Cell Reports Medicine (May 2020)

Persistence of HIV-1 Env-Specific Plasmablast Lineages in Plasma Cells after Vaccination in Humans

  • Madhubanti Basu,
  • Michael S. Piepenbrink,
  • Czestochowa Francois,
  • Fritzlaine Roche,
  • Bo Zheng,
  • David A. Spencer,
  • Ann J. Hessell,
  • Christopher F. Fucile,
  • Alexander F. Rosenberg,
  • Catherine A. Bunce,
  • Jane Liesveld,
  • Michael C. Keefer,
  • James J. Kobie

Journal volume & issue
Vol. 1, no. 2
p. 100015

Abstract

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Summary: Induction of persistent HIV-1 Envelope (Env) specific antibody (Ab) is a primary goal of HIV vaccine strategies; however, it is unclear whether HIV Env immunization in humans induces bone marrow plasma cells, the presumed source of long-lived systemic Ab. To define the features of Env-specific plasma cells after vaccination, samples were obtained from HVTN 105, a phase I trial testing the same gp120 protein immunogen, AIDSVAX B/E, used in RV144, along with a DNA immunogen in various prime and boost strategies. Boosting regimens that included AIDSVAX B/E induced robust peripheral blood plasmablast responses. The Env-specific immunoglobulin repertoire of the plasmablasts is dominated by VH1 gene usage and targeting of the V3 region. Numerous plasmablast-derived immunoglobulin lineages persisted in the bone marrow >8 months after immunization, including in the CD138+ long-lived plasma cell compartment. These findings identify a cellular linkage for the development of sustained Env-specific Abs following vaccination in humans.

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