A Thermal-Stable Protein Nanoparticle That Stimulates Long Lasting Humoral Immune Response

Author:

Wong Ten-Tsao1ORCID,Liou Gunn-Guang23ORCID,Kan Ming-Chung4ORCID

Affiliation:

1. Department of Marine Biotechnology & Institute of Marine and Environmental Technology, University of Maryland Baltimore County, Baltiomre, MD 21202, USA

2. Institute of Biological Chemistry, Academia Sinica, Taipei 11529, Taiwan

3. Office of Research and Development, College of Medicine, National Taiwan University, Taipei 10051, Taiwan

4. Vaxsia Biomedical Inc., Taipei 11503, Taiwan

Abstract

A thermally stable vaccine platform is considered the missing piece of vaccine technology. In this article, we reported the creation of a novel protein nanoparticle and assessed its ability to withstand extended high temperature incubation while stimulating a long-lasting humoral immune response. This protein nanoparticle was assembled from a fusion protein composed of an amphipathic helical peptide derived from the M2 protein of the H5N1 influenza virus (AH3) and a superfolder green fluorescent protein (sfGFP). Its proposed structure was modeled according to transmission electronic microscope (TEM) images of protein nanoparticles. From this proposed protein model, we created a mutant with two gain-of-function mutations that work synergistically on particle stability. A protein nanoparticle assembled from this gain-of-function mutant is able to remove a hydrophobic patch from its surface. This gain-of-function mutant also contributes to the higher thermostability of protein nanoparticles and stimulates a long lasting humoral immune response after a single immunization. This assembled nanoparticle showed increasing particle stability at higher temperatures and salt concentrations. This novel protein nanoparticle may serve as a thermally-stable platform for vaccine development.

Funder

MOEA

University of Maryland Baltimore County

Publisher

MDPI AG

Subject

Pharmacology (medical),Infectious Diseases,Drug Discovery,Pharmacology,Immunology

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