Molecular Therapy: Methods & Clinical Development (Mar 2020)

Induction of Transient Virus Replication Facilitates Antigen-Independent Isolation of SIV-Specific Monoclonal Antibodies

  • Nuria Pedreño-Lopez,
  • Christine M. Dang,
  • Brandon C. Rosen,
  • Michael J. Ricciardi,
  • Varian K. Bailey,
  • Martin J. Gutman,
  • Lucas Gonzalez-Nieto,
  • Matthias G. Pauthner,
  • Khoa Le,
  • Ge Song,
  • Raiees Andrabi,
  • Kim L. Weisgrau,
  • Nicholas Pomplun,
  • José M. Martinez-Navio,
  • Sebastian P. Fuchs,
  • Jens Wrammert,
  • Eva G. Rakasz,
  • Jeffrey D. Lifson,
  • Mauricio A. Martins,
  • Dennis R. Burton,
  • David I. Watkins,
  • Diogo M. Magnani

Journal volume & issue
Vol. 16
pp. 225 – 237

Abstract

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Structural characterization of the HIV-1 Envelope (Env) glycoprotein has facilitated the development of Env probes to isolate HIV-specific monoclonal antibodies (mAbs). However, preclinical studies have largely evaluated these virus-specific mAbs against chimeric viruses, which do not naturally infect non-human primates, in contrast to the unconstrained simian immunodeficiency virus (SIV)mac239 clone. Given the paucity of native-like reagents for the isolation of SIV-specific B cells, we examined a method to isolate SIVmac239-specific mAbs without using Env probes. We first activated virus-specific B cells by inducing viral replication after the infusion of a CD8β-depleting mAb or withdrawal of antiretroviral therapy in SIVmac239-infected rhesus macaques. Following the rise in viremia, we observed 2- to 4-fold increases in the number of SIVmac239 Env-reactive plasmablasts in circulation. We then sorted these activated B cells and obtained 206 paired Ab sequences. After expressing 122 mAbs, we identified 14 Env-specific mAbs. While these Env-specific mAbs bound to both the SIVmac239 SOSIP.664 trimer and to infected primary rhesus CD4+ T cells, five also neutralized SIVmac316. Unfortunately, none of these mAbs neutralized SIVmac239. Our data show that this method can be used to isolate virus-specific mAbs without antigenic probes by inducing bursts of contemporary replicating viruses in vivo. Keywords: SIV, monoclonal antibodies, rhesus macaques, CD8b depletion, antiretroviral therapy interruption