PLoS Neglected Tropical Diseases (Jun 2017)

Therapeutic administration of a recombinant human monoclonal antibody reduces the severity of chikungunya virus disease in rhesus macaques.

  • Rebecca Broeckel,
  • Julie M Fox,
  • Nicole Haese,
  • Craig N Kreklywich,
  • Soila Sukulpovi-Petty,
  • Alfred Legasse,
  • Patricia P Smith,
  • Michael Denton,
  • Carsten Corvey,
  • Shiv Krishnan,
  • Lois M A Colgin,
  • Rebecca M Ducore,
  • Anne D Lewis,
  • Michael K Axthelm,
  • Marie Mandron,
  • Pierre Cortez,
  • Jonathan Rothblatt,
  • Ercole Rao,
  • Ingo Focken,
  • Kara Carter,
  • Gopal Sapparapau,
  • James E Crowe,
  • Michael S Diamond,
  • Daniel N Streblow

DOI
https://doi.org/10.1371/journal.pntd.0005637
Journal volume & issue
Vol. 11, no. 6
p. e0005637

Abstract

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Chikungunya virus (CHIKV) is a mosquito-borne virus that causes a febrile syndrome in humans associated with acute and chronic debilitating joint and muscle pain. Currently no licensed vaccines or therapeutics are available to prevent or treat CHIKV infections. We recently isolated a panel of potently neutralizing human monoclonal antibodies (mAbs), one (4N12) of which exhibited prophylactic and post-exposure therapeutic activity against CHIKV in immunocompromised mice. Here, we describe the development of an engineered CHIKV mAb, designated SVIR001, that has similar antigen binding and neutralization profiles to its parent, 4N12. Because therapeutic administration of SVIR001 in immunocompetent mice significantly reduced viral load in joint tissues, we evaluated its efficacy in a rhesus macaque model of CHIKV infection. Rhesus macaques that were treated after infection with SVIR001 showed rapid elimination of viremia and less severe joint infiltration and disease compared to animals treated with SVIR002, an isotype control mAb. SVIR001 reduced viral burden at the site of infection and at distant sites and also diminished the numbers of activated innate immune cells and levels of pro-inflammatory cytokines and chemokines. SVIR001 therapy; however, did not substantively reduce the induction of CHIKV-specific B or T cell responses. Collectively, these results show promising therapeutic activity of a human anti-CHIKV mAb in rhesus macaques and provide proof-of-principle for its possible use in humans to treat active CHIKV infections.