Chimeric hepatitis B surface antigen virus-like particles expressing the strep A epitope p*17 elicit a humoral immune response in mice

Article


Dooley, Leanne, Ahmad, Tarek, Ozberk, Victoria, Pandey, Manisha, Good, Michael and Kotiw, Mkie. 2024. "Chimeric hepatitis B surface antigen virus-like particles expressing the strep A epitope p*17 elicit a humoral immune response in mice ." Heliyon. 10 (9). https://doi.org/10.1016/j.heliyon.2024.e30606
Article Title

Chimeric hepatitis B surface antigen virus-like particles expressing the strep A epitope p*17 elicit a humoral immune response in mice

ERA Journal ID212685
Article CategoryArticle
AuthorsDooley, Leanne, Ahmad, Tarek, Ozberk, Victoria, Pandey, Manisha, Good, Michael and Kotiw, Mkie
Journal TitleHeliyon
Journal Citation10 (9)
Article Numbere30606
Number of Pages9
Year2024
PublisherElsevier
Place of PublicationUnited Kingdom
ISSN2405-8440
Digital Object Identifier (DOI)https://doi.org/10.1016/j.heliyon.2024.e30606
Web Address (URL)https://www.sciencedirect.com/science/article/pii/S2405844024066374
Abstract

To optimize immunogenicity, bacterial epitopes in putative vaccine constructs can be presented to immune cells as multiple repeated structures on a defined nanoparticle. Virus-like particles (VLPs) are viral capsid proteins that self-assemble to form compact and highly ordered nanoparticles that are within the optimal size range for uptake by dendritic cells. VLPs mimic the live virus in size and form but contain no viral genetic material, are therefore noninfective and are the basis of safe and effective vaccines against hepatitis B virus (HBV) and human papillomavirus (HPV). Due to their particulate nature, molecular stability, and expression of high density and repetitive antigen displays, recombinant cell culture-derived VLPs are ideal platforms for the delivery of small molecules, including bacterial epitopes. We developed a putative vaccine by expressing a minimal epitope from the bacterium Streptococcus pyogenes (Strep A) on the surface of a recombinant VLP comprising multiple copies of HBV small envelope protein (HBsAg-S). Strep A is responsible for a wide spectrum of human infections and postinfectious diseases that disproportionately affect children and young adults living in resource-poor communities. No vaccine is currently available to offer sufficiently broad protection from the numerous and diverse strains of Strep A endemic in these at-risk populations. The Strep A antigen targeted by our vaccine construct is p*17, a cryptic epitope from a highly conserved region of the Strep A M-protein with demonstrated enhanced immunogenicity and broad protective potential against Strep A. To ensure surface expression and optimal immunogenicity, we expressed p*17 within the immunodominant “a” determinant of HBsAg-S. The recombinant VLPs (VLP-p*17) expressed in HEK293T cells spontaneously formed 22 nm particles and induced the production of high titers of p*17-specific IgG in BALB/c mice immunized with three 0.5 μg doses of VLP-p*17 formulated with adjuvant.

Keywordshepatitis B; immune
Contains Sensitive ContentDoes not contain sensitive content
ANZSRC Field of Research 2020320701. Medical bacteriology
Byline AffiliationsSchool of Health and Medical Sciences
Institute for Life Sciences and the Environment
Griffith University
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