition between new and pre-existing PCs regulates the survival of new PCs and the durability of antibody responses.