Development of a novel dual-domain nanoparticle antigen construct for universal influenza vaccine.

Vaccine

Department of Veterinary Pathobiology, College of Veterinary Medicine and Biomedical Science, Texas A&M University, College Station, Texas, United States.

Published: December 2017

AI Article Synopsis

  • A novel dual-domain nanoparticle fusion protein (DDNFP) was developed to enhance the presentation of conserved antigens for a universal influenza vaccine, featuring M2e from M2 and fusion peptide or alpha helix from HA2.
  • The DDNFP utilizes a unique dodecameric nanoparticle protein (Dps) from bacteria, allowing simultaneous fusion and surface presentation at both ends while forming stable nanoparticles around 9 nm.
  • The DDNFPs triggered strong antibody responses and provided full protection against a lethal H1N1 virus challenge, with the M2e-EcDps-CD construct showing superior protective effects compared to other versions.

Article Abstract

A highly effective antigen construct for presenting conserved antigen domains is essential to the development of a universal influenza vaccine. We have developed a novel dual-domain nanoparticle fusion protein (DDNFP) which allows independent presentation of two conserved domains. The conserved domains used were from two separate viral surface proteins, M2e of M2 and fusion peptide (FP) or long alpha helix (CD) of HA2. The carrier is a novel nanoparticle protein - the dodecameric DNA binding protein from starved cells (Dps) of bacteria or archaea. Dps was found to be uniquely capable of simultaneous fusion and surface presentation at both N- and C-termini while retaining the ability to form nanoparticles. Thus, DDNFPs with M2e and FP or CD fused at N- and C-termini of Dps from E. coli (EcDps) or other bacteria were first constructed based on the H1 subtype sequences along with corresponding single-domain nanoparticle fusion proteins (SDNFPs). They were expressed at high levels in bacteria and found to form nanoparticles of the expected size (∼9 nm). They were stable against treatment at high temperatures. The DDNFPs (M2e-EcDps-FP and M2e-EcDps-CD) induced strong antibody responses against individual antigen domains and provided full protection against lethal challenge with PR8 virus (H1N1). Importantly, the protection by DDNFPs was synergistically enhanced as compared to SDNFPs. The M2e-EcDps-CD provided an even stronger protection than M2e-EcDps-FP and therefore appeared to be the superior construct. Together, with novel domain combination, enhanced protection and ease of production, this M2e/CD DDNFP could potentially be a highly effective antigen construct for the universal influenza vaccine.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5715465PMC
http://dx.doi.org/10.1016/j.vaccine.2017.10.051DOI Listing

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