Molecular Therapy: Methods & Clinical Development (Sep 2022)

AAV-monoclonal antibody expression protects mice from Ebola virus without impeding the endogenous antibody response to heterologous challenge

  • Laura P. van Lieshout,
  • Amira D. Rghei,
  • Wenguang Cao,
  • Shihua He,
  • Geoff Soule,
  • Wenjun Zhu,
  • Sylvia P. Thomas,
  • Debra Sorensen,
  • Kathy Frost,
  • Kevin Tierney,
  • Brad Thompson,
  • Stephanie Booth,
  • David Safronetz,
  • Raveendra R. Kulkarni,
  • Byram W. Bridle,
  • Xiangguo Qiu,
  • Logan Banadyga,
  • Sarah K. Wootton

Journal volume & issue
Vol. 26
pp. 505 – 518

Abstract

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Filoviruses cause severe hemorrhagic fever with case fatality rates as high as 90%. Filovirus-specific monoclonal antibodies (mAbs) confer protection in nonhuman primates as late as 5 days after challenge, and FDA-approved mAbs REGN-EB3 and mAb114 have demonstrated efficacy against Ebola virus (EBOV) infection in humans. Vectorized antibody expression mediated by adeno-associated virus (AAV) can generate protective and sustained concentrations of therapeutic mAbs in animal models for a variety of infectious diseases, including EBOV. Here we demonstrate that AAV6.2FF-mediated expression of murine IgG2a EBOV mAbs, 2G4 and 5D2, protects from mouse-adapted (MA)-EBOV infection with none of the surviving mice developing anti-VP40 antibodies above background. Protective serum concentrations of AAV6.2FF-2G4/AAV6.2FF-5D2 did not alter endogenous antibody responses to heterologous virus infection. AAV-mediated expression of EBOV mAbs 100 and 114, and pan-ebolavirus mAbs, FVM04, ADI-15878, and CA45, as human IgG1 antibodies conferred protection against MA-EBOV at low serum concentrations, with minimum protective serum levels as low as 2 μg/mL. Vectorized expression of murine IgG2a or human IgG1 mAbs led to sustained expression in the serum of mice for >400 days or for the lifetime of the animal, respectively. AAV6.2FF-mediated mAb expression offers an alternative to recombinant antibody administration in scenarios where long-term protection is preferable to passive immunization.

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