Memory B cell subset formation is influenced by naive precursor frequency. Memory B cells were generated from the indicated numbers of naive NP-specific B cells after adoptive transfer of Vh186.2 Sd-Tg donor splenocytes into AM14 × Vκ8R CB.17 recipients, i.p. immunization with NP-CGG precipitated in alum, and ≥12 wk rest. The number of naive NP-reactive B cells adoptively transferred is indicated above each column. The percentage of the parent population is indicated adjacent to the gates or within the respective quadrant. Representative plots from three to five individual mice per cell dose are shown. A, FACS plots of live splenic B cells demonstrating NIP binding and κ L chain expression. B, FACS graphs and plots of NIP-binding B cells gated as in A, stained with Abs to the indicated markers.

Surface expression of PD-L2 (CD273), CD80, and CD73 define phenotypic subsets of IgM and isotype-switched memory B cells. Memory cells were generated after adoptive transfer of Vh186.2 Sd-Tg BALB/c splenic B cells into AM14 × Vκ8R Tg CB.17 recipients, immunization with NP-CGG precipitated in alum, and 12–20 wk rest. Naive cells were harvested from unimmunized Vh186.2 Sd-Tg mice. The percentage of the parent population of each quadrant or gate is indicated for individual mice shown. A, FACS plots of splenocytes stained with Abs to the indicated markers gated on live, NIP-binding κ^neg splenic B cells. Representative plots for >11 mice are shown. B, Representative graphs of IgM staining of memory B cell subpopulations defined as in A. Individual quadrants are depicted clockwise, beginning with the upper right. Parallel stains with anti-IgG₁ (data not shown) confirmed the IgM⁻ gates. Naive B cells were lacking IgM⁻ and IgG₁⁺ populations (data not shown). Representative plots from at least five individual mice per dose are shown. Specific memory subpopulations discussed in the text are highlighted in color.