Human Vaccines & Immunotherapeutics (Sep 2020)

Active immunoprophylaxis with a synthetic DNA-encoded monoclonal anti-respiratory syncytial virus scFv-Fc fusion protein confers protection against infection and durable activity

  • Katherine Schultheis,
  • Holly M Pugh,
  • Janet Oh,
  • Jacklyn Nguyen,
  • Bryan Yung,
  • Charles Reed,
  • Neil Cooch,
  • Jing Chen,
  • Jian Yan,
  • Kar Muthumani,
  • Laurent M. Humeau,
  • David B. Weiner,
  • Kate E. Broderick,
  • Trevor R. F. Smith

DOI
https://doi.org/10.1080/21645515.2020.1748979
Journal volume & issue
Vol. 16, no. 9
pp. 2165 – 2175

Abstract

Read online

Respiratory Syncytial virus (RSV) is a major threat to many vulnerable populations. There are currently no approved vaccines, and RSV remains a high unmet global medical need. Here we describe the employment of a novel synthetic DNA-encoded antibody technology platform to develop and deliver an engineered human DNA-encoded monoclonal antibody (dMAbTM) targeting the fusion protein (F) of RSV as a new approach to prevention or therapy of at risk populations. In in vivo models, a single administration of synthetic DNA-encoding the single-chain fragment variable-constant fragment (scFv-Fc) RSV-F dMAb resulted in robust and durable circulating levels of a functional antibody systemically and in mucosal tissue. In cotton rats, which are the gold-standard animals to model RSV infection, we observed sustained scFv-Fc RSV-F dMAb in the sera and lung-lavage samples, demonstrating the potential for both long-lasting immunity to RSV and effective biodistribution. The scFv-Fc RSV-F dMAb harbored in the sera exhibited RSV antigen-specific binding and potent viral neutralizing activity. Importantly, in vivo delivery of synthetic DNA-encoding, the scFv-Fc RSV-F dMAb protected animals against viral challenge. Our findings support the significance of dMAbs as a potential platform technology for durable protection against RSV disease.

Keywords