RNA and Toll-Like Receptor 7 License the Generation of Superior Secondary Plasma Cells at Multiple Levels in a B Cell Intrinsic Fashion

Secondary plasma cells (PCs) originate from memory B cells and produce increased
levels of antibodies with higher affinity compared to PCs generated during primary
responses. Here we demonstrate that virus-like particles (VLPs) only induce secondary
PCs in the presence of toll-like receptor (TLR) 7 and if they are loaded with RNA.
Furthermore, adoptive transfer experiments demonstrate that RNA and TLR7 signaling
are required for secondary PC generation, both at the level ofmemory B cell as well as PC
differentiation. TLR7-signaling occurred in a B cell intrinsic manner as TLR7-deficient B
cells in an otherwise TLR7-competent environment failed to differentiate into secondary
PCs. Therefore, RNA inside VLPs is essential for the generation of memory B cells, which
are competent to differentiate to secondary PCs and for the differentiation of secondary
PCs themselves. While we have not tested all other TLR or non-TLR adjuvants with our
VLPs, these data have obvious implications for vaccine design, as RNA packaged into
VLPs is a simple way to enhance induction of memory B cells capable of generating
secondary PCs.