Mixed Origins: HIV gp120-specific memory develops from pre-existing memory and naive B cells following vaccination in humans [article]

Madhubanti Basu, Michael S Piepenbrink, Christopher Fucile, Catherine A Bunce, Li-Xing Man, Jane Liesveld, Alexander F Rosenberg, Michael C Keefer, James J Kobie
2021 bioRxiv   pre-print
The most potent and broad HIV envelope (Env)-specific antibodies often when reverted to their inferred germline versions representing the naive B cell receptor, fail to bind Env suggesting that the initial responding B cell population is not exclusively comprised of a naive population, but also a pre-existing cross-reactive antigen-experienced B cell pool that expands following Env exposure. Previously we isolated gp120-reactive monoclonal antibodies (mAbs) from participants in HVTN 105, an HIV
more » ... vaccine trial. Using deep sequencing VH-lineage tracking we identified several of these mAb lineages in pre-immune peripheral blood. Several of these pre-immune lineages also persisted in the bone marrow, including CD138+ long-lived plasma cell compartment, ~7 months after the final vaccination. The majority of the pre-immune lineage members included IgM, however IgG and IgA members were also prevalent and exhibited somatic hypermutation. These results suggest that vaccine-induced gp120-specific antibody lineages originate from both naive and cross-reactive memory B cells.
doi:10.1101/2021.09.01.458551 fatcat:bkbzslnclrc6poy22srksai5nu