Cell Reports (Oct 2017)

Elicitation of Neutralizing Antibodies Targeting the V2 Apex of the HIV Envelope Trimer in a Wild-Type Animal Model

  • James E. Voss,
  • Raiees Andrabi,
  • Laura E. McCoy,
  • Natalia de Val,
  • Roberta P. Fuller,
  • Terrence Messmer,
  • Ching-Yao Su,
  • Devin Sok,
  • Salar N. Khan,
  • Fernando Garces,
  • Laura K. Pritchard,
  • Richard T. Wyatt,
  • Andrew B. Ward,
  • Max Crispin,
  • Ian A. Wilson,
  • Dennis R. Burton

DOI
https://doi.org/10.1016/j.celrep.2017.09.024
Journal volume & issue
Vol. 21, no. 1
pp. 222 – 235

Abstract

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Recent efforts toward HIV vaccine development include the design of immunogens that can engage B cell receptors with the potential to affinity mature into broadly neutralizing antibodies (bnAbs). V2-apex bnAbs, which bind a protein-glycan region on HIV envelope glycoprotein (Env) trimer, are among the most broad and potent described. We show here that a rare “glycan hole” at the V2 apex is enriched in HIV isolates neutralized by inferred precursors of prototype V2-apex bnAbs. To investigate whether this feature could focus neutralizing responses onto the apex bnAb region, we immunized wild-type rabbits with soluble trimers adapted from these Envs. Potent autologous tier 2 neutralizing responses targeting basic residues in strand C of the V2 region, which forms the core epitope for V2-apex bnAbs, were observed. Neutralizing monoclonal antibodies (mAbs) derived from these animals display features promising for subsequent broadening of the response.

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